Endocrine and local control of the primate corpus luteum

Stouffer, Richard L.; Bishop, Cecily V.; Bogan, Randy L.; Xu, Fan; Hennebold, Jon D.

doi:10.1016/j.repbio.2013.08.002

Cited by 69 publications

(55 citation statements)

References 108 publications

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“…The main function of luteal cells is the synthesis of steroid hormones. Stouffer et al (). We find that progesterone secretion is significantly increased by POP overexpression.…”

Section: Resultsmentioning

confidence: 99%

Prolyl oligopeptidase regulates progesterone secretion via the ERK signaling pathway in murine luteal cells

Bao

Zhang

et al. 2019

Molecular Reproduction Devel

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Prolyl oligopeptidase (POP), one of the most widely distributed serine endopeptidases, is highly expressed in the ovaries. However, the physiological role of POP in the ovaries is not clear. In this study, we investigated the significance of POP in the corpus luteum. Murine luteal cells were cultured in vitro and treated with a POP selective inhibitor, (2S)‐1[[(2 S)‐1‐(1‐oxo‐4‐phenylbutyl)‐2‐pyrrolidinyl carbonyl]‐2‐pyrrolidinecarbonitrile (KYP‐2047). We found that KYP‐2047 treatment decreased progesterone secretion. In contrast, POP overexpression increased progesterone secretion. Three essential steroidogenic enzymes, including p450 cholesterol side‐chain cleavage enzyme (CYP11A), 3β‐hydroxysteroid dehydrogenase (3β‐HSD), and the steroidogenic acute regulatory protein (StAR), were regulated by POP. Further studies showed that POP overexpression increased ERK1/2 phosphorylation and increased the expression of steroidogenic factor 1 (SF1), while KYP‐2047 treatment decreased ERK1/2 phosphorylation and SF1 expression. To clarify the role of ERK1/2 signaling in POP‐regulated progesterone synthesis, U0126‐EtOH, an inhibitor of the ERK signaling pathway, was used to treat luteal cells. We found that U0126‐EtOH decreased progesterone production and the expression of steroidogenic enzymes and SF1. POP overexpression did not reverse the effects of U0126‐EtOH. Overall, POP regulates progesterone secretion by stimulating the expression of CYP11A, 3β‐HSD, and StAR in luteal cells. ERK signaling and downstream SF1 expression contribute to this process.

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“…The main function of luteal cells is the synthesis of steroid hormones. Stouffer et al (). We find that progesterone secretion is significantly increased by POP overexpression.…”

Section: Resultsmentioning

confidence: 99%

Prolyl oligopeptidase regulates progesterone secretion via the ERK signaling pathway in murine luteal cells

Bao

Zhang

et al. 2019

Molecular Reproduction Devel

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“…The main function of the corpus luteum is to synthesize and secrete progesterone, which is indispensable for maintenance of pregnancy and regulation of the estrous cycle (Stouffer 2003; Devoto et al, 2009). The luteal phase can be divided into three main stages, namely development, maintenance, and regression, according to the macroscopic appearance of corpus luteum tissues (Stouffer et al, 2013). The pathway for progesterone synthesis mainly involves three steroidogenic enzymes, namely steroidogenic acute regulatory protein (known as StAR), p450 cholesterol side-chain cleavage enzyme (p450), and 3β-hydroxysteroid dehydrogenase, and two cellular organelles (mitochondria and ER) (Niswender 2002; Rekawiecki et al, 2008).…”

Section: Activation Of the Upr In The Ovarian Cyclementioning

confidence: 99%

Dual role for the unfolded protein response in the ovary: adaption and apoptosis

Qiao

2016

Protein &Amp; Cell

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The endoplasmic reticulum (ER) is the principal organelle responsible for several specific cellular functions including synthesis and folding of secretory or membrane proteins, lipid metabolism, and Ca2+ storage. Different physiological as well as pathological stress conditions can, however, perturb ER homeostasis, giving rise to an accumulation of unfolded or misfolded proteins in the ER lumen, a condition termed ER stress. To deal with an increased folding demand, cells activate the unfolded protein response (UPR), which is initially protective but can become detrimental if ER stress is severe and prolonged. Accumulating evidence demonstrates a link between the UPR and ovarian development and function, including follicular growth and maturation, follicular atresia, and corpus luteum biogenesis. Additionally, ER stress and the UPR may also play an important role in the ovary under pathological conditions. Understanding the molecular mechanisms related to the dual role of unfolded protein response in the ovarian physiology and pathology may reveal the pathogenesis of some reproductive endocrine diseases and provide a new guidance to improve the assisted reproductive technology. Here we review the current literature and discuss concepts and progress in understanding the UPR, and we also analyze the role of ER stress and the UPR in the ovary.

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“…Specifically, inhibiting P4 synthesis results in structural changes similar to those associated with luteal regression (See review by (Stouffer, et al 2013). These changes are prevented by supplemental P4 treatment (Stouffer, et al 2013). However, the effect of RU486 treatment is variable; at times increasing while at other times decreasing P4 secretion.…”

Section: Introduction and Historical Perspectivementioning

confidence: 99%

Non-canonical progesterone signaling in granulosa cell function

Peluso¹,

Pru²

2014

Reproduction

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It has been known for over three decades that progesterone (P4) suppresses follicle growth. It has been assumed that P4 acts directly on granulosa cells of developing follicles to slow their development, since P4 inhibits both mitosis and apoptosis of cultured granulosa cells. However, granulosa cells of developing follicles of mice, rats, monkeys and humans do not express the A or B form of the classic nuclear receptor for progesterone (PGR). In contrast, these granulosa cells express other progesterone binding proteins, one of which is referred to as Progesterone Receptor Membrane Component 1 (PGRMC1). PGRMC1 specifically binds P4 with high affinity and mediates P4’s anti-mitotic and anti-apoptotic action as evidenced by the lack of these P4-dependent effects in PGRMC1-depleted cells. In addition, mice in which PGRMC1 is conditionally depleted in granulosa cells show diminished follicle development. While the mechanism through which P4 activation of PGRMC1 affects granulosa cell function is not well defined, it appears that PGRMC1 controls granulosa cell function in part by regulating gene expression in T cell specific transcription factor/lymphoid enhancer factor (Tcf/Lef)-dependent manner. Clinically, altered PGRMC1 expression has been correlated with premature ovarian failure/insufficiency, polycystic ovarian syndrome and infertility. These collective studies provide strong evidence that PGRMC1 functions as a receptor for P4 in granulosa cells and that altered expression results in compromised reproductive capacity. Ongoing studies seek to define the components of the signal transduction cascade through which P4-activation of PGRMC1 results in the regulation of granulosa cell function.

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Endocrine and local control of the primate corpus luteum

Cited by 69 publications

References 108 publications

Prolyl oligopeptidase regulates progesterone secretion via the ERK signaling pathway in murine luteal cells

Prolyl oligopeptidase regulates progesterone secretion via the ERK signaling pathway in murine luteal cells

Dual role for the unfolded protein response in the ovary: adaption and apoptosis

Non-canonical progesterone signaling in granulosa cell function

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