Summary Basis of Decision for Jcovden (previously the Janssen COVID-19 Vaccine)

Review decision

The Summary Basis of Decision explains why the product was approved for sale in Canada. The document includes regulatory, safety, effectiveness and quality (in terms of chemistry and manufacturing) considerations.


Product type:

Drug

Summary Basis of Decision (SBD) documents provide information related to the original authorization of a product. The SBD for Jcovden (previously the Janssen COVID-19 Vaccine) is located below.

Recent Activity for Jcovden (previously the Janssen COVID-19 Vaccine)

SBDs written for eligible drugs approved after September 1, 2012 will be updated to include post-authorization information. This information will be compiled in a Post-Authorization Activity Table (PAAT). The PAAT will include brief summaries of activities such as submissions for new uses of the product, and whether Health Canada's decisions were negative or positive. PAATs will be updated regularly with post-authorization activity throughout the product's life cycle.

Post-Authorization Activity Table (PAAT) for Jcovden (previously the Janssen COVID-19 Vaccine)

Updated: 2024-01-19

The following table describes post-authorization activity for the Jcovden (previously the Janssen COVID-19 Vaccine), a product which contains the medicinal ingredient Ad26.COV2.S (recombinant). For more information on the type of information found in PAATs, please refer to the Frequently Asked Questions: Summary Basis of Decision (SBD) Project: Phase II and to the List of abbreviations found in Post-Authorization Activity Tables (PAATs).

For additional information about the drug submission process, refer to the Guidance Document: The Management of Drug Submissions and Applications.

Drug Identification Number (DIN):

  • DIN 02513153 - 5 x 1010 virus particles/0.5 mL Ad26.COV2.S (recombinant), suspension, intramuscular administration

Post-Authorization Activity Table (PAAT)

Activity/submission type, control number Date submitted Decision and date Summary of activities
PBRER # 274921 2023-05-02 Review completed 2023-09-25 Submission filed in response to commitments made as per the Food and Drug Regulations. PBRER #4 for the period 2022-08-25 to 2023-02-24. The information was reviewed and found acceptable. No further action was required.
DIN 02513153 cancelled (post market) Not applicable Discontinuation date: 2023-06-30 The manufacturer notified Health Canada that sale of the drug has been discontinued post market. Health Canada cancelled the DIN pursuant to section C.01.014.6(1)(a) of the Food and Drug Regulations.

Amended Terms and Conditions
Control # 253702

Not applicable

Terms and conditions amended post authorization
2023-06-09

Health Canada updated the Risk Management Plan Terms and Conditions for Jcovden to reflect the accumulation of safety data and information gained in the post-market setting for this vaccine.

Risk Management Plan update
Control # 270886

2022-12-21 Review completed 2023-05-17 The updated Core (European Union [EU]) Risk Management Plan (RMP) version 6.0 and Canadian Addendum version 4.0 dated December 2022 were filed as per the terms and conditions imposed on the authorization issued under the Food and Drug Regulations. The review concluded that the RMP and Canadian Addendum are acceptable at this time. The current post-market safety data are consistent with the labelled safety profile of Jcvoden.
PBRER # 269194 2022-10-31 Review completed 2023-03-13 Submission filed in response to commitments made as per the Food and Drug Regulations. PBRER #3 for the period 2022-02-25 to 2022-08-24. The sponsor was asked to provide updated assessments for the ongoing monitoring of safety events.
Post-Market Information Request Review Control # 268172 2022-07-26 Review completed
2023-03-10

Health Canada conducted a third ad-hoc review of available data on the risk of thrombosis with thrombocytopenia syndrome (TTS) with viral vector vaccines Jcvoden and Vaxzevria. The sponsors were requested to submit all available data to Health Canada for review. The information was assessed, and Health Canada will continue to monitor the safety of these vaccines.

SNDS # 267263 2022-08-24 Issued NOC
2023-02-16

Submission filed as a Level I – Supplement to seek authorization for a booster dose of Jcovden, following primary vaccination with an mRNA COVID-19 vaccine in subjects 18 years of age and older. The submission was reviewed and considered acceptable, and an NOC was issued. A Regulatory Decision Summary was published.

SNDS # 268236 2022-09-28 Issued NOC
2022-12-23

Submission filed as a Level II – Supplement (Safety) to update the PM with pooled analyses of safety data from studies COV1001, COV1002, COV2001, COV3001, and COV3009. The submission was reviewed and considered acceptable. As a result of the SNDS, modifications were made to the Adverse Reactions section of the PM. An NOC was issued.

SNDS # 267768 2022-09-12 Issued NOC
2022-12-12

Submission filed as a Level II – Supplement (Safety) to update the PM with new safety information related to facial paralysis. The submission was reviewed and considered acceptable. As a result of the SNDS, modifications were made to the Adverse Reactions section of the PM, and corresponding changes were made to Part III: Patient Medication Information. An NOC was issued.

SNDS # 264886 2022-07-06 Issued NOC
2022-10-27

Submission filed as a Level II – Supplement (Safety) to update the PM. The changes were in response to an Advisement Letter issued by Health Canada dated 2022-06-06, requesting revisions related to small-vessel vasculitis with cutaneous manifestation. The submission was reviewed and considered acceptable. As a result of the SNDS, modifications were made to the Adverse Reactions section of the PM. An NOC was issued.

PBRER # 263656 2022-04-25 Review completed
2022-09-08

Submission filed in response to commitments made as per the Food and Drug Regulations. PBRER #2 for the period 2021-08-25 to 2022-02-24. The sponsor was asked to provide updated assessments for the ongoing monitoring of safety events.

SNDS # 264578 2022-05-26 Issued NOC (subject to terms and conditions)
2022-08-05

Submission filed as a Level II – Supplement to change the brand name from the Janssen COVID-19 Vaccine to Jcvoden, and to introduce Canadian-specific labels. The information was reviewed and considered acceptable. An NOC was issued. Terms and conditions were imposed on the authorization.

NC # 262955 2022-03-31 Issued NOL
2022-07-05

Submission filed as a Level II (90 day) Notifiable Change (Moderate Quality Changes) to transfer quality control testing activities between sites. The submission was reviewed and considered acceptable, and an NOL was issued.

Post-Market Information Request Review Control # 264026 2022-05-13 Review completed
2022-06-21

Health Canada reviewed information under a memorandum issued by the United States Food and Drug Administration based on an updated analysis of reported cases of thrombosis with thrombocytopenia syndrome. Health Canada issued a letter to the sponsor requesting further information. The response was reviewed, and the sponsor was asked to provide updated assessments for the ongoing monitoring of safety events.

NC # 262027 2022-03-04 Issued NOL
2022-06-06

Submission filed as a Level II (90 day) Notifiable Change to extend the shelf life from 6 to 11 months and to update the release specifications for the drug substance and drug product. The submission was reviewed and considered acceptable, and an NOL was issued.

Bi-monthly safety report
Control # 261495
2022-02-14 Review completed
2022-05-18

Information filed as per the terms and conditions imposed on the authorization issued under the Food and Drug Regulations. Bi-monthly safety report #1 for the period 2021-11-01 to 2022-01-15. The sponsor was asked to provide updated assessments for the ongoing monitoring of safety events.

SNDS # 259715 2021-12-17 Issued NOC
2022-05-11

Submission filed as a Level I – Supplement to seek authorization for a booster dose of the Janssen COVID-19 Vaccine. The submission was reviewed and considered acceptable, and an NOC was issued. A Regulatory Decision Summary was published.

Risk Management Plan update
Control # 259715
2021-12-17 Review completed
2022-05-11

The updated Core (European Union [EU]) Risk Management Plan (RMP) version 4.0 and Canadian Addendum version 3.0 dated December 2021 were filed as per the terms and conditions imposed on the authorization issued under the Food and Drug Regulations. The review concluded that the RMP and Canadian Addendum are acceptable at this time. The current post-market safety data are consistent with the labelled safety profile of the Janssen COVID-19 Vaccine.

SNDS # 261307 2022-02-09 Issued NOC
2022-03-24
Submission filed as a Level II – Supplement (Safety) to update the Product Monograph (PM). The Product Monograph was updated to include information related to myocarditis and pericarditis, thrombosis with thrombocytopenia syndrome, and other adverse drug reactions. Changes were made to the Contraindications, Warnings and Precautions, Adverse Reactions and Patient Medication Information sections. The submission was reviewed and considered acceptable, and an NOC was issued.
NC # 259668 2021-12-16 Issued NOL
2022-03-21
Submission filed as a Level II (90 day) Notifiable Change to transfer of quality control testing activities between sites. The submission was reviewed and considered acceptable, and an NOL was issued.
Amended Terms and Conditions Control # 253702 Not applicable Terms and conditions amended post authorization
2022-03-17

Health Canada imposed a new Term and Condition to the authorization of the Janssen COVID-19 Vaccine. Health Canada considered the Term and Condition of bi-monthly safety reports closed. This Term and Condition has been replaced with the requirement to submit Periodic Safety Update Reports / Periodic Benefit Risk Evaluation Reports every 6 months.

Post-Market Information Request Review Control # 259124, 259125 2021-12-07 Review completed
2022-03-11
Health Canada requested that the sponsor submit their plan to address the impact of the new variant of concern (Omicron) on the effectiveness and on any associated safety issues of their COVID-19 vaccine. In addition, the sponsor was requested to submit any detailed analyses of the effectiveness of the vaccine against the new variant. The information was assessed and Health Canada will continue to monitor the safety and effectiveness of this vaccine.
NC # 259501 2021-12-13 Issued NOL
2022-02-28
Submission filed as a Level II (90 day) Notifiable Change to add a new site to be used in drug substance production. The submission was reviewed and considered acceptable, and an NOL was issued.
Monthly safety report
Control # 259630
2021-12-15 Review completed
2022-02-18
Information filed in response to commitments made as per the terms and conditions imposed on the authorization issued under the Food and Drug Regulations. Monthly safety report #9 for the period 2021-11-01 to 2021-11-30. The sponsor was asked to provide updated assessments for the ongoing monitoring of safety events.
PBRER # 258149 2021-10-29 Review completed
2022-02-03
Submission filed in response to commitments made as per the terms and conditions imposed on the authorization issued under the Interim Order Respecting the Importation, Sale and Advertising of Drugs for Use in Relation to COVID-19 (Interim Order). PBRER #1 for the period 2021-02-25 to 2021-08-24. The sponsor was asked to provide updated assessments for the ongoing monitoring of safety events.
Monthly safety report
Control # 258695
2021-11-16 Review completed
2022-01-14
Submission filed in response to commitments made as per the terms and conditions imposed on the authorization issued under the Interim Order Respecting the Importation, Sale and Advertising of Drugs for Use in Relation to COVID-19 (Interim Order). Monthly safety report #8 for the period 2021-10-01 to 2021-10-31. The sponsor was asked to provide updated assessments for the ongoing monitoring of safety events.
Monthly safety report
Control # 257658
2021-10-18 Review completed
2021-11-30
Submission filed in response to commitments made as per the terms and conditions imposed on the authorization issued under the Interim Order Respecting the Importation, Sale and Advertising of Drugs for Use in Relation to COVID-19 (Interim Order). Monthly safety report #7 for the period 2021-09-01 to 2021-09-30. The sponsor was asked to provide updated assessments for the ongoing monitoring of safety events.
Drug product (DIN 02513153) market notification Not applicable Date of first sale:
2021-11-23
The manufacturer notified Health Canada of the date of first sale pursuant to C.01.014.3 of the Food and Drug Regulations.
NDS # 253702 2021-06-14 Issued NOC (subject to terms and conditions)
2021-11-23

NOC issued for New Drug Submission. The submission was reviewed and considered acceptable, and an NOC was issued. Terms and conditions were imposed on the authorization. A Regulatory Decision Summary was published. DIN 02513153 was issued.

Public advisory Not applicable Posted
2021-11-09
Public Advisory posted (Health Canada is updating the labels of the Janssen and Vaxzevria [AstraZeneca] COVID-19 vaccines), containing important information about product safety for the general public.
Health Product Risk Communication Not applicable Posted
2021-11-05
Health Product Risk Communication posted (Importation of Janssen COVID-19 Vaccine with European Union [EU] English-only Vial and Carton Labels), containing important information about packaging and supply for healthcare professionals.
Monthly safety report
Control # 256682
2021-09-15 Review completed
2021-10-15
Information filed as per the terms and conditions imposed on the authorization issued under the Interim Order Respecting the Importation, Sale and Advertising of Drugs for Use in Relation to COVID-19 (Interim Order). Monthly safety report #6 for the period 2021-08-01 to 2021-08-31. The sponsor was asked to provide updated assessments for the ongoing monitoring of safety events.
Monthly safety report
Control # 255695
2021-08-16 Review completed
2021-09-14
Information filed as per the terms and conditions imposed on the authorization issued under the Interim Order Respecting the Importation, Sale and Advertising of Drugs for Use in Relation to COVID-19 (Interim Order). Monthly safety report #5 for the period 2021-07-01 to 2021-07-31. The current post-market safety data are consistent with the labelled safety profile of the Janssen COVID-19 Vaccine.
Amendment # 254486 2021-07-07 Authorization amended
2021-08-18

An application submitted to amend the authorization in respect of this drug (relating to a Product Monograph update) has been reviewed and it has been determined that the changes are acceptable. The Product Monograph was updated to include information related to Guillain-Barré syndrome, capillary leak syndrome and other adverse drug reactions. Changes were made to the Contraindications, Warnings and Precautions, Adverse Reactions and Patient Medication Information sections. The authorization under the Interim Order has been amended to permit these changes.

