Expression and regulation of oestrogen receptors in the human corpus luteum

Driesche, Sander van den; Smith, Victoria M.; Myers, Michelle; Duncan, W. Colin

doi:10.1530/rep-07-0427

Cited by 28 publications

(13 citation statements)

References 51 publications

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“…360 In luteinized human granulosa cells, Chiang et al found ERα levels to remain relatively constant over a period of 10 days in culture but always much lower than ERα mRNA levels. 398 Recent reports in human ovarian samples collected during elective hysterectomy demonstrate that ERα is expressed in granulosa cells of antral follicles, with weak to no positive immunohistochemical staining in luteinized granulosa cells 399 supporting previous data.…”

Section: Primatessupporting

confidence: 76%

“…This study also used in vitro luteinized granulosa cells, treated with hCG or E2. Treatment of the luteinized granulosa cells with hCG reduced expression of ERα, ERβ1, and ERβ2 by approximately 50%, while treatment with E2 reduced expression of ERα and ERβ1 with no significant change in ERβ2, 399 suggesting that human granulosa cells may respond to LH by reducing ERβ in a manner similar to that found in rodent ovaries.…”

Section: Primatesmentioning

confidence: 69%

See 1 more Smart Citation

Steroid Receptors in the Uterus and Ovary

Binder

Winuthayanon

Hewitt

et al. 2015

Knobil and Neill's Physiology of Reproduction

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Section: Primatessupporting

confidence: 76%

Section: Primatesmentioning

confidence: 69%

Steroid Receptors in the Uterus and Ovary

Binder

Winuthayanon

Hewitt

et al. 2015

Knobil and Neill's Physiology of Reproduction

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“…Nevertheless, the localization of both androgen receptors (AR) and Es receptors (ER) within the human CL (3,4) suggests a paracrine/autocrine role for these steroids in regulating luteal function (2).…”

mentioning

confidence: 99%

Estrogens and androgens affect human luteal cell function

Tropea

Lanzone

Tiberi³

et al. 2010

Fertility and Sterility

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“…ERα, ERβ, and the plasma membrane estrogen receptor GPR30 have been reported in luteal tissues of rodents, domestic animals, monkeys, and women, with most studies suggesting that ERβ predominates (Duffy et al 2000, Hosokawa et al 2001, Diaz & Wiltbank 2004, Shibaya et al 2007, Wang et al 2007, van den Driesche et al 2008, Hazell et al 2009, Maranesi et al 2010). Additional studies have shown that estrogen acts directly at luteal cells to regulate functions as diverse as apoptosis, steroidogenesis, and inhibin production (Diaz & Wiltbank 2004, van den Driesche et al 2008). While expression of enzymes involved in estrogen synthesis increases as luteolysis approaches (Benyo et al 1993, Diaz & Wiltbank 2004), it is widely accepted that tissue estrogen concentrations within the corpus luteum are receptor-saturating throughout the luteal phase (Duffy et al 1999a).…”

Section: Discussionmentioning

confidence: 99%

Estrogen promotes luteolysis by redistributing prostaglandin F2α receptors within primate luteal cells

Kim¹,

Markosyan²,

Pepe³

et al. 2015

Reproduction

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Prostaglandin F2α (PGF2α) has been proposed as a functional luteolysin in primates. However, administration of PGF2α or prostaglandin synthesis inhibitors in vivo both initiate luteolysis. These contradictory findings may reflect changes in PGF2α receptors (PTGFR) or responsiveness to PGF2α at a critical point during the life span of the corpus luteum. The current study addressed this question using ovarian cells and tissues from female cynomolgus monkeys and luteinizing granulosa cells from healthy women undergoing follicle aspiration. PTGFRs were present in the cytoplasm of monkey granulosa cells, while PTGFRs were localized to the perinuclear region of large, granulosa-derived monkey luteal cells by mid-late luteal phase. A PTGFR agonist decreased progesterone production by luteal cells obtained at mid-late and late luteal phases but did not decrease progesterone production by granulosa or luteal cells from younger corpora lutea. These findings are consistent with a role for perinuclear PTGFRs in functional luteolysis. This concept was explored using human luteinizing granulosa cells maintained in vitro as a model for luteal cell differentiation. In these cells, PTGFRs relocated from the cytoplasm to the perinuclear area in an estrogen- and estrogen receptor-dependent manner. Similar to our findings with monkey luteal cells, human luteinizing granulosa cells with perinuclear PTGFRs responded to a PTGFR agonist with decreased progesterone production. These data support the concept that PTGFR stimulation promotes functional luteolysis only when PTGFRs are located in the perinuclear region. Estrogen receptor-mediated relocation of PTGFRs within luteal cells may be a necessary step in the initiation of luteolysis in primates.

show abstract

Expression and regulation of oestrogen receptors in the human corpus luteum

Cited by 28 publications

References 51 publications

Steroid Receptors in the Uterus and Ovary

Steroid Receptors in the Uterus and Ovary

Estrogens and androgens affect human luteal cell function

Estrogen promotes luteolysis by redistributing prostaglandin F2α receptors within primate luteal cells

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