Summary Basis of Decision for Stivarga
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:
Summary Basis of Decision (SBD) documents provide information related to the original authorization of a product. The SBD for Stivarga is located below.
Recent Activity for Stivarga
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 Stivarga
Updated: 2023-04-24
The following table describes post-authorization activity for Stivarga, a product which contains the medicinal ingredient regorafenib (as regorafenib monohydrate). 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 that are found in PAATs.
For additional information about the drug submission process, refer to the Management of Drug Submissions Guidance.
Drug Identification Number (DIN):
DIN 02403390 - 40 mg regorafenib (as regorafenib monohydrate), tablet, oral administration
Post-Authorization Activity Table (PAAT)
Activity/submission type, control number | Date submitted | Decision and date | Summary of activities |
---|---|---|---|
NC # 233755 | 2020-01-20 | Issued NOL 2020-03-11 | Submission filed as a Level II (90 day) Notifiable Change to update the PM with new safety information. The changes were in response to an Advisement Letter issued by Health Canada, dated 2019-11-22, requesting revisions related to the risk of artery dissection and artery aneurysm. As a result of the NC, modifications were made to the Warnings and Precautions, and Adverse Reactions sections of the PM, and corresponding changes were made to Part III: Consumer Information. The submission was reviewed and considered acceptable, and an NOL was issued. |
SNDS # 214314 | 2018-03-08 | Issued NOC 2019-02-04 | Submission filed as a Level I – Supplement to update the PM with new safety information and to add pediatric data. The submission was reviewed and considered acceptable. As a result of the SNDS, modifications were made to the Adverse Reactions and Action and Clinical Pharmacology sections of the PM. An NOC was issued. |
Summary Safety Review posted | Not applicable | Posted 2018-12-03 |
Summary Safety Review posted for vascular endothelial growth factor receptor tyrosine kinase inhibitors (Assessing the potential risk of abnormal structural changes of the artery walls including rupture [Artery Dissections and Artery Aneurysms]). |
SNDS # 203322 | 2017-02-28 | Issued NOC 2017-09-18 |
Submission filed as a Level I - Supplement for a new indication for use in the treatment of patients with hepatocellular carcinoma (HCC) who have been previously treated with one systemic therapy. A Regulatory Decision Summary was published. |
NC # 212813 | 2018-01-15 | Issued NOL 2018-05-31 |
Submission filed as a Level II (90 day) Notifiable Change (Risk Management Change) to update the PM with new safety information. As a result of the NC, modifications were made to the Adverse Reactions section of the PM. The submission was reviewed and considered acceptable, and an NOL was issued. |
New safety review started by Health Canada | Not applicable | Started between 2017-11-01 and 2017-11-30 |
Health Canada started a safety review for vascular endothelial growth factor receptor tyrosine kinase inhibitors related to aortic dissection (serious condition in which the inner layer of the aorta, the large blood vessel branching off the heart, tears). |
SNDS # 199667 | 2016-10-25 | Issued NOC 2017-08-29 |
SNDS was filed subsequent to NC # 198233. Submission filed as a Level I - Supplement to update the PM to reflect revisions in the company core data sheet. The inclusion of this information in the PM does not change the previously established favourable benefit/risk ratio of Stivarga for its approved indication. As a result of the submission, the following sections of the PM were updated: Warnings and Precautions, Drug Interactions, Dosage and Administration, and the PM Part III: Patient Medication Information. In addition, a minor change was made to the indication to change the "KRAS wild type" specification to "RAS wild type" in patients previously treated with an anti-epidermal growth factor receptor therapy. The submission was reviewed and considered acceptable, and an NOC was issued. A Regulatory Decision Summary was published. |
NC # 198233 | 2016-09-08 | Cancellation Letter Received 2016-10-06 |
Submission filed as a Level II (90 day) Notifiable Change (Risk Management Change) to update the PM to reflect revisions in the company core data sheet. The proposed revisions in the PM exceeded the scope of an NC. The submission was therefore cancelled administratively by the sponsor, so as to be filed as an SNDS. |
NC # 190396 | 2015-12-10 | Issued No Objection Letter Notice 2016-03-21 |
