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水通道蛋白在正常人体肾脏及肾脏疾病中的表达

Aquaporin expression in normal human kidney and in renal disease.

作者信息

Bedford Jennifer J, Leader John P, Walker Robert J

机构信息

Department of Physiology, University of Otago, Dunedin, New Zealand.

出版信息

J Am Soc Nephrol. 2003 Oct;14(10):2581-7. doi: 10.1097/01.asn.0000089566.28106.f6.

Abstract

Aquaporins (AQPs), membrane-inserted water channel proteins, play a highly important role in the reabsorption of water from the renal tubular fluid. Experimentally, both in rats and mice, failure to insert functional AQP molecules into renal tubular membranes leads to nephrogenic diabetes insipidus. In humans, most forms of renal disease lead to a reduction in the water handling capacity of the kidney. AQP distribution in various forms of human renal disease has not been documented. Immunohistochemical studies of biopsy samples from a wide range of renal diseases revealed a substantial and striking upregulation of AQP-1 in the glomeruli of most diseased kidneys. AQP-1 expression remained prominent in proximal tubules in all lesions. In contrast, there was judged qualitatively to be a reduction in the amounts of AQP-2 and AQP-3 expression, especially in lesions with substantial interstitial fibrosis and nephron loss, as compared with a healthy region of normal kidneys. The results were quantitatively confirmed by real-time reverse transcriptase-PCR. This is the first documentation of altered AQP expression in human renal disease. The significance of the increased AQP-1 expression requires further studies.

摘要

水通道蛋白(AQPs)是插入细胞膜的水通道蛋白,在肾小管液中水的重吸收过程中发挥着极其重要的作用。在实验中,无论是大鼠还是小鼠,若未能将功能性AQP分子插入肾小管膜,都会导致肾性尿崩症。在人类中,大多数形式的肾脏疾病都会导致肾脏处理水的能力下降。目前尚未有关于各种人类肾脏疾病中水通道蛋白分布情况的文献记载。对来自多种肾脏疾病的活检样本进行免疫组织化学研究发现,在大多数患病肾脏的肾小球中,水通道蛋白-1(AQP-1)有显著且惊人的上调。在所有病变中,近端小管中AQP-1的表达仍然显著。相比之下,与正常肾脏的健康区域相比,定性判断AQP-2和AQP-3的表达量有所减少,尤其是在有大量间质纤维化和肾单位丢失的病变中。这些结果通过实时逆转录聚合酶链反应得到了定量证实。这是首次关于人类肾脏疾病中水通道蛋白表达改变的文献记载。AQP-1表达增加的意义需要进一步研究。

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