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doi.org/10.1016/j.ejmech.2018.10.068

Enhancement of the tail hydrophobic interactions within the carbonic anhydrase IX active site via structural extension: Design and synthesis of novel N-substituted isatins-SLC-0111 hybrids as carbonic anhydrase inhibitors and antitumor agents

..., Claudiu T. Supuran
128
European Journal of Medicinal Chemistry
Volume: 162, Pages: 147 - 160
Published: Jan 1, 2019
Abstract
Herein we report the design and synthesis of novel N-substituted isatins-SLC-0111 hybrids (6a-f and 9a-l). A structural extension approach was adopted via N-alkylation and N-benzylation of isatin moiety to enhance the tail hydrophobic interactions within the carbonic anhydrase (CA) IX active site. Thereafter, a hybrid pharmacophore approach was utilized via merging the pharmacophoric elements of isatin and SLC-0111 in a single chemical...
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Paper Details
Title
Enhancement of the tail hydrophobic interactions within the carbonic anhydrase IX active site via structural extension: Design and synthesis of novel N-substituted isatins-SLC-0111 hybrids as carbonic anhydrase inhibitors and antitumor agents
DOI
doi.org/10.1016/j.ejmech.2018.10.068
Published Date
Jan 1, 2019
Journal
European Journal of Medicinal Chemistry
Volume
162
Pages
147 - 160
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