Constraints for genetic association studies imposed by attributable fraction and familial risk

doi:10.1093/carcin/bgl182

Carcinogenesis Advance Access originally published online on September 28, 2006
Carcinogenesis 2007 28(3):648-656; doi:10.1093/carcin/bgl182

This Article

	Full Text
	FREE Full Text (PDF)
	All Versions of this Article: 28/3/648 most recent bgl182v1
	Alert me when this article is cited
	Alert me if a correction is posted

Services

	Email this article to a friend
	Similar articles in this journal
	Similar articles in ISI Web of Science
	Similar articles in PubMed
	Alert me to new issues of the journal
	Add to My Personal Archive
	Download to citation manager
	Search for citing articles in: ISI Web of Science (6)
	Request Permissions

Google Scholar

	Articles by Hemminki, K.
	Articles by Bermejo, J. L.
	Search for Related Content

PubMed

	PubMed Citation
	Articles by Hemminki, K.
	Articles by Bermejo, J. L.

Social Bookmarking

	What's this?

Constraints for genetic association studies imposed by attributable fraction and familial risk

Kari Hemminki¹^,2^,* and Justo Lorenzo Bermejo¹

¹ Division of Molecular Genetic Epidemiology, German Cancer Research Center (DKFZ) Im Neuenheimer Feld 580, D-69120 Heidelberg, Germany
² Center for Family Medicine, Karolinska Institute 141 83 Huddinge, Sweden

^*To whom correspondence should be addressed. Email: k.hemminki{at}dkfz.de

Candidate gene studies have become very popular but some oftheir implicit constraints, such as the familial risk and thepopulation attributable fraction (PAF) conferred by the geneunder study, are poorly understood. We model here these parametersfor susceptibility genes in terms of genotype relative risk(GRR), allele frequency and statistical power in simulated geneticassociation studies, assuming 500 or 2000 case–controlpairs and different modes of inheritance. The results show thatthe common association studies on genes with minor allele frequency>10% have sufficient power to detect disease-causing variantsconferring PAFs >10%, which can be compared to known genes,such as BRCA1 with a PAF of 1.8%. Yet, common low-risk variantsconfer low familial relative risks (FRRs), typically <1.1.The models show that candidate gene studies may be able to identifygenes conferring close to 100% of the PAF, but they may notexplain the empirical FRRs. In order to explain FRRs, rare,high-penetrant genes or interacting combinations of common variantsneed to be uncovered. However, the candidate gene studies forcommon alleles do not target this class of genes. The resultsmay challenge the common disease–common variant hypothesis,which posits common variants with low GRRs and large PAFs, howeverfailing to accommodate the empirical FRRs.

Abbreviations: CDCV, common disease–common variant; FRR, familialrelative risk; GRR, genotype relative risk; PAF, population attributable fractions; SNP, single nucleotide polymorphism.

Received July 26, 2006; revised September 13, 2006; accepted September 15, 2006.

Add to CiteULike CiteULike Add to Connotea Connotea Add to Del.icio.us Del.icio.us What's this?

This article has been cited by other articles:

K. Hemminki, J. Sundquist, and J. Lorenzo Bermejo
Familial Risks for Cancer as the Basis for Evidence-Based Clinical Referral and Counseling
Oncologist, March 1, 2008; 13(3): 239 - 247.
[Abstract] [Full Text] [PDF]

K Hemminki, A Forsti, and J L Bermejo
Estimating risks of common complex diseases: familial and population risks
J. Med. Genet., February 1, 2008; 45(2): 126 - 127.
[Full Text] [PDF]

				K Hemminki, A Forsti, and J L Bermejo Estimating risks of common complex diseases: familial and population risks J. Med. Genet., February 1, 2008; 45(2): 126 - 127. [Full Text] [PDF]