Abstract

Substantial evidence has conclusively demonstrated that aspirin reduces risk of colorectal neoplasia. Nonetheless, the U.S. Preventive Services Task Force recommended against routine of use of aspirin to prevent colorectal cancer (CRC) largely due to uncertainty regarding its mode of action and concerns about the dose-related risk of gastrointestinal bleeding (GIB). In the current funding period, we made several important, high-impact contributions to address these issues and advance the field of chemoprevention. First, aspirin inhibits neoplasia through multiple interrelated biological mechanisms, including prostaglandin synthesis (prostaglandin-endoperoxidase synthase-2 [PTGS-2 or COX-2]); prostaglandin catabolism (15-hydroxyprostaglandin dehydrogenase [15-PGDH]); chronic inflammation (macrophage inhibitory cytokine-1 [MIC-1/GDF15]); and the TCF7L2/TCF4 transcription factor, a component of Wnt signaling at the 8q24 CRC risk locus that is a known enhancer to MYC. Second, aspirin chemoprevention may be tailored according to biomarkers of prostaglandin tone, such as urinary prostaglandin metabolites (PGE-M). Third, we and others have shown that use of aspirin, including low, anti-platelet doses, is associated with a lower risk of death from CRC as well as multiple cancers. Last, aspirin improves survival among CRC patients, particularly those with somatic PIK3CA mutations. Nonetheless, there remains a limited understanding of aspirin's overall risk- benefit profile after incorporating other cancer outcomes and cardiovascular disease (CVD) for which aspirin has established benefit. The field is now at crucial juncture to translate these findings into the clinic. There remains a high unmet need to 1) define the optimal dose, timing, and duration of aspirin use in relation to absolute ris of cancer, CVD, and GIB in the overall population as well as according to specific subgroups (e.g. sex or comorbidities); 2) identify individuals most likely to benefit and advance mechanistic understanding of aspirin's anti-cancer effect. Our central hypothesis is that aspirin, by reducing risk of multiple cancers and CVD, has a favorable risk-benefit profile for most individuals and influences several neoplastic pathways which can be exploited as biomarkers of chemopreventive efficacy. In this competing renewal, we will test this hypothesis through first-of-its kind human studies that 1) assess aspirin, at a range of dose, timing, and duration of use within sufficiently large and well-characterized cohorts to provide robust estimates of risk-benefit; 2) determine if randomized aspirin treatment, at anti-platelet (81 mg/d) or standard doses (325 mg/d), influences specific mechanistic biomarkers of colorectal carcinogenesis to advance correlation to causality. Because these data are critical to inform ongoing efforts to formulate recommendations for aspirin chemoprevention, our study has the potential for transformative public health impact.

Public Health Relevance

Compelling evidence has shown that aspirin reduces risk of colorectal as well as other cancers. This study will determine the overall long-term risks and benefits of aspirin within appropriate populations and uncover mechanisms of its anti-cancer effect in humans that could lead to the discovery of novel biomarkers of chemopreventive efficacy. Because these data are critical to inform ongoing efforts to formulate recommendations for routine aspirin use for prevention of cancer and other chronic diseases, our study has the potential for transformative public health impact.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA137178-09
Application #
9487909
Study Section
Chemo/Dietary Prevention Study Section (CDP)
Program Officer
Umar, Asad
Project Start
2009-09-29
Project End
2020-05-31
Budget Start
2018-06-01
Budget End
2019-05-31
Support Year
9
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Massachusetts General Hospital
Department
Type
DUNS #
073130411
City
Boston
State
MA
Country
United States
Zip Code

  Publications

Kosumi, Keisuke; Hamada, Tsuyoshi; Koh, Hideo et al. (2018) The Amount of Bifidobacterium Genus in Colorectal Carcinoma Tissue in Relation to Tumor Characteristics and Clinical Outcome. Am J Pathol 188:2839-2852
Liu, Li; Tabung, Fred K; Zhang, Xuehong et al. (2018) Diets That Promote Colon Inflammation Associate With Risk of Colorectal Carcinomas That Contain Fusobacterium nucleatum. Clin Gastroenterol Hepatol 16:1622-1631.e3
Yang, Wanshui; Liu, Li; Masugi, Yohei et al. (2018) Calcium intake and risk of colorectal cancer according to expression status of calcium-sensing receptor (CASR). Gut 67:1475-1483
Van Dyke, Alison L; Langhamer, Margaret S; Zhu, Bin et al. (2018) Family History of Cancer and Risk of Biliary Tract Cancers: Results from the Biliary Tract Cancers Pooling Project. Cancer Epidemiol Biomarkers Prev 27:348-351
Hamada, Tsuyoshi; Liu, Li; Nowak, Jonathan A et al. (2018) Vitamin D status after colorectal cancer diagnosis and patient survival according to immune response to tumour. Eur J Cancer 103:98-107
Liu, Po-Hong; Wu, Kana; Ng, Kimmie et al. (2018) Association of Obesity With Risk of Early-Onset Colorectal Cancer Among Women. JAMA Oncol :
Song, Mingyang; Chan, Andrew T (2018) The Potential Role of Exercise and Nutrition in Harnessing the Immune System to Improve Colorectal Cancer Survival. Gastroenterology 155:596-600
Neumeyer, Sonja; Banbury, Barbara L; Arndt, Volker et al. (2018) Mendelian randomisation study of age at menarche and age at menopause and the risk of colorectal cancer. Br J Cancer 118:1639-1647
He, Xiaosheng; Wu, Kana; Ogino, Shuji et al. (2018) Association Between Risk Factors for Colorectal Cancer and Risk of Serrated Polyps and Conventional Adenomas. Gastroenterology 155:355-373.e18
Hu, Yang; Ding, Ming; Yuan, Chen et al. (2018) Association Between Coffee Intake After Diagnosis of Colorectal Cancer and Reduced Mortality. Gastroenterology 154:916-926.e9

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