Ordered subset analysis for case‐control studies
TL;DR: It is demonstrated that OSACC is a useful method for improving SNP association signals in genetically heterogeneous datasets and its ability to identify a more informative subset of cases that may be subjected to more detailed molecular analysis.
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Abstract: Genetic heterogeneity, which may manifest on a population level as different frequencies of a specific disease susceptibility allele in different subsets of patients, is a common problem for candidate gene and genome-wide association studies of complex human diseases. The ordered subset analysis (OSA) was originally developed as a method to reduce genetic heterogeneity in the context of family-based linkage studies. Here, we have extended a previously proposed method (OSACC) for applying the OSA methodology to case-control datasets. We have evaluated the type I error and power of different OSACC permutation tests with an extensive simulation study. Case-control datasets were generated under two different models by which continuous clinical or environmental covariates may influence the relationship between susceptibility genotypes and disease risk. Our results demonstrate that OSACC is more powerful under some disease models than the commonly used trend test and a previously proposed joint test of main genetic and gene-environment interaction effects. An additional unique benefit of OSACC is its ability to identify a more informative subset of cases that may be subjected to more detailed molecular analysis, such as DNA sequencing of selected genomic regions to detect functional variants in linkage disequilibrium with the associated polymorphism. The OSACC-identified covariate threshold may also improve the power of an additional dataset to replicate previously reported associations that may only be detectable in a fraction of the original and replication datasets. In summary, we have demonstrated that OSACC is a useful method for improving SNP association signals in genetically heterogeneous datasets.
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Citations
•Journal Article
A Susceptibility Locus for Age–Related Macular Degeneration on Chromosome 16p12
Kylee L. Spencer,Silke Schmidt,Michael A. Hauser,William K. Scott,Lana M. Olson,Paul Gallins,Anita Agarwal,Eric A. Postel,M.A. Pericak–Vance,Jonathan L. Haines +9 more
TL;DR: The results suggest that a susceptibility gene on chromosome 16p12 may predispose to AMD, particularly to the neovascular form, and that further research into the previously suggested association of neov vascular AMD and systemic hypertension is warranted.
59
TDT-HET: A new transmission disequilibrium test that incorporates locus heterogeneity into the analysis of family-based association data
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TL;DR: The development of a test that extends the classic transmission disequilibrium test (TDT) to one that accounts for locus heterogeneity among coded trios is developed and it is conjecture that the TDT-HET may be a useful method for correctly identifying linked trios.
IGF-I gene variability is associated with an increased risk for AD
Teo Vargas,Ana Martínez-García,Desiree Antequera,Elisabet Vilella,Jordi Clarimón,Ignacio Mateo,Pascual Sánchez-Juan,Eloy Rodríguez-Rodríguez,Ana Frank,Marcel Rosich-Estrago,Alberto Lleó,Laura Molina-Porcel,Rafael Blesa,Teresa Gomez-Isla,Onofre Combarros,Félix Bermejo-Pareja,Fernando Valdivieso,María J. Bullido,Eva Carro +18 more
TL;DR: It is suggested that polymorphisms within the IGF-I gene could infer greater risk for AD through their effect on IGF-i levels, and the physiological role IGF- I in the pathogenesis of AD is confirmed.
39
The role of phenotype in gene discovery in the whole genome sequencing era.
TL;DR: Statistical genetic methods and analytical approaches that are concerned with optimizing phenotypes for gene discovery for complex traits offer two general categories of advantages: they may increase power to localize genes of interest and also aid in interpreting associations between genetic variants and disease outcomes.
29
Ordered subset analysis of copy number variation association with age at onset of Alzheimer's disease.
Kinga Szigeti,Blanka Kellermayer,Jenna M. Lentini,Brian Trummer,Deepika Lal,Rachelle S. Doody,Li Yan,Song Liu,Changxing Ma +8 more
TL;DR: OSA, using AAO as a quantitative trait, optimized power and detected replicable signals suggesting that AD is genetically heterogeneous between AAO subsets, thus improving power under some disease models.
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