Antimycobacterial Rufomycin Analogues from Streptomyces atratus Strain MJM3502

Zhou, Bin; Shetye, Gauri; Yu, Yang; Santarsiero, Bernard D.; Klein, Larry L.; Abad-Zapatero, Cele; Wolf, Nina M.; Cheng, Jinhua; Jin, Yingyu; Lee, Hanki; Suh, Joo-Won; Lee, Hyun; Bisson, Jonathan; McAlpine, James B.; Chen, Shao-Nong; Cho, Sang-Hyun; Franzblau, Scott G.; Pauli, Guido F.

doi:10.1021/acs.jnatprod.9b01095.s002

np9b01095_si_002.pdf (7.57 MB)

Antimycobacterial Rufomycin Analogues from Streptomyces atratus Strain MJM3502

journal contribution

posted on 2020-02-07, 14:10 authored by Bin Zhou, Gauri Shetye, Yang Yu, Bernard D. Santarsiero, Larry L. Klein, Cele Abad-Zapatero, Nina M. Wolf, Jinhua Cheng, Yingyu Jin, Hanki Lee, Joo-Won Suh, Hyun Lee, Jonathan Bisson, James B. McAlpine, Shao-Nong Chen, Sang-Hyun Cho, Scott G. Franzblau, Guido F. Pauli

This study represents a systematic chemical and biological study of the rufomycin (RUF) class of cyclic heptapeptides, which our anti-TB drug discovery efforts have identified as potentially promising anti-TB agents that newly target the caseinolytic protein C1, ClpC1. Eight new RUF analogues, rufomycins NBZ1–NBZ8 (1–8), as well as five known peptides (9–13) were isolated and characterized from the Streptomyces atratus strain MJM3502. Advanced Marfey’s and X-ray crystallographic analysis led to the assignment of the absolute configuration of the RUFs. Several isolates exhibited potent activity against both pathogens M. tuberculosis H37Rv and M. abscessus, paired with favorable selectivity (selectivity index >60), which collectively underscores the promise of the rufomycins as potential anti-TB drug leads.