The authorization in respect of this drug (so amended) continues to be subject to terms and conditions that pertain to matters other than these changes. No additional terms and conditions were imposed when the authorization was amended to reflect these changes.

Monthly safety report
Control # 254484
2021-07-15 Review completed
2021-08-15

Information filed as per the terms and conditions imposed on the authorization issued under the Interim Order Respecting the Importation, Sale and Advertising of Drugs for Use in Relation to COVID-19 (Interim Order). Monthly safety report #4 for the period 2021-06-01 to 2021-06-30 as well as other post-market safety data. The sponsor was asked to provide updated assessments for the ongoing monitoring of safety events.

Amendment # 253751 2021-06-22 Authorization amended
2021-08-04

An application submitted to amend the authorization in respect of this drug (relating to a Product Monograph update) has been reviewed and it has been determined that the changes are acceptable. The changes were in response to an Advisement Letter issued by Health Canada requesting the sponsor update the Product Monograph to include information related to thrombosis and thrombocytopenia in the Warnings and Precautions and Post-Market Adverse Reactions sections. The authorization under the Interim Order has been amended to permit these changes.

The authorization in respect of this drug (so amended) continues to be subject to terms and conditions that pertain to matters other than these changes. No additional terms and conditions were imposed when the authorization was amended to reflect these changes.

Amendment # 253284 2021-06-02 Authorization amended
2021-07-28

An application submitted to amend the authorization in respect of this drug (relating to the use of carton and vial labels approved in the United States) has been reviewed and it has been determined that the changes are acceptable. The authorization under the Interim Order has been amended to permit these changes.

The authorization in respect of this drug (so amended) continues to be subject to terms and conditions that pertain to matters other than these changes. No additional terms and conditions were imposed when the authorization was amended to reflect these changes.

Monthly safety report
Control # 253341
2021-06-17 Review completed
2021-07-08

Information filed as per the terms and conditions imposed on the authorization issued under the Interim Order Respecting the Importation, Sale and Advertising of Drugs for Use in Relation to COVID-19 (Interim Order). Monthly safety report #3 for the period 2021-05-01 to 2021-05-31 as well as other post-market safety data. The sponsor was asked to provide updated assessments for the ongoing monitoring of safety events.

Risk Management Plan update
Control # 252207
2021-06-08 Review completed
2021-07-07

The updated Core (European Union [EU]) Risk Management Plan (RMP) and Canadian Addendum were filed as per the terms and conditions imposed on the authorization issued under the Interim Order Respecting the Importation, Sale and Advertising of Drugs for Use in Relation to COVID-19. The review of the Core EU RMP in conjunction with the Canadian Addendum is acceptable at this time. The safety concerns and their corresponding pharmacovigilance and risk minimization activities may be updated in a timely manner as more data becomes available in the clinical trial programs and in the real world use setting. The sponsor was requested to submit an updated RMP to include thrombosis as an important potential risk.

Amendment # 252997 2021-05-21 Authorization amended
2021-06-11
An application submitted to amend the authorization in respect of this drug (relating to an alternative quality control testing site for the drug substance and drug product) has been reviewed and it has been determined that the changes are acceptable. The authorization under the Interim Order has been amended to permit these changes.

The authorization in respect of this drug (so amended) continues to be subject to terms and conditions that pertain to matters other than these changes. No additional terms and conditions were imposed when the authorization was amended to reflect these changes.
Monthly safety report
Control # 252742
2021-05-14 Review completed
2021-06-04
Information filed as per the terms and conditions imposed on the authorization issued under the Interim Order Respecting the Importation, Sale and Advertising of Drugs for Use in Relation to COVID-19 (Interim Order). Monthly safety report #2 for the period 2021-04-01 to 2021-04-30 as well as other post-market safety data. The sponsor was asked to provide updated assessments for the ongoing monitoring of safety events.
Amendment # 252182 2021-04-30 Authorization amended
2021-05-19
An application submitted to amend the authorization in respect of this drug (relating to a transfer of quality control testing activities between sites) has been reviewed and it has been determined that the changes are acceptable. The authorization under the Interim Order has been amended to permit these changes.

The authorization in respect of this drug (so amended) continues to be subject to terms and conditions that pertain to matters other than these changes. No additional terms and conditions were imposed when the authorization was amended to reflect these changes.
Monthly safety report
Control # 251806
2021-04-14 Review completed
2021-05-07
Information filed as per the terms and conditions imposed on the authorization issued under the Interim Order Respecting the Importation, Sale and Advertising of Drugs for Use in Relation to COVID-19 (Interim Order). Monthly safety report #1 for the period 2021-02-25 to 2021-03-31. The current post-market safety data are consistent with the labelled safety profile of the Janssen COVID-19 Vaccine.
Risk Management Plan update
Control # 251230
2021-03-31 Review completed
2021-05-07
Updated Core (European Union) Risk Management Plan (RMP) and Canadian Addendum filed as per the terms and conditions imposed on the authorization issued under the Interim Order Respecting the Importation, Sale and Advertising of Drugs for Use in Relation to COVID-19 (Interim Order). The review concluded that the RMP is acceptable at this time. The safety concerns identified and their corresponding pharmacovigilance and risk minimization activities may be updated in a timely manner as more data becomes available in the clinical trial programs and in the real world use setting.
Summary Safety Review posted Not applicable Posted
2021-05-04
Summary Safety Review posted for the Janssen COVID-19 Vaccine (Assessing the Potential Risk of Thrombosis in Combination with Thrombocytopenia).
Post-Market Information Request Review Control # 251516 2021-04-16 Review completed 2021-04-30 Health Canada conducted an ad-hoc review of available data on the risk of thrombosis with thrombocytopenia syndrome (TTS) with Jcvoden. The sponsor was requested to submit all available data to Health Canada for review. The information was assessed, and Health Canada will continue to monitor the safety of the vaccine.
New safety review started by Health Canada Not applicable Started between
2021-04-01 and 2021-04-30

Health Canada started a safety review for Janssen COVID-19 Vaccine, in response to case reports from the United States of thrombosis (blood clots) in combination with thrombocytopenia (low blood platelets).

Dear Healthcare Professional Letter Not applicable Published
2021-04-26
Dear Healthcare Professional Letter posted (Janssen COVID-19 Vaccine and the Risk of Thrombosis with Thrombocytopenia), containing new safety information for healthcare professionals.
Dear Healthcare Professional Letter Not applicable Published
2021-04-26
Dear Healthcare Professional Letter posted (Importation of Janssen COVID-19 Vaccine with Two Types of English-only Vial and Carton Labels), containing important information about supply and product safety for healthcare professionals.
Amendment # 250716 2021-03-19 Authorization amended
2021-04-23
An application submitted to amend the authorization in respect of this drug (relating to a new manufacturing site for the drug product and a Product Monograph update) has been reviewed and it has been determined that the changes are acceptable. Safety information related to the risk of thrombosis in combination with thrombocytopenia was added to the Product Monograph. The authorization under the Interim Order has been amended to permit these changes.

Additional terms and conditions were imposed on this authorization when it was amended to permit this change, to ascertain the continued quality of the product manufactured at the new site and the continued safe use of the product.
Dear Healthcare Professional Letter Not applicable Published
2021-03-08
Dear Healthcare Professional Letter posted (Authorization of Janssen COVID‑19 Vaccine with English-only Vial and Carton Labels), containing important information about supply and product safety for healthcare professionals.
Application # 246758 2020-11-30 Authorized (with terms and conditions)
2021-03-05
Authorized with terms and conditions under the Interim Order Respecting the Importation, Sale and Advertising of Drugs for Use in Relation to COVID‑19.
Summary Basis of Decision (SBD) for Jcovden (previously the Janssen COVID-19 Vaccine)

Date SBD issued: 2021-03-19

The following information relates to the interim authorization of Jcovden (previously the Janssen COVID-19 Vaccine).

Ad26.COV2.S (recombinant)

Drug Identification Number (DIN):

  • DIN 02513153 - 5 x 1010 virus particles/0.5 mL Ad26.COV2.S (recombinant), suspension, intramuscular administration

Janssen Inc.

Application Control Number: 246758

 

On March 5, 2021, Health Canada issued an authorization under the Interim Order Respecting the Importation, Sale and Advertising of Drugs for Use in Relation to COVID‑19 (Interim Order) to Janssen Inc. for the Janssen COVID‑19 Vaccine. The Interim Order, signed by the Minister of Health on September 16, 2020, establishes new authorization pathways with the intent to expedite the authorization for the importation, sale and advertising of drugs used in relation to coronavirus disease 2019 (COVID‑19), while taking into consideration urgent public health needs caused by COVID‑19.

The interim authorization of the Janssen COVID‑19 Vaccine was based on quality (chemistry and manufacturing), non‑clinical (pharmacology and toxicology), and clinical (immunogenicity, safety, and efficacy) information. Following review of the available information, Health Canada considers that the evidence provided meets the Health Canada standards published in the Guidance for Market Authorization Requirements for COVID-19 Vaccines. The evidence supports the conclusion that the benefits associated with the Janssen COVID‑19 Vaccine outweigh the risks, having regard to the uncertainties relating to the benefits and risks and the necessity of addressing the urgent public health need related to COVID‑19. Based on these considerations, the benefit‑risk profile of the Janssen COVID‑19 Vaccine is considered favourable for active immunization for the prevention of coronavirus disease 2019 (COVID‑19) caused by severe acute respiratory syndrome coronavirus 2 (SARS‑CoV‑2) virus in individuals 18 years of age and older.

The interim authorization of the Janssen COVID‑19 Vaccine is subject to terms and conditions that need to be met by the sponsor to ascertain the continued quality, safety, and efficacy of the product. The terms and conditions may be amended at any time. Furthermore, this authorization may be revoked if new information does not support the safe and effective use of the product.

For further information on authorization under this pathway, refer to Health Canada's Interim Order Respecting the Importation, Sale, and Advertising of Drugs for Use in Relation to COVID‑19 and the Information and Application Requirements for Drugs Authorized under the Interim Order: Guidance Document.

1 What was approved?

The Janssen COVID‑19 Vaccine (Ad26.COV2.S, recombinant) is indicated for active immunization for the prevention of coronavirus disease 2019 (COVID‑19) caused by severe acute respiratory syndrome coronavirus 2 (SARS‑CoV‑2) virus in individuals 18 years of age and older.

The authorization of the Janssen COVID‑19 Vaccine under the Interim Order Respecting the Importation, Sale, and Advertising of Drugs for Use in Relation to COVID‑19 (Interim Order) is supported by an interim efficacy analysis of an ongoing pivotal Phase III study (Study COV3001 or the ENSEMBLE Study) which includes 43,783 participants.

Based on the data submitted to and reviewed by Health Canada, the safety and efficacy of the Janssen COVID‑19 Vaccine have been established in participants 18 years of age and older. The safety and efficacy of the Janssen COVID‑19 Vaccine in individuals under 18 years of age have not been established.

Clinical studies of the Janssen COVID‑19 Vaccine include participants 65 years of age and older and their data contribute to the overall assessment of safety and efficacy.

The Janssen COVID‑19 Vaccine is contraindicated in individuals who are hypersensitive to the active ingredient, any other adenovirus-based vaccines, or to any ingredient in the formulation, including any non‑medicinal ingredient or component of the container.

The Janssen COVID‑19 Vaccine (Ad26.COV2.S [recombinant], 5 x 1010 virus particles/0.5 mL) is presented as a suspension. In addition to the medicinal ingredient, the suspension contains 2‑hydroxypropyl‑β‑cyclodextrin (HBCD), citric acid monohydrate, ethanol, hydrochloric acid, polysorbate‑80, sodium chloride, sodium hydroxide, trisodium citrate dihydrate, and water for injection.

For more information, refer to the Clinical, Non‑clinical, and Quality (Chemistry and Manufacturing) Basis for Decision sections.

Additional information may be found in the Janssen COVID‑19 Vaccine Product Monograph, approved by Health Canada and available through the Drug Product Database and on the Health Canada COVID‑19 vaccines and treatments portal.

2 Why was Jcovden (previously the Janssen COVID-19 Vaccine) approved?

Health Canada considers that sufficient evidence has been provided to support the conclusion that the benefits associated with the Janssen COVID‑19 Vaccine outweigh the risks, having regard to the uncertainties relating to the benefits and risks and the necessity of addressing the urgent public health need related to coronavirus disease 2019 (COVID‑19). Based on these considerations, the benefit‑risk profile of the Janssen COVID‑19 Vaccine is deemed favourable for active immunization for the prevention of coronavirus disease 2019 (COVID‑19) caused by severe acute respiratory syndrome coronavirus 2 (SARS‑CoV‑2) virus in individuals 18 years of age and older.

