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Literature DB >> 11890312

Two-stage designs for gene-disease association studies.

Jaya M Satagopan¹, David A Verbel, E S Venkatraman, Kenneth E Offit, Colin B Begg.

Abstract

The goal of this article is to describe a two-stage design that maximizes the power to detect gene-disease associations when the principal design constraint is the total cost, represented by the total number of gene evaluations rather than the total number of individuals. In the first stage, all genes of interest are evaluated on a subset of individuals. The most promising genes are then evaluated on additional subjects in the second stage. This will eliminate wastage of resources on genes unlikely to be associated with disease based on the results of the first stage. We consider the case where the genes are correlated and the case where the genes are independent. Using simulation results, it is shown that, as a general guideline when the genes are independent or when the correlation is small, utilizing 75% of the resources in stage 1 to screen all the markers and evaluating the most promising 10% of the markers with the remaining resources provides near-optimal power for a broad range of parametric configurations. This translates to screening all the markers on approximately one quarter of the required sample size in stage 1.

Entities: Chemical

Mesh：

Year: 2002 PMID： 11890312 PMCID： PMC8978151 DOI： 10.1111/j.0006-341x.2002.00163.x

Source DB: PubMed Journal: Biometrics ISSN： 0006-341X Impact factor: 2.571

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7. The relative power of family-based and case-control designs for linkage disequilibrium studies of complex human diseases. II. Individual genotyping.

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9. Multifactor dimensionality reduction-phenomics: a novel method to capture genetic heterogeneity with use of phenotypic variables.

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10. Quantifying and correcting for the winner's curse in genetic association studies.

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Two-stage designs for gene-disease association studies.

Review 1. A look at linkage disequilibrium.

2. The lifetime risks of breast cancer in Ashkenazi Jewish carriers of BRCA1 and BRCA2 mutations.

3. Tests for linkage and association in nuclear families.

4. Use of parents, sibs, and unrelated controls for detection of associations between genetic markers and disease.

5. General score tests for associations of genetic markers with disease using cases and their parents.

6. Genetic heterogeneity and penetrance analysis of the BRCA1 and BRCA2 genes in breast cancer families. The Breast Cancer Linkage Consortium.

7. The relative power of family-based and case-control designs for linkage disequilibrium studies of complex human diseases. II. Individual genotyping.

1. Group sequential methods and sample size savings in biomarker-disease association studies.

2. Efficient computation of significance levels for multiple associations in large studies of correlated data, including genomewide association studies.

3. Don't split your data.

4. Designing a multistage, SNP-based, genome screen for common diseases.

5. Quantitative trait locus study design from an information perspective.

6. Ranks of genuine associations in whole-genome scans.

Review 7. Recent developments in genomewide association scans: a workshop summary and review.

8. Two-stage designs in case-control association analysis.

9. Multifactor dimensionality reduction-phenomics: a novel method to capture genetic heterogeneity with use of phenotypic variables.

10. Quantifying and correcting for the winner's curse in genetic association studies.