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Activation of Cl Channels by Human Chorionic Gonadotropin in Luteinized Granulosa Cells of the Human Ovary Modulates Progesterone Biosynthesis

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2008-09
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Olivero, Pablo
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Activation of Cl Channels by Human Chorionic Gonadotropin in Luteinized Granulosa Cells of the Human Ovary Modulates Progesterone Biosynthesis
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Author
  • Olivero, Pablo;
  • Leiva Salcedo, Elías;
  • Devoto, Luigi;
  • Stutzin Schottlander, Andrés;
Abstract
Chloride permeability pathways and progesterone (P4) secretion elicited by human chorionic gonadotropin (hCG) in human granulosa cells were studied by electrophysiological techniques and single-cell volume, membrane potential and Ca2 i measurements. Reduction in extracellular Cl and equimolar substitution by the membrane-impermeant anions glutamate or gluconate significantly increased hCGstimulated P4 accumulation. A similar result was achieved by exposing the cells to hCG in the presence of a hypotonic extracellular solution. Conversely, P4 accumulation was drastically reduced in cells challenged with hCG exposed to a hypertonic solution. Furthermore, conventional Cl channel inhibitors abolished hCG-mediated P4 secretion. In contrast, 25-hydroxycholesterol-mediated P4 accumulation was unaffected by Cl channel blockers. In human granulosa cells, hCG triggered the activation of a tamoxifen-sensitive outwardly rectifying Cl current comparable to the volume-sensitive outwardly rectifying Cl current. Exposure of human granulosa cells to hCG induced a rapid 4,4 -diisothiocyanatostilbene- 2,2-disulphonic acid-sensitive cell membrane depolarization that was paralleled with an approximately 20% decrease in cell volume. Treatment with hCG evoked oscillatory and nonoscillatory intracellular Ca2 signals in human granulosa cells. Extracellular Ca2 removal and 4,4 -diisothiocyanatostilbene-2,2-disulphonic acid abolished the nonoscillatory component while leaving the Ca2 oscillations unaffected. It is concluded that human granulosa cells express functional the volume-sensitive outwardly rectifying Cl channels that are activated by hCG, which are critical for plasma membrane potential changes, Ca2 influx, and P4 production.
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This work was supported by Fondo de Areas Prioritarias Grant 15010006 (Chile).
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URI: https://repositorio.uchile.cl/handle/2250/128094
ISSN: 0013-7227
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ENDOCRINOLOGY, Volume: 149, Issue: 9, Pages: 4680-4687, 2008
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