The use of the Janssen COVID‑19 Vaccine is permitted under an authorization issued in accordance with section 5 of the Interim Order Respecting the Importation, Sale, and Advertising of Drugs for Use in Relation to COVID‑19 (Interim Order). The interim authorization is subject to terms and conditions that need to be met by the sponsor to ascertain the continued quality, safety, and efficacy of the product.

Coronavirus disease 2019 is the infectious disease caused by the recently discovered coronavirus, SARS‑CoV‑2, in late 2019, which has spread rapidly and globally since its emergence. In Canada, there have been 881,761 confirmed cases of COVID‑19 and 22,192 deaths as of March 5, 2021, the date of authorization of the Janssen COVID‑19 Vaccine. It is predominantly a respiratory illness passed from person to person primarily by droplets and aerosols from the nose or mouth when an infected person coughs, sneezes, or speaks. Once a person is infected with the SARS-CoV-2 virus, the disease can affect other organs. People with COVID‑19 can be asymptomatic, or can experience a range of symptoms from mild to severe illness. Symptoms may appear 1 to 14 days after exposure to the virus. Symptoms may include fever (≥38 °C) or chills, cough, shortness of breath, fatigue, muscle or body aches, headache, loss of taste or smell, sore throat, congestion or runny nose, nausea or vomiting, and diarrhea. The highest disease burden is in older adults and individuals with certain underlying comorbid conditions such as obesity, heart disease, chronic kidney disease, type 2 diabetes, cancer, and, pulmonary obstructive disease.

Care for individuals who have COVID‑19 has improved with clinical experience, and clinical management of COVID‑19 with a variety of therapies has continued to improve. Health Canada has authorized, under the Interim Order Respecting the Importation, Sale, and Advertising of Drugs for Use in Relation to COVID‑19 (Interim Order), several vaccines (Pfizer‑BioNTech COVID‑19 Vaccine, COVID‑19 Vaccine Moderna, AstraZeneca COVID‑19 Vaccine, and Covishield) for protection against COVID‑19. Nevertheless, there remains an urgent need for further prophylactic vaccine options in the context of the ongoing pandemic. The Janssen COVID‑19 Vaccine is the first single-dose vaccine to be authorized in Canada for active immunization to prevent COVID‑19 caused by the SARS‑CoV‑2 virus.

The Janssen COVID‑19 Vaccine is a monovalent vaccine composed of a recombinant, replication‑incompetent human adenovirus serotype 26 (Ad26) vector, constructed to encode the SARS‑CoV‑2 spike (S) protein. The S protein on the surface of the coronavirus binds to the angiotensin‑converting enzyme 2 (ACE2) receptor of a host cell, allowing the virus to infect the cell. Vaccination with the Janssen COVID‑19 Vaccine induces both neutralizing antibody and cellular immune responses directed against the spike S protein which may contribute to protection against COVID-19.

Clinical evidence for the efficacy of the Janssen COVID‑19 Vaccine is based primarily on the interim data from the ENSEMBLE Study (Study COV3001), an ongoing Phase III pivotal clinical study. The ENSEMBLE Study is a randomized, double‑blind, placebo‑controlled study designed to evaluate the efficacy, safety, and immunogenicity of the Janssen COVID‑19 Vaccine (Ad26.COV2.S, recombinant) in adults aged 18 years and older who have no known history of SARS‑CoV‑2 infection. The ENSEMBLE Study is currently being conducted in the United States, South Africa, Brazil, Chile, Argentina, Columbia, Peru, and Mexico.

At the time of analysis, a total of 44,325 participants 18 years of age and older were randomized in the ENSEMBLE Study and included in the interim efficacy analysis. Randomization was stratified by age (18 to 59 years, 60 years and older) and presence or absence of comorbidities associated with an increased risk of progression to severe COVID-19. Comorbidities consisted of stable pre-existing medical conditions, defined as disease not requiring significant change in therapy during the 3 months preceding vaccination, as well stable human immunodeficiency virus (HIV) infection. The most common pre-existing medical conditions were obesity (27.5%), hypertension (10.3%), type 2 diabetes mellitus (7.2%), serious heart conditions (2.4%), and asthma (1.3%). Other comorbidities were present in ≤1% of the participants. Human immunodeficiency virus (HIV) infection was reported at baseline in 2.5% of the participants. Participants with comorbidities were phased into the ENSEMBLE Study only after the safety review of 2,000 participants without comorbidities (for participants ≥18 to <60 years of age in stage 1, and for participants ≥60 years of age in stage 2).

Enrolled participants were randomized in a 1:1 ratio between two groups. The first group (vaccine group; number of participants [n] = 19,630) received a single intramuscular injection of the Janssen COVID‑19 Vaccine at a dose of 5 × 1010 virus particles. The second group (placebo group; n = 19,691) received a single intramuscular injection of 0.9% sodium chloride. Of the 39,321 participants included in the efficacy analysis, 38,059 were SARS‑CoV‑2 seronegative at baseline, and 1,262 had an unknown serostatus. The study included a median follow‑up of 58 days, and 56.4% of participants were followed for at least 8 weeks. Participants are planned to be followed for up to 24 months, for assessments of safety and efficacy against COVID‑19.

ENSEMBLE Study, Phase III; Participants in final efficacy analysis
  Vaccine group Placebo group
Male 10,924 (55.6%) 10,910 (55.4%)
Female 8,702 (44.3%) 8,777 (44.6%)
Total number of participants
(18 years of age and older)
19,630 19,691
Participants in safety analysis
Total number of participants
(18 years of age and older)
21,895 21,888

The primary efficacy endpoint of the ENSEMBLE Study was defined as a symptomatic moderate to severe/critical COVID‑19 case, confirmed by positive SARS‑CoV-2 viral ribonucleic acid (RNA) results using a polymerase chain reaction (PCR)‑based test in a central laboratory. To conduct the evaluation, the ENSEMBLE Study contained two co‑primary endpoints: to demonstrate the efficacy of a single intramuscular injection of the Janssen COVID‑19 Vaccine in the prevention of molecularly confirmed, moderate to severe/critical COVID‑19 with onset at least 14 days (Day 15) and at least 28 days (Day 29) post vaccination, as compared to placebo, in adults SARS‑CoV‑2 seronegative at baseline.

Moderate COVID‑19 was defined based on the following criteria:

  • the participant must have experienced any one of the following new or worsening signs or symptoms: respiratory rate ≥20 breaths/minute, abnormal saturation of oxygen (SpO2) but still >93% on room air at sea level, clinical or radiologic evidence of pneumonia, radiologic evidence of deep vein thrombosis (DVT), shortness of breath, or difficulty breathing; or
  • any two of the following new or worsening signs or symptoms: fever (≥38.0 °C or ≥100.4 °F), heart rate ≥90 beats/minute, shaking chills or rigors, sore throat, cough, malaise, headache, muscle pain (myalgia), gastrointestinal symptoms, new or changing olfactory or taste disorders, red or bruised appearing feet or toes.

Severe/critical COVID‑19 was defined based on the following criteria:

  • the participant must have experienced any one of the following at any time during the course of observation: clinical signs at rest indicative of severe systemic illness (respiratory rate ≥30 breaths/minute, heart rate ≥125 beats/minute, oxygen saturation [SpO2] ≤93% on room air at sea level, or partial pressure of oxygen/fraction of inspired oxygen [PaO2/FiO2] <300 mmHg), respiratory failure (defined as needing high-flow oxygen, non‑invasive ventilation, mechanical ventilation, or extracorporeal membrane oxygenation [ECMO]), evidence of shock (defined as systolic blood pressure <90 mmHg, diastolic blood pressure <60 mmHg, or requiring vasopressors), significant acute renal, hepatic, or neurologic dysfunction, admission to intensive care unit (ICU), death.

Final determination of severe/critical COVID‑19 cases were made by an independent adjudication committee.

The vaccine efficacy success criteria for the co‑primary endpoints, predefined by the sponsor, was a vaccine efficacy greater than 50%, with a lower bound of the 95% confidence interval (CI) above 30%.

At the time of the final primary efficacy analysis (cut‑off date of January 22, 2021), participants had been followed for symptomatic COVID‑19 disease for a median of 8 weeks post vaccination, corresponding to 3,143.7 person‑years for the Janssen COVID‑19 Vaccine and 3,146.7 person‑years in the placebo group.

As demonstrated through the results of the final primary efficacy analysis, the Janssen COVID‑19 Vaccine met both co‑primary endpoints of the ENSEMBLE Study and exceeded the success criterion of a vaccine efficacy greater than 50% and with the lower bound of the 95% CI above 30% set out by Health Canada's Guidance for Market Authorization Requirements for COVID‑19 Vaccines.

Vaccine efficacy success criteria
As defined in Health Canada's Guidance for Market Authorization Requirements for COVID-19 Vaccines
Target threshold of at least 50% vaccine efficacy, with a lower bound of the 95% confidence interval above 30%

Predefined by sponsor for ENSEMBLE Study, Phase III
A vaccine efficacy success criteria for the co‑primary endpoints greater than 50% with a lower bound of the 95% confidence interval (CI) above 30%
Efficacy rates observed in interim efficacy analysis (ENSEMBLE Study, Phase III)
  Vaccine efficacy rate 95% CI
14 days post vaccination
Against moderate to severe/critical COVID‑19:
Participants 18 years of age and older who were
seronegative or with unknown serostatus
66.9% 59.03% to 73.40%
28 days post vaccination
Against moderate to severe/critical COVID‑19:
Participants 18 years of age and older who were
seronegative or with unknown serostatus
66.1% 55.01% to 74.80%
14 days post vaccination
Against severe/critical COVID‑19:
Participants 18 years of age and older who were
seronegative or with unknown serostatus
76.7% 54.56% to 89.09%
28 days post vaccination
Against severe/critical COVID‑19:
Participants 18 years of age and older against who
were seronegative or with unknown serostatus
85.4% 54.15% to 96.90%

Vaccine efficacy for the co‑primary endpoints against molecularly confirmed moderate to severe/critical COVID-19 in individuals who were seronegative or who had an unknown serostatus at baseline was 66.9% (95% CI: 59.03; 73.40) as of 14 days after vaccination and 66.1% (95% CI: 55.01; 74.80) as of 28 days after vaccination. Higher vaccine efficacy was seen against moderate to severe/critical COVID‑19. The vaccine efficacy was 76.7% (95% CI: 54.56; 89.09) as of 14 days after vaccination and 85.4% (95% CI: 54.15; 96.90) as of 28 days after vaccination.

In the ENSEMBLE Study, 34.6% of participants were ≥60 years of age. The Janssen COVID‑19 Vaccine showed consistent efficacy across age groups against moderate to severe/critical COVID‑19, as well as against severe/critical COVID‑19. Vaccine efficacy was also consistent between genders, between Hispanics and non‑Hispanics, and between Black/African Americans and Caucasians. Across geographical regions, vaccine efficacy ranged from 52.0% to 74.4%, due to the impact of variants of concern. Though the presence of variants of concern in certain study sites appears to have impacted the overall vaccine efficacy in those regions, the vaccine seems to have maintained its efficacy against severe and critical COVID-19.

The Janssen COVID‑19 Vaccine was observed to have a positive impact on COVID‑19‑related hospitalization and COVID‑19‑associated death. As of 14 days after vaccination, 2 versus 29 cases of COVID‑19‑related hospitalizations were observed in the vaccine group compared to placebo. As of 28 days after vaccination, 0 versus 16 cases of COVID‑19‑related hospitalizations were observed in the vaccine group compared to placebo. There were no COVID‑19‑related deaths reported in vaccine recipients, compared to 5 COVID‑19‑related deaths reported in placebo recipients (all from South Africa), who were SARS‑CoV‑2 PCR‑negative at baseline.

The immunogenicity of the Janssen COVID‑19 Vaccine was evaluated based on Phase I and Phase II studies (COV1001, COV1002, and COV2001), and one Phase III ENSEMBLE Study (COV3001). Results from these studies indicate the Janssen COVID‑19 Vaccine elicited SARS‑CoV‑2 immune responses.

Evidence of the clinical safety of the Janssen COVID-19 Vaccine was based primarily on an interim analysis from the ongoing Phase III ENSEMBLE Study, with a cut-off date of January 22, 2021. At the time of the analysis, a total of 43,783 participants ≥18 years of age had been randomized and received either the Janssen COVID‑19 Vaccine (n = 21,895) or a placebo (n = 21,888) as a single intramuscular injection. At the time of the analysis, the median follow‑up was 58 days from vaccination. Enrollment was stratified by age (18 to 59 and ≥60 years of age), with 7,331 (33%) of participants in the Janssen COVID‑19 Vaccine group ≥60 years old.

