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促黄体生成素(LH)刺激单个卵巢(颗粒)细胞内的钙离子([Ca2+]i)动员和跨膜阳离子内流:作为LH-[Ca2+]i剂量反应细胞机制的募集

Luteinizing hormone (LH) stimulates both intracellular calcium ion ([Ca2+]i) mobilization and transmembrane cation influx in single ovarian (granulosa) cells: recruitment as a cellular mechanism of LH-[Ca2+]i dose response.

作者信息

Flores J A, Aguirre C, Sharma O P, Veldhuis J D

机构信息

Department of Internal Medicine, University of Virginia Health Sciences Center, and National Science Foundation Center for Biology Timing, Charlottesville 22908, USA.

出版信息

Endocrinology. 1998 Aug;139(8):3606-12. doi: 10.1210/endo.139.8.6162.

DOI:10.1210/endo.139.8.6162
PMID:9681514
Abstract

The gonadotropic hormones, LH and FSH, activate adenylyl cyclase in their respective target cells and thereby initiate many biochemical responses. In addition to stimulating cAMP production, both LH and FSH promote agonist-specific increases in the cytoplasmic concentration of free calcium ions ([Ca2+]i) in gonadal cells. Here, we have applied single cell fluorescence video microscopy with the Ca2+-sensitive dye fura-2 to investigate the mechanism(s) by which LH induces a rise in the [Ca2+]i in individual (swine) granulosa cells collected from single Graafian follicles. Stimulation with LH induced a rapid onset, biphasic, spike- and plateau-like [Ca2+]i signal in responsive granulosa cells. The cellular mechanisms mediating this biphasic LH-stimulated increase in [Ca2+]i were examined by external Ca2+ removal and via the manganese (Mn2+) quench technique, which showed that LH triggers initial intracellular Ca2+ mobilization followed by delayed transmembrane Ca2+ influx. Single cell Ca2+ assessment of the LH dose-response mechanism(s) revealed that higher concentrations of LH progressively recruit a larger number of responding individual granulosa cells. Further analyses disclosed a marked [Ca2+]i response heterogeneity among individual granulosa cells harvested from the same Graafian follicle. In addition, the percentage of cells responding to LH [but not to an alternative putative agonist of the phospholipase C (PLC) pathway, viz. endothelin-1] with a biphasic [Ca2+]i rise increased with maturational development of the follicle. Pretreatment of granulosa cells with a specific PLC inhibitor, U-73122 (but not with its inactive congener U-73343), significantly reduced the percentage of cells responding to a LH challenge from 78% to 25% (P < 0.0001) and prolonged the time required to achieve a half-maximal value of the [Ca2+]i transient, viz. from 22 +/- 1.5 sec (n = 27 cells) to 39 +/- 7.2 sec (n = 12 cells; P = 0.002). In cell population studies, LH stimulated in a concentration- and time-dependent manner the accumulation of inositol phosphate in porcine granulosa cells. In summary, the present single cell investigations in mature granulosa cells demonstrate that LH drives initial intracellular Ca2+ mobilization followed by transmembrane divalent cation influx. The PLC inhibitor U-73122 antagonizes this action of LH. By analyzing [Ca2+]i responses in individual living granulosa cells, we further show that, despite within-follicle diversity, the LH dose biphasic [Ca2+]i response arises via the recruitment of a larger number of responding gonadal cells rather than by increased [Ca2+]i signal amplitude. Finally, the percentage of individual LH (but not endothelin-1)-responding granulosa cells increases with follicular maturation. Collectively, these data highlight the potential importance of the LH-stimulatable, PLC-transduced [Ca2+]i signaling mechanism in the later stages of granulosa cell differentiation.

摘要

促性腺激素LH和FSH可激活各自靶细胞中的腺苷酸环化酶,从而引发许多生化反应。除了刺激cAMP生成外,LH和FSH均能促进性腺细胞中游离钙离子([Ca2+]i)胞质浓度的激动剂特异性增加。在此,我们应用对Ca2+敏感的染料fura-2进行单细胞荧光视频显微镜观察,以研究LH诱导从单个格拉夫卵泡采集的单个(猪)颗粒细胞中[Ca2+]i升高的机制。用LH刺激可在反应性颗粒细胞中诱导快速起始、双相、峰状和平台状的[Ca2+]i信号。通过去除细胞外Ca2+并采用锰(Mn2+)淬灭技术研究介导这种双相LH刺激的[Ca2+]i增加的细胞机制,结果表明LH触发最初的细胞内Ca2+动员,随后是延迟的跨膜Ca2+内流。对LH剂量反应机制的单细胞Ca2+评估显示,较高浓度的LH逐渐募集更多有反应的单个颗粒细胞。进一步分析发现,从同一个格拉夫卵泡采集的单个颗粒细胞之间存在明显的[Ca2+]i反应异质性。此外,随着卵泡的成熟发育,对LH(而非磷脂酶C(PLC)途径的另一种假定激动剂内皮素-1)产生双相[Ca2+]i升高反应的细胞百分比增加。用特异性PLC抑制剂U-73122(而非其无活性类似物U-73343)预处理颗粒细胞,可使对LH刺激有反应的细胞百分比从78%显著降低至25%(P<0.0001),并延长达到[Ca2+]i瞬变半最大值所需的时间,即从22±1.5秒(n = 27个细胞)延长至39±7.2秒(n = 12个细胞;P = 0.002)。在细胞群体研究中,LH以浓度和时间依赖性方式刺激猪颗粒细胞中肌醇磷酸的积累。总之,目前对成熟颗粒细胞的单细胞研究表明,LH驱动最初的细胞内Ca2+动员,随后是跨膜二价阳离子内流。PLC抑制剂U-73122拮抗LH的这一作用。通过分析单个活颗粒细胞中的[Ca2+]i反应,我们进一步表明,尽管卵泡内存在差异,但LH剂量双相[Ca2+]i反应是通过募集更多有反应的性腺细胞而非通过增加[Ca2+]i信号幅度产生的。最后,对LH(而非内皮素-1)有反应的单个颗粒细胞百分比随卵泡成熟而增加。这些数据共同突出了LH可刺激的、PLC转导的[Ca2+]i信号传导机制在颗粒细胞分化后期的潜在重要性。

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