摘要
通过组织血管紧张素Ⅱ肾素(AngⅡ)1型受体(AT1R)信号,肾素-血管紧张素系统的过度激活对心血管、肾脏及内分泌系统产生不利影响,引起高血压及相关靶器官损害。此外,基础和临床研究表明,生理受体的信号对正常器官如肾脏的发育以及心血管和肾脏稳态的维护也发挥着不可或缺的作用。AT1R信号等功能的多样性,促使我们寻求一种新的AT1R信号选择性调节策略。为了达到这一目的,在研究功能和选择性调节AT1R信号的过程中,通过小鼠肾cDNA库双杂交酵母筛选,一种与AT1R羧基端胞质域直接相互作用的分子是被发现证明,并命名为AT1R相关蛋白(ATRAP)。功能分析结果表明,ATRAP促进培养细胞构AT1R内化和抑制小鼠远曲细胞AngⅡ介导的病理反应。ATRAP在各种组织如肾脏中得到表达并大量分布在肾小管上皮细胞。遗传工程小鼠修饰后的ATRAP表达表明为应对诸如慢性注射血管紧张素II的病理刺激,ATRAP在调节肾脏钠的处理和调节血压的过程中起着关键作用,并表明ATRAP是一个有趣的目标对象。
关键词: 心血管疾病,高血压,肾,受体,肾疾病,钠离子重吸收。
Current Medicinal Chemistry
Title:Angiotensin II Type 1 Receptor Binding Molecule ATRAP as a Possible Modulator of Renal Sodium Handling and Blood Pressure in Pathophysiology
Volume: 22 Issue: 28
Author(s): K. Tamura, H. Wakui, K. Azushima, K. Uneda, S. Haku, R. Kobayashi, K. Ohki, K. Haruhara, S. Kinguchi and M. Matsuda, A. Yamashita and S. Umemura
Affiliation:
关键词: 心血管疾病,高血压,肾,受体,肾疾病,钠离子重吸收。
摘要: Exaggerated activation of the renin-angiotensin system via tissue angiotensin II (Ang II) type 1 receptor (AT1R) signaling exerts detrimental effects on cardiovascular, renal and endocrine systems to provoke hypertension and related target organ damage. On the other hand, accumulated research evidence of both basic and clinical studies shows that physiological AT1R signaling also plays an indispensable role for the normal organ development such as the kidney and the maintenance of cardiovascular and renal homeostasis. Such functional diversity of AT1R signaling prompts us to seek a new strategy of selective modulation of AT1R signaling in pathophysiology. In the course of an investigational search for a means to functionally and selectively modulate AT1R signaling for that purpose, a molecule directly interacting with the carboxyl-terminal cytoplasmic domain of AT1R was identified by employing yeast two-hybrid screening of a mouse kidney cDNA library and named AT1R-associated protein (ATRAP). The results of functional analysis showed that ATRAP promotes constitutive AT1R internalization in cultured cells and inhibits Ang II-mediated pathological response in mouse distal convoluted cells. The ATRAP is expressed in a variety of tissues including the kidney where ATRAP is abundantly distributed in epithelial cells along the renal tubules. The results employing genetic engineered mice with modified ATRAP expression showed that ATRAP plays a key role in the regulation of renal sodium handling and the modulation of blood pressure in response to pathological stimuli such as chronic Ang II infusion, and suggest ATRAP to be a target of interest.
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K. Tamura, H. Wakui, K. Azushima, K. Uneda, S. Haku, R. Kobayashi, K. Ohki, K. Haruhara, S. Kinguchi and M. Matsuda, A. Yamashita and S. Umemura , Angiotensin II Type 1 Receptor Binding Molecule ATRAP as a Possible Modulator of Renal Sodium Handling and Blood Pressure in Pathophysiology, Current Medicinal Chemistry 2015; 22 (28) . https://dx.doi.org/10.2174/0929867322666150821095036
DOI https://dx.doi.org/10.2174/0929867322666150821095036 |
Print ISSN 0929-8673 |
Publisher Name Bentham Science Publisher |
Online ISSN 1875-533X |
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