Solicited adverse events and unsolicited adverse events to Day 28 post vaccination were collected in a subset of participants called the safety subset. This set included 6,376 participants from 45 sites in the United States, Brazil and South Africa, of whom 2,651 (39.4%) were ≥60 years of age. In this safety subset, 3,356 participants received the Janssen COVID‑19 Vaccine and 3,380 received a placebo.

In the safety subset, the Janssen COVID‑19 Vaccine exhibited moderate reactogenicity. The most frequently reported adverse reactions after a single‑dose administration were: pain at the injection site (48.7%), headache (39.0%), fatigue (38.3%), and myalgia (33.2%). The majority of these adverse reactions were mild to moderate in severity and resolved within 1 to 3 days.

Hypersensitivity adverse events were more common in the Janssen COVID‑19 Vaccine group (0.4%) than in the placebo group (0.3%). Hypersensitivity events in the vaccine group included rash and urticaria, which are likely related to vaccination. Additional hypersensitivity events considered related to vaccination were noted in an ongoing open‑label study (COV3012). These events included two cases of facial swelling and the serious adverse event of type IV hypersensitivity.

Imbalances in thromboembolic events between the Janssen COVID‑19 Vaccine group and the placebo group (15 vs. 10), tinnitus (6 vs. 0), vertigo (13 vs. 7) and seizures (4 vs. 1) were noted at the participant level. As a contributory effect of the Janssen COVID‑19 Vaccine could not be excluded for a minority of these events, they will be followed post‑market.

No imbalances in events were noted for Guillain-Barré syndrome or facial paralysis (Bell's palsy).

Overall, serious adverse event rates were lower in the Janssen COVID‑19 Vaccine group compared to the placebo group (0.4%; n = 90) and (0.6%; n = 137) respectively. When serious adverse events related to COVID-19 were excluded, serious adverse events were reported by 0.4% of participants in both the vaccine and placebo groups (83 and 95 participants respectively).

A total of 7 participants in the Janssen COVID‑19 Vaccine group, compared to 3 participants in the placebo group, experienced serious adverse events that were considered possibly related to the Janssen COVID‑19 Vaccine by the investigator. Three of these serious adverse events in the vaccine group were:

  • one case of fever, headache and asthenia in a 35‑year‑old male that occurred less than a day after vaccination;
  • one case of severe injection site pain in a 30‑year‑old male that occurred immediately after vaccination and was ongoing 10 weeks later; and
  • one case of type IV hypersensitivity in a 42‑year‑old male that occurred 3 days after vaccination.

The remaining four serious adverse events considered possibly related by the investigator, for which a contributing role for the vaccine could not be ruled out, were:

  • one case of Guillain-Barré Syndrome in a 60‑year‑old female that occurred 16 days after vaccination;
  • two cases of facial paralysis, one in a 62‑year‑old male that occurred 3 days after vaccination, and one in a 43‑year‑old male that occurred 16 days after vaccination; and
  • one case of pericarditis in a 68‑year‑old male that occurred 17 days after vaccination.

A contributory effect of the Janssen COVID‑19 Vaccine also could not be excluded for two additional serious adverse events: a case of transverse sinus thrombosis in a 25‑year‑old male that occurred 21 days after vaccination, and a case of hemiparesis in a 49‑year‑old female that occurred 26 days after vaccination.

No participants withdrew from the study due to an adverse event. There were 3 fatal adverse events in the vaccine group and 16 in the placebo group. None of the deaths were considered related to the Janssen COVID‑19 Vaccine.

The safety and efficacy of the Janssen COVID‑19 Vaccine in pregnant women have not been established. To date, women who were pregnant were excluded from the clinical studies. Up to the cut-off date of January 22, 2021, a total of 8 pregnancies were reported in the ENSEMBLE Study: 4 in the vaccine group and 4 in the placebo group. Of the pregnancies in the vaccine group, 2 are ongoing, one ended in spontaneous abortion, and one was an ectopic pregnancy. These participants continue to be followed for pregnancy outcomes. There is a pregnancy exposure registry that monitors pregnancy outcomes in women exposed to the Janssen COVID‑19 Vaccine during pregnancy. Women who are vaccinated with the Janssen COVID‑19 Vaccine during pregnancy are encouraged to enroll in the registry.

It is not known whether the components of the Janssen COVID-19 Vaccine or antibodies induced by the Janssen COVID-19 Vaccine are excreted in human breast milk. Human data are not available to assess the impact of the Janssen COVID-19 Vaccine on milk production or its effects on the breastfed child. The developmental and health benefits of breastfeeding should be considered along with the mother's clinical need for immunization against COVID‑19.

Adults with stable/well-controlled human immunodeficiency virus (HIV) infection or adults receiving chronic low‑dose immunosuppressive therapy (less than 20 mg of prednisone or equivalent) were included in Janssen COVID‑19 Vaccine Phase III clinical studies. Immunocompromised individuals including those receiving substantial immunosuppressive therapy may have a diminished immune response to the Janssen COVID‑19 Vaccine.

In regard to COVID‑19 variants, sera obtained 28 days after vaccination with the Janssen COVID‑19 Vaccine in the COV1001 study (in participants aged ≥18 to ≤55 years) showed an almost 9‑fold reduction in the ability to neutralize the B1.1.7 SARS‑CoV‑2 variant relative to the SARS‑CoV‑2 Victoria strain, which has high homology to the Wuhan‑Hu‑1 S sequence used to construct the vector‑based vaccine. With a more mature antibody response in sera obtained 70 days after vaccination, the reduction in neutralizing activity against the B1.1.7 variant was 3.3‑fold. Definitive data regarding protection against emerging SARS‑CoV‑2 variants (e.g., those originating in the United Kingdom, Brazil and South Africa) are not yet available. The potential impact on vaccine efficacy and safety will be monitored. As outlined in the terms and conditions, data regarding protection against emerging variants will be provided, when available.

Collectively, the results of the clinical efficacy and safety evaluation demonstrated that the Janssen COVID‑19 Vaccine met the safety requirements as specified in Health Canada's Guidance for Market Authorization Requirements for COVID-19 Vaccines. The vaccine was determined to be safe and well tolerated in participants 18 years of age and older when used according to the recommended dosage regimen (one standard dose of 5 x 1010 virus particles administered by intramuscular injection).

A Core Risk Management Plan (RMP) for the Janssen COVID-19 Vaccine was submitted by Janssen Inc. to Health Canada. The RMP is designed to describe known and potential safety issues, to present the monitoring scheme and when needed, to describe measures that will be put in place to minimize risks associated with the product. The RMP for the Janssen COVID-19 Vaccine includes information about the important potential risk of vaccine-associated enhanced disease (VAED) including vaccine-associated enhanced respiratory disease (VAERD). The RMP also identified seven areas of missing information: "use during pregnancy", "use in breastfeeding women", "use in immunocompromised patients", "use in patients with autoimmune or inflammatory disorders", "use in frail patients with comorbidities (e.g., chronic obstructive pulmonary disease, diabetes, chronic neurological disease, cardiovascular disorders)", "interaction with other vaccines", and "long-term safety". Upon review, Health Canada recommended the addition of additional important potential risks ("anaphylaxis" and "venous thromboembolism") and missing information ("use in the pediatric population <18 years of age" and "long-term effectiveness").

Overall, the RMP was considered to be acceptable and identified appropriate monitoring (pharmacovigilance) activities and risk minimization measures (i.e., Product Monograph and labelling) based on the safety profile of the product. The identified limitations and areas of missing information are managed through labelling and the RMP, and will continue to be investigated through ongoing and planned studies. The Phase III ENSEMBLE Study (COV3001) is ongoing and will continue to collect information on the long‑term safety and efficacy of the vaccine. In addition, there are post‑authorization commitments for monitoring the long‑term safety and efficacy of the Janssen COVID‑19 Vaccine. As outlined in the terms and conditions, the RMP will be updated to reflect additional safety information, including that which is relevant to the Canadian-specific context, as it becomes available. In addition to regulatory requirements for post-market monitoring and prioritized reporting of adverse events following immunization, monthly safety summary reports will be provided to Health Canada and will include information related to special populations (e.g., pregnant women). Results related to safety and effectiveness from ongoing and planned studies will be submitted as they become available. For more information, refer to the complete list of terms and conditions available on the Health Canada COVID‑19 vaccines and treatments portal.

Terms and conditions related to developing and implementing Canadian-specific labelling have also been put in place.

Given the high unmet medical need and the emergency context of the COVID‑19 pandemic, Health Canada considers that the Janssen COVID‑19 Vaccine has a favourable benefit‑risk balance and an acceptable safety profile.

Pursuant to Section 5 of the Interim Order, the Janssen COVID‑19 Vaccine has been authorized for sale in Canada, with associated terms and conditions set out to ascertain the continued quality, safety and efficacy of the product. At any time, the terms and conditions may be amended. In addition, the authorization may be revoked if new information does not support the safe and effective use of the product.

For more information, refer to the Clinical, Non‑clinical, and Quality (Chemistry and Manufacturing) Basis for Decision sections.

3 What steps led to the approval of Jcovden (previously the Janssen COVID-19 Vaccine)?

The application for authorization of the Janssen COVID-19 Vaccine (Ad26.COV2.S, recombinant) was filed on November 30, 2020, in accordance with section 3 of the Interim Order Respecting the Importation, Sale and Advertising of Drugs for Use in Relation to COVID-19 (Interim Order).

The intent of the Interim Order (signed by the Minister of Health on September 16, 2020), is to expedite the authorization of coronavirus disease 2019 (COVID-19) drugs, while still protecting the health and safety of Canadians who will use these drugs. Authorizations under this Interim Order will be granted only if Health Canada determines that the benefits and risks of the product are supported by evidence that the drug is safe, effective and of high quality, taking into consideration the uncertainties related to the drug in the context of the urgent public health needs related to COVID-19. As outlined in the Guidance Document: Information and Application Requirements for Drugs Authorized under the Interim Order, the Interim Order recognizes that applications may not be complete at the time of initial filing and information may be submitted as it becomes available, until the application is deemed complete. This process can reduce time to authorization for these important drugs while maintaining appropriate standards of safety, efficacy, and quality.

The Interim Order sets out a modified set of application requirements with the potential for a rolling submission of information. This allows Health Canada to begin its assessment using the information submitted by the applicant and accept new evidence as it becomes available until the application is deemed complete.

Following an expedited review of the clinical, non-clinical, and quality data submitted, Health Canada determined that sufficient evidence was provided to support the conclusion that the benefits associated with the Janssen COVID-19 Vaccine outweigh the risks, taking into consideration the uncertainties relating to the benefits and risks and the necessity of addressing the urgent public health need related to COVID-19. An authorization for sale of the Janssen COVID-19 Vaccine, with imposed terms and conditions, was issued by Health Canada on March 5, 2021.

 

Submission Milestones: Jcovden (previously the Janssen COVID-19 Vaccine)

Submission Milestone Date
Pre-application meeting 2020-10-28
Pre-application meeting 2020-11-03
Initial application filed by sponsor 2020-11-30
Initial non-clinical data submitted by sponsor 2020-11-30
Initial quality data submitted by sponsor 2020-11-30
Initial clinical data submitted by sponsor 2020-11-30
Risk Management Plan submitted by sponsor 2021-02-19
Educational material submitted by sponsor 2021-02-26
Health Canada Biostatistics Evaluation complete 2021-03-04
Health Canada Quality Evaluation complete 2021-03-04
Health Canada Review of Risk Management Plan complete 2021-03-04
Terms and Conditions finalized by Health Canada 2021-03-04
Health Canada Clinical/Medical Evaluation complete 2021-03-04
Final Product Monograph (English and French) submitted by sponsor 2021-03-04
Health Canada Labelling Review complete 2021-03-04
Interim authorization issued by Director General, Biologic and Radiopharmaceutical Drugs Directorate, Health Canada 2021-03-05

The Canadian regulatory decision on the review of the Janssen COVID-19 Vaccine was based on a critical assessment of the data package submitted to Health Canada. Correspondence between the sponsor and the European Medicines Agency and the Food and Drug Administration (FDA) was also consulted. Information presented by the sponsor to the FDA Vaccines and Related Biological Products Advisory Committee was used as an added reference.

For further information on authorization under this pathway, refer to Health Canada's Interim Order Respecting the Importation, Sale, and Advertising of Drugs for Use in Relation to COVID‑19 and the Information and Application Requirements for Drugs Authorized under the Interim Order: Guidance Document.

4 What follow-up measures will the company take?

In accordance with section 10 of the Interim Order Respecting the Importation, Sale, and Advertising of Drugs for Use in Relation to COVID-19 (Interim Order), terms and conditions were imposed on the authorization issued in respect of the Janssen COVID-19 Vaccine.

These terms and conditions set out requirements relating to clinical information, quality (chemistry and manufacturing), risk management plan (RMP) elements, and labelling, and were put in place to ascertain the continued quality, safety, and efficacy of the product.

