A risk prediction algorithm based on family history and common genetic variants: application to prostate cancer with potential clinical impact.

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Authors

Macinnis, RJ
Antoniou, AC
Eeles, RA
Severi, G
Al Olama, AA
McGuffog, L
Kote-Jarai, Z
Guy, M
O'Brien, LT
Hall, AL
Wilkinson, RA
Sawyer, E
Ardern-Jones, AT
Dearnaley, DP
Horwich, A
Khoo, VS
Parker, CC
Huddart, RA
Van As, N
McCredie, MR
English, DR
Giles, GG
Hopper, JL
Easton, DF

Document Type

Journal Article

Date

2011-07-18

Date Accepted

2011-05-31

Abstract

Genome wide association studies have identified several single nucleotide polymorphisms (SNPs) that are independently associated with small increments in risk of prostate cancer, opening up the possibility for using such variants in risk prediction. Using segregation analysis of population-based samples of 4,390 families of prostate cancer patients from the UK and Australia, and assuming all familial aggregation has genetic causes, we previously found that the best model for the genetic susceptibility to prostate cancer was a mixed model of inheritance that included both a recessive major gene component and a polygenic component (P) that represents the effect of a large number of genetic variants each of small effect, where . Based on published studies of 26 SNPs that are currently known to be associated with prostate cancer, we have extended our model to incorporate these SNPs by decomposing the polygenic component into two parts: a polygenic component due to the known susceptibility SNPs, , and the residual polygenic component due to the postulated but as yet unknown genetic variants, . The resulting algorithm can be used for predicting the probability of developing prostate cancer in the future based on both SNP profiles and explicit family history information. This approach can be applied to other diseases for which population-based family data and established risk variants exist.

Citation

Genetic epidemiology, 2011, 35 (6), pp. 549 - 556

Source Title

Publisher

WILEY

ISSN

0741-0395

eISSN

1098-2272

Research Team

Clinical Academic Radiotherapy (Dearnaley)
Clinical Academic Radiotherapy (Huddart)
Oncogenetics
Stereotactic and Precision Body Radiotherapy

Notes