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Tuning the ion selectivity of tetrameric cation channels by changing the number of ion binding sites.


ABSTRACT: Selective ion conduction across ion channel pores is central to cellular physiology. To understand the underlying principles of ion selectivity in tetrameric cation channels, we engineered a set of cation channel pores based on the nonselective NaK channel and determined their structures to high resolution. These structures showcase an ensemble of selectivity filters with a various number of contiguous ion binding sites ranging from 2 to 4, with each individual site maintaining a geometry and ligand environment virtually identical to that of equivalent sites in K(+) channel selectivity filters. Combined with single channel electrophysiology, we show that only the channel with four ion binding sites is K(+) selective, whereas those with two or three are nonselective and permeate Na(+) and K(+) equally well. These observations strongly suggest that the number of contiguous ion binding sites in a single file is the key determinant of the channel's selectivity properties and the presence of four sites in K(+) channels is essential for highly selective and efficient permeation of K(+) ions.

SUBMITTER: Derebe MG 

PROVIDER: S-EPMC3021048 | biostudies-literature | 2011 Jan

REPOSITORIES: biostudies-literature

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Tuning the ion selectivity of tetrameric cation channels by changing the number of ion binding sites.

Derebe Mehabaw G MG   Sauer David B DB   Zeng Weizhong W   Alam Amer A   Shi Ning N   Jiang Youxing Y  

Proceedings of the National Academy of Sciences of the United States of America 20101227 2


Selective ion conduction across ion channel pores is central to cellular physiology. To understand the underlying principles of ion selectivity in tetrameric cation channels, we engineered a set of cation channel pores based on the nonselective NaK channel and determined their structures to high resolution. These structures showcase an ensemble of selectivity filters with a various number of contiguous ion binding sites ranging from 2 to 4, with each individual site maintaining a geometry and li  ...[more]

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