Submission filed as a Level II (90 day) Notifiable Change (Risk Management Change) to update the Product Monograph (PM) with new hepatotoxicity and skin toxicity safety information. As a result of the Notifiable Change, modifications were made to the Warnings and Precautions and Adverse Reactions sections of the PM. |
SNDS # 182560 | 2015-03-02 | Issued NOC 2015-09-22 |
Submission filed as a Level I - Supplement to seek approval for a change in the drug product specifications and an extension of the in-use shelf-life of the drug product. The data were reviewed and considered acceptable, and an NOC was issued. As a result of the SNDS, changes were made to the Part III: Patient Medication Information section of the Product Monograph. |
NC # 180592 | 2014-12-11 | No Objection Letter 2015-03-19 |
Submission filed as a Level II (90 day) Notifiable Change (Safety Change) to make revisions to the Product Monograph (PM). As a result of the Notifiable Change (NC), updates were made to the Warnings and Precautions, Adverse Reactions, and Drug Interactions sections of the PM. Corresponding changes were made to the PM Part III: Consumer Information. The submission was reviewed and considered acceptable. A No Objection Letter was issued. |
Summary Safety Review posted | Not applicable | Posted 2015-01-14 |
Summary Safety Review posted for Vascular Endothelial Growth Factor (VEGF) receptor inhibitors (Thrombotic microangiopathy). |
SNDS # 159750 | 2012-10-31 | Issued NOC 2013-10-04 |
Submission filed for an expanded indication for Stivarga. The submission included data from one international, multicentre, randomised, placebo-controlled Phase III pivotal study examining the efficacy and safety of Stivarga for advanced gastrointestinal stromal tumours (GIST) after failure of imatinib and sunitinib. The results of this study were supported by the results of an earlier Phase II study in the same patient population. Stivarga with best supportive care significantly increased Progression Free Survival (PFS) as compared to placebo with best supportive care under the proposed conditions of use. Stivarga has a manageable safety profile considered acceptable in this group of patients with no other treatment options. The risk/benefit profile for the administration of Stivarga for the revised indication was considered acceptable and an NOC was issued for the expanded indication of 'Treatment of adult patients with metastatic and/or unresectable GIST who have had disease progression on or intolerance to imatinib mesylate and sunitinib malate treatment. Approval of Stivarga is based on PFS.' |
Drug product (DIN 02403390) market notification | Not applicable | Date of first sale: 2013-04-02 |
The manufacturer notified Health Canada of the date of first sale pursuant to C.01.014.3 of the Food and Drug Regulations. |
NDS # 157970 | 2012-08-15 | Issued NOC 2013-03-11 |
Notice of Compliance issued for New Drug Submission. |
Summary Basis of Decision (SBD) for Stivarga
Date SBD issued: 2013-11-07
The following information relates to the New Drug Submission for Stivarga.
Regorafenib (as regorafenib monohydrate), 40 mg, tablet, oral
Drug Identification Number (DIN):
- 02403390
Bayer Inc.
New Drug Submission Control Number: 157970
On March 11, 2013, Health Canada issued a Notice of Compliance to Bayer Inc. for the drug product, Stivarga.
The market authorization was based on quality (chemistry and manufacturing), non-clinical (pharmacology and toxicology), and clinical (pharmacology, safety, and efficacy) information submitted. Based on Health Canada's review, the benefit/risk profile of Stivarga is favourable for the treatment of patients with metastatic colorectal cancer (CRC) who have been previously treated with fluoropyrimidine-based chemotherapy, oxaliplatin, irinotecan, an anti-vascular endothelial growth factor (anti-VEGF) therapy, and, if KRAS wild type, an anti-epidermal growth factor receptor (anti-EGFR) therapy.
1 What was approved?
Stivarga, a multikinase inhibitor and antineoplastic agent, was authorized for the treatment of patients with metastatic colorectal cancer (CRC) who have been previously treated with fluoropyrimidine-based chemotherapy, oxaliplatin, irinotecan, an anti-vascular endothelial growth factor (anti-VEGF) therapy, and, if KRAS wild type, an anti-epidermal growth factor receptor (anti-EGFR) therapy.
No differences in safety or efficacy were observed between older and younger patients.
The safety and efficacy of Stivarga in pediatric patients have not been established.
Stivarga is contraindicated for patients who are hypersensitive to regorafenib, sorafenib, drugs in the same class (other multikinase inhibitors), or any ingredient in the formulation. Stivarga was approved for use under the conditions stated in the Stivarga Product Monograph taking into consideration the potential risks associated with the administration of this drug product.
