| Literature DB >> 15137031 |
Yuliya V Korolkova1, Gea-Ny Tseng, Eugene V Grishin.
Abstract
ERG potassium channels specify one component of the delayed rectifier in the heart and are likely to play an important functional role in other excitable cells. Compared to other K+ channels, the human ERG (hERG) channel possesses an unusually long S5-P linker that presumably forms an alpha-helix important for channel function. hERG-specific toxins bind to the outer mouth of the hERG channel. Channel residues in the middle of the S5-P linker and at the pore entrance are critical for toxin binding. One of these scorpion toxins is BeKm-1. Residues critical for BeKm-1 binding to the hERG channel are located in the alpha-helix and the following loop, whereas the "traditional" interaction surface of other short scorpion toxins is formed by residues on the beta-sheet. This unique localization of BeKm-1's interaction surface and its specific action on the hERG channel suggest a unique outer mouth structure of the hERG channel. We used the mutant cycle analysis approach to define contacts in the toxin-channel complex. This information provides critical constraints and is important for molecular modeling of the hERG pore structure. Copyright 2004 John Wiley & Sons, Ltd.Entities:
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Year: 2004 PMID: 15137031 DOI: 10.1002/jmr.667
Source DB: PubMed Journal: J Mol Recognit ISSN: 0952-3499 Impact factor: 2.137