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利钠肽激活的鸟苷酸环化酶mRNA在大鼠脑中的定位

Localization of natriuretic peptide-activated guanylate cyclase mRNAs in the rat brain.

作者信息

Herman J P, Dolgas C M, Rucker D, Langub M C

机构信息

Department of Anatomy and Neurobiology, University of Kentucky College of Medicine, Lexington 40536-0084, USA.

出版信息

J Comp Neurol. 1996 May 27;369(2):165-87. doi: 10.1002/(SICI)1096-9861(19960527)369:2<165::AID-CNE1>3.0.CO;2-1.

Abstract

Physiological actions of atrial natriuretic peptide (ANP) and C-type natriuretic peptide (CNP) are elaborated by membrane-bound natriuretic peptide receptors (NPRs). These receptors possess intracellular guanylate cyclase domains that mobilize cyclic guanosine monophosphate upon binding of peptide. Two distinct NPR subtypes have been described in brain: the NPR-A selectively binds ANP, whereas NPR-B exhibits high affinity for CNP. To define further the potential domains of ANP and CNP action in brain, the present study used in situ hybridization histochemistry to map NPR-A and NPR-B mRNA-expressing cell populations. Significant levels of neuronal NPR-A mRNA expression were observed only in the mitral cell layer of the olfactory bulb, medial habenula, subfornical organ, and area postrema. Expression of NPR-A mRNA was observed in forebrain white matter tracts, suggesting synthesis in glial cells. In contrast, NPR-B mRNA was widely expressed throughout the neuraxis. In the telencephalon, signal was abundant throughout limbic cortex and neocortex, olfactory bulb, hippocampus, and amygdala. Intense NPR-B mRNA hybridization was observed in preoptic-hypothalamic neuroendocrine circuits and in motor nuclei of cranial nerves. Intermediate expression of NPR-B mRNA was observed in brainstem nuclei controlling autonomic function. Labeling for NPR-B but not NPR-A mRNA was observed in pituicytes in the neural lobe of the pituitary and in scattered cells of the anterior pituitary. These results suggest that CNP is the primary biologically active natriuretic peptide in brain. In contrast with NPR-B, NPR-A appears to be expressed largely in restricted cell populations containing high levels of ANP and in circumventricular organs. These data implicate the NPR-A in autoregulation of ANP neurons and central registration of cardiac ANP release.

摘要

心房利钠肽(ANP)和C型利钠肽(CNP)的生理作用是由膜结合型利钠肽受体(NPRs)介导的。这些受体具有细胞内鸟苷酸环化酶结构域,在肽结合后可激活环磷酸鸟苷。在脑中已描述了两种不同的NPR亚型:NPR-A选择性结合ANP,而NPR-B对CNP具有高亲和力。为了进一步明确ANP和CNP在脑中的潜在作用区域,本研究采用原位杂交组织化学技术来定位表达NPR-A和NPR-B mRNA的细胞群。仅在嗅球的二尖瓣细胞层、内侧缰核、穹窿下器官和最后区观察到显著水平的神经元NPR-A mRNA表达。在脑前白质束中观察到NPR-A mRNA的表达,提示其在胶质细胞中合成。相比之下,NPR-B mRNA在整个神经轴广泛表达。在端脑,信号在整个边缘皮质和新皮质、嗅球、海马和杏仁核中丰富。在视前 - 下丘脑神经内分泌回路和颅神经运动核中观察到强烈的NPR-B mRNA杂交信号。在控制自主功能的脑干核中观察到NPR-B mRNA的中等水平表达。在垂体神经叶的垂体细胞和垂体前叶的散在细胞中观察到NPR-B mRNA而非NPR-A mRNA的标记。这些结果表明CNP是脑中主要的生物活性利钠肽。与NPR-B不同,NPR-A似乎主要在含有高水平ANP的受限细胞群和室周器官中表达。这些数据提示NPR-A参与ANP神经元的自身调节以及心脏ANP释放的中枢记录。

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