Stivarga (40 mg regorafenib, as regorafenib monohydrate) is presented as a tablet. In addition to the medicinal ingredient, the tablet core contains: cellulose microcrystalline; croscarmellose sodium; magnesium stearate; povidone; and silica colloidal anhydrous. The film-coating of the tablet contains iron oxide red, iron oxide yellow, lecithin (soy), macrogol, polyvinyl alcohol (partially hydrolyzed), talc, and titanium dioxide.
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 Stivarga Product Monograph, approved by Health Canada and available through the Drug Product Database.
2 Why was Stivarga approved?
Health Canada considers that the benefit/risk profile of Stivarga is favourable for the treatment of patients with metastatic colorectal cancer (CRC) who have been previously treated with fluoropyrimidine-based chemotherapy, oxaliplatin, irinotecan, an anti-vascular endothelial growth factor (anti-VEGF) therapy, and, if KRAS wild type, an anti-epidermal growth factor receptor (anti-EGFR) therapy.
One out of every 14 people in Canada has a life-time risk of developing CRC. For metastatic CRC, palliative treatments include fluoropyrimidine-based therapies either in combination with oxaliplatin or in combination with irinotecan. In addition, bevacizumab in combination with fluoropyrimidine-based chemotherapy and cetuximab, and panitumumab in combination with fluoropyrimidine-based chemotherapy or as monotherapy have been shown to increase the beneficial results of well-established combination regimens. Despite the various treatment options outlined above, no treatment options are available for patients with metastatic CRC that progresses after all approved standard therapies. For these patients, the prognosis is dismal with a median survival time of 3-6 months.
Stivarga (regorafenib) has been shown to be efficacious in patients with metastatic CRC who have failed standard therapy. The efficacy results were mainly derived from a Phase III randomized, double-blind, placebo-controlled study (Study 14387), and were supported by a Phase I study (Study 11650) which provided initial evidence of the anti-tumour activity of regorafenib in a similar patient population. Data from the Phase III study showed a statistically significant benefit in overall survival for patients treated with Stivarga. The observed improvement in overall survival of 29% for the Stivarga plus Best Supportive Care (BSC) group over the placebo plus BSC group [median 6.4 months versus (vs.) 5.0 months] corresponded to a 23% reduction in hazard over placebo plus BSC. This reduction is important and clinically significant in patients who have failed all standard therapies. The prognosis of these patients is generally poor due to the lack of effective treatment. The progression-free survival results were consistent with the overall survival results, showing progression-free benefit for the Stivarga group compared to the control group.
In the pivotal Study 14387, the most frequently observed treatment-emergent adverse events (≥30%) in the Stivarga plus BSC group included decreased appetite (47%), hand-foot skin reaction (HFSR) or palmar-plantar erythrodysesthesia syndrome (47%), diarrhea (43%), fatigue (40%), decreased weight (32%), hypertension (30%), and dysphonia (30%). The most common (≥5%) Grade 3 adverse events in the Stivarga plus BSC group were HFSR (17%), fatigue (9%), diarrhea (8%), hypertension (8%) and asthenia (7%). Significantly more patients in the Stivarga plus BSC group (67%) than in the placebo plus BSC group (22%) had dose modifications due to adverse events. The incidence of adverse events leading to permanent treatment discontinuation with Stivarga (17.6%) was relatively low compared to placebo (12.6%) indicating that most adverse reactions in the Stivarga-treated patients could be managed by dose modifications.
The important identified risks are severe drug-induced liver injury (DILI), hemorrhage, myocardial ischemia and infarction, arterial hypertension and hypertensive crisis, palmar-plantar erythrodysesthesia syndrome/hand-foot skin reaction (HFSR), gastrointestinal perforation and fistula, reversible posterior leukoencephalopathy syndrome (RPLS), and Stevens-Johnson syndrome (SJS). These are considered identified risks due to pharmacological plausibility and clinical safety data suggesting a causal link to regorafenib. Severe DILI, hemorrhage, myocardial infarction/ischemia, SJS and RPLS are considered important because of their potential to result in severe or fatal outcomes. Hypertension and HFSR are important in that they are very common and may adversely impact effective therapy delivery and quality of life. A Serious Warnings and Precautions box in the Stivarga Product Monograph contains warnings regarding hepatotoxicity, hemorrhage involving the respiratory and gastrointestinal tracts, cardiac ischemia and infarction, RPLS, gastrointestinal perforation and fistula, arterial hypertension, and HFSR. The cardiovascular section of the Stivarga Product Monograph contains explicit warnings regarding the increased incidence of cardiac adverse events (8.4 vs. 5.5%) including cardiac arrhythmia (3% vs. 0.8%), cardiac ischemia and infarction (1.2% vs. 0.4%) and severe (Grade 3/4) congestive heart failure (1.2% vs.0.4%) in Stivarga-treated patients compared to placebo-treated patients.
