Structural Pharmacology of Cation-Chloride Cotransporters.

Membranes (Basel)

Department of Biochemistry, University of Utah School of Medicine, Salt Lake City, UT 84102, USA.

Published: November 2022

Loop and thiazide diuretics have been cornerstones of clinical management of hypertension and fluid overload conditions for more than five decades. The hunt for their molecular targets led to the discovery of cation-chloride cotransporters (CCCs) that catalyze electroneutral movement of Cl together with Na and/or K. CCCs consist of two 1 Na-1 K-2 Cl (NKCC1-2), one 1 Na-1 Cl (NCC), and four 1 K-1 Cl (KCC1-4) transporters in human. CCCs are fundamental in trans-epithelia ion secretion and absorption, homeostasis of intracellular Cl concentration and cell volume, and regulation of neuronal excitability. Malfunction of NKCC2 and NCC leads to abnormal salt and water retention in the kidney and, consequently, imbalance in electrolytes and blood pressure. Mutations in KCC2 and KCC3 are associated with brain disorders due to impairments in regulation of excitability and possibly cell volume of neurons. A recent surge of structures of CCCs have defined their dimeric architecture, their ion binding sites, their conformational changes associated with ion translocation, and the mechanisms of action of loop diuretics and small molecule inhibitors. These breakthroughs now set the stage to expand CCC pharmacology beyond loop and thiazide diuretics, developing the next generation of diuretics with improved potency and specificity. Beyond drugging renal-specific CCCs, brain-penetrable therapeutics are sorely needed to target CCCs in the nervous system for the treatment of neurological disorders and psychiatric conditions.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9784483PMC
http://dx.doi.org/10.3390/membranes12121206DOI Listing

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