New C25 Carbamate Rifamycin Derivatives Are Resistant to Inactivation by ADP-ribosyl Transferases
Overview
Authors
Affiliations
A novel series of 3-morpholino rifamycins in which the C25 acetate group was replaced by a carbamate group were prepared and found to exhibit significantly improved antimicrobial activity than rifampin against Mycobacterium smegmatis. Further characterization of such compounds suggests that relatively large groups attached to the rifamycin core via a C25 carbamate linkage prevent inactivation via ribosylation of the C23 alcohol as catalyzed by the endogenous rifampin ADP-ribosyl transferase of M. smegmatis. SAR studies of the C25 carbamate rifamycin series against M. smegmatis and other bacteria are reported.
C25-modified rifamycin derivatives with improved activity against .
Paulowski L, Beckham K, Johansen M, Berneking L, Van N, Degefu Y PNAS Nexus. 2023; 1(4):pgac130.
PMID: 36714853 PMC: 9802118. DOI: 10.1093/pnasnexus/pgac130.
Redesign of Rifamycin Antibiotics to Overcome ADP-Ribosylation-Mediated Resistance.
Lan T, Ganapathy U, Sharma S, Ahn Y, Zimmerman M, Molodtsov V Angew Chem Int Ed Engl. 2022; 61(45):e202211498.
PMID: 36222275 PMC: 9633546. DOI: 10.1002/anie.202211498.
Kanglemycin A Can Overcome Rifamycin Resistance Caused by ADP-Ribosylation by Arr Protein.
Harbottle J, Mosaei H, Allenby N, Zenkin N Antimicrob Agents Chemother. 2021; 65(12):e0086421.
PMID: 34606341 PMC: 8597724. DOI: 10.1128/AAC.00864-21.
Ganapathy U, Lan T, Krastel P, Lindman M, Zimmerman M, Ho H Antimicrob Agents Chemother. 2021; 65(9):e0097821.
PMID: 34228543 PMC: 8370238. DOI: 10.1128/AAC.00978-21.
Macrocycle-Antibiotic Hybrids: A Path to Clinical Candidates.
Surur A, Sun D Front Chem. 2021; 9:659845.
PMID: 33996753 PMC: 8120311. DOI: 10.3389/fchem.2021.659845.