Abstract

An ever increasing fraction of the estimated total complement of human genes is being identified. Projects focused on either the biology of a particular functional or structural element or those carrying out a comprehensive cataloguing of genes in particular chromosomal regions or tissue types add daily to the lists of genes. Currently, in excess of 1500 well characterized human coding sequences have been identified with another 3,000 unique sequences identified via analysis of fragments from cDNA libraries. It seems likely that the next decade will see substantial additions to these totals as positional cloning efforts, exon trapping technology, massive sequencing efforts and homology screening programs expand. Project 3 will exploit this ongoing work in three ways to provide genetically useful expressed sequence reagents to the scientific community. First, we will incorporate into the linkage maps being developed by Project 5 polymorphic cDNAs identified from the literature. We will use published sequence based DNA variants for this, as well as new variants identified in Project 2. We will also incorporate into the evolving linkage map polymorphic short tandem repeats (STRPs) identified in Project 1 that will be derived from subcloned and STRP enriched cDNA libraries. Next we will identify the parent cDNA clone for a subset of the STRPs identified from coding sequences in Project 1. This will provide us with a benchmark for how frequently we can expect to identify particular classes of STRPs in true expressed coding sequences. Our third goal will be to provide the linkage maps and polymorphic cDNAs as a resource to outside investigators who wish to characterize their own families or populations using linkage or association studies. As part of this goal, we will pilot test the feasibility of obtaining and characterizing population based samples from a range of normal and disease based groups with multiple geographical origins. This will be done in close collaboration with the ELSI core to explore the ethical, legal and social aspects of issues including cooperation, consent and the scope and effects of erroneous typing. Project 3 will undertake extensive data validation in concert with Project 4 and error checking with Projects 4 and 5. The ultimate product will be a collection of 2,000 polymorphic cDNAs that have linkage assignments and can serve as candidate genes. Over 4,000 cDNA STSs will be defined which can be integrated into a physical map. A better understanding of how to carry out registry based surveys focused on abnormalities of candidate genes will be developed.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Human Genome Research Institute (NHGRI)
Type
Specialized Center (P50)
Project #
1P50HG000835-01
Application #
3843226
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
1
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
University of Iowa
Department
Type
DUNS #
041294109
City
Iowa City
State
IA
Country
United States
Zip Code
52242

  Publications

Taillon-Miller, P; Bauer-Sardina, I; Saccone, N L et al. (2000) Juxtaposed regions of extensive and minimal linkage disequilibrium in human Xq25 and Xq28. Nat Genet 25:324-8
Gleeson, C M; Sloan, J M; McGuigan, J A et al. (1998) Barrett's oesophagus: microsatellite analysis provides evidence to support the proposed metaplasia-dysplasia-carcinoma sequence. Genes Chromosomes Cancer 21:49-60
Scott, D A; Kraft, M L; Carmi, R et al. (1998) Identification of mutations in the connexin 26 gene that cause autosomal recessive nonsyndromic hearing loss. Hum Mutat 11:387-94
el-Shanti, H; Murray, J C; Semina, E V et al. (1998) Assignment of gene responsible for progressive pseudorheumatoid dysplasia to chromosome 6 and examination of COL10A1 as candidate gene. Eur J Hum Genet 6:251-6
Greinwald Jr, J H; Scott, D A; Marietta, J R et al. (1997) Construction of P1-derived artificial chromosome and yeast artificial chromosome contigs encompassing the DFNB7 and DFNB11 region of chromosome 9q13-21. Genome Res 7:879-86
Yuan, B; Vaske, D; Weber, J L et al. (1997) Improved set of short-tandem-repeat polymorphisms for screening the human genome. Am J Hum Genet 60:459-60
Sheffield, V C; Pierpont, M E; Nishimura, D et al. (1997) Identification of a complex congenital heart defect susceptibility locus by using DNA pooling and shared segment analysis. Hum Mol Genet 6:117-21
Peiffer-Schneider, S; Schutte, B C; Murray, J C et al. (1997) Exclusion of Ifa and Ifb as the Lps gene and mapping of three markers near the Lps locus. Mamm Genome 8:785-6
Gleeson, C M; Sloan, J M; McGuigan, J A et al. (1997) Allelotype analysis of adenocarcinoma of the gastric cardia. Br J Cancer 76:1455-65
Bonne-Tamir, B; Nystuen, A; Seroussi, E et al. (1997) Usher syndrome in the Samaritans: strengths and limitations of using inbred isolated populations to identify genes causing recessive disorders. Am J Phys Anthropol 104:193-200

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