The terms and conditions include (but are not limited to) the following:

  • Provide updated clinical study reports on vaccine efficacy, safety and immunogenicity from Study COV3001, as soon as they are available.
  • Provide safety updates for participants in Study COV3001 when 6‑month data that is representative of the overall trial population is available, which includes elderly participants.
  • Provide a discussion describing how Janssen intends to monitor long‑term efficacy and safety once Study COV3001 is unblinded and the placebo group is administered the vaccine.
  • Provide updated clinical study reports on vaccine efficacy, safety and immunogenicity from Studies COV2001, COV1002, and COV1001, as soon as they are available.
  • Provide the results of the coagulopathy assessments in Study COV2001 as soon as they are available.
  • Provide updated clinical study reports on vaccine efficacy, safety and immunogenicity from Study 3009, as soon as they are available.
  • Provide a list and brief descriptions of all clinical trials currently underway.
  • Provide data regarding protection against variants of concerns (e.g., B.1.1.7, B.1.351 [501Y.V2], P1), including new or emerging variants (e.g., CAL.20C [L452R], B.1.525, A.23.1) when available, if their clinical presentation and/or epidemiological distribution warrants it.

Additionally, the sponsor will:

  • Submit prompt reporting of adverse reactions to the Canada Vigilance Program.
  • Submit monthly safety reports for the period of the Interim Order authorization, unless otherwise determined by Health Canada.
  • Provide, prior to distribution, patient information cards to support traceability, where required, which will include elements such as manufacturer name, name of vaccinee, space for recording date of administration, and associated batch/lot numbers, and information on how to report any adverse events.
  • Provide a Canadian addendum to the Core RMP that will include anaphylaxis and venous thromboembolism as important potential risks and describe planned pharmacovigilance monitoring activities for use in pregnant and breastfeeding women. It will also specify use in pediatric populations (i.e., younger than 18 years of age) and long‑term effectiveness data as missing information.
  • Provide an updated Core RMP and a Canadian Addendum in a timely manner if a signal of safety issue is observed in post‑authorization surveillance.
  • Submit final snapshots of all components of the electronic platform (linked to on the global labels), containing Canadian-specific labelling information for the Janssen COVID-19 Vaccine in French and English for Health Canada's review and records, prior to launch of the electronic platform.
  • Develop and distribute a Health Product Risk Communication, in French and English, with Health Canada approval and endorsement, to inform healthcare professionals about the authorization of the Janssen COVID‑19 Vaccine under the Interim Order with the English‑only vial and carton labels to expedite global access of the drug in the context of the pandemic.
    • The letter should direct healthcare professionals to the electronic platform where they can find information about the approved Canadian‑specific labelling and expiry date information in both official languages and should be issued prior to, and alongside, the distribution of the vaccine until such time as Canadian-specific labelling is implemented.
  • Commit to developing Canadian‑specific bilingual labelling for the Janssen COVID‑19 Vaccine and implementing such labelling at a point when the global supply and pandemic situation will allow. Health Canada should be kept informed of estimated timelines and proposed strategies concerning the development and implementation of Canadian‑specific bilingual labels.
  • Commit to revising all inner and outer labels for the Janssen COVID‑19 Vaccine to include the printed expiry date information at a point when the global supply and pandemic situation will allow.
  • Submit a certificate of analysis for each lot distributed in Canada, as outlined in the Guidance for market authorization requirements for COVID‑19 vaccines: Quality, manufacturing and lot release requirements. A summary of batch disposition should be submitted on a biannual basis.
  • Promptly provide information with regard to additional process and assay validation, stability studies and any new manufacturing facilities or manufacturing changes to ensure continued alignment with the authorization under the Interim Order.
  • Provide stability information in a timely manner to support extension of the expiry date. Once approved, relevant databases should be updated with the new expiry date.
  • Provide notification of changes in the Good Manufacturing Practices status, when available, for any of the facilities included in the authorization as well as any new facilities relevant to the Canadian supply chain.
6 What other information is available about drugs?

Health Canada is committed to providing up‑to‑date information related to vaccines and treatments for COVID‑19. Up‑to‑date information can be found at the following links:

7 What was the scientific rationale for Health Canada's decision?
7.1 Clinical Basis for Decision

The clinical data provided in the application for authorization of the Janssen COVID-19 Vaccine (Ad26.COV2.S, recombinant) under the Interim Order Respecting the Importation, Sale, and Advertising of Drugs for Use in Relation to COVID-19 (Interim Order) included results based on the interim efficacy analysis data from the ongoing Phase III efficacy, safety, and immunogenicity study (Study COV3001 or the ENSEMBLE Study), in which the two co‑primary efficacy endpoints were met. Data from the first-in-human study (COV1001), Phase I and II studies (COV1002 and COV2001), and a Phase III study (COV3009) have also been submitted in support of the vaccine, dosage regimen, and the safety and immunogenicity of the vaccine. The clinical data reviewed in this application were submitted on a rolling basis, as is permitted under the Interim Order. Correspondence between the sponsor and the European Medicines Agency and the Food and Drug Administration was also consulted. Information presented by the sponsor to the Vaccines and Related Biological Products Advisory Committee was used as an added reference.

Initial immunogenicity and safety data (28 days post Dose 1 data from Cohort 1a and available data from Cohort 3) from the COV1001 study demonstrated that a single‑dose of Ad26.COV2.S, (recombinant), the medicinal ingredient in the Janssen COVID‑19 Vaccine, at dose levels of 5 x 1010 virus particles induced a sufficient immune response and is safe. The sponsor therefore chose to proceed with the single‑dose regimen at a dose level of 5 x 1010 virus particles in the ENSEMBLE Study.

Following review, terms and conditions were imposed upon the authorization of the Janssen COVID-19 Vaccine to ascertain the continued quality, safety, and efficacy of the product.

Clinical Pharmacology

The Janssen COVID‑19 Vaccine is a monovalent vaccine composed of a recombinant, replication‑incompetent human adenovirus type 26 (Ad26) vector, constructed to encode the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) spike (S) protein in a stabilized conformation. The S protein on the surface of the coronavirus binds to the angiotensin‑converting enzyme 2 (ACE2) receptor of a host cell, allowing the virus to infect the cell. Vaccination with the Janssen COVID-19 Vaccine leads to humoral and cellular immune responses directed against the S protein and in particular the production of neutralizing and other functional anti‑S antibodies which can block the binding of the S protein to the ACE2 receptor, contributing to protection against COVID‑19.

Immunogenicity was assessed as part of the clinical efficacy evaluation of the Janssen COVID‑19 Vaccine.

For further details, please refer to the Janssen COVID‑19 Vaccine Product Monograph, approved by Health Canada and available through the Drug Product Database and on the Health Canada COVID‑19 vaccines and treatments portal.

Clinical Efficacy

Evidence of the clinical efficacy of the Janssen COVID‑19 Vaccine (Ad26.COV2.S, recombinant) is based primarily on the available data from the pivotal ENSEMBLE Study (Study COV3001) which assessed the efficacy, safety, and immunogenicity of the Janssen COVID‑19 Vaccine. The interim analysis results are based on a cut-off date of January 22, 2021.

The ENSEMBLE Study is an ongoing Phase III randomized, double‑blind, placebo‑controlled study that evaluated a single intramuscular injection of the Janssen COVID‑19 Vaccine (5 x 1010 virus particles/0.5 mL) for the prevention of COVID-19 in adults aged 18 years and older. The study is currently being conducted in the United States, South Africa, Brazil, Chile, Argentina, Columbia, Peru, and Mexico.

The ENSEMBLE Study has enrolled 44,325 participants 18 years of age and older, of whom 43,783 were vaccinated (21,895 in the Janssen COVID‑19 Vaccine group and 21,888 in the placebo group). A total of 39,321 participants were included in the per‑protocol set with 19,630 in the Janssen COVID‑19 Vaccine group and 19,691 in the placebo group.

The median age in the per‑protocol set was 53.0 years. In total, 66.4% of participants were ≥18 to <60 years of age and 34.6% of the participants were ≥60 years of age, and 20.4% and 3.6% of the participants were ≥65 and ≥75 years of age, respectively. The majority of participants were Caucasian (62.1%), Black/African American (17.2%), Native American (8.4%), or Asian (3.7%). Lastly, 39.9% of the participants had one or more comorbidities, consisting of stable pre-existing medical conditions, defined as disease not requiring significant change in therapy during the 3 months preceding vaccination, as well as individuals with stable human immunodeficiency virus (HIV) infection. The most common pre-existing medical conditions were obesity, hypertension, type 2 diabetes mellitus, serious heart conditions, and asthma. Other comorbidities were present in ≤1% of the participants. Human immunodeficiency virus infection was reported at baseline in 2.5% of the participants. Participants with comorbidities were phased into the ENSEMBLE Study only after the safety review of 2,000 participants without comorbidities (for participants ≥18 to <60 years of age in stage 1, and for participants ≥60 years of age in stage 2).

Participants who had previously received a coronavirus vaccine, pregnant women, and participants with abnormal function of the immune system were ineligible to participate in the ENSEMBLE Study. Participants were also excluded if they had known or suspected allergy or a history of anaphylaxis or serious adverse reactions to vaccines or their excipients.

The study design included stratification of the participants by age (18 to 59 years, 60 years and older) in addition to the presence or absence of comorbidities associated with an increased risk of progression to severe COVID‑19. Participants were then randomized in a 1:1 ratio to receive either an intramuscular injection of the Janssen COVID‑19 Vaccine (at a dose level of 5 x 1010 virus particles; number of participants [n] = 21,895) or a placebo (0.9% sodium chloride; n = 21,888). The study included a median follow‑up of 2 months after vaccination. It is planned that participants will be followed for up to 2 years for assessment of safety and efficacy against COVID‑19.

The primary efficacy endpoint of the ENSEMBLE Study was defined as a symptomatic moderate to severe/critical COVID‑19 case, confirmed by positive SARS COV-2 viral ribonucleic acid (RNA) results using a polymerase chain reaction (PCR)‑based test in a central laboratory. To conduct the evaluation, the ENSEMBLE Study contained two co‑primary endpoints as follows:

  • first occurrence of molecularly confirmed moderate to severe/critical COVID‑19, with onset at least 14 days post vaccination (Day 15);
  • first occurrence of molecularly confirmed moderate to severe/critical COVID‑19, with onset at least 28 days post vaccination (Day 29).

Moderate COVID‑19 was defined based on the following criteria:

  • the participant must have experienced any one of the following new or worsening signs or symptoms: respiratory rate ≥20 breaths/minute, abnormal saturation of oxygen (SpO2) but still >93% on room air at sea level, clinical or radiologic evidence of pneumonia, radiologic evidence of deep vein thrombosis (DVT), shortness of breath or difficulty breathing; or
  • any two of the following new or worsening signs or symptoms: fever (≥38.0 °C or ≥100.4 °F), heart rate ≥90 beats/minute, shaking chills or rigors, sore throat, cough, malaise, headache, muscle pain (myalgia), gastrointestinal symptoms, new or changing olfactory or taste disorders, red or bruised appearing feet or toes.

Severe/critical COVID‑19 was defined based on the following criteria:

  • the participant must have experienced any one of the following at any time during the course of observation: clinical signs at rest indicative of severe systemic illness (respiratory rate ≥30 breaths/minute, heart rate ≥125 beats/minute, oxygen saturation [SpO2] ≤93% on room air at sea level, or partial pressure of oxygen/fraction of inspired oxygen [PaO2/FiO2] <300 mmHg), respiratory failure (defined as needing high-flow oxygen, non‑invasive ventilation, mechanical ventilation, or extracorporeal membrane oxygenation [ECMO]), evidence of shock (defined as systolic blood pressure <90 mmHg, diastolic blood pressure <60 mmHg, or requiring vasopressors), significant acute renal, hepatic, or neurologic dysfunction, admission to intensive care unit (ICU), death.

Final determination of severe/critical COVID‑19 cases was made by an independent adjudication committee.

At the time of the interim efficacy analysis cut-off date January 22, 2021, participants had been followed for symptomatic COVID‑19 for a median of 2 months, corresponding to 3,143.7 person‑years in the Janssen COVID‑19 Vaccine group and 3,146.7 person‑years in the placebo group.

Results from the ENSEMBLE Study demonstrated that both co‑primary efficacy endpoints were met. For the first co‑primary endpoint with onset as of 14 days after vaccination, there were 116 cases of moderate to severe/critical COVID-19 in the vaccine group and 348 in the placebo group. For the second co‑primary endpoint with onset as of 28 days after vaccination, there were 66 cases of moderate to severe/critical COVID‑19 in the vaccine group and 193 in the placebo group. Vaccine efficacy for the co‑primary endpoints against moderate to severe/critical COVID‑19 in individuals who were seronegative (or of unknown serostatus) at baseline was 66.9% (95% confidence interval [CI]: 59.0; 73.4) as of 14 days after vaccination and 66.1% (95% CI: 55.0; 74.8) as of 28 days after vaccination. Higher vaccine efficacy was observed against severe/critical COVID‑19. The vaccine efficacy as of 14 days after vaccination was 76.7%, and was 85.4% as of 28 days after vaccination. Efficacy against COVID‑19 was consistent across age, gender, race, and ethnicity demographics.

