Involvement of a novel C-terminal kinase domain of Kir6.2 in the K-ATP channel rundown reactivation

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作者
Kuo-Long Lou
Hsiu-Chuan Chou
Yau-Wie Tsai
Yu-Shuan Shiau
Po-Tsang Huang
Ting-Yu Chen
Yuh-Yuan Shiau
Robert J. French
机构
[1] Graduate Institute of Oral Biology,
[2] College of Medicine,undefined
[3] National Taiwan University,undefined
[4] Taipei 10042,undefined
[5] Taiwan E-mail: kllou@ha.mc.ntu.edu.tw Phone: +886 2 23562340 Fax: +886 2 23820785,undefined
[6] Institute of Statistical Science,undefined
[7] Academia Sinica,undefined
[8] Taipei,undefined
[9] Taiwan,undefined
[10] Department of Biophysics & Neuroscience Research Groups,undefined
[11] Faculty of Medicine,undefined
[12] Health Sciences Centre,undefined
[13] University of Calgary,undefined
[14] T2N 4N1,undefined
[15] Canada,undefined
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关键词
Keywords. Channel gating; 3D homology modeling; Kinase domain; Kir6.2; Rundown reactivation;
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摘要
Rundown is a generally encountered problem while recording KATP channel activity with inside-out patches. No assigned structural fragment related to this mechanism has yet been derived from any of the functional analyses performed. Therefore, based on a combined sequence and secondary structure alignment against known crystal structure of segments from closely related proteins, we propose here the three-dimensional structural model of an intracellular C-terminal domain of the Kir6.2 subunit in KATP channels. An E. coli CMP-kinase was suggested as template for the model building. The subdomain arrangement of this novel kinase domain and the structural correlation for UDP-docking are described. With structural-functional interpretation, we conclude that the reactivation of KATP channel rundown by MgATP or UDP is very possibly regulated by this intracellular kinase domain at the C-terminus of Kir6.2 subunit in KATP channels.
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页码:20 / 25
页数:5
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