Awardee OrganizationUNIVERSITY OF CALIFORNIA, SAN DIEGO
Description
Abstract Text
DESCRIPTION (provided by applicant): Bone Morphogenetic Protein-15 (BMP-15), a
member of the TGF-beta superfamily, is an oocyte-specific growth factor. Recent
studies of a naturally occurring mutation in sheep [Inverdale (FecX')] have
suggested an essential role for BMP-15 in folliculogenesis and fertility. In
the homozygous FecX' female, follicular development arrests at the primary
stage, resulting in infertility. In contrast, the heterozygous FecX1 females
exhibit increases in ovulation rate and in twin and triplet births. It has now
been shown that a substitution of valine by aspartic acid at residue 31 (V31D)
of the BMP-15 gene is present in FecX' carriers. Therefore, BMP-15 mutation
appears to be associated with infertility and super fertility in a
dosage-sensitive manner. Our laboratory has recently produced recombinant
BMP-15 and identified granulosa cells (GCs) as target cells for this factor.
Using the recombinant protein, we have found that BMP-15 (i) stimulates rat GC
proliferation, (ii) inhibits FSH receptor expression, and (iii) stimulates kit
ligand expression in the GCs. These findings establish the new concept that
oocyte-derived BMP-15 is functionally involved in regulating three major
aspects of follicle development, namely GC proliferation, GC
cytodifferentiation, and oogenesis. Here, we propose to elucidate the molecular
basis of BMP-15 action from the receptors to the target genes by characterizing
BMP-15 receptor and signaling molecules (Aim 1) and the molecular mechanisms by
which BMP-15 regulates FSH receptor and kit ligand gene expression (Aim 2). We
have also found that, despite lacking the inter-subunit disulfide bonds seen in
most of the dimeric TGF-beta superfamily members, BMP-15 and the closely
related GDF-9 are homodimers. Furthermore, we have obtained evidence that
BMP-15 and GDF-9 can form heterodimers, and thus we propose to explore the
biological roles of BMP-15/GDF-9 heterodimers (Aim 3). Although the V31D
mutation in the BMP15 gene was found in Inverdale sheep, the role of
BMP-15-V31D mutation in Inverdale sheep is yet unclear. We will explore the
biological activities of the BMP-15-V31D mutation and test our hypothesis that
BMP-15-V31D could influence the biosynthesis of GDF-9 (Aim 4). Finally we will
generate the same mutation in mice and determine the in vivo effect of the
BMP-15-V31D mutation on folliculogenesis and ovulation (Aim 5). These studies
should provide significant advances in understanding regulation of the events
central to female fertility and ultimately improve approaches for birth control
and for treating gonadal abnormalities and infertility.
Eunice Kennedy Shriver National Institute of Child Health and Human Development
CFDA Code
865
DUNS Number
804355790
UEI
UYTTZT6G9DT1
Project Start Date
01-May-2002
Project End Date
31-July-2008
Budget Start Date
01-May-2006
Budget End Date
31-July-2008
Project Funding Information for 2006
Total Funding
$333,964
Direct Costs
$219,713
Indirect Costs
$114,251
Year
Funding IC
FY Total Cost by IC
2006
Eunice Kennedy Shriver National Institute of Child Health and Human Development
$333,964
Year
Funding IC
FY Total Cost by IC
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