Important potential risks that have been reported with other tyrosine kinase inhibitor agents include gastrointestinal perforation and fistula, wound-healing impairment, SJS/toxic epidermal necrolysis, and interstitial lung disease. Therefore, precautionary measures are indicated in the Stivarga Product Monograph.
In addition to the important risks mentioned above, metabolic and biochemical abnormalities have been frequently reported, but are generally mild and not associated with clinical complications. Corresponding advice on monitoring and clinical management is included in the finalized Stivarga Product Monograph.
For the patient subpopulations analyzed, no relevant safety differences were observed except for the higher incidence of drug-related serious adverse events in female patients treated with Stivarga as compared to placebo. No dose adjustments are required for age, body mass index, sex, ethnicity, mild hepatic impairment, or mild and moderate renal impairment. Because there is no data for patients with severe and end-stage renal impairment or severe hepatic impairment, precautionary statements advise to avoid the use of Stivarga in these patients.
A Risk Management Plan (RMP) for Stivarga was submitted by Bayer Inc. to Health Canada. Upon review, the RMP was considered to be acceptable. 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.
Overall, Stivarga demonstrated a statistically significant and clinically relevant improvement in overall survival in patients with metastatic CRC who had failed standard therapy. When administered according to the recommended dosing schedule of 160 mg once daily, for the first 21 days of each 28-day cycle, Stivarga shows an acceptable and manageable toxicity profile.
The benefit/risk assessment was based on data from adequate and comprehensive non-clinical and clinical development programs. Known unfavorable effects of the drug class and findings from non-clinical investigations, as well as potential risks, were adequately addressed, as were all relevant requests from Health Canada during the review of this submission.
Based on the observed survival benefit, and together with a tolerable safety profile, the benefit of Stivarga outweighs the risk for patients with metastatic CRC previously treated with fluoropyrimidine-based chemotherapy, oxaliplatin, irinotecan, an anti-VEGF therapy, and, if KRAS wild type, an anti-EGFR therapy.
This New Drug Submission complies with the requirements of sections C.08.002 and C.08.005.1 and therefore Health Canada has granted the Notice of Compliance pursuant to section C.08.004 of the Food and Drug Regulations. 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 Stivarga?
The drug submission for Stivarga was reviewed under the Priority Review Policy. Stivarga demonstrated a significant increase in effectiveness with an improved benefit/risk profile compared to existing therapies for patients with metastatic colorectal cancer (CRC) who have been previously treated with fluoropyrimidine-based chemotherapy, an anti-vascular endothelial growth factor (anti-VEGF) therapy, and, if KRAS wild type, an anti-epidermal growth factor receptor (anti-EGFR) therapy. This condition is regarded as serious and life-threatening and is not adequately managed by a drug presently marketed in Canada.
Submission Milestones: Stivarga
Submission Milestone | Date |
---|---|
Pre-submission meeting: | 2012-06-13 |
Request for priority status | |
Filed: | 2012-06-29 |
Approval issued by Director, Bureau Of Metabolism, Oncology, and Reproductive Sciences | 2012-08-07 |
Submission filed: | 2012-08-15 |
Screening | |
Screening Acceptance Letter issued: | 2012-09-13 |
Review | |
Biopharmaceutics Evaluation complete: | 2012-11-29 |
Quality Evaluation complete: | 2013-03-06 |
Clinical Evaluation complete: | 2013-03-08 |
Biostatistics Evaluation complete: | 2012-12-27 |
Labelling Review complete: | 2013-03-06 |
Notice of Compliance issued by Director General | 2013-03-11 |
For additional information about the drug submission process, refer to the Management of Drug Submissions Guidance.
