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正常和缺血性肾脏中人类肾素的生物合成与分泌

Human renin biosynthesis and secretion in normal and ischemic kidneys.

作者信息

Pratt R E, Carleton J E, Richie J P, Heusser C, Dzau V J

机构信息

Department of Medicine, Brigham and Women's Hospital, Boston, MA 02115.

出版信息

Proc Natl Acad Sci U S A. 1987 Nov;84(22):7837-40. doi: 10.1073/pnas.84.22.7837.

Abstract

The pathway of renin biosynthesis and secretion in normal and ischemic human kidneys has been investigated by pulse-labeling experiments. The results indicate that in normal human kidney, preprorenin is rapidly processed to 47-kDa prorenin. Microradiosequencing showed that this molecule was generated by cleavage between Gly-23 and Leu-24, yielding a 43-amino acid proregion. Analysis of prorenin secreted by the kidney tissue yielded an identical sequence, indicating that prorenin is secreted without any further proteolysis. An examination of the kinetics of processing and secretion suggested that a majority of the newly synthesized prorenin is quickly secreted, while only a small fraction is processed intracellularly to the mature renin. The differences in secretion kinetics between prorenin and mature renin and the selective inhibition of prorenin secretion by monensin suggest that they are secreted independently via two pathways: a constitutive pathway probably from the Golgi or protogranules that rapidly release prorenin and a regulated pathway that secretes mature renin from the mature granules. A comparison of the kinetics of processing between normal and ischemic tissues suggests that renal ischemia leads to an overall increase in the rate of processing of prorenin to mature renin. In addition, prolonged biosynthetic labeling of renin in the ischemic kidney yielded two smaller molecular weight immunoreactive forms suggestive of renin fragments that may be degradative products. These fragments were not detected in normal kidney tissue labeled for similar lengths of time.

摘要

通过脉冲标记实验研究了正常和缺血性人肾脏中肾素生物合成和分泌的途径。结果表明,在正常人类肾脏中,前肾素原迅速加工为47 kDa的肾素原。微量放射测序表明,该分子是由甘氨酸-23和亮氨酸-24之间的切割产生的,产生了一个43个氨基酸的前区。对肾脏组织分泌的肾素原的分析产生了相同的序列,表明肾素原在没有任何进一步蛋白水解的情况下被分泌。对加工和分泌动力学的研究表明,大多数新合成的肾素原迅速分泌,而只有一小部分在细胞内加工为成熟肾素。肾素原和成熟肾素分泌动力学的差异以及莫能菌素对肾素原分泌的选择性抑制表明,它们通过两条途径独立分泌:一条可能来自高尔基体或原颗粒的组成型途径,迅速释放肾素原;另一条调节途径从成熟颗粒中分泌成熟肾素。正常组织和缺血组织加工动力学的比较表明,肾缺血导致肾素原加工为成熟肾素的速率总体增加。此外,对缺血性肾脏中肾素进行长时间的生物合成标记产生了两种较小分子量的免疫反应形式,提示可能是降解产物的肾素片段。在标记相同时间的正常肾脏组织中未检测到这些片段。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7f10/299413/5e32eac01992/pnas00337-0047-a.jpg

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