SPRINTR: Nicotinamide Chemoprevention for Keratinocyte Carcinoma in Solid Organ Transplant Recipients - Pivotal Trial
Study Details
Study Description
Brief Summary
As patients live longer after receiving an organ transplant, there is a need to reduce the longterm side effects of the drugs used to prevent organ rejection. In particular, long-term use of these drugs increases the risk of skin cancer. Skin cancer is now a leading cause of illness and disfigurement after kidney, liver, heart, and lung transplantation. Given the increased risk and burden of skin cancer in transplant recipients, prevention is critical.
Nicotinamide is a form of Vitamin B3 that has been shown to protect against skin cancer in the general population. However, it is unclear whether nicotinamide is effective among immune-suppressed transplant recipients. We will conduct a clinical trial involving multiple transplant centres in Canada to evaluate whether oral nicotinamide (500 mg twice daily) is effective and safe for preventing skin cancer. We will recruit 396 high-risk adult kidney, liver, heart, and lung transplant patients who have previously had at least one skin cancer. Patients will receive nicotinamide or sham tablets for up to 4 years. The results will inform efforts to improve the long-term health of transplant recipients.
Condition or Disease | Intervention/Treatment | Phase |
---|---|---|
|
Phase 3 |
Detailed Description
Improved survival after solid organ transplantation has created the need to better prevent the long-term adverse effects of immunosuppressant drugs in transplant survivors - particularly cancer development. Keratinocyte carcinoma (non-melanoma skin cancer) is by far the most common form of post-transplant malignancy and has a more aggressive clinical course than in the general population. Preventive measures are thus critical to reduce the burden of skin cancer in the high-risk transplant population.
Nicotinamide is a low cost, commercially available, over-the-counter Vitamin B3 derivative that has been found to safely reduce the rate of keratinocyte carcinoma in immunocompetent patients with a history of skin cancer. It is unclear whether its efficacy and safety translate to the immunosuppressed transplant population.
Given this uncertainty, we plan to build on our internal pilot study (N=120) to conduct the SPRINTR (Skin cancer PRevention with Nicotinamide in Transplant Recipients) pivotal trial to address these specific aims:
Primary question: Does oral nicotinamide (500 mg twice daily) reduce the rate of further keratinocyte carcinoma compared with placebo when used in addition to standard care for up to 208 weeks in high-risk solid organ transplant recipients?
Secondary questions:
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What is the safety of nicotinamide when used in addition to standard care for up to 208 weeks in the transplant population?
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What is the effect of nicotinamide on quality of life related to skin cancer?
We will conduct a multicentre, pragmatic, parallel group, investigator- and patient-blinded, randomized trial with a superiority framework. This pivotal trial will evaluate the efficacy and safety of oral nicotinamide versus placebo to prevent further keratinocyte carcinoma in 396 high-risk solid organ transplant recipients. Data from our previous internal pilot study (N=120 participants) will be combined with data from the current pivotal trial (N=276 additional patients) in the final analysis.
Study Design
Arms and Interventions
Arm | Intervention/Treatment |
---|---|
Experimental: Nicotinamide Intervention Drug : Nicotinamide |
Drug: Nicotinamide
Oral nicotinamide (500 mg) twice daily
Other Names:
|
Placebo Comparator: Placebo Intervention: Placebo Oral Capsule |
Drug: Placebo
Matching placebo capsule twice daily
|
Outcome Measures
Primary Outcome Measures
- Time to first biopsy-confirmed keratinocyte carcinoma (basal cell carcinoma or invasive cutaneous squamous cell carcinoma) [Up to 208 weeks]
Secondary Outcome Measures
- Time to first invasive squamous cell carcinoma during follow-up [Up to 208 weeks]
- Time to first basal cell carcinoma during follow-up [Up to 208 weeks]
- Time to multiple keratinocyte carcinomas over follow-up [Up to 208 weeks]
- Occurrence of adverse events during follow-up [208 weeks]
Overall and by body system, frequency, seriousness, and severity
- Acute graft rejection (biopsy-confirmed) [208 weeks]
Adverse event
- Graft loss or retransplantation [208 weeks]
Adverse event
- High/low cyclosporine or tacrolimus blood concentration requiring dose adjustment [208 weeks]
Adverse event
- Change from baseline in annual Basal and Squamous Cell Carcinoma Quality of Life (BaSQoL) score [52 weeks]
- Change from baseline in annual Basal and Squamous Cell Carcinoma Quality of Life (BaSQoL) score [104 weeks]
- Change from baseline in annual Basal and Squamous Cell Carcinoma Quality of Life (BaSQoL) score [156 weeks]
- Change from baseline in annual Basal and Squamous Cell Carcinoma Quality of Life (BaSQoL) score [208 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Montreal Cognitive Assessment (MoCA) [52 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Montreal Cognitive Assessment (MoCA) [104 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Montreal Cognitive Assessment (MoCA) [156 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Montreal Cognitive Assessment (MoCA) [208 weeks]
- Neurocognitive substudy - Proportion of participants with cognitive impairment [52 weeks]
As defined by the International Cognition and Cancer Task Force (T scores ≥2 standard deviations below the normative population mean on a single test, or ≥1.5 standard deviations below the mean on at least two tests, or both)
- Neurocognitive substudy - Proportion of participants with cognitive impairment [104 weeks]
