SuFEx-based antitubercular compound irreversibly inhibits Pks13

Inna V Krieger; Paridhi Sukheja; Baiyuan Yang; Su Tang; Daniel Selle; Ashley Woods; Curtis Engelhart; Pradeep Kumar; Michael B Harbut; Dongdong Liu; Brendan Tsuda; Bo Qin; Grant A L Bare; Gencheng Li; Victor Chi; Julian Gambacurta; Janine Hvizdos; Matthew Reagan; Isabelle L Jones; Lisa M Massoudi; Lisa K Woolhiser; Alessandro Cascioferro; Erica Kundrick; Parul Singh; William Reiley; Thomas R Ioerger; Dilipkumar Reddy Kandula; Jacob W McCabe; Taijie Guo; David Alland; Helena I Boshoff; Dirk Schnappinger; Gregory T Robertson; Khisi Mdluli; Kyoung-Jin Lee; Jiajia Dong; Shuangwei Li; Peter G Schultz; Sean B Joseph; Melissa S Love; K Barry Sharpless; H Michael Petrassi; Arnab K Chatterjee; James C Sacchettini; Case W McNamara

doi:10.1038/s41586-025-09286-3

SuFEx-based antitubercular compound irreversibly inhibits Pks13

Nature. 2025 Sep;645(8081):755-763. doi: 10.1038/s41586-025-09286-3. Epub 2025 Jul 30.

Authors

Inna V Krieger^#¹, Paridhi Sukheja^#², Baiyuan Yang^#², Su Tang¹, Daniel Selle¹, Ashley Woods², Curtis Engelhart³, Pradeep Kumar^{4

5}, Michael B Harbut², Dongdong Liu², Brendan Tsuda², Bo Qin², Grant A L Bare⁶, Gencheng Li⁶, Victor Chi², Julian Gambacurta⁷, Janine Hvizdos⁷, Matthew Reagan⁷, Isabelle L Jones⁷, Lisa M Massoudi⁸, Lisa K Woolhiser⁸, Alessandro Cascioferro², Erica Kundrick², Parul Singh^{4

5}, William Reiley⁷, Thomas R Ioerger⁹, Dilipkumar Reddy Kandula¹⁰, Jacob W McCabe¹⁰, Taijie Guo¹¹, David Alland^{4

5}, Helena I Boshoff¹², Dirk Schnappinger³, Gregory T Robertson⁸, Khisi Mdluli¹³, Kyoung-Jin Lee², Jiajia Dong¹¹, Shuangwei Li², Peter G Schultz^{2

14}, Sean B Joseph², Melissa S Love², K Barry Sharpless⁶, H Michael Petrassi², Arnab K Chatterjee², James C Sacchettini¹⁵, Case W McNamara¹⁶

Affiliations

¹ Department of Biochemistry and Biophysics, Texas A&M University, College Station, TX, USA.
² Calibr-Skaggs Institute for Innovative Medicines, A Division of Scripps Research, La Jolla, CA, USA.
³ Department of Microbiology and Immunology, Weill Cornell Medicine, New York, NY, USA.
⁴ New Jersey Medical School Division of Infectious Disease, Department of Medicine, Rutgers University, Newark, NJ, USA.
⁵ Ruy V. Lourenco Center for the Study of Emerging and Re-emerging Pathogens, Rutgers University, Newark, NJ, USA.
⁶ Department of Chemistry, The Scripps Research Institute, La Jolla, CA, USA.
⁷ Trudeau Institute, Saranac Lake, NY, USA.
⁸ Mycobacteria Research Laboratories, Department of Microbiology, Immunology and Pathology, Colorado State University, Fort Collins, CO, USA.
⁹ Department of Computer Science, Texas A&M University, College Station, TX, USA.
¹⁰ AB Sciex LLC, Framingham, MA, USA.
¹¹ Institute of Translational Medicine, Shanghai Jiao Tong University, Shanghai, China.
¹² Tuberculosis Research Section, Laboratory of Clinical Immunology and Microbiology, National Institute of Allergy and Infectious Diseases (NIAID), National Institutes of Health (NIH), Bethesda, MD, USA.
¹³ Gates Medical Research Institute, Cambridge, MA, USA.
¹⁴ The Department of Chemistry and The Skaggs Institute for Chemical Biology, The Scripps Research Institute, La Jolla, CA, USA.
¹⁵ Department of Biochemistry and Biophysics, Texas A&M University, College Station, TX, USA. sacchett@tamu.edu.
¹⁶ Calibr-Skaggs Institute for Innovative Medicines, A Division of Scripps Research, La Jolla, CA, USA. cmcnamara@scripps.edu.

^# Contributed equally.

Abstract

Mycobacterium tuberculosis (Mtb) remains the world's deadliest bacterial pathogen¹. There is an urgent medical need to develop new drugs that shorten the treatment duration to combat widespread multi-drug-resistant and extensive-drug-resistant Mtb. Here, we present a preclinical covalent compound, CMX410, that contains an aryl fluorosulfate (SuFEx)² warhead and uniquely targets the acyltransferase domain of Pks13, an essential enzyme in cell-wall biosynthesis. CMX410 is equipotent against drug-sensitive and drug-resistant strains of Mtb and efficacious in multiple mouse models of infection. Inhibition by CMX410 is irreversible through a previously undescribed mechanism: CMX410 reacts with the catalytic serine of the AT domain of Pks13, rapidly and irreversibly disabling the active site by forming a β-lactam. CMX410 is highly selective for its target and thus demonstrates excellent pharmacological and safety profiles, including no adverse effects in a 14-day rat toxicity study up to 1,000 mg kg^-1 per day. The distinctive mode of action from current drugs, high potency across all tested clinical isolates, oral bioavailability, favourable performance in drug combination testing and superior pharmacological and safety characteristics make CMX410 a promising first-in-class candidate to replace outdated cell-wall biosynthesis inhibitors, such as isoniazid and ethambutol, in tuberculosis regimens.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

Animals
Antitubercular Agents* / adverse effects
Antitubercular Agents* / chemistry
Antitubercular Agents* / pharmacokinetics
Antitubercular Agents* / pharmacology
Antitubercular Agents* / therapeutic use
Bacterial Proteins* / antagonists & inhibitors
Bacterial Proteins* / chemistry
Bacterial Proteins* / metabolism
Catalytic Domain / drug effects
Cell Wall / drug effects
Cell Wall / enzymology
Disease Models, Animal
Female
Humans
Male
Mice
Microbial Sensitivity Tests
Mycobacterium tuberculosis* / drug effects
Mycobacterium tuberculosis* / enzymology
Rats
Tuberculosis / drug therapy
Tuberculosis / microbiology

Substances

Antitubercular Agents
Bacterial Proteins

Grants and funding

P01 AI095208/AI/NIAID NIH HHS/United States