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首页> 外文期刊>Life sciences >The expression and biological role of the non-neuronal cholinergic system in the ovary.
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The expression and biological role of the non-neuronal cholinergic system in the ovary.

机译:非神经胆碱能系统在卵巢中的表达及其生物学作用。

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Functioning of the ovary depends on an interplay between hormones, locally produced growth factors and neurotransmitters. Neurotransmitters are delivered to the ovary via its sympathetic innervation and originate from intrinsic nerve cells expressing catecholaminergic and peptidergic traits. We found that the nerve fibers and nerve cells of the ovary were however not immunoreactive for the ACh-synthesizing enzyme, choline-acetyl transferase (ChAT). Immunoreactivity was instead detected in ovarian endocrine cells, namely granulosa cells (GCs), of rodents and primates. Importantly, isolated GCs produce ACh. Thus, endocrine cells are an unexpected non-neuronal source of ACh in the ovary. GCs in vivo and in vitro also contain ACh-receptors of the muscarinic subtype (MR), namely M1 and M5. MR of human GCs are functional and linked to rapid increases in intracellular calcium levels. A role of ovarian ACh/MR in the crucial process of cell proliferation is suggested by the observation that in growing follicles, ChAT-immunoreactive GCs co-express "proliferating cell nuclear antigen" (PCNA) and that cholinergic agents stimulate cell proliferation of human GCs in vitro. This proliferative effect is associated with rapid disruption of gap junction communication and phosphorylation of connexin 43. In addition, calcium-dependent channels are activated. Ongoing studies have begun to identify down-stream effects of M1/5 activation in GCs, which include, for example, expression of a transcription factor (egr-1). In summary, ovarian endocrine cells are sources and targets of ACh. We propose that an as yet unexplored intraovarian cholinergic system exists, which contributes to physiological ovarian tissue remodeling by stimulation of cell proliferation.
机译:卵巢的功能取决于激素,局部产生的生长因子和神经递质之间的相互作用。神经递质通过其交感神经传递到卵巢,并起源于表达儿茶酚胺能和肽能特性的内在神经细胞。我们发现卵巢的神经纤维和神经细胞对ACh合成酶胆碱乙酰基转移酶(ChAT)没有免疫反应。而是在啮齿动物和灵长类动物的卵巢内分泌细胞,即颗粒细胞(GC)中检测到免疫反应性。重要的是,孤立的GC会产生ACh。因此,内分泌细胞是卵巢中ACh的意外非神经源。体内和体外的GC也含有毒蕈碱亚型(MR)的ACh受体,即M1和M5。人类GC的MR具有功能,并与细胞内钙水平的快速升高有关。观察到,在生长的卵泡中,ChAT免疫反应性GC共表达“增殖细胞核抗原”(PCNA),并且胆碱能剂刺激人GC的细胞增殖,表明了卵巢ACh / MR在细胞增殖的关键过程中的作用。体外。这种增殖作用与间隙连接通讯的迅速破坏和连接蛋白43的磷酸化有关。此外,钙依赖性通道被激活。正在进行的研究已经开始确定GC中M1 / 5激活的下游效应,例如包括转录因子(egr-1)的表达。总之,卵巢内分泌细胞是ACh的来源和靶标。我们建议存在一个尚未探索的卵巢内胆碱能系统,它通过刺激细胞增殖来促进卵巢的生理组织重塑。

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