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大鼠肾脏中钠/肌醇共转运体的定位与快速调节

Localization and rapid regulation of Na+/myo-inositol cotransporter in rat kidney.

作者信息

Yamauchi A, Miyai A, Shimada S, Minami Y, Tohyama M, Imai E, Kamada T, Ueda N

机构信息

First Department of Medicine, Osaka University School of Medicine, Japan.

出版信息

J Clin Invest. 1995 Sep;96(3):1195-201. doi: 10.1172/JCI118151.

Abstract

myo-inositol, a major compatible osmolyte in renal medulla, is accumulated in several kinds of cells under hypertonic conditions via Na+/myo-inositol cotransporter (SMIT). To investigate the physiological role of the SMIT, we sought to determine its localization by in situ hybridization and its acute regulation by NaCl and furosemide administration. Northern analysis demonstrated that SMIT is strongly expressed in the medulla and at low levels in the cortex of kidney. Intraperitoneal injection of NaCl rapidly induced SMIT mRNA in both the cortex and medulla, and furosemide completely abolished this induction. In situ hybridization revealed that SMIT it predominantly present in the medullary and cortical thick ascending limbs of Henle's loop (TALH) and macula densa cells. Less intense signals were seen in the inner medullary collecting ducts (IMCD). NaCl loading increased the signals throughout the TALH, and furosemide reduced the signals. SMIT in the IMCD is less sensitive to these kinds of acute regulation. Thus, the distribution pattern of SMIT does not correspond to the corticomedullary osmotic gradient, and SMIT in the TALH and macula densa cells is regulated very rapidly. These results suggest that SMIT expression in TALH may be regulated by intracellular and/or peritubular tonicity close to the basolateral membrane, which is supposed to be proportional to the magnitude of NaCl reabsorption.

摘要

肌醇是肾髓质中一种主要的相容性渗透溶质,在高渗条件下,它通过钠/肌醇协同转运蛋白(SMIT)在多种细胞中蓄积。为了研究SMIT的生理作用,我们试图通过原位杂交确定其定位,并通过给予氯化钠和呋塞米来研究其急性调节作用。Northern印迹分析表明,SMIT在肾髓质中强烈表达,而在肾皮质中表达水平较低。腹腔注射氯化钠可迅速诱导皮质和髓质中的SMIT mRNA表达,而呋塞米可完全消除这种诱导作用。原位杂交显示,SMIT主要存在于亨氏袢的髓质和皮质厚升支(TALH)以及致密斑细胞中。在内髓集合管(IMCD)中可见较弱的信号。氯化钠负荷增加了整个TALH中的信号,而呋塞米则降低了信号。IMCD中的SMIT对这类急性调节不太敏感。因此,SMIT的分布模式与皮质-髓质渗透梯度不对应,并且TALH和致密斑细胞中的SMIT受到非常快速的调节。这些结果表明,TALH中SMIT的表达可能受靠近基底外侧膜的细胞内和/或肾小管周张力调节,而这种张力被认为与氯化钠重吸收的程度成正比。

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