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Testing for association with a case‐parents design in the presence of genotyping errors
Author(s) -
Morris Richard W.,
Kaplan Norman L.
Publication year - 2004
Publication title -
genetic epidemiology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.301
H-Index - 98
eISSN - 1098-2272
pISSN - 0741-0395
DOI - 10.1002/gepi.10297
Subject(s) - type i and type ii errors , genotyping , mendelian inheritance , statistics , genotype , likelihood ratio test , haplotype , genetics , single nucleotide polymorphism , observational error , snp , biology , mathematics , gene
Genotyping errors can create a problem for the analysis of case‐parents data because some families will exhibit genotypes that are inconsistent with Mendelian inheritance. The problem with correcting Mendelian inconsistent genotype errors by regenotyping or removing families in which they occur is that the remaining unidentified genotype errors can produce excess type I (false positive) error for some family‐based tests for association. We address this problem by developing a likelihood ratio test (LRT) for association in a case‐parents design that incorporates nuisance parameters for a general genotype error model. We extend the likelihood approach for a single SNP to include short haplotypes consisting of 2 or 3 SNPs. The extension to haplotypes is based on assumptions of random mating, multiplicative penetrances, and at most a single genotype error per family. For a single SNP, we found, using Monte Carlo simulation, that type I error rate can be controlled for a number of genotype error models at different error rates. Simulation results suggest the same is true for 2 and 3 SNPs. In all cases, power declined with increasing genotyping error rates. In the absence of genotyping errors, power was similar whether nuisance parameters for genotype error were included in the LRT or not. The LRT developed here does not require prior specification of a particular model for genotype errors and it can be readily computed using the EM algorithm. Consequently, this test may be generally useful as a test of association with case‐parents data in which Mendelian inconsistent families are observed. Genet Epidemiol 26:142–154, 2004. Published 2004 Wiley‐Liss, Inc.