| Literature DB >> 33712547 |
Xiaojing Pan1, Zhangqiang Li2, Xueqin Jin2, Yanyu Zhao3,4, Gaoxingyu Huang3,4, Xiaoshuang Huang2, Zilin Shen2, Yong Cao5, Mengqiu Dong5, Jianlin Lei6, Nieng Yan7.
Abstract
Among the nine subtypes of human voltage-gated sodium (Nav) channels, the brain and cardiac isoforms, Nav1.1 and Nav1.5, each carry more than 400 missense mutations respectively associated with epilepsy and cardiac disorders. High-resolution structures are required for structure-function relationship dissection of the disease variants. We report the cryo-EM structures of the full-length human Nav1.1-β4 complex at 3.3 Å resolution here and the Nav1.5-E1784K variant in the accompanying paper. Up to 341 and 261 disease-related missense mutations in Nav1.1 and Nav1.5, respectively, are resolved. Comparative structural analysis reveals several clusters of disease mutations that are common to both Nav1.1 and Nav1.5. Among these, the majority of mutations on the extracellular loops above the pore domain and the supporting segments for the selectivity filter may impair structural integrity, while those on the pore domain and the voltage-sensing domains mostly interfere with electromechanical coupling and fast inactivation. Our systematic structural delineation of these mutations provides important insight into their pathogenic mechanism, which will facilitate the development of precise therapeutic interventions against various sodium channelopathies.Entities:
Keywords: Dravet syndrome; Nav1.1; cryo-EM structure; epileptic seizure; fast inactivation
Year: 2021 PMID: 33712547 PMCID: PMC7980448 DOI: 10.1073/pnas.2100066118
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205