4 What follow-up measures will the company take?
Requirements for post-market commitments are outlined in the Food and Drugs Act and Regulations.
6 What other information is available about drugs?
Up to date information on drug products can be found at the following links:
- See MedEffect Canada for the latest advisories, warnings and recalls for marketed products.
- See the Notice of Compliance (NOC) Database for a listing of the authorization dates for all drugs that have been issued an NOC since 1994.
- See the Drug Product Database (DPD) for the most recent Stivarga Product Monograph. The DPD contains product-specific information on drugs that have been approved for use in Canada and have been market notified (that is, the company has told Health Canada the product is being marketed).
- See the Notice of Compliance with Conditions (NOC/c)-related documents for the latest fact sheets and notices for products which were issued an NOC under the Notice of Compliance with Conditions (NOC/c) Guidance, if applicable. Clicking on a product name links to (as applicable) the Fact Sheet, Qualifying Notice, and Dear Health Care Professional Letter.
- See the Patent Register for patents associated with medicinal ingredients, if applicable.
- See the Register of Innovative Drugs for a list of drugs that are eligible for data protection under C.08.004.1 of the Food and Drug Regulations, if applicable.
7 What was the scientific rationale for Health Canada's decision?
7.1 Clinical Basis for Decision
Clinical Pharmacology
Regorafenib, the active ingredient in Stivarga, is a multikinase inhibitor that blocks several enzymes involved in tumour angiogenesis, oncogenesis, and the tumour microenvironment.
The data from the submitted clinical pharmacokinetic studies are considered sufficient and there are no major concerns to prevent the approval of Stivarga for the specified indication. Extensive labelling changes were proposed for the clinical pharmacokinetic parts of the Stivarga Product Monograph and the sponsor accepted all of the proposed changes. Appropriate warnings and precautions are in place in the approved Stivarga Product Monograph to address the identified safety concerns.
For further details, please refer to the Stivarga Product Monograph, approved by Health Canada and available through the Drug Product Database.
Clinical Efficacy
The clinical efficacy and safety of Stivarga were evaluated in an international, multicentre, randomized, double-blind, placebo-controlled Phase III study (Study 14387) in patients with metastatic colorectal cancer (CRC) who had progressed after failure of standard therapy [including fluoropyrimidine-based chemotherapy, an anti-vascular endothelial growth factor (anti-VEGF) therapy, and, if KRAS wild type, an anti-epidermal growth factor receptor (anti-EGFR) therapy].
In total, 760 patients were randomized 2:1 to receive 160 mg regorafenib (4 tablets Stivarga, each containing 40 mg regorafenib) orally once daily plus best supportive care (BSC; n = 505) or matching placebo plus BSC (n = 255), for 3 weeks on therapy followed by 1 week off therapy. Patients continued therapy until disease progression or unacceptable toxicity were identified.
Demographics and baseline disease characteristics were comparable between the Stivarga and placebo groups with regard to age, gender, and Eastern Cooperative Oncology Group (ECOG) performance status. The primary site of disease was colon (64% vs. 67.5%), rectum (29.9% vs. 27.1%) or colon and rectum (5.9% vs. 5.5%). KRAS mutation was reported in 54.1% of the patients in the Stivarga group vs. 61.6% in the placebo group. All patients received prior treatment with fluoropyrimidine, oxaliplatin, irinotecan, and bevacizumab. Of the patients with a KRAS wild type tumour, 99.5% in the Stivarga group and 100% in the placebo group had received prior treatment with cetuximab and/or panitumumab.
The primary efficacy endpoint was overall survival (OS). Secondary endpoints were progression-free survival (PFS), overall response rate (ORR), and disease control rate (DCR).
The median duration of treatment phase was 7 weeks (approximately 2 cycles). The addition of Stivarga to BSC resulted in a statistically significant improvement in survival compared to placebo plus BSC.
The results of this pivotal Phase III study demonstrated a statistically significant reduction in the risk of death in patients treated with Stivarga compared to placebo [hazard ratio (HR) 0.77 (95% Confidence Interval (CI): 0.64, 0.94); p = 0.010356]. The median survival time (OS) was 6.4 months (95% CI: 5.8, 7.3) in the Stivarga-treated patients compared to 5.0 months (95% CI: 4.4, 5.8) in placebo-treated patients. Although there was a statistically significant reduction in the estimated risk of progression [HR 0.49 (95% CI: 0.42, 0.58); p <0.000001], a 7-day improvement in the median PFS (59 days vs. 52 days) with Stivarga over placebo is not considered to be clinically meaningful.
