Targeted protein degradation in mycobacteria uncovers antibacterial effects and potentiates antibiotic efficacy

Author:

Won Harim I.ORCID,Zinga SamuelORCID,Kandror Olga,Akopian Tatos,Wolf Ian D.,Schweber Jessica T. P.,Schmid Ernst W.,Chao Michael C.ORCID,Waldor Maya,Rubin Eric J.ORCID,Zhu Junhao

Abstract

AbstractProteolysis-targeting chimeras (PROTACs) represent a new therapeutic modality involving selectively directing disease-causing proteins for degradation through proteolytic systems. Our ability to exploit targeted protein degradation (TPD) for antibiotic development remains nascent due to our limited understanding of which bacterial proteins are amenable to a TPD strategy. Here, we use a genetic system to model chemically-induced proximity and degradation to screen essential proteins in Mycobacterium smegmatis (Msm), a model for the human pathogen M. tuberculosis (Mtb). By integrating experimental screening of 72 protein candidates and machine learning, we find that drug-induced proximity to the bacterial ClpC1P1P2 proteolytic complex leads to the degradation of many endogenous proteins, especially those with disordered termini. Additionally, TPD of essential Msm proteins inhibits bacterial growth and potentiates the effects of existing antimicrobial compounds. Together, our results provide biological principles to select and evaluate attractive targets for future Mtb PROTAC development, as both standalone antibiotics and potentiators of existing antibiotic efficacy.

Funder

U.S. Department of Health & Human Services | NIH | National Institute of Allergy and Infectious Diseases

Private funding provided by Grace Wang and Josef Tatelbaum.

National Science Foundation

The Harvard GSAS Herchel Smith Graduate Fellowship and the Marcus Urann Graduate Fellowship.

U.S. Department of Health & Human Services | NIH | National Institute of General Medical Sciences

Publisher

Springer Science and Business Media LLC

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