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Review
. 2022 Sep:126:105920.
doi: 10.1016/j.bioorg.2022.105920. Epub 2022 Jun 1.

A decade of tail-approach based design of selective as well as potent tumor associated carbonic anhydrase inhibitors

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Review

A decade of tail-approach based design of selective as well as potent tumor associated carbonic anhydrase inhibitors

Amit Kumar et al. Bioorg Chem. 2022 Sep.

Abstract

Human carbonic anhydrase (hCA) isoforms hCA IX and hCA XII are well established anticancer drug targets and their selective inhibition is highly desired for the proper treatment of cancer. Lack of isoform-selectivity in current clinically used CA inhibitors (CAIs) is a major concern as it leads to undesired side effects, associated with off-target inhibition. Thus, there is need to explore alternative approaches for the design of isoform-selective inhibitors and the leading promising approach for the design of isoform-selective CAIs is "the tail-approach". Virtually, most drug design studies in the last decade were done by considering the tail-approach reported in 1999. The past decade of 2010-2020 witnessed progressive maturation of this approach as a large number of CAIs have been designed and synthesised based on it, many of which turned out to be effective as well as selective hCA IX and hCA XII inhibitors. This review covers the past decade (2010-2020) research, considering selective as well as potent inhibitors of tumor associated isoforms, hCA IX and hCA XII, which include newer generation inhibitors containing sulfonamides or their bioisosteres, non-classical inhibitors (including carboxylic acid/ester, coumarin and sulfocoumarin classes) and various other novel classes of inhibitors belonging to newly identified chemotypes/scaffolds.

Keywords: Cancer; Carbonic anhydrase inhibitors; Potent inhibitors; SLC-0111; Selective inhibitors; Tail-approach; hCA IX; hCA XII.

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