Abstract

Investigating the genetics of autism presents particular challenges (due to features such as limited vertical transmission, and small family size), over and above the usual difficulties of modeling complex and heterogeneous disorders. Therefore, clarification of the phenotypic expression of the genetic liability underlying autism is a critical first step. A method for exploring the phenotypic boundaries of autism and identifying relatives of autistic probands affected with a broad or multidimensional phenotype will be developed using data from the Baltimore Family Study of Autism. The method will then be replicated, in a quasi- validation step, with data from two additional sets of autism families (one simplex and one multiplex) collected in Iowa with the use of instruments and measures similar or identical to those used in the Baltimore study. The method for identifying the affected will be tested for its utility in improving the power of genetic modeling, including segregation and linkage analyses. The segregation analyses will be carried out on the two data sets described above. The linkage studies will be carried out with simulated data; both trait and marker genotypes will be simulated for pedigrees with the phenotypic characteristics of the families we have actually observed. Then both likelihood-based and non-parametric linkage analysis will be carried out to determine statistical power under various models and misclassification schemes. More generally, I hope this work will contribute to the development of methods for correctly classifying affected relatives in families expressing other complex disorders with ambiguous phenotypic expression, and to the search for genes for other neuropsychiatric disorders.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Scientist Development Award (K21)
Project #
5K21MH001338-05
Application #
2889860
Study Section
Epidemiology and Genetics Review Committee (EPI)
Program Officer
Goldschmidts, Walter L
Project Start
1995-08-01
Project End
2001-07-31
Budget Start
1999-08-01
Budget End
2001-07-31
Support Year
5
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Tufts University
Department
Type
DUNS #
City
Boston
State
MA
Country
United States
Zip Code
02111

  Publications

Wassink, Thomas H; Piven, Joseph; Vieland, Veronica J et al. (2005) Evaluation of the chromosome 2q37.3 gene CENTG2 as an autism susceptibility gene. Am J Med Genet B Neuropsychiatr Genet 136B:36-44
Wassink, Thomas H; Piven, Joseph; Vieland, Veronica J et al. (2002) Evaluation of FOXP2 as an autism susceptibility gene. Am J Med Genet 114:566-9
Collaborative Linkage Study of Autism (2001) An autosomal genomic screen for autism. Am J Med Genet 105:609-15
Collaborative Linkage Study of Autism (2001) Incorporating language phenotypes strengthens evidence of linkage to autism. Am J Med Genet 105:539-47
Van Eerdewegh, P; Dowd, M; Dupuis, J et al. (2001) On the detection of linkage in multiple data sets: a comparison of various statistical approaches. Genet Epidemiol 21 Suppl 1:S67-72
Wassink, T H; Piven, J; Vieland, V J et al. (2001) Evidence supporting WNT2 as an autism susceptibility gene. Am J Med Genet 105:406-13
Wassink, T H; Piven, J; Patil, S R (2001) Chromosomal abnormalities in a clinic sample of individuals with autistic disorder. Psychiatr Genet 11:57-63
Bradford, Y; Haines, J; Hutcheson, H et al. (2001) Incorporating language phenotypes strengthens evidence of linkage to autism. Am J Med Genet 105:539-47
Barrett, S; Beck, J C; Bernier, R et al. (1999) An autosomal genomic screen for autism. Collaborative linkage study of autism. Am J Med Genet 88:609-15
Folstein, S E; Santangelo, S L; Gilman, S E et al. (1999) Predictors of cognitive test patterns in autism families. J Child Psychol Psychiatry 40:1117-28

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