MECHANISMS & MOLECULAR GENETICS OF HYPERHOMOCYSTEINEMIA
Project Number1R01HL058984-01
Contact PI/Project LeaderBANERJEE, RUMA V
Awardee OrganizationUNIVERSITY OF NEBRASKA LINCOLN
Description
Abstract Text
DESCRIPTION
(Adapted from applicant's abstract) Hyperhomocysteinemia is graded risk
factor for atherosclerotic cardiovascular diseases, a leading cause of
mortality in the United States. Two housekeeping enzymes that directly
"manage" cellular homocysteine are methionine synthase (MS) and
cystathionine Beta-synthase (CBS). The human genes encoding both proteins
have been cloned, and mutations in these genes leading to severe
hyperhomocysteinemia have been described. Polymorphisms in these genes
independently, or in concert with the environment (viz. Nutritional
status), may contribute to mild hyperhomocysteinemia. The proposed goals
are (1) to test the hypothesis that one or more common polymorphisms in the
MS gene correlates with "risk" for cardiovascular diseases. (2) To develop
rapid genetic and biochemical screens for detecting MS mutations in patients
(3) To characterize the cellular and organismal consequences of severe MS
deficiency using a cell culture model and MS knockout mice. (4) To
characterize the catalytic penalties attendant with individual mutations in
CBS isolated from homocystinuric patients and MS polymorphisms that have
been discovered so far. (End of Abstract)
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