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Submitted on April 17, 2003
Accepted on July 7, 2003
stimulated gene 6 blocks cumulus cell-oocyte complex expansion
1 Department of Molecular and Cellular Biology, Baylor College of Medicine, Houston, Texas 77030 (S.A.O., J.S.R.); MRC Immunochemistry Unit, Department of Biochemistry, University of Oxford, OX13QU Oxford, United Kingdom (A.J.D., M.S.R.); Departments of Medicine (Division of Nephrology) and Pharmacology, Vanderbilt University School of Medicine, S3223 MCN, 1161 21Avenue South, Nashville, Tennessee 37232-2372 (R.M.B.); and Howard Hughes Medical Institute and Department of Biochemistry and Cell Biology MS-140, Rice University, 6100 South Main Street, Houston, Texas 77005-1892 (R.H.G.)
* To whom correspondence should be addressed. E-mail: joanner{at}bcm.tmc.edu.
During ovulation the oocyte and surrounding somatic cumulus cells contained within a specialized, mucoid matrix are released from the ovary. One matrix component, TNF-
stimulated gene 6 (TSG-6), is a hyaluronan binding protein induced in cumulus cells of preovulatory follicles by the LH surge and is decreased in cumulus cells of COX-2 and EP2 null mice which exhibit impaired ovulation and cumulus expansion. To determine if TSG-6 was hormonally induced in cumulus cells in vitro and was functional during the formation of the expanded matrix, we established a cumulus cell-oocyte complex (COC) culture system. This system was used to analyze the effects of FSH, PGE2, EP2 receptor, and selected protein kinase inhibitors on TSG-6 production as well as specific antibodies to the TSG-6 link module on TSG-6 function. We document that TSG-6 message and protein are induced by cAMP/PKA/MAPK signaling pathways and that blocking these cascades prevents expansion and the production of TSG-6. FSH but not PGE2 rescued expansion and production of TSG-6 in the EP2 null COCs, indicating that generation of a cAMP signal is essential. Furthermore, disruption of the functional interactions between TSG-6, I
I, and hyaluronan with specific antibodies severely altered matrix formation and cumulus expansion, as recoded by time-lapse imaging. Collectively, these results indicate that TSG-6 mRNA is induced in cumulus cells in culture by cAMP and that the secreted TSG-6 protein is a key structural component of the mouse COC matrix.
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