There were no complete tumour responses according to Response Evaluation Criteria In Solid Tumors (RECIST) criteria. Five (1%) Stivarga-treated patients and 1 (0.4%) placebo-treated patient achieved a partial response with no difference in ORR (p = 0.19). Disease control rate (DCR) was assessed after 6-8 weeks post randomization and was comprised of stable disease, non-complete response or non-progressive disease. The median duration of stable disease was 60 days in the Stivarga group and 52 days in the placebo group. Given a high rate of missing/out of schedule assessment and lack of independent review, the DCR data could be biased. Stable disease was reported in 43% vs. 14% of patients in the Stivarga group compared to the placebo group.
Exploratory subgroup analyses were conducted for subgroups such as age, gender, number of prior therapies and various disease characteristics in 25 pre-specified sub-group analyses across OS and PFS. All subgroup analyses were descriptive in nature where a HR of less than 1 suggested a beneficial trend in efficacy in favour of Stivarga and a HR of greater than 1 suggested a trend in favor of placebo. A HR of approximately 1 represented no trend in favour of either treatment. All tests were one-sided. The results showed a beneficial trend towards improvement in OS in 24/25 subgroups analysed, including 11 subgroups with statistically significant prolongation in OS (p<0.05). A HR <1 was maintained in all but one subgroup (metastatic CRC of both colon and rectum) of patients. The results of PFS analysis strongly supported the OS results showing HR <1 in all 25 subgroups tested. The effect of Stivarga over placebo was more pronounced in a subgroup of patients with KRAS wild type (n = 299) based on the HR = 0.653 (95% CI: 0.476, 0.895) corresponding to 35% reduction in the risk of death. In contrast, Stivarga-treated patients with KRAS mutations (n = 430) demonstrated a statistically insignificant reduction in the risk of death by 13% based on the HR = 0.867 (95% CI: 0.670, 1.123). The Stivarga Product Monograph contains information to highlight this difference in survival benefit based on historical KRAS mutational status.
Health Related Quality of Life (HRQoL) data showed deterioration in patients' quality of life of similar magnitude in both treatment arms, with a trend to worsening the HRQoL with Stivarga compared to placebo. However, a higher attrition rate in the placebo arm compared to the Stivarga arm and a short observation time (median 8 weeks) preclude any meaningful conclusion regarding the patient reported outcome.
The results of several ad hocsensitivity analyses of OS and PFS demonstrated consistency with the primary analyses results, thus confirming prolongation of survival time with Stivarga over placebo. These results are considered to be supportive for a definite survival benefit of the Stivarga treatment.
In conclusion, the efficacy results from the pivotal Phase III study are considered positive with regard to clinical and statistical relevance as well as internal consistency. The credibility of the results in this pivotal study is confirmed by the primary endpoint, which demonstrates a statistically significant benefit of Stivarga in OS. Moreover, all the sensitivity analyses confirmed the primary analyses, indicating that the data are robust.
For more information, refer to the Stivarga Product Monograph, approved by Health Canada and available through the Drug Product Database.
Clinical Safety
The clinical safety evaluation was based on results from the pivotal Phase III, randomized, double-blind, placebo-controlled Study 14387 (described in Clinical Efficacy), in which 500 patients received Stivarga at a dose of 160 mg daily plus BSC, and 253 patients received placebo plus BSC, for 3 weeks of each 4-week treatment cycle, until disease progression or unacceptable toxicity were identified. The median duration of treatment was 7 weeks and safety observation was <3 months (median time) in both treatment groups.
A dose modification occurred in 67% and 22% of patients in the Stivarga and placebo group, respectively. Due to adverse reactions, 61% of the Stivarga-treated patients required a dose interruption and 38% of the patients had their dose reduced. Treatment cessations occurred with similar incidence (18% vs. 13%) indicating that most adverse events in the Stivarga-treated patients could be managed by dose modifications. There appears to be a narrow safety margin between therapeutic and toxic doses of Stivarga. Dose-limiting toxicities included hepatotoxicity, hemorrhage, gastrointestinal (GI), and dermatological toxicities.
