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口服卵泡刺激素受体激动剂对颗粒细胞的影响不同于重组人卵泡刺激素。

Oral follicle-stimulating hormone receptor agonist affects granulosa cells differently than recombinant human FSH.

机构信息

Center for Drug Discovery, Baylor College of Medicine, Houston, Texas; Division of Reproductive Endocrinology and Infertility, Department of Obstetrics and Gynecology, University of Southern California, Los Angeles, California.

Center for Drug Discovery, Baylor College of Medicine, Houston, Texas; Department of Pathology and Immunology, Baylor College of Medicine, One Baylor Plaza, Houston, Texas.

出版信息

Fertil Steril. 2023 Nov;120(5):1061-1070. doi: 10.1016/j.fertnstert.2023.07.024. Epub 2023 Jul 31.

Abstract

OBJECTIVE

To determine whether TOP5300, a novel oral follicle-stimulating hormone (FSH) receptor (FSHR) allosteric agonist, elicits a different cellular response than recombinant human FSH (rh-FSH) in human granulosa cells from patients undergoing in vitro fertilization.

DESIGN

Basic science research with a preclinical allosteric FSHR agonist.

SETTING

University hospital.

PATIENT(S): Patients with infertility at a single academic fertility clinic were recruited under an Institutional Review Board-approved protocol. Primary granulosa cell cultures were established for 41 patients, of whom 8 had normal ovarian reserve (NOR), 17 were of advanced reproductive age (ARA), 12 had a diagnosis of polycystic ovary syndrome (PCOS), and 4 had a combination of diagnoses, such as ARA and PCOS.

INTERVENTION(S): Primary granulosa-lutein (GL) cell cultures were treated with rh-FSH, TOP5300, or vehicle.

MAIN OUTCOME MEASURE(S): Estradiol (E) production using enzyme-linked immunosorbent assay, steroid pathway gene expression of StAR and aromatase using quantitative polymerase chain reaction, and FSHR membrane localization using immunofluorescence were measured in human GL cells.

RESULT(S): TOP5300 consistently stimulated E production among patients with NOR, ARA, and PCOS. Recombinant FSH was the more potent ligand in GL cells from patients with NOR but was ineffective in cells from patients with ARA or PCOS. The lowest level of FSHR plasma membrane localization was seen in patients with ARA, although FSHR localization was more abundant in cells from patients with PCOS; the highest levels were present in cells from patients with NOR. The localization of FSHR was not affected by TOP5300 relative to rh-FSH in any patient group. TOP5300 stimulated greater expression of StAR and CYP19A1 across cells from all patients with NOR, ARA, and PCOS combined, although rh-FSH was unable to stimulate StAR and aromatase (CYP19A1) expression in cells from patients with PCOS. TOP5300-induced expression of StAR and CYP19A1 mRNA among patients with ARA and NOR was consistently lower than that observed in cells from patients with PCOS.

CONCLUSION(S): TOP5300 appears to stimulate E production and steroidogenic gene expression from GL cells more than rh-FSH in PCOS, relative to patients with ARA and NOR. It does not appear that localization of FSHR at cell membranes is a limiting step for TOP5300 or rh-FSH stimulation of steroidogenic gene expression and E production.

摘要

目的

确定新型口服卵泡刺激素(FSH)受体(FSHR)变构激动剂 TOP5300 是否在接受体外受精的患者的人颗粒细胞中引起与重组人 FSH(rh-FSH)不同的细胞反应。

设计

基础科学研究与临床前变构 FSHR 激动剂。

地点

大学医院。

患者

根据机构审查委员会批准的方案,在一家学术生育诊所招募患有不育症的患者。为 41 名患者建立了原发性颗粒细胞培养物,其中 8 名患者具有正常卵巢储备(NOR),17 名患者处于高龄生育期(ARA),12 名患者患有多囊卵巢综合征(PCOS),4 名患者同时患有 ARA 和 PCOS 等多种诊断。

干预措施

用 rh-FSH、TOP5300 或载体处理原发性颗粒-黄体(GL)细胞培养物。

主要观察指标

采用酶联免疫吸附试验检测雌二醇(E)的产生,采用定量聚合酶链反应检测 StAR 和芳香化酶的类固醇途径基因表达,采用免疫荧光法检测人 GL 细胞中的 FSHR 膜定位。

结果

TOP5300 始终刺激 NOR、ARA 和 PCOS 患者的 E 产生。重组 FSH 是 NOR 患者 GL 细胞中更有效的配体,但对 ARA 或 PCOS 患者的细胞无效。ARA 患者的 FSHR 质膜定位最低,尽管 PCOS 患者的细胞中 FSHR 定位更丰富;最高水平存在于 NOR 患者的细胞中。与 rh-FSH 相比,TOP5300 在任何患者组中均未影响 FSHR 的定位。TOP5300 刺激 NOR、ARA 和 PCOS 所有患者的 GL 细胞中 StAR 和 CYP19A1 的表达增加,尽管 rh-FSH 不能刺激 PCOS 患者的 StAR 和芳香化酶(CYP19A1)表达。TOP5300 诱导的 ARA 和 NOR 患者的 StAR 和 CYP19A1 mRNA 表达始终低于 PCOS 患者的细胞。

结论

与 ARA 和 NOR 患者相比,TOP5300 似乎在 PCOS 患者的 GL 细胞中比 rh-FSH 更能刺激 E 产生和类固醇生成基因表达。FSHR 在细胞膜上的定位似乎不是 TOP5300 或 rh-FSH 刺激类固醇生成基因表达和 E 产生的限制步骤。

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