Soluble gp130 is Up-Regulated in the Implantation Window and Shows Altered Secretion in Patients with Primary Unexplained Infertility
J. R. A. Sherwin,
S. K. Smith,
A. Wilson and
A. M. Sharkey
The Reproductive Molecular Research Group, Department of Obstetrics and Gynecology, University of Cambridge, The Rosie Maternity Hospital, Cambridge, CB2 2SW, United Kingdom
Address all correspondence and requests for reprints to: Dr. R. Sherwin, Department of Obstetrics and Gynecology, University of Cambridge, Box 223, The Rosie Hospital, Cambridge, CB2 2SW, United Kingdom. E-mail: . jras100{at}cam.ac.uk
Abstract
Members of the IL-6 family of cytokines, which includes leukemiainhibitory factor (LIF) and IL-11, play important roles in implantation.The activity of these cytokines is modified by soluble receptorssuch as the IL-6 receptor (sIL-6R). gp130 is a signal transductionmolecule common to the receptor complexes of this family, andits soluble form (sgp130) antagonizes their actions. The purposeof this study was to determine whether secretion of IL-6, LIF,sIL-6R, and sgp130 was different in the endometrium of womenwith primary unexplained infertility compared with normal fertilewomen. Endometrial biopsies were taken between d LH+6 and +13and cultured in serum-free medium for 4 h. Secretion of IL-6,LIF, sIL-6R, and sgp130 was measured in the supernatant by ELISA.We also measured the secretion of IL-6, sIL-6R, and sgp130 byendometrial biopsies taken throughout the menstrual cycle innormal fertile women. Secretion of sgp130 increased 20-foldbetween d 20 and 26 of the cycle, coinciding with the implantationwindow (proliferative phase, median, 27.0 pg/ml·mg; range,2336; d 2026, median, 501.5 pg/ml·mg; range,26.11344; P = 0.03). RT-PCR showed that none of the knownsplice variants of gp130 were present in endometrium, indicatingthat sgp130 is produced by proteolytic cleavage of the membrane-boundform. IL-6 secretion varied considerably between patients andwas greatest during the secretory phase and at menstruation.No significant change was seen in sIL-6R during the cycle. BetweenLH+6 and +13, secretion of sgp130 was significantly reducedin the infertile group (median, 93.1 pg/ml·mg; range,28.5256; compared with the fertile group, median, 223pg/ml·mg; range, 63534; U-statistic = 37; P =0.017). Secretion of IL-6, LIF, and sIL-6R did not differ betweenthe two groups. Immunolocalization of gp130, IL-6R, and theLIF receptor showed that the glandular epithelium and also endothelialcells are targets for IL-6 and LIF. These findings show thatduring a normal menstrual cycle, sgp130 secretion is greatlyincreased between d LH+6 and +13, due to proteolytic cleavageof membrane-bound gp130. Infertile patients show reduced secretionof sgp130 compared with fertile controls during this period,which coincides with the implantation window.
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