Abstract

During the next granting period I plan to continue our research along three major lines. First, we will complete the mapping of the WAGR region of 11p13. Our initial efforts will be directed toward completing a long range restriction map of this region followed by the isolation of the genomic DNA of this region by molecular cloning techniques. From these cloned DNA sequences we will develop a transcriptional map of this region. We will then identify transcripts responsible for the specific functional phenotypes identified with deletions of this region, aniridia, Wilms tumor, urogenital malformations and mental retardation by correlating the location of deletion and translocation breakpoints with the occurrence of these conditions in patients. A second goal of this proposal will be to extend our studies of homology between human chromosome 11 and other mammalian species. One main focus will be to characterize the region of mouse chromosome 2 which is likely to be homologous to the WAGR region of human chromosome 11. We will undertake a detailed effort to study the genetics and functional basis of mutations at the Sey locus on mouse chromosome 2 which we believe is likely to be a homologue to the human aniridia (AN-2) locus on chromosome 11. We will attempt to develop mice which are functionally hemozygous for the mouse homologue to the Wilms tumor gene and determine whether such animals exhibit a high frequency of malignancies derived from embryonic kidney tissue. A further goal of our mouse genetics program will be to continue to characterize homology relationships between other portions of human chromosome II and segments of mouse chromosomes 7 (llp15), 19 (llq13) and 9 (llq23). The third major objective of this proposal will be to continue develop and utilize molecular genetic and somatic genetic techniques to map chromosome 11 in its entirety. Continued effort will be directed towards the extension of studies on the short arm of the chromosome. Increased effort and emphasis will be placed on the long arm of the chromosome during the next granting period. In particular, we will utilize techniques and reagents developed during the previous granting period to isolate somatic cell hybrids for the long arm of the chromosome analogous to those which have been so useful in mapping IIp. Additional cloned genomic DNA segments for IIq will be isolated using these hybrids, and RFLPs will be identified for a subset of these genomic DNA clones, A detailed map of IIq will then be constructed using the combined power of somatic cell genetics, genetic linkage techniques and long range restriction mapping methods. We will utilize map information derived from our studies to test hypotheses regarding the location of genes for specific genetic disorders or predispositions on chromosome 11.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM027882-10
Application #
3275106
Study Section
Mammalian Genetics Study Section (MGN)
Project Start
1980-04-01
Project End
1993-06-30
Budget Start
1989-07-01
Budget End
1990-06-30
Support Year
10
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
Massachusetts Institute of Technology
Department
Type
Organized Research Units
DUNS #
City
Cambridge
State
MA
Country
United States
Zip Code
02139

  Publications

Park, S; Schalling, M; Bernard, A et al. (1993) The Wilms tumour gene WT1 is expressed in murine mesoderm-derived tissues and mutated in a human mesothelioma. Nat Genet 4:415-20
Oettinger, M A; Stanger, B; Schatz, D G et al. (1992) The recombination activating genes, RAG 1 and RAG 2, are on chromosome 11p in humans and chromosome 2p in mice. Immunogenetics 35:97-101
Haber, D A; Timmers, H T; Pelletier, J et al. (1992) A dominant mutation in the Wilms tumor gene WT1 cooperates with the viral oncogene E1A in transformation of primary kidney cells. Proc Natl Acad Sci U S A 89:6010-4
Schwartz, C E; Haber, D A; Stanton, V P et al. (1991) Familial predisposition to Wilms tumor does not segregate with the WT1 gene. Genomics 10:927-30
Pelletier, J; Schalling, M; Buckler, A J et al. (1991) Expression of the Wilms' tumor gene WT1 in the murine urogenital system. Genes Dev 5:1345-56
Warburton, D; Gersen, S; Yu, M T et al. (1990) Monochromosomal rodent-human hybrids from microcell fusion of human lymphoblastoid cells containing an inserted dominant selectable marker. Genomics 6:358-66
Glaser, T; Rose, E; Morse, H et al. (1990) A panel of irradiation-reduced hybrids selectively retaining human chromosome 11p13: their structure and use to purify the WAGR gene complex. Genomics 6:48-64
Glaser, T; Lane, J; Housman, D (1990) A mouse model of the aniridia-Wilms tumor deletion syndrome. Science 250:823-7
Lichter, P; Tang, C J; Call, K et al. (1990) High-resolution mapping of human chromosome 11 by in situ hybridization with cosmid clones. Science 247:64-9
Glaser, T; Housman, D; Lewis, W H et al. (1989) A fine-structure deletion map of human chromosome 11p: analysis of J1 series hybrids. Somat Cell Mol Genet 15:477-501

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