In Vivo Structure-Function Analyses of Caenorhabditis elegans MEC-4, a Candidate Mechanosensory Ion Channel Subunit

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The Journal of Neuroscience, April 1, 2000, 20(7):2575-2588

In Vivo Structure-Function Analyses of Caenorhabditis elegans MEC-4, a Candidate Mechanosensory Ion Channel Subunit
Kyonsoo Hong, Itzhak Mano, and Monica Driscoll
Department of Molecular Biology and Biochemistry, Rutgers, The State University of New Jersey, Piscataway, New Jersey 08854
Mechanosensory signaling mediated by mechanically gated ion channels constitutes the basis for the senses of touch and hearingand contributes fundamentally to the development and homeostasisof all organisms. Despite this profound importance in biology,little is known of the molecular identities or functional requirementsof mechanically gated ion channels. We report a genetically basedstructure-function analysis of the candidate mechanotransducingchannel subunit MEC-4, a core component of a touch-sensing complexin Caenorhabditis elegans and a member of the DEG/ENaC superfamily.We identify molecular lesions in 40 EMS-induced mec-4 allelesand further probe residue and domain function using site-directedapproaches. Our analysis highlights residues and subdomains criticalfor MEC-4 activity and suggests possible roles of these in channelassembly and/or function. We describe a class of substitutionsthat disrupt normal channel activity in touch transduction butremain permissive for neurotoxic channel hyperactivation, andwe show that expression of an N-terminal MEC-4 fragment interfereswith in vivo channel function. These data advance working modelsfor the MEC-4 mechanotransducing channel and identify residues,unique to MEC-4 or the MEC-4 degenerin subfamily, that might bespecifically required for mechanotransducing function. Becausemany other substitutions identified by our study affect residuesconserved within the DEG/ENaC channel superfamily, this work alsoprovides a broad view of structure-function relations in the superfamilyas a whole. Because the C. elegans genome encodes representativesof a large number of eukaryotic channel classes, we suggest thatsimilar genetic-based structure-activity studies might be generallyapplied to generate insight into the in vivo function of diversechanneltypes.

Key words: MEC-4; touch sensation; mechanosensation; mechanotransduction; neurodegeneration; degenerin; Na⁺ channel; ENaC; mutagenesis
Copyright © 2000 Society for Neuroscience 0270-6474/00/2072575-14$05.00/0

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