Awardee OrganizationUNIVERSITY OF CALIFORNIA AT DAVIS
Description
Abstract Text
This proposal is focused on developing a new contraceptive method for
men. The project begins with our previous finding that immunization of
male rodents with sperm surface proteins leads to either of two effects:
anti-sperm antibody becomes bound to sperm in the epididymis or sperm are
completely eliminated from the epididymis, leading to infertility. In this
project we propose to use rodent studies to define the mechanisms of these
two phenomena and to develop optimal protocols for obtaining each effect.
These immunization protocols will then be tested in monkeys to determine
if they affect primate sperm and induce infertility. Simultaneously, a new
approach to male contraception will be tested that is designed to cause
the disruption (by immunological or pharmacological means) of cell-cell
interactions in the testis, thus blocking sperm development.
Our first aim is to systematically optimize immunization conditions
in mice by altering four variables: choice of antigen, adjuvant, dose and
route of administration. The mice will first be evaluated for antibody
bound to epididymal sperm or loss of sperm in the epididymis. The
immunized male mice will also be scored for presence of orchitis or
epididymitis which may be relatively minimal or absent with specific
choices among the four variables. The optimal protocol(s) that leads to
antibody-bound sperm in the epididymis or ejaculate will be tested for the
ability of the sperm to function in vitro fertilization and in vivo
fertility of immunized mice. An efficacious protocol will then be tested
in male monkeys. The optimal protocol that leads to loss of epididymal
sperm in mice will be used to study the mechanism of this loss and tested
to determine if epididymal sperm will be eliminated in male monkeys. If
contraceptive efficacy is obtained, but inflammation is present, we will
test peptide immunogen specifically designed to produce antibodies without
an inflammatory response. We will also study early germ cell to identify
cell adhesion molecules present outside the blood-testis barrier and
therefore subject to inhibition by antibodies or pharmacological agents,
that will not have to cross the barrier.
Eunice Kennedy Shriver National Institute of Child Health and Human Development
CFDA Code
DUNS Number
047120084
UEI
TX2DAGQPENZ5
Project Start Date
01-March-2001
Project End Date
30-June-2002
Budget Start Date
01-October-1997
Budget End Date
30-September-1998
Project Funding Information for 2001
Total Funding
$165,579
Direct Costs
$165,579
Indirect Costs
Year
Funding IC
FY Total Cost by IC
2001
Eunice Kennedy Shriver National Institute of Child Health and Human Development
$165,579
Year
Funding IC
FY Total Cost by IC
Sub Projects
No Sub Projects information available for 5U54HD029125-11 0002
Publications
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Outcomes
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Clinical Studies
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