Abstract

Genetic surveys in human populations often involve a mixture of subpopulations. Recognition of the presence of mixtures and identification of mixture components is essential in understanding the maintenance of genetic variation, and for reconstructing evolutionary history. This project aims at a quantitative assessment of the effect of admixture on genetic variation in natural populations. Two types of mixtures will be studied: (a) mixture due to amalgamation of subpopulations; and (b) admixture due to gene flow among source populations. In both instances, we will develop statistical methods to identify the source of mixtures, and estimate the mixing components. Since the presence of mixture affects the observed allele frequency distribution, adjustment for the effects of mixture components will provide reliable estimates of locus-specific mutation rates (v's) and effective population size (e's) from multi-locus allele frequency data. The utility of admixed populations for genetic- epidemiological studies of complex diseases will be examined by the dynamics of allelic association among loci and its relationship with the history of admixture. The maximum likelihood principle will be used to develop analytical methods for such analyses, and numerical algorithms will be provided to encompass the possibility of missing data and unknown source populations. The theory will be applied to allozyme data from the Amerindians, and the three major ethnic groups, to test its validity, and to provide empirical observations on the effect of mixtures on genetic variation. Genetic evidence of admixture will be studied in the Siddis of India, and the Sinhalese of Sri Lanka, whose parental populations are not precisely known. Extensive computer simulations and re-analysis of published data from Asian Macaques and Drosophila will be used to test the theories and to study the statistical properties of the estimators. The estimation of locus-specific mutation rates will contribute to an understanding of the variation of mutability at different loci, or at DNA segments in different parts of the human genome. Simultaneous estimates of v's and Ne's will allow effective comparisons of the rate of spontaneous mutations in different organisms. The relationship between admixture levels and the multi-locus association of alleles will aid (a) in understanding the genetic etiology of complex diseases, and (b) in developing efficient survey strategies for mapping genes underlying such diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM041399-03
Application #
3299581
Study Section
Mammalian Genetics Study Section (MGN)
Project Start
1990-04-01
Project End
1994-03-31
Budget Start
1992-04-01
Budget End
1993-03-31
Support Year
3
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
University of Texas Health Science Center Houston
Department
Type
Schools of Medicine
DUNS #
City
Houston
State
TX
Country
United States
Zip Code
77225

  Publications

Missoni, Sasa; Durakovic, Zijad; Sahay, Rashmi et al. (2013) Smoking habits according to metabolic traits in an island population of the eastern Adriatic Coast. Coll Antropol 37:745-53
Li, Biao; Kimmel, Marek (2013) Factors influencing ascertainment bias of microsatellite allele sizes: impact on estimates of mutation rates. Genetics 195:563-72
Ge, Jianye; Budowle, Bruce; Aranda, Xavier G et al. (2009) Mutation rates at Y chromosome short tandem repeats in Texas populations. Forensic Sci Int Genet 3:179-84
Guha, S; Chakraborty, R (2008) Correlation analyses reveal a substantial influence of allelic gaps on the investigation of genetic diversity of modern human populations with microsatellites. Ann Hum Genet 72:644-53
Raskin, Salmo; Pereira-Ferrari, Lilian; Reis, Francisco Caldeira et al. (2008) Incidence of cystic fibrosis in five different states of Brazil as determined by screening of p.F508del, mutation at the CFTR gene in newborns and patients. J Cyst Fibros 7:15-22
Wilding, Craig S; Curwen, Gillian B; Tawn, E Janet et al. (2007) Influence of polymorphisms at loci encoding DNA repair proteins on cancer susceptibility and G2 chromosomal radiosensitivity. Environ Mol Mutagen 48:48-57
Chakraborty, Bandana M; Chakraborty, Ranajit (2007) Sensitivity and specificity of body mass index as a definition of the obesity component of metabolic syndrome. Coll Antropol 31:943-7
Raj, Srilakshmi M; Chakraborty, Ranajit; Wang, Ning et al. (2006) Linkage disequilibria and haplotype structure of four SNPs of the interleukin 1 gene cluster in seven Asian Indian populations. Hum Biol 78:109-19
Wen, Bo; Li, Hui; Gao, Song et al. (2005) Genetic structure of Hmong-Mien speaking populations in East Asia as revealed by mtDNA lineages. Mol Biol Evol 22:725-34
Klaric, Irena Martinovic; Pericic, Marijana; Lauc, Lovorka Barac et al. (2005) Genetic variation at nine short tandem repeat loci among islanders of the eastern Adriatic coast of Croatia. Hum Biol 77:471-86

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