Vaccine efficacy against moderate to severe/critical COVID‑19 as of 14 days after vaccination was 67.6% (95% CI: 59.38; 74.30) in participants without comorbidities and 64.2% (95% CI: 52.68; 73.14) in participants with comorbidities. Vaccine efficacy against moderate to severe/critical COVID‑19 as of 28 days after vaccination was 68.8% (95% CI: 58.98; 76.58) in participants without comorbidities and 58.6% (95% CI: 40.57; 71.55) in participants with comorbidities. The slightly lower vaccine efficacy observed in participants with comorbidities could be due to differences in length of follow‑up, since participants with comorbidities were included in the later stages of the study by design.

Janssen COVID‑19 Vaccine was observed to have a positive impact on COVID‑19‑related hospitalization and COVID‑19‑associated death. As of 14 days after vaccination, 2 versus 29 cases of COVID‑19‑related hospitalizations were observed in the vaccine group compared to placebo. As of 28 days after vaccination, 0 versus 16 cases of COVID‑19‑related hospitalizations were observed in the vaccine group compared to placebo. There were no COVID‑19‑related deaths reported in vaccine recipients, compared to 5 COVID‑19‑related deaths reported in placebo recipients (all from South Africa), who were SARS‑CoV‑2 PCR‑negative at baseline.

Among the 39,321 participants in the ENSEMBLE Study, a total of 20.4% (8,021) and 3.7% (1,455) of the participants were ≥65 and ≥75 years of age, respectively. When the Janssen COVID‑19 Vaccine was assessed in this subpopulation, vaccine efficacy against moderate to severe/critical COVID‑19 as of 14 and as of 28 days after vaccination in participants ≥65 years of age was 76.5% (95% Confidence Interval [CI]: 59.12; 87.30) and 68.6% (95% CI: 38.60; 85.06), respectively. For participants ≥75 years vaccine efficacy was 89.7% (95% CI: 25.95; 99.77) as of 14 days after vaccination. In regard to COVID‑19 cases reported with onset at least 28 days after vaccination, there were 0 cases in the Janssen COVID‑19 Vaccine and 4 cases in the placebo group.

A difference in the point estimates of vaccine efficacy against moderate to severe/critical COVID‑19 was observed in participants ≥60 years of age with and without comorbidities. As of 28 days after vaccination, the point estimate for vaccine efficacy against moderate to severe/critical COVID‑19 in participants ≥60 years of age without comorbidities was 72.4% (95% CI: 45.04; 87.25), while the point estimate for participants ≥60 years with comorbidities was 42.3% (95% CI: ‑13.14; 71.57). The observed differences in vaccine efficacy are partially driven by the relatively low number of cases, which explains the relatively wide confidence intervals around the point estimates of the vaccine efficacy in these subgroup analyses. This could also be due to differences in the length of follow‑up, since older participants and participants with comorbidities were included in the later stages of the study. For participants ≥60 years of age without comorbidities, approximately 50% and 25% of participants were followed for at least 56 days and 72 days after vaccination, respectively. In contrast, only 25% of participants ≥60 years of age with comorbidities were followed for approximately 56 days after vaccination, and none were followed at least 72 days after vaccination.

Exploratory subgroup analyses of vaccine efficacy against moderate to severe/critical COVID‑19 in different regions (Brazil, South Africa, and the United States) were conducted in parallel with strain sequencing. For these subgroup analyses, all COVID‑19 cases (PCR‑positive cases confirmed and pending confirmation by the central laboratory) accrued up to the primary efficacy analysis data cut-off date of January 22, 2021 were included.

Strain sequencing was conducted on available samples with sufficient viral load from centrally confirmed COVID‑19 cases (one sequence per case). A total of 71.7% of central laboratory confirmed primary analysis cases have been sequenced (United States [73.5%], South Africa [66.9%] and Brazil [69.3%]). In the United States, 96.4% of strains were identified as the Wuhan‑H1 variant D614G; in South Africa, 94.5% were identified as the 20H/501Y.V2 variant (B.1.351 lineage); in Brazil, 69.4% were identified to be a variant of the P.2 lineage and 30.6% as the Wuhan‑H1 variant D614G. As of February 12, 2021, SARS‑CoV‑2 variants from the B1.1.7 or P.1 lineages were not found in any of the sequenced samples.

In the United States specifically, the vaccine efficacy against all moderate to severe/critical cases of COVID‑19 was 74.4% (95% CI: 65.00; 81.57) as of Day 14, and 72.0% (95% CI: 58.19; 81.71) as of Day 28. In South Africa the corresponding vaccine efficacy rates were 52.0% (95% CI: 30.26; 67.44) and 64.0% (95% CI: 41.19; 78.66), respectively. In Brazil the corresponding vaccine efficacy rates were 66.2% (95% CI: 51.01; 77.14) and 68.1% (95% CI: 48.81; 80.74), respectively. Vaccine efficacy against all severe/critical cases of COVID‑19 in the United States was 78.0% (95% CI: 33.13; 94.58) 14 days after vaccination, and 85.9% (95% CI: 99.38; 99.69) 28 days after vaccination. In South Africa the corresponding vaccine efficacy rates were 73.1% (95% CI: 40.03; 89.36) and 81.7% (95% CI: 46.18; 95.42), respectively. In Brazil the corresponding vaccine efficacy rates were 81.9% (95% CI: 17.01; 98.05) and 87.6% (95% CI: 7.84; 99.72), respectively.

Collectively, the results of the efficacy analysis demonstrated that the Janssen COVID-19 Vaccine met the vaccine efficacy success criteria as specified in Health Canada's Guidance Document, Guidance for Market Authorization Requirements for COVID-19 Vaccines. The Phase III ENSEMBLE Study is ongoing and data will be submitted to assess longer-term safety. In addition, the study will continue to provide additional information on the safety and efficacy of the Janssen COVID‑19 vaccine over a period of 2 years.

Immunogenicity

The immunogenicity of the Janssen COVID-19 Vaccine was evaluated in four studies, one Phase I, two Phase I/II, and one Phase III.

  • Study COV1001 is a randomized, double‑blind, placebo‑controlled, Phase I/IIa study, conducted in adults ≥18 to ≤55 years of age (Cohort 1 and Cohort 2) and adults ≥65 years of age (Cohort 3).
  • Study COV1002 is a randomized, double‑blind, placebo‑controlled, Phase I study, conducted in adults ≥20 to ≤55 years of age and ≥65 years of age.
  • Study COV2001 is a randomized, double‑blind, placebo‑controlled, Phase IIa study, conducted in adults ≥18 to ≤55 years of age and adults ≥65 years of age.
  • Study COV3001 (ENSEMBLE Study) is a randomized, double‑blind, placebo‑controlled, Phase III study, conducted in adults ≥18 years of age.

The immunogenicity of the Janssen COVID‑19 Vaccine was evaluated using the following methods: neutralizing antibodies were measured with a wild type SARS‑CoV‑2 neutralization assay (wtVNA), spike protein‑binding antibody responses were measured using a spike‑enzyme‑linked immunosorbent assay (S-ELISA), and cellular immunogenicity was measured using S‑specific CD4+ and CD8+ T‑cell responses.

For both the wtVNA and S‑ELISA assays, a participant was considered to have responded to vaccination if one of the following criteria were met:

  • If the baseline sample value was negative (i.e., below the lower limit of quantification) and the post‑vaccination sample value was positive; or
  • If the baseline sample value was positive (i.e., above the lower limit of quantification) and the post‑vaccination sample value was ≥4‑fold over the baseline sample.

The immunogenicity data should be interpreted with caution, because there is no immune correlate of protection. These analyses were exploratory, and the results are based on small groups of subjects.

Humoral Immunogenicity

Across the Phase I and II studies (COV1001, COV1002, and COV2001), a SARS‑CoV‑2 neutralizing antibody response was observed at Day 29 in at least 88% of participants ≥18 to ≤55 years of age and at least 93% of participants ≥65 years of age.

In study COV1001, neutralizing antibody responses were 96% at Day 29, and 100% at Day 57, Day 71 and Day 85, in individuals ≥18 to ≤55 years of age. In individuals ≥65 years of age, neutralizing antibody responses were 100% at Day 15, 96% at Day 29, and 90% at Day 87.

In the Phase III ENSEMBLE Study (COV3001), S‑specific binding antibody concentrations increased from baseline (geometric mean concentration [GMC] <lower limit of quantification [LLOQ]) to Day 29 with a GMC of 462 (95% CI: 381; 560) in participants ≥18 to 59 years of age, and a GMC of 347 (95% CI: 278; 434) in participants ≥60 years of age. No major difference was observed in S‑specific binding antibody levels induced by the Janssen COVID‑19 Vaccine between participants from Brazil, South Africa, and the United States.

In the placebo groups, no overall humoral response was observed at any of the time points.

Cellular Immunogenicity

In COV1001, a single dose of the Janssen COVID‑19 vaccine elicited CD4 and CD8 T‑cell responses in participants ≥18 to ≤55 years of age and individuals ≥65 years of age, at Day 28. The CD4 T‑cell responses were skewed towards a Th1 phenotype.

Immunogenicity Against the B1.1.7 SARS‑CoV‑2 Variant

Sera obtained 28 days after vaccination with the Janssen COVID‑19 vaccine in the COV1001 study (in participants aged ≥18 to ≤55 years) showed an almost 9‑fold reduction in the ability to neutralize the B1.1.7 SARS‑CoV‑2 variant relative to the SARS‑CoV‑2 Victoria strain, which has high homology to the WuhanHu‑1 S sequence used to construct the vector‑based vaccine. With a more mature antibody response in sera obtained 70 days after vaccination, the reduction in neutralizing activity against the B1.1.7 variant was 3.3‑fold.

Indication

The sponsor filed the application for authorization of the Janssen COVID‑19 Vaccine under the Interim Order with the following indication:

  • Janssen COVID‑19 Vaccine (Ad26.COV2.S, recombinant) is indicated for active immunization against coronavirus disease 2019 (COVID‑19) caused by severe acute respiratory syndrome coronavirus 2 (SARS‑CoV‑2) in persons 18 years of age and older.

Health Canada approved the following indication:

  • Janssen COVID‑19 Vaccine (SARS‑CoV‑2 Vaccine [Ad26.COV2.S, recombinant]) is indicated for active immunization for the prevention of coronavirus disease 2019 (COVID‑19) caused by SARS‑CoV‑2 virus in individuals 18 years of age and older.

For more information, refer to the Janssen COVID-19 Vaccine Product Monograph, approved by Health Canada and available through the Drug Product Database and on the Health Canada COVID‑19 vaccines and treatments portal.

 

Clinical Safety

The evidence of safety for the Janssen COVID-19 Vaccine is largely based on data from the ongoing pivotal Phase III COV3001 study (ENSEMBLE Study) with a cut-off date of January 22, 2021.

The full analysis set included 43,783 participants aged 18 years and older, of whom 21,895 received the Janssen COVID-19 Vaccine (dose 5 x 1010 virus particles) and 21,888 received a saline placebo. At the time of the analysis, the median follow‑up was 58 days from vaccination. Enrollment was stratified by age (18 to 59 and ≥60 years of age) and 7,331 (33%) of participants in the Janssen COVID‑19 Vaccine group were ≥60 years old.The median age of individuals was 53 years. The safety analysis was performed once the median follow‑up duration of 2 months after vaccination was reached. The participants were monitored for solicited local and systemic reactions, unsolicited adverse events and serious adverse events.

Solicited adverse reactions and unsolicited adverse events were collected in a subset of participants called the safety subset. This set included 6,376 participants from 45 sites in the United States, Brazil, and South Africa. Of the 6,376 participants, 2,651 (39.4%) participants were ≥60 years of age. A total of 3,356 participants received the Janssen COVID-19 Vaccine and 3,380 received the placebo.

Solicited Adverse Reactions

Solicited local and systemic adverse reactions were collected in the safety subset for the first 7 days after vaccination. Assessments included local reactions (pain, erythema, and swelling) and systemic reactions (fatigue, headache, myalgia, nausea, and fever). Both solicited local and systemic adverse reactions were more common in participants who received the Janssen COVID‑19 Vaccine compared with placebo (66.0% vs. 41.9% respectively). Solicited events were more commonly reported by younger adults (18 to 59 years of age) than by older adults (≥60 years of age). The majority of these events were mild to moderate in severity, with slightly lower rates of Grade ≥3 events in the older age group. No Grade 4 adverse reactions were reported. Time to onset and duration of both local and systemic adverse reactions were similar in younger and older adults and in participants with and without comorbidities.

Solicited local adverse reactions were more common in participants who received the Janssen COVID‑19 Vaccine than in those who received placebo (50.3 and 41.9% respectively). The most common solicited local adverse reaction was vaccination site pain, which occurred in 48.7% of participants in the Janssen COVID‑19 Vaccine group and 16.7% in the placebo group. The majority of local adverse reactions occurred within the first 2 to 3 days post vaccination, with a median duration of 2 to 3 days.

