Awardee OrganizationMASSACHUSETTS GENERAL HOSPITAL
Description
Abstract Text
Specifically, the long-term objective of the proposed research is
to identify and characterize genes that are important in the
pathogenesis of human parathyroid neoplasms (both adenomas and
carcinomas). Although the majority of these genes have yet to be
identified, genetic rearrangement and overexpression of a cell
cycle regulator (PRAD1 or human cyclin D1) has been implicated in
the pathogenesis of about 5% of parathyroid tumors. The underlying
hypothesis for the proposed studies, then, is that abnormalities in
other cell cycle regulators (p53, retinoblastoma (Rb) and cyclins
other than PRAD1) and/or additional candidate oncogenes (some
perhaps by their overexpression) are likely to be important in the
pathogenesis of these tumors. To begin to test this hypothesis,
human parathyroid adenomas will be examined for: (i) abnormalities
in the p53 and Rb genes using "loss of heterozygosity" (LOH)
studies and subsequent characterization of the remaining, non-
deleted allele in tumors showing LOH; and (il) tumor-specific
overexpression (or unique expression) of cDNAs isolated by
subtractive hybridization, one or more of which may encode a
putative oncogene or a gene functionally linked to an oncogene.
These studies should provide important insights into the molecular
mechanisms of tumorigenesis in these neoplasms, and could
potentially have broader clinical and biological ramifications as
has been the case for PRAD1).
No Sub Projects information available for 5K08CA001752-02
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