The most frequently observed treatment-emergent adverse events (≥30%) in the Stivarga group were fatigue (64%), decreased appetite (47%), hand foot skin reaction (HFSR, 47%), diarrhea (43%), decreased weight (32%), hypertension (30%), and dysphonia (32%). The most common Grade 3 events in the Stivarga group were HFSR (17%), fatigue (15%), diarrhea (8%), hypertension (8%) infection (7%) and hyperbilirubinemia (6%).
The important identified risks are severe drug-induced liver injury (DILI), hemorrhage, myocardial ischemia and infarction, arterial hypertension and hypertensive crisis, palmar-plantar erythrodysesthesia syndrome/HFSR, GI perforation and fistula, reversible posterior leukoencephalopathy syndrome (RPLS), and Stevens-Johnson syndrome (SJS). These identified risks are due to the known class effects and clinical safety data suggesting a causal link to regorafenib, the medicinal ingredient of Stivarga. Severe DILI, hemorrhage, myocardial infarction/ischemia, SJS and RPLS are considered important because of their potential to result in severe or fatal outcomes. Hypertension and HFSR are important in that they are very common and may adverselyimpact effective therapy delivery and quality of life. The Stivarga Product Monograph has a Serious Warnings and Precautions box containing warnings regarding hepatotoxicity, hemorrhage involving the respiratory and gastrointestinal tracts, RPLS, GI perforation and fistula, arterial hypertension, and HFSR. All of the important identified risks are appropriately labelled to raise the physicians' and patients' awareness, and statements including advice on clinical management are provided in the corresponding sections of the finalized Product Monograph for Stivarga.
The cardiovascular section of the Stivarga Product Monograph contains explicit warnings regarding the increased incidence of cardiac adverse events (8.4 vs. 5.5%) including cardiac arrhythmia (3% vs. 0.8%), cardiac ischemia and infarction (1.2% vs. 0.4%) and severe (Grade 3/4) congestive heart failure (1.2% vs. 0.4%) in Stivarga-treated patients compared to placebo-treated patients. Arterial hypertension was the most common vascular disorder, reported in 30% of Stivarga-treated patients. Adequate monitoring, conventional management, and dose interruption/reduction are recommended for patients with persisting hypertension. In the event of a hypertensive crisis, Stivarga should be discontinued. Based on the cardiosafety review, Stivarga may decrease heart rate. Caution should be observed in patients with a low heart rate at baseline, a history of syncope or arrhythmia, sick sinus syndrome, sinoatrial block, atrioventricular (AV) block, ischemic heart disease, or congestive heart failure. Concomitant medications that result in a decrease in heart rate should be avoided to the extent possible during treatment with Stivarga.
Stivarga increased the incidence of hypothyroidism (4.2% vs. 0.4%) and incidence of fistula (0.8% vs. 0.4%), compared to placebo. A precautionary statement recommends the discontinuation of Stivarga in patients who develop GI perforation or fistula.
Stivarga increased the incidence of hemorrhage (21% vs. 8%) compared to placebo. Fatal hemorrhage involving the respiratory, genitourinary and GI tracts was reported in 4 (0.8%) Stivarga-treated patients. No placebo-treated patients had a fatal bleeding event. Treatment with Stivarga should be stopped in patients with severe and life-threatening hemorrhage. Close monitoring of the International Normalized Ratio (INR) in patients receiving warfarin is advised.
Data from a regorafenib safety database indicated that severe DILI with fatal outcomes was reported in 3 of 1,100 patients treated with regorafenib. All cases occurred within the first 2 months of therapy and exhibited hepatocellular necrosis and clinical manifestations of hepatic failure including ascites, neurological deterioration, and abnormal coagulation.
In Study 14387, the incidence of hepatobiliary disorders was higher in Stivarga-treated patients (20% vs. 12%) compared to placebo-treated patients. Fatal events of hepatic dysfunction were reported in 10/500 (2%) Stivarga-treated patients compared to 4 (1.6%) placebo-treated patients. Adverse events of hepatic dysfunction led to the treatment cessation in 7 (1.4%) Stivarga-treated patients and 3 (1.2%) placebo-treated patients. Hepatic injury/failure adverse events (fibrosis, cirrhosis and other liver damage-related conditions) were reported in 37/500 (7.4%) Stivarga-treated patients compared to 13/253 (5.1%) placebo-treated patients. Dose modifications should be carried out in cases of liver dysfunction. Early discontinuation is the most important risk mitigation in cases of DILI.
