Pharmacological tools to target NKCC1 in brain disorders
- PMID: 34620512
- DOI: 10.1016/j.tips.2021.09.005
Pharmacological tools to target NKCC1 in brain disorders
Abstract
The chloride importer NKCC1 and the chloride exporter KCC2 are key regulators of neuronal chloride concentration. A defective NKCC1/KCC2 expression ratio is associated with several brain disorders. Preclinical/clinical studies have shown that NKCC1 inhibition by the United States FDA-approved diuretic bumetanide is a potential therapeutic strategy in preclinical/clinical studies of multiple neurological conditions. However, bumetanide has poor brain penetration and causes unwanted diuresis by inhibiting NKCC2 in the kidney. To overcome these issues, a growing number of studies have reported more brain-penetrating and/or selective bumetanide prodrugs, analogs, and new molecular entities. Here, we review the evidence for NKCC1 pharmacological inhibition as an effective strategy to manage neurological disorders. We also discuss the advantages and limitations of bumetanide repurposing and the benefits and risks of new NKCC1 inhibitors as therapeutic agents for brain disorders.
Keywords: NKCC1; brain disorders; bumetanide; chloride homeostasis; selective NKCC1 inhibitors.
Copyright © 2021 The Authors. Published by Elsevier Ltd.. All rights reserved.
Conflict of interest statement
Declaration of interests The authors declare the following competing financial interest(s): L.C. is named as a co-inventor on the granted patent: US 9,822,368; EP 3083959; JP 6490077; L.C. is named as a co-inventor on the patent application WO 2018/189225. A.S., M.B., M.D.V., and L.C. are named as co-inventors on patent application IT 102019000004929.
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