Abstract

Fertilization involves a series of signal transduction events that serve to activate the block to polyspermy, induce resumption of the cell cycle, incorporate the paternal genome, and activate egg metabolism. Key steps in this process include the actin cytoskeleton modifications that physically incorporate the sperm nucleus into the egg and subsequently reorganize the egg cortex. Recent findings by this laboratory revealed that the cytoskeleton-associated PYK2 kinase is rapidly activated during fertilization and functional studies indicate a role for PYK2 in sperm incorporation and egg activation. The objective of the proposed study is to test the hypothesis that PYK2 kinase participates in the signaling events triggered by sperm-egg adhesion or fusion that are critical for sperm incorporation and modification of the egg cytoskeleton. The project will make use of the economical zebrafish fertilization system which provides unique advantages for identification of signaling events at the point of sperm-egg contact as well as for proteomic analysis of substrates of the PYK2 kinase. The first specific aim will identify the specific function(s) of PYK2 kinase in egg activation.
The second aim will identify the signals which activate PYK2 at fertilization.
The third aim will identify the protein targets phosphorylated by PYK2 in order to work out the downstream pathways that it controls. The results of this study will provide important details regarding control of the egg cytoskeleton at fertilization and possibly help resolve the question of signaling pathways activated by sperm-egg recognition and fusion. These findings will have significant application to the development of techniques for assisted reproductive technologies to enhance human fertility. Lay Summary: This study will work out the mechanism by which the sperm activates the egg during fertilization. The specific role of PYK2 kinase in bringing the sperm nucleus into the egg will be analyzed with the ultimate aim of enhancing the success of human in vitro fertilization.

Public Health Relevance

Assisted reproductive technologies such as in vitro oocyte maturation, in vitro fertilization and intracytoplasmic sperm injection have remained fairly inefficient processes. The proposed experiments will provide basic knowledge regarding the signal transduction process initiated by sperm-egg contact which could be used to improve these clinical methods.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
5R01HD062860-03
Application #
8280385
Study Section
Cellular, Molecular and Integrative Reproduction Study Section (CMIR)
Program Officer
Moss, Stuart B
Project Start
2010-08-13
Project End
2015-05-31
Budget Start
2012-06-01
Budget End
2013-05-31
Support Year
3
Fiscal Year
2012
Total Cost
$259,200
Indirect Cost
$86,400

  Institution

Name
University of Kansas
Department
Anatomy/Cell Biology
Type
Schools of Medicine
DUNS #
016060860
City
Kansas City
State
KS
Country
United States
Zip Code
66160

  Publications

Wang, Huizhen; Luo, Jinping; Carlton, Carol et al. (2017) Sperm-oocyte contact induces outside-in signaling via PYK2 activation. Dev Biol 428:52-62
Czirok, Andras; Isai, Dona Greta; Kosa, Edina et al. (2017) Optical-flow based non-invasive analysis of cardiomyocyte contractility. Sci Rep 7:10404
McGinnis, Lynda K; Kinsey, William H (2015) Role of focal adhesion kinase in oocyte-follicle communication. Mol Reprod Dev 82:90-102
Kinsey, William H (2014) SRC-family tyrosine kinases in oogenesis, oocyte maturation and fertilization: an evolutionary perspective. Adv Exp Med Biol 759:33-56
Luo, Jinping; McGinnis, Lynda K; Carlton, Carol et al. (2014) PTK2b function during fertilization of the mouse oocyte. Biochem Biophys Res Commun 450:1212-7
McGinnis, Lynda K; Pelech, Steven; Kinsey, William H (2014) Post-ovulatory aging of oocytes disrupts kinase signaling pathways and lysosome biogenesis. Mol Reprod Dev 81:928-45
McGinnis, Lynda K; Luo, Jinping; Kinsey, William H (2013) Protein tyrosine kinase signaling in the mouse oocyte cortex during sperm-egg interactions and anaphase resumption. Mol Reprod Dev 80:260-72
Kinsey, William H (2013) Intersecting roles of protein tyrosine kinase and calcium signaling during fertilization. Cell Calcium 53:32-40
Sharma, Dipika; Kinsey, William H (2013) PYK2: a calcium-sensitive protein tyrosine kinase activated in response to fertilization of the zebrafish oocyte. Dev Biol 373:130-40
McGinnis, Lynda K; Carroll, David J; Kinsey, William H (2011) Protein tyrosine kinase signaling during oocyte maturation and fertilization. Mol Reprod Dev 78:831-45