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鉴定沿皮质小管表达的真正替代肾素转录本,并研究其在体内促进胰岛素抵抗的潜在作用,而不会显著升高血浆肾素活性。

Identification of bona fide alternative renin transcripts expressed along cortical tubules and potential roles in promoting insulin resistance in vivo without significant plasma renin activity elevation.

机构信息

From the Department of Medical Science and Cardio-Renal Medicine, Yokohama City University, Graduate School of Medicine, Yokohama, Japan.

出版信息

Hypertension. 2014 Jul;64(1):125-33. doi: 10.1161/HYPERTENSIONAHA.114.03394. Epub 2014 Apr 28.

Abstract

Renin belongs to a family of aspartyl proteases and is the rate-limiting enzyme in the synthesis of the potent vasoactive peptide angiotensin II. Processing of renal renin has been extensively investigated in juxtaglomerular granular cells, in which prorenin and active renin are present in secretory condensed granules. Previous studies demonstrated alternative renin transcription in rat adrenal glands. Different studies reported novel intracellular forms of renin deduced from novel 5' variants derived from renin mRNA in both mice and humans. Comprehensive detailed studies in genetically engineered mice showed that both a secreted and an intracellular form of renin plays divergent mechanism regulating fluid intake and metabolism by the brain renin-angiotensin system; however, the presence, regulation, and functions of these renin isoforms in kidney and adrenal gland are not fully understood in mice. To investigate the characteristics of renin isoforms in mice, we performed a systematic inventory of renin transcripts of mice with and without a duplication of the renin gene alternatively from previous studies. We discovered a novel isoform of renin of the Ren2 gene, which conserved functionally important residues of the prosegment and incomplete isoforms of the Ren1C/D gene lacking a pre-pro segment. In situ hybridization assays revealed alternative renin isoforms expressed along cortical tubules. Newly generated transgenic mice with systemic overexpression of alternative renin transcript showed enhanced local angiotensin II generation without elevation of plasma renin activity and systemic insulin resistance in vivo, providing new pathophysiological insights into insulin resistance exaggerated by bona fide renin isoform.

摘要

肾素属于天冬氨酸蛋白酶家族,是合成强效血管活性肽血管紧张素 II 的限速酶。在肾小球旁颗粒细胞中,对肾素的加工进行了广泛的研究,其中前肾素和活性肾素存在于分泌浓缩颗粒中。先前的研究表明,在大鼠肾上腺中有替代的肾素转录。不同的研究报道了新型的肾素,它是从老鼠和人类的肾素 mRNA 的新型 5'变体推导出来的。在基因工程小鼠中的综合详细研究表明,脑肾素-血管紧张素系统中,无论是分泌型还是细胞内型的肾素,都通过不同的机制调节液体摄入和代谢;然而,这些肾素同工型在肾脏和肾上腺中的存在、调节和功能在小鼠中尚未完全了解。为了研究小鼠肾素同工型的特征,我们对有和没有肾素基因重复的小鼠进行了系统的肾素转录本分析,这是从前人的研究中得到的。我们发现了 Ren2 基因的一种新型肾素同工型,它保守了前肽段的功能重要残基和缺少前肽段的 Ren1C/D 基因的不完全同工型。原位杂交试验显示,沿着皮质小管表达了替代的肾素同工型。具有系统过表达替代肾素转录本的新生成的转基因小鼠显示局部血管紧张素 II 生成增强,而血浆肾素活性和全身胰岛素抵抗没有升高,为胰岛素抵抗通过真正的肾素同工型而加剧提供了新的病理生理学见解。

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