Abstract

The primary goals of this revised project are; 1) to study the etiology of trisomy 21 including the mechanisms of disfunction and the factor that influence its frequency, and 2) to investigate the phenotypic consequences of the extra chromosome 21. We will use cytogenetic, molecular and epidemiological tools to investigate specific hypotheses generated from our previous work on Down syndrome (DS). These include hypotheses to explain the two established correlates of nondisjunction, advanced maternal age and aberrant levels of recombination, as well as hypotheses concerning environmental exposures. Additionally, we will examine a chromosome 21 gene-speficic dosage model to explain the phenotypic variation seen among DS individuals. Our innovative approach is similar to the strategy used to genetically map disease genes based on affected relative pairs. All studies will take advantage of our well-established resource of DNA results on over 1000 DS individuals and their parents, our Atlanta population epidemiology DS study, our on-going collaborations with the Denmark and California population based DS studies, and our strong team of investigators who have a long-term commitment to understanding the tillage of trisomy 21 and its consequences. The results from this project will provide essential data to elucidate mechanisms of nondisjunction and factors and influence its frequency and will be directly applicable to related studies in Projects II and III. Moreover, mechanisms responsible for maternal age effect will be identified and may point to new strategies of clinical intervention, possibly changing from prevention to preconception therapy. In addition, this will be the first study to provide direct evidence for a specific model to explain the effect of an extra chromosome 21. Identification of susceptibility genes may be used to predict phenotypic outcomes and may lead to possible treatments. Our analytical model to investigate mechanisms of chromosomal disease due to increased gene dosage will be complementary to the genome- based approach to study the pathogenesis of X chromosome abnormalities, as proposed in Project IV. Furthermore, the identification of genes involved in developmental processes or leukemia pathways may be applicable to other disorders found among chromosomally normal individuals.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Program Projects (P01)
Project #
5P01HD032111-05
Application #
6108739
Study Section
Project Start
1999-03-01
Project End
2001-02-28
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
5
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Case Western Reserve University
Department
Type
DUNS #
077758407
City
Cleveland
State
OH
Country
United States
Zip Code
44106

  Publications

Kokotas, Haris; Grigoriadou, Maria; Mikkelsen, Margareta et al. (2009) Investigating the impact of the Down syndrome related common MTHFR 677C>T polymorphism in the Danish population. Dis Markers 27:279-85
Lamb, N E; Sherman, S L; Hassold, T J (2005) Effect of meiotic recombination on the production of aneuploid gametes in humans. Cytogenet Genome Res 111:250-5
Lamb, Neil E; Yu, Kai; Shaffer, John et al. (2005) Association between maternal age and meiotic recombination for trisomy 21. Am J Hum Genet 76:91-9
Schueler, M G; Higgins, A W; Rudd, M K et al. (2001) Genomic and genetic definition of a functional human centromere. Science 294:109-15
Tsuchiya, K; Schueler, M G; Dev, V G (2001) Familial X centromere variant resulting in false-positive prenatal diagnosis of monosomy X by interphase FISH. Prenat Diagn 21:852-5
Brown, A S; Feingold, E; Broman, K W et al. (2000) Genome-wide variation in recombination in female meiosis: a risk factor for non-disjunction of chromosome 21. Hum Mol Genet 9:515-23
Hassold, T; Sherman, S; Hunt, P (2000) Counting cross-overs: characterizing meiotic recombination in mammals. Hum Mol Genet 9:2409-19
Feingold, E; Brown, A S; Sherman, S L (2000) Multipoint estimation of genetic maps for human trisomies with one parent or other partial data. Am J Hum Genet 66:958-68
Hassold, T; Sherman, S (2000) Down syndrome: genetic recombination and the origin of the extra chromosome 21. Clin Genet 57:95-100
Freeman, S B; Yang, Q; Allran, K et al. (2000) Women with a reduced ovarian complement may have an increased risk for a child with Down syndrome. Am J Hum Genet 66:1680-3

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