Cancer Diagnosis, Polygenic Risk, and Longevity-Associated Variants

Author:

Goetz Laura H.ORCID,Don JanithORCID,Schork Andrew J.ORCID,Duggan David,Price Nathan D.,Evans Daniel S.,Cummings Steve,Perls ThomasORCID,Sebastiani PaolaORCID,Schork Nicholas J.ORCID

Abstract

ABSTRACTBackgroundPolygenic risk scores (PRS) have been developed to predict individual cancer risk and their potential clinical utility is receiving a great deal of attention. However, the degree to which the predictive utility of individual cancer-specific PRS may be augmented or refined by the incorporation of other cancer PRS, non-cancer disease PRS, or the protective effects of health and longevity-associated variants, is largely unexplored.MethodsWe constructed PRS for different cancers from public domain data as well as genetic scores for longevity (‘Polygenic Longevity Scores’ or ‘PLS’) for individuals in the UK Biobank. We then explored the relationships of these multiple PRS and PLS among those with and without various cancers.ResultsWe found statistically significant associations between some PLS and individual cancers, even after accounting for cancer-specific PRS. None of the PLS in their current form had an effect pronounced enough to motivate clinical cancer risk stratification based on its combined use with cancer PRS. A few variants at loci used in the PLS had known associations with Alzheimer’s disease and other diseases.ConclusionUnderlying heterogeneity behind cancer susceptibility in the population at large is not captured by PRS derived from analytical models that only consider marginal associations of individual variants with cancer diagnoses. Our results have implications for the derivation and calculation of PRS and their use in clinical and biomedical research settings.ImpactExtensions of analyses like ours could result in a more refined understanding of cancer biology and how to construct PRS for cancer.

Publisher

Cold Spring Harbor Laboratory

Reference69 articles.

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4. Variation in cancer risk among tissues can be explained by the number of stem cell divisions

5. Cancer genes and the pathways they control

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