Wakui Hiromichi, Uneda Kazushi, Tamura Kouichi, Ohsawa Masato, Azushima Kengo, Kobayashi Ryu, Ohki Kohji, Dejima Toru, Kanaoka Tomohiko, Tsurumi-Ikeya Yuko, Matsuda Miyuki, Haruhara Kotaro, Nishiyama Akira, Yabana Machiko, Fujikawa Tetsuya, Yamashita Akio, Umemura Satoshi
Department of Medical Science and Cardiorenal Medicine, Yokohama City University Graduate School of Medicine, Yokohama, Japan (H.W., K.U., K.T., M.O., K.A., R.K., K.O., T.D., T.K., Y.T.I., M.M., K.H., M.Y., T.F., S.U.).
Department of Pharmacology, Kagawa University School of Medicine, Kagawa, Japan (A.N.).
J Am Heart Assoc. 2015 Mar 19;4(3):e001594. doi: 10.1161/JAHA.114.001594.
Angiotensin II type 1 receptor (AT1R)-associated protein (ATRAP; Agtrap gene) promotes AT1R internalization along with suppression of pathological AT1R activation. In this study, we examined whether enhancement of ATRAP in the renal distal tubules affects sodium handling and blood pressure regulation in response to high salt (HS) loading, using ATRAP transgenic mice on a salt-sensitive C57BL/6J background.
Renal ATRAP transgenic (rATRAP-Tg) mice, which exhibit renal tubule-dominant ATRAP enhancement, and their wild-type littermate C57BL/6J mice on a normal salt diet (0.3% NaCl) at baseline were subjected to dietary HS loading (4% NaCl) for 7 days. In rATRAP-Tg mice, the dietary HS loading-mediated blood pressure elevation was suppressed compared with wild-type mice, despite similar baseline blood pressure. Although renal angiotensin II level was comparable in rATRAP-Tg and wild-type mice with and without HS loading, urinary sodium excretion in response to HS loading was significantly enhanced in the rATRAP-Tg mice. In addition, functional transport activity of the amiloride-sensitive epithelial Na(+) channel was significantly decreased under saline volume-expanded conditions in rATRAP-Tg mice compared with wild-type mice, without any evident change in epithelial Na(+) channel protein expression. Plasma membrane AT1R expression in the kidney of rATRAP-Tg mice was decreased compared with wild-type mice.
These results demonstrated that distal tubule-dominant enhancement of ATRAP inhibits pathological renal sodium reabsorption and blood pressure elevation in response to HS loading. The findings suggest that ATRAP-mediated modulation of sodium handling in renal distal tubules could be a target of interest in salt-sensitive blood pressure regulation.
1型血管紧张素II受体(AT1R)相关蛋白(ATRAP;Agtrap基因)可促进AT1R内化,同时抑制病理性AT1R激活。在本研究中,我们使用盐敏感C57BL/6J背景的ATRAP转基因小鼠,研究肾远曲小管中ATRAP的增强是否会影响高盐(HS)负荷下的钠处理和血压调节。
肾ATRAP转基因(rATRAP-Tg)小鼠表现出肾小管为主的ATRAP增强,其野生型同窝C57BL/6J小鼠在基线时接受正常盐饮食(0.3% NaCl),然后进行7天的高盐饮食(4% NaCl)。在rATRAP-Tg小鼠中,尽管基线血压相似,但与野生型小鼠相比,高盐饮食介导的血压升高受到抑制。尽管在有或无高盐负荷的rATRAP-Tg和野生型小鼠中肾血管紧张素II水平相当,但rATRAP-Tg小鼠对高盐负荷的尿钠排泄显著增强。此外,与野生型小鼠相比,在生理盐水扩容条件下,rATRAP-Tg小鼠中氨氯地平敏感的上皮钠通道的功能转运活性显著降低,而上皮钠通道蛋白表达没有明显变化。与野生型小鼠相比,rATRAP-Tg小鼠肾脏中的质膜AT1R表达降低。
这些结果表明,远曲小管为主的ATRAP增强可抑制病理性肾钠重吸收和高盐负荷引起的血压升高。这些发现表明,ATRAP介导的肾远曲小管钠处理调节可能是盐敏感性血压调节中一个有意义的靶点。
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