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ROMK1通道的加工与转运对温度敏感。

Processing and transport of ROMK1 channel is temperature-sensitive.

作者信息

Brejon M, Le Maout S, Welling P A, Merot J

机构信息

Department de Biologie Cellulaire, et Moléculaire, Gif/Yvette, 91191, France.

出版信息

Biochem Biophys Res Commun. 1999 Aug 2;261(2):364-71. doi: 10.1006/bbrc.1999.1016.

Abstract

To investigate the biosynthetic mechanisms involved in the expression of the renal epithelial inward rectifying K(+) channel, ROMK1 (Kir1.1a), a six amino acid epitope (AU1) was introduced onto the extreme N-terminus for efficient immunoprecipitation. As expressed in Xenopus oocytes, the AU1 epitope did not modify the functional properties of the ROMK1 channel. To analyze kinetics of ROMK1 synthesis in renal epithelial cells, the AU1-ROMK1 construct was stably transfected in MDCK cells and pulse chase experiments were conducted. When the cells are grown at 37 degrees C, the ROMK1 protein was unstable, being rapidly degraded with a t(1/2) < 1 hour. Furthermore, whole cell patch clamp experiments failed to detect functional ROMK1 channels at the plasma membrane in cells grown at 37 degrees C. In contrast, the degradation process was minimized when the cells were grown at 26 degrees C (t(1/2) > 4 hours), allowing ROMK1 channels to be functionally expressed on the plasma membrane. In summary, in a mammalian epithelial expression system maintained at a physiological temperature, wild-type ROMK1 is bio-synthetically labile and incapable of efficient traffic to the plasmalemma. These observations are reminiscent of temperature sensitive biosynthetic defects in mutant plasma membrane proteins, suggesting that wild-type ROMK1 may require other factors, like the association of a surrogate subunit, for appropriate biosynthetic processing.

摘要

为了研究参与肾上皮内向整流钾通道ROMK1(Kir1.1a)表达的生物合成机制,在其极端N端引入了一个六氨基酸表位(AU1)以进行高效免疫沉淀。在非洲爪蟾卵母细胞中表达时,AU1表位未改变ROMK1通道的功能特性。为了分析肾上皮细胞中ROMK1的合成动力学,将AU1-ROMK1构建体稳定转染至MDCK细胞中并进行脉冲追踪实验。当细胞在37℃下生长时,ROMK1蛋白不稳定,以t(1/2) < 1小时的速度迅速降解。此外,全细胞膜片钳实验未能在37℃下生长的细胞的质膜上检测到功能性ROMK1通道。相比之下,当细胞在26℃下生长时(t(1/2) > 4小时),降解过程最小化,使得ROMK1通道能够在质膜上功能性表达。总之,在维持在生理温度的哺乳动物上皮表达系统中,野生型ROMK1在生物合成上不稳定,无法有效地转运到质膜。这些观察结果让人联想到突变体质膜蛋白中温度敏感的生物合成缺陷,表明野生型ROMK1可能需要其他因子,如替代亚基的结合,来进行适当的生物合成加工。

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