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Active- and Allosteric-Site Cyclic Peptide Inhibitors of Secreted M. tuberculosis Chorismate Mutase

ACS Infectious Diseases. 2025-03; 
Renier H P van Neer, Patricia K Dranchak, Mahesh Aitha, Lijun Liu, Emma K Carlson, Isabella E Jacobsen, Kevin Battaile, Yuhong Fang, Dingyin Tao, Ganesha Rai, Janak Padia, Scott Lovell, Hiroaki Suga, James Inglese
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Peptide Synthesis and high-purity macrocyclic peptides, L2.1 and D1.3, were synthesized by GenScript (Piscataway, NJ). MtbCM HiBiT Tag His10 pET21a+ expression plasmids were prepared by Genscript. Get A Quote
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摘要

The secreted Chorismate mutase enzyme of Mycobacterium tuberculosis (*MtbCM) is an underexplored potential target for the development of new antitubercular agents that are increasingly needed as antibiotic resistance rises in prevalence. As an enzyme suspected to be involved in virulence and host-pathogen interactions, disruption of its function could circumvent the difficulty of treating tuberculosis-infected granulomas. Drug development, however, is limited by novel ligand discovery. Currently, *MtbCM activity is measured by using a low throughput acid/base-mediated product derivatization absorbance assay. Here, we utilized an RNA-display affinity selection approach enabled by the Random Peptides Integrated D... More

關鍵詞

Mycobacterium tuberculosis; allosteric binding; assay development; cyclic peptides; isomerase; ligand displacement
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