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神经元或神经胶质细胞特异性清除分泌型肾素不会影响肾脏肾素、基础动脉压或代谢。

Neuron- or glial-specific ablation of secreted renin does not affect renal renin, baseline arterial pressure, or metabolism.

机构信息

Interdisciplinary Genetics Program, Roy J. and Lucille A. Carver College of Medicine, University of Iowa, Iowa City, Iowa, USA.

出版信息

Physiol Genomics. 2011 Mar 29;43(6):286-94. doi: 10.1152/physiolgenomics.00208.2010. Epub 2010 Dec 28.

Abstract

The renin-angiotensin system (RAS), known for its roles in cardiovascular, metabolic, and developmental regulation, is present in both the circulation and in many individual tissues throughout the body. Substantial evidence supports the existence of a brain RAS, though quantification and localization of brain renin have been hampered by its low expression levels. We and others have previously determined that there are two isoforms of renin expressed in the brain. The classical isoform encoding secreted renin (sREN) and a novel isoform encoding intracellular renin (icREN), the product of an alternative promoter and first exon (exon 1b). The differential role that these two isoforms play in cardiovascular and metabolic regulation remains unclear. Here we examined the physiological consequences of neuron- and glia-specific knockouts of sREN by crossing mice in which the sREN promoter and isoform-specific first exon (exon-1a) is flanked by LoxP sequences (sREN(flox) mice) with mice expressing Cre-recombinase controlled by either the neuron-specific Nestin promoter or the glia-specific GFAP promoter. Resulting offspring exhibited selective knockout of sREN in either neurons or glia, while preserving expression of icREN. Consistent with a hypothesized role of icREN in the brain RAS, neuron- and glia-specific knockout of sREN had no effect on blood pressure or heart rate; food, water, or sodium intake; renal function; or metabolic rate. These data demonstrate that sREN is dispensable within the brain for normal physiological regulation of cardiovascular, hydromineral, and metabolic regulation, and thereby indirectly support the importance of icREN in brain RAS function.

摘要

肾素-血管紧张素系统(RAS)在心血管、代谢和发育调节中起着重要作用,存在于循环系统和全身许多组织中。大量证据支持脑 RAS 的存在,尽管脑肾素的定量和定位受到其低表达水平的阻碍。我们和其他人之前已经确定,脑中有两种肾素同工型表达。经典同工型编码分泌型肾素(sREN)和一种新型同工型编码细胞内肾素(icREN),其产物是一个替代启动子和第一外显子(外显子 1b)。这两种同工型在心血管和代谢调节中的作用尚不清楚。在这里,我们通过将 sREN 启动子和同工型特异性第一外显子(exon-1a)侧翼带有 LoxP 序列的小鼠(sREN(flox) 小鼠)与表达 Cre 重组酶的小鼠进行杂交,研究了神经元和神经胶质特异性敲除 sREN 的生理后果,该 Cre 重组酶由神经元特异性 Nestin 启动子或神经胶质特异性 GFAP 启动子控制。由此产生的后代表现出神经元或神经胶质中 sREN 的选择性敲除,而 icREN 的表达得到保留。与 icREN 在脑 RAS 中的作用假设一致,神经元和神经胶质特异性敲除 sREN 对血压或心率、食物、水或钠摄入、肾功能或代谢率没有影响。这些数据表明,sREN 在大脑中对于心血管、水盐和代谢调节的正常生理调节是可有可无的,从而间接支持 icREN 在脑 RAS 功能中的重要性。

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