As defined by the International Cognition and Cancer Task Force (T scores ≥2 standard deviations below the normative population mean on a single test, or ≥1.5 standard deviations below the mean on at least two tests, or both)
- Neurocognitive substudy - Proportion of participants with cognitive impairment [156 weeks]
As defined by the International Cognition and Cancer Task Force (T scores ≥2 standard deviations below the normative population mean on a single test, or ≥1.5 standard deviations below the mean on at least two tests, or both)
- Neurocognitive substudy - Proportion of participants with cognitive impairment [208 weeks]
As defined by the International Cognition and Cancer Task Force (T scores ≥2 standard deviations below the normative population mean on a single test, or ≥1.5 standard deviations below the mean on at least two tests, or both)
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Hopkins Verbal Learning Test - Revised [52 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Hopkins Verbal Learning Test - Revised [104 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Hopkins Verbal Learning Test - Revised [156 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Hopkins Verbal Learning Test - Revised [208 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Trail Making A and B [52 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Trail Making A and B [104 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Trail Making A and B [156 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Trail Making A and B [208 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Controlled Oral Word Association [52 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Controlled Oral Word Association [104 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Controlled Oral Word Association [156 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Controlled Oral Word Association [208 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Animal Naming Task [52 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Animal Naming Task [104 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Animal Naming Task [156 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Animal Naming Task [208 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Wechsler Adult Intelligence Scale (Fourth Edition - Canadian, WAIS-IV-CDN) [52 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Wechsler Adult Intelligence Scale (Fourth Edition - Canadian, WAIS-IV-CDN) [104 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Wechsler Adult Intelligence Scale (Fourth Edition - Canadian, WAIS-IV-CDN) [156 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Wechsler Adult Intelligence Scale (Fourth Edition - Canadian, WAIS-IV-CDN) [208 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Digit Span subtest [52 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Digit Span subtest [104 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Digit Span subtest [156 weeks]
- Neurocognitive substudy - Change from baseline in demographically-corrected T score for Digit Span subtest [208 weeks]
Eligibility Criteria
Criteria
Inclusion Criteria:
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Age ≥ 18 years old
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Kidney, liver, heart, or lung transplant at least two years ago
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History of at least one prior histologically-confirmed keratinocyte carcinoma or squamous cell carcinoma in situ
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Currently immunosuppressed with a calcineurin inhibitor-based regimen (cyclosporine or tacrolimus)
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Able to attend follow-up visits
Exclusion Criteria:
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Use of nicotinamide or niacin (≥250 mg daily) within past 12 weeks
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Untreated localized skin cancer at baseline (patient can enrol after skin cancer treatment)
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Biopsy-confirmed acute rejection episode within the past 12 weeks
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Active liver disease (high AST >3 times or bilirubin >1.5 times)
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Severe kidney disease (estimated glomerular filtration rate <20 mL/min/1.73 m2)
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Solid organ or hematologic malignancy, invasive melanoma, Merkel cell carcinoma, or metastatic skin cancer within the past five years
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Pregnancy or lactation
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Need for ongoing carbamazepine or primidone
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Allergy to nicotinamide or any ingredient of the vitamin or placebo capsules
Contacts and Locations
Locations
Site | City | State | Country | Postal Code | |
---|---|---|---|---|---|
1 | University of Calgary | Calgary | Alberta | Canada | T2N 1N4 |
2 | University of Alberta | Edmonton | Alberta | Canada | T6G 2R3 |
3 | Vancouver General Hospital | Vancouver | British Columbia | Canada | V5Z 1M9 |
4 | St. Paul's Hospital | Vancouver | British Columbia | Canada | V6Z 1Y6 |
5 | The Ottawa Hospital | Ottawa | Ontario | Canada | K1Y 4E9 |
6 | University of Ottawa Heart Institute | Ottawa | Ontario | Canada | K1Y 4W7 |
7 | Toronto General Hospital | Toronto | Ontario | Canada | M5G 2C4 |
8 | Women's College Hospital | Toronto | Ontario | Canada | M5S 1B2 |
Sponsors and Collaborators
- Women's College Hospital
- Canadian Institutes of Health Research (CIHR)
- University Health Network, Toronto
- NOW Foods
Investigators
- Principal Investigator: An-Wen Chan, Women's College Hospital
- Principal Investigator: Sang Joseph Kim, University Health Network, Toronto
Study Documents (Full-Text)
None provided.More Information
Publications
None provided.- SPRINTR-pivotal