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[下丘脑神经激素的亚细胞分布及其释放的体外刺激]

[Subcellular distribution of hypothalamic neurohormones and in vitro stimulation of their release].

作者信息

Kordon C, Epelbaum J, Gautron J P

出版信息

Bull Schweiz Akad Med Wiss. 1978 Mar;34(1-3):131-44.

PMID:208691
Abstract

Neuronal compartments can be separated by differential spinning or by centrifugation on continuous or discontinuous density gradients. Application of these fractionation techniques to brain structures containing neurosecretory neurons shows that LHRH, somatostatin and a non dopamine prolactin inhibiting factor (PIF) are exclusively recovered from synaptosomal fractions. This indicates that biologically and/or immunologically reactive forms of these hormones are almost entirely concentrated in nerve-endings of neurosecretory neurons. In contrast, other neuropeptides - posterior pituitary hormone, but also TRH, a vasoactive intestinal peptide (VIP), substance P or endorphins - are also found in supernatant fractions. The existence of multiple molecular forms of neuropeptides is likely to explain these differences. Current theories postulate that they are synthetized on ribosomes as precursor forms. Their active structure is only achieved by enzymatic splitting of the pre- or the prohormone within nerve endings. This mode of synthesis is probably common to all neuropeptides, although it has only been well substantiated in a few cases, in particular for the hormones of the posterior pituitary. Thus, the lack of immunologically detectable LHRH or SRIF outside the synaptosomal fraction may reflect masking of the active immunological sites by inert peptide chains associated with prohormonal forms. Fractionation methods can also be applied to physiological or pharmacological experiments. In particular, they permit to characterize, on presynaptic membranes of neurosecretory neurons, specific receptors to neurotransmitters involved in the control of neurohormone secretion. Interaction of dopamine and acetylcholine with LHRH and CRF release are presented as examples of such applications.

摘要

神经元区室可以通过差速离心或在连续或不连续密度梯度上离心来分离。将这些分级分离技术应用于含有神经分泌神经元的脑结构时发现,促黄体生成素释放激素(LHRH)、生长抑素和一种非多巴胺类催乳素抑制因子(PIF)仅从突触体级分中回收。这表明这些激素的生物活性和/或免疫反应性形式几乎完全集中在神经分泌神经元的神经末梢中。相比之下,其他神经肽——后叶垂体激素,还有促甲状腺激素释放激素(TRH)、血管活性肠肽(VIP)、P物质或内啡肽——也存在于上清级分中。神经肽多种分子形式的存在可能解释了这些差异。目前的理论假定它们在核糖体上以前体形式合成。它们的活性结构只有通过在神经末梢内对前激素或激素原进行酶切才能实现。这种合成方式可能对所有神经肽都很常见,尽管仅在少数情况下得到了充分证实,特别是对于后叶垂体的激素。因此,在突触体级分之外缺乏免疫可检测的LHRH或生长抑素释放抑制因子(SRIF)可能反映了与激素原形式相关的惰性肽链对活性免疫位点的掩盖。分级分离方法也可应用于生理学或药理学实验。特别是,它们能够在神经分泌神经元的突触前膜上表征参与神经激素分泌控制的神经递质的特异性受体。多巴胺和乙酰胆碱与LHRH和促肾上腺皮质激素释放因子(CRF)释放的相互作用作为此类应用的例子进行了介绍。

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