A 30-year journey from volume-regulated anion currents to molecular structure of the LRRC8 channel

Author:

Strange Kevin12ORCID,Yamada Toshiki1ORCID,Denton Jerod S.1

Affiliation:

1. Department of Anesthesiology, Vanderbilt University Medical Center, Nashville, TN

2. Novo Biosciences, Inc., Bar Harbor, ME

Abstract

The swelling-activated anion channel VRAC has fascinated and frustrated physiologists since it was first described in 1988. Multiple laboratories have defined VRAC’s biophysical properties and have shown that it plays a central role in cell volume regulation and possibly other fundamental physiological processes. However, confusion and intense controversy surrounding the channel’s molecular identity greatly hindered progress in the field for >15 yr. A major breakthrough came in 2014 with the demonstration that VRAC is a heteromeric channel encoded by five members of the Lrrc8 gene family, Lrrc8A–E. A mere 4 yr later, four laboratories described cryo-EM structures of LRRC8A homomeric channels. As the melee of structure/function and physiology studies begins, it is critical that this work be framed by a clear understanding of VRAC biophysics, regulation, and cellular physiology as well as by the field’s past confusion and controversies. That understanding is essential for the design and interpretation of structure/function studies, studies of VRAC physiology, and studies aimed at addressing the vexing problem of how the channel detects cell volume changes. In this review we discuss key aspects of VRAC biophysics, regulation, and function and integrate these into our emerging understanding of LRRC8 protein structure/function.

Funder

National Institute of Diabetes and Digestive and Kidney Diseases

Publisher

Rockefeller University Press

Subject

Physiology

Reference145 articles.

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