The long term objective of this project is to understand the creation and maintenance of sperm surface topography and the molecular basis of fertilization. Previous evidence indicates that the PH-20 surface protein functions is sperm-zona binding.
Aim I asks how the PH-20 membrane protein is targeted to two different membranes during spermiogenesis. Experiments using techniques of gene cloning and sequencing will test the hypothesis that either two genes or two mRNAs encoded two forms of the PH-20 protein that are differentially targeted.
In Aim II the change in localization of PH-20 during epididymal passage will be studied, using techniques of fluorescence intensity measurements and fluorescence redistribution after photobleaching (FRAP). Another alteration that occurs during epididymal passage is the appearance of the integral membrane protein, PH-30 which our evidence indicates has a role in sperm-egg plasma membrane fusion. The mechanism of its appearance will be investigated. Because of the previous finding that two membrane proteins, PT-1 and PH-20, are freely diffusing on the sperm surface, it will be tested if these proteins are anchored in the membrane by covalent attachment to a lipid, phosphatidyl inositol (PI). During the last grant period, it was discovered that acrosome-intact and acrosome-reacted guinea pig sperm can both initiate sperm-zona binding. We will identify sperm and zona components involved in the binding of each type of sperm. In addition, sperm interactions with the egg plasma membrane will be analyzed. These studies on sperm surface topography and sperm-egg interactions are designed to advance the knowledge of sperm surface organization and regulation of sperm function during fertilization. Understanding of these phenomena are important in both the areas of infertility and contraception.

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
5R01HD016580-11
Application #
3313765
Study Section
Reproductive Biology Study Section (REB)
Project Start
1981-09-01
Project End
1992-12-31
Budget Start
1992-01-01
Budget End
1992-12-31
Support Year
11
Fiscal Year
1992
Total Cost
Indirect Cost
Name
University of Connecticut
Department
Type
Schools of Dentistry
DUNS #
City
Farmington
State
CT
Country
United States
Zip Code
06030
Nishimura, Hitoshi; Gupta, Surabhi; Myles, Diana G et al. (2011) Characterization of mouse sperm TMEM190, a small transmembrane protein with the trefoil domain: evidence for co-localization with IZUMO1 and complex formation with other sperm proteins. Reproduction 141:437-51
He, Zhi-Yong; Gupta, Surabhi; Myles, Diana et al. (2009) Loss of surface EWI-2 on CD9 null oocytes. Mol Reprod Dev 76:629-36
Zhu, Guo-Zhang; Gupta, Surabhi; Myles, Diana Gold et al. (2009) Testase 1 (ADAM 24) a sperm surface metalloprotease is required for normal fertility in mice. Mol Reprod Dev 76:1106-14
Gupta, Surabhi; Primakoff, Paul; Myles, Diana G (2009) Can the presence of wild-type oocytes during insemination rescue the fusion defect of CD9 null oocytes? Mol Reprod Dev 76:602
Nishimura, Hitoshi; Myles, Diana G; Primakoff, Paul (2007) Identification of an ADAM2-ADAM3 complex on the surface of mouse testicular germ cells and cauda epididymal sperm. J Biol Chem 282:17900-7
Runge, Kathryn E; Evans, James E; He, Zhi-Yong et al. (2007) Oocyte CD9 is enriched on the microvillar membrane and required for normal microvillar shape and distribution. Dev Biol 304:317-25
Primakoff, Paul; Myles, Diana G (2007) Cell-cell membrane fusion during mammalian fertilization. FEBS Lett 581:2174-80
Stein, Kathryn K; Go, Jowell C; Lane, William S et al. (2006) Proteomic analysis of sperm regions that mediate sperm-egg interactions. Proteomics 6:3533-43
Ellerman, Diego A; Myles, Diana G; Primakoff, Paul (2006) A role for sperm surface protein disulfide isomerase activity in gamete fusion: evidence for the participation of ERp57. Dev Cell 10:831-7
Stein, Kathryn K; Go, Jowell C; Primakoff, Paul et al. (2005) Defects in secretory pathway trafficking during sperm development in Adam2 knockout mice. Biol Reprod 73:1032-8

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