Status and phase
Conditions
Treatments
About
A randomised double blind dose non-inferiority trial of a daily dose of 600mg versus 300mg versus 100mg of enteric coated aspirin as a cancer preventive in carriers of a germline pathological mismatch repair gene defect, Lynch Syndrome. Project 3 in the Cancer Prevention Programme (CaPP3).
Full description
Study design: A randomised, double-blind, dose non-inferiority study.
Study Intervention: Enteric-coated aspirin 100mg, 300mg or 600mg blinded dose daily followed by daily 100mg open label dose daily.
Primary objective: To determine whether the cancer preventive properties of enteric coated aspirin in Lynch syndrome are dose sensitive by comparing overall cumulative Lynch syndrome cancer incidence rates after 5 years in people who took 100mg, 300mg or 600mg enteric coated aspirin for at least 2 years.
Secondary objectives: Compare overall cumulative incidence of primary colorectal cancers using Poisson regression to allow for multiple primaries in individual patients in the three treatment groups.
Compare overall cumulative incidence of primary endometrial cancers using Poisson regression to allow for multiple primaries in individual patients in the three treatment groups.
Compare overall cumulative incidence of cancers of all types, using Poisson regression to allow for multiple primaries in individual patients in the three treatment groups.
The burden of adverse events associated with the different aspirin doses in this relatively young and healthy population will be documented.
Primary outcome: The number of new primary mismatch repair deficient cancers ("Lynch syndrome cancers") at 5 years and beyond which develop in participants who remain on prescribed treatment for a minimum of 2 years.
Number of study sites: 4 ISRAEL sites. 20 sites all over the world.
Study population/size: 300 patients in ISRAEL. UK 1000-1500 patients. Total with International 3,000 patients.
Study duration: 7 years.
Enrollment
Sex
Ages
Volunteers
Inclusion criteria
Exclusion criteria
Regular use of a non-steroidal anti-inflammatory agent (except aspirin*) on a prescription and/or long-term basis. Regular is defined as > 3 doses per week.
Regular use of aspirin (> 3 doses per week or on a prescription basis) that cannot be replaced with any one of the randomised arms of the study followed by 100mg dose.
Current methotrexate use at a weekly dose of ≥ 15mg.
Known aspirin intolerance or hypersensitivity, including aspirin-sensitive asthma.
Existing clinically significant liver impairment.
Existing renal failure.
Confirmed active peptic ulcer disease within the previous three months.
Known bleeding diathesis or concomitant warfarin therapy.
Inability to comply with study procedures and agents.
Women reporting that they are pregnant or actively planning to achieve a pregnancy within the next two years.
Women who are breastfeeding.
Any significant medical illness that would interfere with study participation.
Primary purpose
Allocation
Interventional model
Masking
1,800 participants in 3 patient groups
Loading...
Central trial contact
Michal Shenhaut, DVM; Maayan Jean, .M.Sc
Data sourced from clinicaltrials.gov
Clinical trials
Research sites
Resources
Legal