Construction of the model for the Genetic Analysis Workshop 14 simulated data: genotype-phenotype relationships, gene interaction, linkage, association, disequilibrium, and ascertainment effects for a complex phenotype.
- Authors
- Greenberg, David A; Zhang, Junying; Shmulewitz, Dvora; Strug, Lisa J; Zimmerman, Regina; Singh, Veena; Marathe, Sudhir
- Year
- 2005
- Journal
- BMC genetics
- PMID
- 16451639
- DOI
- 10.1186/1471-2156-6-S1-S3
- PMCID
- PMC1866756
The Genetic Analysis Workshop 14 simulated dataset was designed 1) To test the ability to find genes related to a complex disease (such as alcoholism). Such a disease may be given a variety of definitions by different investigators, have associated endophenotypes that are common in the general population, and is likely to be not one disease but a heterogeneous collection of clinically similar, but genetically distinct, entities. 2) To observe the effect on genetic analysis and gene discovery of a complex set of gene x gene interactions. 3) To allow comparison of microsatellite vs. large-scale single-nucleotide polymorphism (SNP) data. 4) To allow testing of association to identify the disease gene and the effect of moderate marker x marker linkage disequilibrium. 5) To observe the effect of different ascertainment/disease definition schemes on the analysis. Data was distributed in two forms. Data distributed to participants contained about 1,000 SNPs and 400 microsatellite markers. Internet-obtainable data consisted of a finer 10,000 SNP map, which also contained data on controls. While disease characteristics and parameters were constant, four "studies" used varying ascertainment schemes based on differing beliefs about disease characteristics. One of the studies contained multiplex two- and three-generation pedigrees with at least four affected members. The simulated disease was a psychiatric condition with many associated behaviors (endophenotypes), almost all of which were genetic in origin. The underlying disease model contained four major genes and two modifier genes. The four major genes interacted with each other to produce three different phenotypes, which were themselves heterogeneous. The population parameters were calibrated so that the major genes could be discovered by linkage analysis in most datasets. The association evidence was more difficult to calibrate but was designed to find statistically significant association in 50% of datasets. We also simulated some marker x marker linkage disequilibrium around some of the genes and also in areas without disease genes. We tried two different methods to simulate the linkage disequilibrium.
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| 40 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | 4. KPD patients may suffer from a form of humor impairment. They frequently report that they have… |
| 41 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | 5. KPD patients show unusual speech patterns. This includes 1) a tendency to form words in the… |
| 42 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | 6. A strong aversion to travel by foot (i.e., walking). Patients will use their vehicles (large,… |
| 43 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | 7. Pathological fear of rain, increasing to horror and terror with the presence of snow.… |
| 44 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | 8. Together with the anxiety caused by weather is an extreme sensitivity to what patients describe… |
| 45 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | 9. A preoccupation with body habitus, both of the patient's own and with that of others. In male… |
| 46 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | 10. Anxiety or panic when innocently approached by a stranger, e.g., for directions. This is the… |
| 47 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | 11. Unusual tolerance, even enjoyment, when surrounded by noxious automobile exhaust. This goes… |
| 48 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | 12. An obsession with automobiles (cf, driving obsession, above). |
| 49 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | 13. A fixation, obsession, or unusual concentration on some popular entertainers. It is generally… |
| 50 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | 14. Tendency to fiscal irresponsibility on an extremely large scale. (Although this trait is of… |
| 51 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | Because of these varied phenotypes, there has been much disagreement about how the disorder should… |
| 52 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | 1. The unusual "communal emotionality" that appears in many KPD patients is classified by some… |
| 53 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | "Communally-shared emotions" |
| 54 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | a. Joining/founding cults |
| 55 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | b. Fear/discomfort with strangers |
| 56 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | c. Dislike of jokes told face to face |
| 57 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | d. Obsession with entertainers |
| 58 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | e. Humor impairment |
| 59 | Background — Description of clinical characteristics of KPD and how the family data were collected and classified | Other investigators focus on the behavior-related symptoms: |
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| Citation | PMID | DOI | Status |
|---|---|---|---|
| Matheson, R, Collected Stories, 1959, The creeping terror | — | — | — |
In this knowledge base
| Title | Year | PMID |
|---|---|---|
| Genetic Analysis Workshop 14: microsatellite and single-nucleotide polymorphism marker loci for genome-wide scans. | 2005 | 16451554 |
External
| Title | Authors | Journal | Year | Link |
|---|---|---|---|---|
| Accurate phenotyping: Reconciling approaches through Bayesian model averaging. | Chen CC et al. | — | 2017 | → |
| Computer simulation is an undervalued tool for genetic analysis: a historical view and presentation of SHIMSHON--a Web-based genetic simulation package. | Greenberg DA | — | 2011 | → |
| A novel analytical framework for dissecting the genetic architecture of behavioral symptoms in neuropsychiatric disorders. | Deo AJ et al. | — | 2010 | → |
| Computation of the posterior probability of linkage using 'high effect' genetic model priors. | Logue MW et al. | — | 2008 | → |
| A power study of bivariate LOD score analysis of a complex trait and fear/discomfort with strangers. | Ji F et al. | — | 2005 | → |
| Application of family-based association testing to assess the genotype-phenotype association involved in complex traits using single-nucleotide polymorphisms. | Wang MH et al. | — | 2005 | → |
| Assessment and implications of linkage disequilibrium in genome-wide single-nucleotide polymorphism and microsatellite panels. | Goode EL et al. | — | 2005 | → |
| Bias of allele-sharing linkage statistics in the presence of intermarker linkage disequilibrium. | Goode EL et al. | — | 2005 | → |
| Comparison of single-nucleotide polymorphisms and microsatellite markers for linkage analysis in the COGA and simulated data sets for Genetic Analysis Workshop 14: Presentation Groups 1, 2, and 3. | Wilcox MA et al. | — | 2005 | → |
| Dissection of heterogeneous phenotypes for quantitative trait mapping. | Bickeböller H et al. | — | 2005 | → |
| Genetic Analysis Workshop 14: microsatellite and single-nucleotide polymorphism marker loci for genome-wide scans. | Bailey-Wilson JE et al. | — | 2005 | → |
| Methods for detecting gene x gene interaction in multiplex extended pedigrees. | Brock GN et al. | — | 2005 | → |
| Summary of contributions to GAW Group 5: linkage mapping methods, Problem 2. | Cordell HJ | — | 2005 | → |