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Literature DB >> 18003629

Genetic model selection in two-phase analysis for case-control association studies.

Abstract

The Cochran-Armitage trend test (CATT) is well suited for testing association between a marker and a disease in case-control studies. When the underlying genetic model for the disease is known, the CATT optimal for the genetic model is used. For complex diseases, however, the genetic models of the true disease loci are unknown. In this situation, robust tests are preferable. We propose a two-phase analysis with model selection for the case-control design. In the first phase, we use the difference of Hardy-Weinberg disequilibrium coefficients between the cases and the controls for model selection. Then, an optimal CATT corresponding to the selected model is used for testing association. The correlation of the statistics used for selection and the test for association is derived to adjust the two-phase analysis with control of the Type-I error rate. The simulation studies show that this new approach has greater efficiency robustness than the existing methods.

Mesh：

Year: 2007 PMID： 18003629 PMCID： PMC3294316 DOI： 10.1093/biostatistics/kxm039

Source DB: PubMed Journal: Biostatistics ISSN： 1465-4644 Impact factor: 5.899

21 in total

1. Use of unlinked genetic markers to detect population stratification in association studies.

Authors: J K Pritchard; N A Rosenberg
Journal: Am J Hum Genet Date: 1999-07 Impact factor: 11.025

2. On power and efficiency robust linkage tests for affected sibs.

Authors: J L Gastwirth; B Freidlin
Journal: Ann Hum Genet Date: 2000-09 Impact factor: 1.670

3. QTL fine mapping by measuring and testing for Hardy-Weinberg and linkage disequilibrium at a series of linked marker loci in extreme samples of populations.

Authors: H W Deng; W M Chen; R R Recker
Journal: Am J Hum Genet Date: 2000-03 Impact factor: 11.025

4. Accounting for unmeasured population substructure in case-control studies of genetic association using a novel latent-class model.

Authors: G A Satten; W D Flanders; Q Yang
Journal: Am J Hum Genet Date: 2001-01-19 Impact factor: 11.025

5. Trend tests for case-control studies of genetic markers: power, sample size and robustness.

Authors: B Freidlin; G Zheng; Z Li; J L Gastwirth
Journal: Hum Hered Date: 2002 Impact factor: 0.444

6. Centralizing the non-central chi-square: A new method to correct for population stratification in genetic case-control association studies.

Authors: Prakash Gorroochurn; Gary A Heiman; Susan E Hodge; David A Greenberg
Journal: Genet Epidemiol Date: 2006-05 Impact factor: 2.135

7. Detecting marker-disease association by testing for Hardy-Weinberg disequilibrium at a marker locus.

Authors: D M Nielsen; M G Ehm; B S Weir
Journal: Am J Hum Genet Date: 1998-11 Impact factor: 11.025

8. From genotypes to genes: doubling the sample size.

Authors: P D Sasieni
Journal: Biometrics Date: 1997-12 Impact factor: 2.571

9. Simple, robust linkage tests for affected sibs.

Authors: A S Whittemore; I P Tu
Journal: Am J Hum Genet Date: 1998-05 Impact factor: 11.025

10. Choice of column scores for testing independence in ordered 2 X K contingency tables.

Authors: B I Graubard; E L Korn
Journal: Biometrics Date: 1987-06 Impact factor: 2.571

31 in total

1. A generalized sequential Bonferroni procedure using smoothed weights for genome-wide association studies incorporating information on Hardy-Weinberg disequilibrium among cases.

Authors: Guimin Gao; Guolian Kang; Jiexun Wang; Wenan Chen; Huaizen Qin; Bo Jiang; Qizhai Li; Chuanyu Sun; Nianjun Liu; Kellie J Archer; David B Allison
Journal: Hum Hered Date: 2011-12-30 Impact factor: 0.444

Genetic model selection in two-phase analysis for case-control association studies.

1. Use of unlinked genetic markers to detect population stratification in association studies.

2. On power and efficiency robust linkage tests for affected sibs.

3. QTL fine mapping by measuring and testing for Hardy-Weinberg and linkage disequilibrium at a series of linked marker loci in extreme samples of populations.

4. Accounting for unmeasured population substructure in case-control studies of genetic association using a novel latent-class model.

5. Trend tests for case-control studies of genetic markers: power, sample size and robustness.

6. Centralizing the non-central chi-square: A new method to correct for population stratification in genetic case-control association studies.

7. Detecting marker-disease association by testing for Hardy-Weinberg disequilibrium at a marker locus.

8. From genotypes to genes: doubling the sample size.

9. Simple, robust linkage tests for affected sibs.

10. Choice of column scores for testing independence in ordered 2 X K contingency tables.

1. A generalized sequential Bonferroni procedure using smoothed weights for genome-wide association studies incorporating information on Hardy-Weinberg disequilibrium among cases.

2. A robust method for testing association in genome-wide association studies.

3. Pseudosibship methods in the case-parents design.

4. Tail strength to combine two p values: their correlation cannot be ignored.

5. Can the allelic test be retired from analysis of case-control association studies?

6. Choosing an optimal method to combine P-values.

7. Test selection with application to detecting disease association with multiple SNPs.

8. A new system identification approach to identify genetic variants in sequencing studies for a binary phenotype.

9. Robust tests for matched case-control genetic association studies.

10. Robust joint analysis allowing for model uncertainty in two-stage genetic association studies.