| Literature DB >> 35830852 |
Hao Shao1, Shuhei Taguwa2, Luke Gilbert3, Arielle Shkedi4, Sara Sannino5, Christopher J Guerriero5, Zachary J Gale-Day4, Zapporah T Young4, Jeffrey L Brodsky5, Jonathan Weissman6, Jason E Gestwicki7, Judith Frydman8.
Abstract
The potential of small molecules to localize within subcellular compartments is rarely explored. To probe this question, we measured the localization of Hsp70 inhibitors using fluorescence microscopy. We found that even closely related analogs had dramatically different distributions, with some residing predominantly in the mitochondria and others in the ER. CRISPRi screens supported this idea, showing that different compounds had distinct chemogenetic interactions with Hsp70s of the ER (HSPA5/BiP) and mitochondria (HSPA9/mortalin) and their co-chaperones. Moreover, localization seemed to determine function, even for molecules with conserved binding sites. Compounds with distinct partitioning have distinct anti-proliferative activity in breast cancer cells compared with anti-viral activity in cellular models of Dengue virus replication, likely because different sets of Hsp70s are required in these processes. These findings highlight the contributions of subcellular partitioning and chemogenetic interactions to small molecule activity, features that are rarely explored during medicinal chemistry campaigns.Entities:
Keywords: Hsp70; allosteric inhibitors; anti-cancer; antivirals; chaperones; chemical biology; subcellular localization
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Year: 2022 PMID: 35830852 PMCID: PMC9513760 DOI: 10.1016/j.chembiol.2022.06.006
Source DB: PubMed Journal: Cell Chem Biol ISSN: 2451-9448 Impact factor: 9.039