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异型 PC-1/PC-2 多囊蛋白复合物被 PC-1 N 端激活。

The heteromeric PC-1/PC-2 polycystin complex is activated by the PC-1 N-terminus.

机构信息

Department of Physiology, University of California, San Francisco, San Francisco, United States.

Department of Biochemistry, University of Utah School of Medicine, Salt Lake City, United States.

出版信息

Elife. 2020 Nov 9;9:e60684. doi: 10.7554/eLife.60684.

Abstract

Mutations in the polycystin proteins, PC-1 and PC-2, result in autosomal dominant polycystic kidney disease (ADPKD) and ultimately renal failure. PC-1 and PC-2 enrich on primary cilia, where they are thought to form a heteromeric ion channel complex. However, a functional understanding of the putative PC-1/PC-2 polycystin complex is lacking due to technical hurdles in reliably measuring its activity. Here we successfully reconstitute the PC-1/PC-2 complex in the plasma membrane of mammalian cells and show that it functions as an outwardly rectifying channel. Using both reconstituted and ciliary polycystin channels, we further show that a soluble fragment generated from the N-terminal extracellular domain of PC-1 functions as an intrinsic agonist that is necessary and sufficient for channel activation. We thus propose that autoproteolytic cleavage of the N-terminus of PC-1, a hotspot for ADPKD mutations, produces a soluble ligand in vivo. These findings establish a mechanistic framework for understanding the role of PC-1/PC-2 heteromers in ADPKD and suggest new therapeutic strategies that would expand upon the limited symptomatic treatments currently available for this progressive, terminal disease.

摘要

多囊蛋白蛋白 PC-1 和 PC-2 的突变导致常染色体显性多囊肾病 (ADPKD),最终导致肾衰竭。PC-1 和 PC-2 在初级纤毛上富集,在那里它们被认为形成异源二聚体离子通道复合物。然而,由于在可靠测量其活性方面存在技术障碍,因此缺乏对假定的 PC-1/PC-2 多囊蛋白复合物的功能理解。在这里,我们成功地在哺乳动物细胞的质膜中重建了 PC-1/PC-2 复合物,并表明它作为一种外向整流通道发挥作用。使用重建的和纤毛多囊蛋白通道,我们进一步表明,PC-1 的 N 末端细胞外结构域产生的可溶性片段作为内在激动剂发挥作用,对于通道激活是必需和充分的。因此,我们提出 PC-1 的 N 端的自蛋白水解切割,ADPKD 突变的热点,在体内产生一种可溶性配体。这些发现为理解 PC-1/PC-2 异源二聚体在 ADPKD 中的作用建立了一个机制框架,并提出了新的治疗策略,这些策略将扩展目前针对这种进行性、终末期疾病的有限对症治疗。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/57da/7728438/73c876d4271e/elife-60684-fig1.jpg

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