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Cx32初始C末端结构域的正电荷抑制间隙连接对二氧化碳的门控敏感性。

Positive charges of the initial C-terminus domain of Cx32 inhibit gap junction gating sensitivity to CO2.

作者信息

Wang X G, Peracchia C

机构信息

Department of Pharmacology and Physiology, University of Rochester School of Medicine and Dentistry, New York 14642-8711, USA.

出版信息

Biophys J. 1997 Aug;73(2):798-806. doi: 10.1016/S0006-3495(97)78112-8.

Abstract

Gap junction channels close with CO2 exposure. To determine whether the carboxy-terminus (CT) of connexin32 (Cx32) participates in gating, the CO2 sensitivity of channels made of Cx32 or Cx32 mutants was studied by double voltage clamp. In Xanopus laevis oocytes expressing Cx32, junctional conductance (Gj) dropped to 85% and 47% of controls with 3- and 15-min CO2 exposures, respectively. In response to the 15-min exposure to CO2, pHi dropped to approximately 6.4 in 5-7 min and did not decrease further, even with 30-min exposures. CT deletion by 84% did not affect CO2 sensitivity, but replacement of five arginines (R215, R219, R220, R223, and R224) with asparagines (N) or threonines at the beginning of CT (CT1) in Cx32 or Cx32 deleted beyond residue 225 greatly enhanced CO2 sensitivity (with 3-min CO2 Gj dropped to approximately 8%). Partial R/N replacement resulted in intermediate CO2 sensitivity enhancement. R215 is a stronger inhibitor than R219-220, whereas R223-224 may diminish the inhibitory efficiency of R215 and R219-220. Therefore, positive charges of CT1 reduce the CO2 sensitivity of Cx32, whereas the rest (> 80%) of CT seems to play no role in CO2-induced gating. The role of presumed electrostatic interactions among Cx32 domains in CO2-induced gating is discussed.

摘要

间隙连接通道在暴露于二氧化碳时会关闭。为了确定连接蛋白32(Cx32)的羧基末端(CT)是否参与门控,通过双电压钳研究了由Cx32或Cx32突变体制成的通道的二氧化碳敏感性。在表达Cx32的非洲爪蟾卵母细胞中,分别在暴露于3分钟和15分钟二氧化碳时,连接电导(Gj)降至对照的85%和47%。响应于15分钟的二氧化碳暴露,细胞内pH值在5 - 7分钟内降至约6.4,即使暴露30分钟也不再进一步降低。CT缺失84%不影响二氧化碳敏感性,但在Cx32或缺失超过225位残基的Cx32中,在CT起始处(CT1)将五个精氨酸(R215、R219、R220、R223和R224)替换为天冬酰胺(N)或苏氨酸会大大增强二氧化碳敏感性(暴露3分钟时Gj降至约8%)。部分R/N替换导致二氧化碳敏感性增强程度居中。R215比R219 - 220是更强的抑制剂,而R223 - 224可能会降低R215和R219 - 220的抑制效率。因此,CT1的正电荷降低了Cx32的二氧化碳敏感性,而CT的其余部分(> 80%)似乎在二氧化碳诱导的门控中不起作用。讨论了Cx32结构域之间假定的静电相互作用在二氧化碳诱导门控中的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7074/1180976/f44a34e3dd66/biophysj00033-0253-a.jpg

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