DESCRIPTION (Adapted from the applicant's abstract): The proposal consists
of three objectives. First, Is GH required for maintenance of thymic and
bone marrow cellularity? Does GH ablation result in reduced cellularity of
thymus and bone marrow? The applicant predicts that in the absence of GH
there will be reduction in thymic size involving loss of cortical thymocytes
and accumulation of CD4- CD8- T cell progenitors. The reduction in bone
marrow cellularity will be accompanied by a reduction in multipotent myeloid
progenitors. He predicts that these changes will be reversed by GH
administration and that this will establish that GH ablation is a valid
model for immunosenescence.
Second, does GH act as a survival factor in lymphoid and myeloid progenitors
in vivo by preventing apoptosis? The applicant hypothesizes that GH
promotes survival by maintaining expression of the protooncogene bcl-2 and
that withdrawal of GH will result in induction of apoptosis in thymocytes
and myeloid progenitors associated with a decrease in BCL-2 levels.
Third, the applicant will use highly purified CD34+ cells and flow cytometry
to ask if pluripotent hematopoietic progenitors express receptors for GH and
IGF-I.
Collectively it is hypothesized that these experiments will establish the
concept that GH maintains lymphoid and myeloid tissues in vivo by promoting
the survival of lymphoid and myeloid progenitors and thus will provide new
and important insights into aging of the immune system.
National Institute of Diabetes and Digestive and Kidney Diseases
CFDA Code
847
DUNS Number
001898142
UEI
V6WTL4T5FFJ3
Project Start Date
26-September-1997
Project End Date
31-August-2000
Budget Start Date
26-September-1997
Budget End Date
31-August-2000
Project Funding Information for 1997
Total Funding
$91,941
Direct Costs
$75,000
Indirect Costs
$16,941
Year
Funding IC
FY Total Cost by IC
1997
NIH Office of the Director
$91,941
Year
Funding IC
FY Total Cost by IC
Sub Projects
No Sub Projects information available for 1R15DK052578-01
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