Solicited systemic adverse reactions were more common in participants who received the Janssen COVID‑19 Vaccine than in those who received placebo (55.2% vs. 35.1%). The most common solicited systemic adverse reactions were headache and fatigue which occurred in almost 40% of participants, and myalgia which occurred in a third of participants. The most common systemic events of Grade ≥3 severity were fatigue and myalgia which each occurred at rates of 1.0%. The majority of local adverse reactions began within the first 2 to 3 days post vaccination and the median duration was 1 to 2 days.

Unsolicited Adverse Events

Within the first 28 days after vaccination, the incidence of unsolicited adverse events was similar for the Janssen COVID‑19 Vaccine group and the placebo group (13.1% and 12.0% respectively). Most unsolicited adverse events were Grade 1 or Grade 2 in severity, with 0.6% in both the vaccine and placebo groups reporting an adverse event of ≥ Grade 3 severity. Related unsolicited adverse events in the first 28 days were higher in the Janssen COVID‑19 Vaccine group than in the placebo group (7.2% vs. 4.6% respectively).The imbalance was primarily due to an imbalance in related adverse events in the General Disorders and Administration Site Conditions category (5.2% vs. 2.6%) which were related to reactogenicity.

Serious Adverse Events

Overall, serious adverse event rates were lower in the Janssen COVID‑19 Vaccine group than in the placebo group (0.4% [n = 90] and 0.6% [n = 137] respectively). When serious adverse events related to COVID-19 were excluded, serious adverse events were reported by 0.4% of participants in both the vaccine and placebo groups (83 and 95 participants, respectively).

A total of 7 participants in the Janssen COVID‑19 Vaccine group compared to 3 participants in the control group experienced serious adverse events that were considered possibly related to the Janssen COVID‑19 Vaccine by the investigator. Three of these serious adverse events in the Janssen COVID‑19 Vaccine group were:

  • one case of fever, headache and asthenia in a 35‑year‑old male that occurred less than a day after vaccination;
  • one case of severe injection site pain in a 30‑year‑old male that occurred immediately after vaccination and was ongoing 10 weeks later; and
  • one case of type IV hypersensitivity in a 42‑year‑old male that occurred 3 days after vaccination.

For the remaining four serious adverse events considered possibly related by the investigator, a contributing role of the Janssen COVID‑19 Vaccine could not be ruled out:

  • one case of Guillain-Barré Syndrome in a 60‑year‑old female that occurred 16 days after vaccination;
  • two cases of facial paralysis, one in a 62‑year‑old male that occurred 3 days after vaccination, and one in a 43‑year‑old male that occurred 16 days after vaccination; and
  • one case of pericarditis in a 68‑year‑old male that occurred 17 days after vaccination.

A contributory effect of the vaccine also could not be excluded for two additional serious adverse events: a case of transverse sinus thrombosis in a 25‑year‑old male that occurred 21 days after vaccination, and a case of hemiparesis in a 49‑year‑old female that occurred 26 days after vaccination.

No participants withdrew from the ENSEMBLE Study due to an adverse event. There were 3 fatal adverse events in the vaccine group and 16 in the placebo group. None of the deaths were considered related to the Janssen COVID‑19 Vaccine.

Other Adverse Events of Interest

Hypersensitivity events, including both serious and non‑serious reactions, occurred more frequently in the Janssen COVID‑19 Vaccine group than in the placebo group (0.4% and 0.3% respectively). Hypersensitivity events in the vaccine group which were considered likely related to vaccination included rash and urticaria, two cases of facial swelling, a case of lip swelling, a case of eyelid swelling and a serious adverse event of type IV hypersensitivity.

An imbalance of thromboembolic events was noted with 15 cases in the Janssen COVID‑19 Vaccine group and 10 in the placebo group. Deep vein thrombosis and pulmonary embolism were more frequent in the Janssen COVID‑19 Vaccine group than in the placebo group (10 vs. 3); receipt of the vaccine was considered a possible contributing factor for two cases of deep vein thrombosis and one case of pulmonary embolism. Receipt of the vaccine could also not be excluded as a contributing factor in the serious adverse events of transverse sinus thrombosis and hemiparesis. The sponsor has undertaken a coagulopathy work up of a subset of participants in Study COV2001, and thromboembolic events will be monitored post authorization.

Imbalance in neurological events was noted for tinnitus, vertigo and seizures. Six cases of tinnitus were reported in the Janssen COVID‑19 Vaccine group and none in the placebo group. Two cases of tinnitus were considered related to the vaccine. Thirteen cases of vertigo occurred in the vaccine group as compared to 7 in the placebo group, of which 5 cases occurred in the vaccine group of the safety subset in the first 28 days. In the full analysis set, four cases of vertigo were considered related to the vaccine by the investigator. Four cases of seizures were reported in the vaccine group and none were reported in the placebo group; none were considered related to the vaccine. One case of Guillain‑Barré syndrome occurred in both groups. Facial paralysis (Bell's palsy) occurred in 3 participants in the vaccine group and in 2 participants in the control group.

Fewer cases of COVID‑19 were reported in the Janssen COVID‑19 Vaccine group compared to the control group. There was no evidence of vaccine‑associated enhanced disease (VAED) at this time. Vaccine‑associated enhanced disease will continue to be assessed as additional data becomes available.

Special Populations

Pregnant and Breastfeeding Women

The safety and efficacy of the Janssen COVID‑19 Vaccine in pregnant women have not yet been established.

To date, women who were pregnant were excluded from the Janssen COVID‑19 clinical studies. Up to the cut-off date of January 22, 2021, a total of 8 pregnancies were reported in the ENSEMBLE Study: 4 in the Janssen COVID‑19 Vaccine group and 4 in the placebo group. Of the pregnancies in the vaccine group, 2 are ongoing, one ended in spontaneous abortion, and one was an ectopic pregnancy. These participants continue to be followed for pregnancy outcomes. There is a pregnancy exposure registry that monitors pregnancy outcomes in women exposed to the Janssen COVID‑19 Vaccine during pregnancy. Women who are vaccinated with the Janssen COVID‑19 Vaccine during pregnancy are encouraged to enroll in the registry.

It is not known whether the components of the Janssen COVID-19 Vaccine or antibodies induced by the Janssen COVID-19 Vaccine are excreted in human breast milk. Human data are not available to assess the impact of the Janssen COVID-19 Vaccine on milk production or its effects on the breastfed child. The developmental and health benefits of breastfeeding should be considered along with the mother's clinical need for immunization against COVID‑19.

Immunocompromised Individuals

Adults with stable/well-controlled human immunodeficiency virus (HIV) infection or adults receiving chronic low‑dose immunosuppressive therapy (less than 20 mg of prednisone or equivalent) were included in Janssen COVID‑19 Vaccine Phase III clinical studies. Immunocompromised individuals including those receiving substantial immunosuppressive therapy may have a diminished immune response to Janssen COVID‑19 Vaccine.

Vaccine Safety from Other Studies

Up to the data cut‑off of January 22, 2021, across studies COV1001, COV1002, COV2001, and COV3009, a total of 26 participants reported one or more serious adverse event. One serious adverse event considered to be vaccine‑related was reported in study COV1001: a case of Grade 3 pyrexia beginning 6 hours post vaccination in a participant who received a high dose of Janssen COVID‑19 Vaccine (1 x 1011 virus particles). No safety concerns were identified in any of these studies.

In COV3012, an ongoing Phase IIIb open‑label single‑arm effectiveness study conducted in South Africa, two additional serious hypersensitivity adverse events (including one confirmed anaphylaxis) were reported. Additional information is pending.

Risk Management Plan

A Core Risk Management Plan (RMP) for the Janssen COVID-19 Vaccine was submitted by Janssen Inc. to Health Canada as part of the application for interim authorization. The RMP is designed to describe known and potential safety issues, to present the monitoring scheme and to describe measures that will be put in place to minimize risks associated with the product, when needed.

The following information relates to the RMP submitted by Janssen Inc., as part of the initial application for interim authorization. It is the sponsor's responsibility to monitor the safety profile of the drug and to submit an update to the RMP if there is a significant change to the benefits, harms or uncertainties associated with the drug. Updates to the RMP will be reflected in the Post-Authorization Activity Table for the Janssen COVID‑19 Vaccine.

Based on results from non-clinical and clinical studies, the RMP included no important identified risks and one important potential risk (vaccine‑associated enhanced disease, including vaccine‑associated enhanced respiratory disease). There were seven areas of missing information identified: "use during pregnancy", "use in breastfeeding women", "use in immunocompromised patients", "use in patients with autoimmune or inflammatory disorders", "use in frail patients with comorbidities" (e.g., Chronic obstructive pulmonary disease, diabetes, chronic neurological disease, and cardiovascular disorders), "interaction with other vaccines", and "long-term safety". The proposed routine and additional pharmacovigilance activities for the above safety concerns are considered to be acceptable and the sponsor confirmed that they would be applied in the Canadian context. Additional pharmacovigilance activities include seven planned post-authorization studies, including two effectiveness studies, a safety and immunogenicity study in immunocompromised patients, two safety studies, a pregnancy registry, and a coadministration study of the Janssen COVID-19 Vaccine with seasonal influenza vaccine. Routine risk minimization measures (i.e., Product Monograph and labelling) are also considered to be appropriate.

Following review of the RMP, Health Canada determined that "anaphylaxis" and "venous thromboembolism" should be included as important potential risks. With respect to missing information, Janssen Inc. was requested to include "use in the pediatric (younger than 18 years of age) population" and "long-term effectiveness". As per the terms and conditions imposed on the interim authorization, the sponsor has agreed to reflect the aforementioned in an updated Canadian Addendum to the RMP, which will also include a description of the planned pharmacovigilance activities for monitoring of use in pregnant and breastfeeding women in Canada (e.g., inclusion of Canadian women in the pregnancy registry). Furthermore, the sponsor will submit an updated Core RMP and Canadian Addendum in a timely manner if a signal of safety issue is observed in post-authorization surveillance.

In addition, the sponsor will provide the following information in the post-market period:

  • Older adults: Older adults were included in the clinical development program. The sponsor will submit monthly safety reports to Health Canada, which will include analyses of subpopulations by age and gender.
  • Children: Children were not included in the clinical development program. This subpopulation was identified as missing information in the RMP. The sponsor will submit monthly safety reports to Health Canada.
  • Pregnant women: More information is needed about the use of the vaccine for pregnant women. This subpopulation was identified as missing information in the RMP. The sponsor will monitor and submit monthly safety reports to Health Canada. The sponsor will assess outcomes in pregnancy and lactation through a pregnancy registry.
  • Breastfeeding women: This subpopulation was identified as missing information in the RMP. The sponsor will submit monthly safety reports to Health Canada. The sponsor will assess outcomes in pregnancy and lactation through a pregnancy registry.
  • Immunocompromised individuals and patients with chronic or debilitating conditions: A small number of these subpopulations were included in the clinical development program. This subpopulation was identified as missing information in the RMP. The sponsor will submit monthly safety reports to Health Canada.
  • Anaphylaxis: This was identified as an important potential risk in the RMP. This will be assessed via routine pharmacovigilance activities, and reported in monthly summary safety reports.
  • Indigenous populations in Canada: Adverse drug reactions (ADRs) from all subpopulations, including indigenous, will be reported as expeditiously as applicable, and will be assessed in the monthly reports. Other government departments as well as the sponsor will continue to be engaged in the assessment of ADRs in the indigenous subpopulation.

The sponsor is required to promptly report adverse reactions and provide monthly safety summary reports. In addition, the sponsor will provide, prior to distribution, patient information cards to support traceability, where required, which will include elements such as manufacturer name, name of vaccinee, space for recording date of administration, associated batch/lot numbers, and information on how to report any adverse events.

Results related to safety and effectiveness from ongoing and planned studies will be submitted for review as they become available. The results from these studies and the monthly safety summary reports are expected to address the data gaps related to the long‑term safety and effectiveness of the vaccine, interactions with other vaccines, and specific subpopulations (e.g., pregnant and breastfeeding women, pediatric [i.e., younger than 18 years of age] population, patients with autoimmune or inflammatory disorders, immunocompromised patients and frail patients with comorbidities).

For more information, refer to the complete list of terms and conditions available on the Health Canada COVID‑19 vaccines and treatments portal.

Collectively, the results of the clinical safety evaluation demonstrated that the Janssen COVID‑19 Vaccine met the vaccine safety requirements as specified in Health Canada's Guidance for Market Authorization Requirements for COVID-19 Vaccines. The vaccine was determined to be safe and well tolerated in participants 18 years of age and older when administered according to the recommended dosage regimen. The Phase III ENSEMBLE Study is ongoing and will continue to collect information on the long‑term safety and efficacy of the Janssen COVID‑19 vaccine.

For more information, refer to the Janssen COVID‑19 Vaccine Product Monograph, approved by Health Canada and available through the Drug Product Database and on the Health Canada COVID‑19 vaccines and treatments portal.