The incidence of skin and subcutaneous disorders was higher in the Stivarga-treated patients (72%) as compared to the placebo-treated patients (24%). There was one event of Grade 4 SJS in a patient treated with Stivarga (0.2%). The overall incidence of HFSR/palmar-plantar erythrodysesthesia syndrome (47% vs. 8%) and Grade 3 HFSR (17% vs. 0%) was increased in Stivarga-treated patients. The overall incidence of rash (29% vs. 5%) and Grade 3 rash (6% vs. 0%) was higher in Stivarga-treated patients as compared to patients in the placebo group. Measures for the prevention and treatment of skin adverse reactions include topical treatments, dose reduction/interruption, or in severe or persistent cases, permanent discontinuation of Stivarga.
In cases of unexplained respiratory symptoms such as non-productive cough, dyspnea, crackles, or radiological pulmonary infiltrates, treatment should be discontinued until further pulmonary investigation excludes interstitial lung disease or pneumonitis. In addition to the important risks mentioned above, metabolic and biochemical abnormalities have been frequently reported, but are generally mild and not associated with clinical complications.
Most of the Stivarga-related adverse drug reactions resolve after drug interruption or discontinuation, however, rare cases with fatal outcomes have been reported. Close monitoring of identified targets of Stivarga toxicity is advised, especially in the first 2 months of treatment. Dose modifications and early discontinuations are the most important risk mitigation in case of severe adverse drug reactions. Corresponding risk minimization measures are included in the Stivarga Product Monograph.
For more information, refer to the Stivarga Product Monograph, approved by Health Canada and available through the Drug Product Database.
7.2 Non-Clinical Basis for Decision
The non-clinical pharmacology, safety pharmacology, pharmacokinetic and toxicology program conducted with regorafenib (the medicinal ingredient of Stivarga), and its metabolites M-2 and M-5 is considered to be sufficient to support the intended clinical use of Stivarga.
The findings in the toxicology studies were generally consistent with other marketed tyrosine kinase inhibitors. These findings included adverse effects in the kidneys, liver, digestive system, heart, hematopoietic system, lymphoid system, and endocrine system, which may have relevance to the clinical use of Stivarga. Also consistent with marketed tyrosine kinase inhibitors, these effects occurred at or below clinical exposures in animals.
Adverse findings in teeth and bone/cartilage were observed in rodents and young adult dogs administered regorafenib. These findings would be relevant for children and adolescents should an indication for regorafenib in these age groups be authorized in the future; however, in view of the cessation of tooth and bone/cartilage growth in adults these findings are not considered of relevance for the safety assessment of regorafenib in adults.
In embryo-fetal development studies in rabbits and rats, regorafenib was associated with pregnancy loss, developmental toxicity and teratogenicity at doses and/or exposure levels lower than in humans. In rats, regorafenib was transferred to milk, therefore, breast feeding is not recommended during treatment with Stivarga. Appropriate warnings and precautionary measures are in place in the Stivarga Product Monograph to address the identified safety concerns.
In conclusion, the non-clinical safety studies characterized the toxicological profile of regorafenib adequately to support the market authorization of Stivarga for the specified indication.
For more information, refer to the Stivarga Product Monograph, approved by Health Canada and available through the Drug Product Database.
7.3 Quality Basis for Decision
The Chemistry and Manufacturing information submitted for Stivarga has demonstrated that the drug substance and drug product can be consistently manufactured to meet the approved specifications. Proper development and validation studies were conducted and adequate controls are in place for the commercial processes. Changes to the manufacturing process and formulation made throughout the pharmaceutical development are considered acceptable upon review. Based on the stability data submitted, the proposed shelf-life is considered acceptable.
Proposed limits of drug-related impurities are considered adequately qualified within International Conference on Harmonisation (ICH) limits and/or from toxicological studies.
All sites involved in production are compliant with Good Manufacturing Practices.
All non-medicinal ingredients (excipients) found in the drug product are acceptable for use in drugs according to the Food and Drug Regulations.
None of the excipients used in the manufacture of Stivarga tablets are of human or animal origin.