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[血管紧张素转换酶:一种在进化过程中保守的蛋白质]

[Angiotensin-converting enzyme: a protein conserved during evolution].

作者信息

Rivière Guillaume

机构信息

UMR M100 IFREMER/UCBN Physiologie et Ecophysiologie des Mollusques Marins, Université de Caen Basse-Normandie, Bâtiment Sciences C, Campus I, Esplanade de la Paix, 14000 Caen, France.

出版信息

J Soc Biol. 2009;203(4):281-93. doi: 10.1051/jbio/2009032. Epub 2010 Feb 1.

DOI:10.1051/jbio/2009032
PMID:20122386
Abstract

The Angiotensin-Converting Enzyme (ACE) is crucial for vascular homeostasis in mammals. Three isoforms are present in the human. the somatic ACE (sACE) generates the vasoactive angiotensin II. The testicular isoform (tACE) is required for male fertility. ACE2 was cloned from another gene and displays an antagonistic role. Several ACEs were cloned from insects, despite their lack of a closed circulatory system. Insect isoforms are implied in reproduction and development. No sequence in the C. elegans genome is able to encode a functional enzyme. Nevertheless, an active ACE was characterized in an even more distant organism, the leech, in which the enzyme is mainly expressed within the digestive tract. The presence of ACE is lophotrochozoans raises questions about the appearance and original functions of the enzyme. Besides, the recent availability of genomic data unraveled the putative presence of orthologues in even more distant phyla such as cnidaria, placozoa and even many procaryotes. Moreover, the characterization of an active ACE in a proteobacteria indicates that the ancestor isoform was already functional. Thus, ACE is present from bacteria to mammals and exhibits incredibly conserved molecular, biochemical as well as structural features. The absence of ACE in all eucaryotic bicounts could thus result from a secondary loss. Taken together, these data suggest that ACE appeared early during the course of evolution. Mammalian ACE features could thus be a result of the long evolutive specialization of an ancient protease whose physiological functions remain to be elucidated.

摘要

血管紧张素转换酶(ACE)对哺乳动物的血管稳态至关重要。人类中有三种同工型。体细胞ACE(sACE)生成血管活性肽血管紧张素II。睾丸同工型(tACE)是雄性生育所必需的。ACE2是从另一个基因克隆而来的,具有拮抗作用。尽管昆虫缺乏封闭的循环系统,但仍从昆虫中克隆出了几种ACE。昆虫同工型与繁殖和发育有关。秀丽隐杆线虫基因组中没有能够编码功能性酶的序列。然而,在一种更为远缘的生物——水蛭中发现了一种活性ACE,该酶主要在消化道中表达。ACE在冠轮动物中的存在引发了关于该酶的出现和原始功能的问题。此外,最近基因组数据的可得性揭示了在更远缘的门类如刺胞动物、扁盘动物甚至许多原核生物中可能存在直系同源物。而且,在一种变形菌中对活性ACE的表征表明祖先同工型已经具有功能。因此,ACE从细菌到哺乳动物都存在,并且展现出令人难以置信的保守的分子、生化以及结构特征。所有真核生物中ACE的缺失可能是次生丢失的结果。综上所述,这些数据表明ACE在进化过程中出现得很早。哺乳动物ACE的特征可能是一种古老蛋白酶长期进化特化的结果,其生理功能仍有待阐明。

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[Angiotensin-converting enzyme: a protein conserved during evolution].[血管紧张素转换酶:一种在进化过程中保守的蛋白质]
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Chicken lacks the testis specific isozyme of angiotensin converting enzyme found in mammals.鸡缺乏在哺乳动物中发现的血管紧张素转换酶的睾丸特异性同工酶。
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New aspects on angiotensin-converting enzyme: from gene to disease.血管紧张素转换酶的新进展:从基因到疾病
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