7.2 Non-Clinical Basis for Decision

The non-clinical data submitted in the application for authorization of the Janssen COVID‑19 Vaccine (Ad26.COV2.S, recombinant) under the Interim Order Respecting the Importation, Sale, and Advertising of Drugs for Use in Relation to COVID-19 included biodistribution, repeat‑dose toxicity, and developmental toxicity studies.

Several vaccine candidates were tested in animals to assess immunogenicity and protective efficacy in both one dose and two dose regimens. Overall, studies in mice, rabbits, Syrian hamsters, and non‑human primates (NHP) show that a single dose of Ad26.COV2.S (recombinant), the medicinal ingredient in the Janssen COVID‑19 Vaccine, is immunogenic by inducing humoral and cellular immune responses. Results demonstrated that Ad26.COV2.S induces neutralizing antibodies and a Th1‑skewed immune response, factors that are theorized to minimize potential risk of vaccine‑associated enhanced respiratory disease (VAERD).

In a Syrian hamster severe acute respiratory syndrome coronavirus 2 (SARS‑CoV‑2) challenge model, Ad26.COV2.S provided dose level‑dependent protection from infectious viral load in the lung. In a SARS-CoV-2 NHP challenge model, immunization with Ad26.COV2.S at dose levels of 1 × 1011 virus particles and 5 × 1010 virus particles fully protected all animals from viral replication in the lung, and protected 14 out of 16 NHP from viral replication in the nose (studies NHP 20‑09 and NHP 20‑14). In both Syrian hamsters and NHP, SARS‑CoV‑2-specific binding and neutralizing antibodies significantly correlate with protection from infection with SARS‑CoV‑2.

Challenge studies in Syrian hamsters and NHP showed no indications of VAERD based on monitoring of clinical signs and viral load of animals vaccinated with Ad26.COV2.S after SARS‑CoV‑2 challenge, and based on histopathologic assessment of lung tissue from these animals compared with challenged control animals. In conclusion, data from the non‑clinical studies that selected the vaccine candidate for clinical development are acceptable, and the available non‑clinical data did not show any adverse vaccine‑related effects.

Biodistribution studies evaluated the potential biodistribution of Ad26.COV2.S using surrogate Ad26‑based vaccines. Rabbits were administered a single dose of 0.5 x 1011 virus particles or 1 x 1011 virus particles of a surrogate vaccine by intramuscular injection. Presence of vector deoxyribonucleic acid (DNA) was observed at the site of injection, as well as the draining lymph nodes and spleen. Thus, the biodistribution data demonstrated limited systemic dissemination of vector DNA. In addition, clearance of vector DNA from these sites was generally observed to occur over time.

In the repeat‑dose toxicity study in rabbits, 3 doses of Ad26.COV2.S (recombinant) were administered 2 weeks apart by intramuscular injection at a dose of 1 x 1011 virus particles/dose (2‑fold the human dose on an absolute basis). Vaccine administration resulted in histopathological inflammation at the site of injection and surrounding tissues, as well as increased germinal centre cellularity in draining lymph nodes and spleen (correlating with enlargement of draining lymph nodes and spleen and increased spleen weights), increase in body temperature, and increased white blood cell counts (including increased monocyte and lymphocyte counts). In addition, clinical chemistry changes (i.e., increased circulating fibrinogen and C‑reactive protein levels, and increased plasma globulin levels with decreased albumin/globulin [A/G] ratios) indicated an acute phase response. Collectively, these changes are consistent with expected immunostimulatory and acute phase responses following intramuscular administration of a vaccine. Full or partial recovery from all findings was observed following a 3-week recovery period.

In the combined embryo‑fetal and pre‑ and postnatal developmental toxicity study, female rabbits were administered Ad26.COV2.S at a dose of 1 x 1011 virus particles/dose by intramuscular injection 7 days prior to mating and on gestation days (GD) 6 and 20 (a total of 3 doses). There was no adverse effect of vaccine administration on reproductive performance, fertility, ovarian and uterine examinations, or parturition; however, one female died on GD 23 from unknown causes. No vaccine‑related adverse effects on pre‑ and postnatal development were observed. This included no vaccine‑related fetal external, visceral, or skeletal malformations, and no vaccine‑related adverse effects on the development and survival of kits (from birth until postnatal day 28). The study did not investigate whether Ad26.COV2.S (recombinant) can distribute across the placental barrier or is present in maternal milk.

Genotoxicity and carcinogenicity studies were not conducted with Ad26.COV2.S (recombinant), which is considered acceptable, as such studies are not considered relevant to vaccines of this nature.

Based on biodistribution data demonstrating vector DNA clearance from tissues, the mechanism of action, and on the available background evidence within the scientific literature, the potential for integration into the host genome is considered to be low.

No concerns are raised with respect to potential for germline integration, as biodistribution data demonstrated no dissemination of vector DNA to the testes and ovaries of rabbits following intramuscular administration.

Overall, the non‑clinical pharmacology and toxicology profile of Ad26.COV2.S, the medicinal ingredient in the Janssen COVID-19 Vaccine, supports its proposed clinical use. The results of the non‑clinical studies as well as the potential risks to humans have been included in the Janssen COVID-19 Vaccine Product Monograph. Considering the intended use of the Janssen COVID-19 Vaccine, there are no pharmacological or toxicological issues within this submission to preclude authorization of the product.

For more information, refer to the Janssen COVID-19 Vaccine Product Monograph, approved by Health Canada and available through the Drug Product Database and on the Health Canada COVID‑19 vaccines and treatments portal.

7.3 Quality Basis for Decision

Quality (chemistry and manufacturing) data were provided in the application for authorization of the Janssen COVID‑19 Vaccine (Ad26.COV2.S, recombinant) under the Interim Order Respecting the Importation, Sale, and Advertising of Drugs for Use in Relation to COVID-19 (Interim Order). The standards Health Canada applied to the review of the submitted data are aligned with those followed by other major regulatory authorities in the assessment of the quality, safety, and efficacy of coronavirus disease 2019 (COVID‑19) vaccines. The interim authorization of the Janssen COVID‑19 Vaccine is associated with terms and conditions that need to be met by the sponsor to ascertain the continued quality, safety, and efficacy of the product.

The Janssen COVID‑19 Vaccine is a prophylactic vaccine developed to prevent COVID‑19, the infectious disease caused by the severe acute respiratory syndrome coronavirus 2 (SARS‑CoV‑2). This vaccine contains a non-replicating adenovirus serotype 26 (Ad26)-based vector constructed to encode the SARS‑CoV‑2 spike protein. The vaccine elicits both neutralizing antibody and cellular immune responses directed against the spike protein, which may contribute to protection against COVID‑19.

Characterization of the Drug Substance

The drug substance, Ad26.COV2.S, is a recombinant, replication-incompetent Ad26‑based vector encoding a full-length and stabilized SARS‑CoV‑2 spike (S) protein, based on the wild-type full-length S gene information obtained from a SARS‑CoV‑2 clinical isolate (Wuhan, 2019, whole genome sequence NC 045512).

The recombinant Ad26-based vector has been rendered replication-incompetent by deletions in the E1 region of the Ad26 genome. In addition, a part of the E3 region has been removed to create sufficient space for the transgene encoding the SARS‑CoV‑2 S protein. Additional genetic engineering enables replication of Ad26.COV2.S in the E1‑complementing PER.C6 TetR cell line, a human cell line capable of supporting the manufacturing of replication-incompetent adenoviral vectors.

Detailed characterization studies were performed to provide assurance that Ad26.COV2.S consistently exhibits the desired characteristic structure and biological activity.

Manufacturing Process and Process Controls of the Drug Substance and Drug Product

The drug substance is manufactured in a multi-stage process consisting of cell expansion and virus production, purification, formulation, filling, and freezing. The process is initiated by thawing of a single bag of PER.C6 TetR cells from a large volume high density cell bank, followed by stages of cell culture expansion until the viable cell density required for inoculation of a virus production bioreactor is obtained. Thereafter, the virus is produced through infection of the expanded cell culture with an Ad26.COV2.S virus seed at a target multiplicity of infection. In subsequent stages, the Ad26.COV2.S virus particles are released from the PER.C6 TetR cells by chemical lysis (permeabilization), the levels of residual host cell deoxyribonucleic acid (DNA) are reduced by precipitation with a detergent, and after sedimentation by gravity, the resulting supernatant is clarified by filtration. Levels of impurities including host cell DNA, host cell protein, process additives, and media components are reduced using a chromatography purification step, followed by a diafiltration step. The diafiltration product is diluted with formulation buffer to the target virus particle titer. Subsequently, the diluted bulk is subjected to a 0.2 µm filtration step. The resulting drug substance is filled into the primary storage container, frozen, and stored.

The drug product manufacturing involves thawing of the drug substance, pre-filtration, pooling, and dilution with pre-filtered formulation buffer. The formulated bulk is homogenized, sterile filtered, and aseptically filled into vials, which are then stoppered and capped. Thereafter, the vials are visually inspected, frozen, and shipped for labelling and packaging. The final drug product is stored at ‑20±5 °C.

As part of the overall process control strategy, the sponsor has determined critical quality attributes, critical material attributes, and critical process parameters. In-process controls and their acceptance criteria have also been established. Importantly, the control strategy for the manufacturing process draws upon the extensive experience of the sponsor with the AdVac/PER.C6 platform technology, which has been utilized in the development of other Ad26-vectored vaccines (e.g., the Ebola vaccine, Ad26.ZEBOV-GP [recombinant], authorized by the European Medicines Agency in 2020). This experience facilitated the rapid transition from early clinical trial material manufacturing to large commercial scale manufacturing. Data were submitted to support comparability of manufacturing processes which included testing results for key critical quality attributes, release specifications for the drug substance and drug product, and additional characterization testing data. The sponsor provided enough information to support the consistency of production. The information submitted, in conjunction with the prior extensive experience of the sponsor with other vaccines based on the same platform, is considered sufficient to support authorization under the Interim Order. In addition, risk mitigation measures are addressed through requirements outlined in the terms and conditions imposed on the interim authorization of the vaccine.

Control of the Drug Substance and Drug Product

The sponsor provided justifications for the release and stability specifications for the drug substance and drug product. Test methods were selected based on relevant regulatory guidance, compendial requirements, and the sponsor's experience with similar products manufactured using the same platform process. The submitted release and stability results were within the proposed specification limits.

Risk mitigation measures are addressed through requirements outlined in the terms and conditions imposed on the interim authorization of the vaccine and the required additional oversight through Health Canada's Guidance for Sponsors: Lot Release Program for Schedule D (Biologic) Drugs.

Stability of the Drug Substance and Drug Product

The stability data provided for the drug substance support the initial shelf life of 24 months when stored frozen at the recommended storage condition of ‑80 (-5/+10) °C to ‑50 (±10) °C. This shelf life claim is largely based on the stability data derived from the AdVac/PER.C6 platform and the ongoing drug substance stability program at ‑60±10 °C. There are limited long-term stability data for drug substance batches manufactured at commercial scale.

The stability data provided for the drug product support the initial shelf life of 24 months when stored frozen at the recommended storage condition of ‑25 °C to ‑15 °C, and within these 24 months, 3 months when stored at 2 °C to 8 °C. The drug product should not be refrozen after it has been placed in storage at 2 °C to 8 °C and must be stored in the original packaging in order to be protected from light. The current shelf life claim is conservatively based on a shelf life model that was constructed from available development and stability data of the Ad26.COV2.S vaccine in addition to other Ad26‑based vaccines manufactured to date using the AdVac/PER.C6 platform. The stability profiles were based on the evaluation and monitoring of all the stability‑indicating attributes, including the composition, potency, and general quality attributes of the drug product.

In-use storage conditions are outlined in the Janssen COVID-19 Vaccine Product Monograph. After the first dose has been withdrawn, the vial/filled syringe may be held at 2 °C to 8 °C for up to 6 hours or at room temperature (maximally 25 °C) for up to 3 hours. If the vaccine is not used within this time, it must be discarded.

Results of the ongoing stability studies will be submitted to Health Canada for review post authorization (see terms and conditions).

The proposed packaging and components are considered acceptable.

Facilities and Equipment

Travel restrictions due to the COVID-19 pandemic prevented Health Canada from conducting on-site evaluations of the drug substance and drug product manufacturing facilities.

Based on the provided information, the design, operations, and controls of the facilities and equipment involved in production are considered suitable for the activities and products manufactured.

The facilities involved in production are compliant with Good Manufacturing Practices.

Adventitious Agents Safety Evaluation

The manufacturing process of Ad26.COV2.S incorporates adequate control measures to prevent contamination and maintain microbial control. Controlled selection and appropriate specifications for raw materials and excipients, specifications, in-process controls and release testing for starting materials, the drug substance and drug product, assure adventitious agents safety for Ad26.COV2.S. Apart from the PER.C6 TetR cell line, which is a human fetal retina cell line developed in the early 1980s, none of the starting and raw materials used in the manufacture of the virus seed banks, cell banks, drug substance or drug product are of direct animal or human origin. No excipients of animal or human origin are used in the drug product formulation.