Controlled human infection with Mycobacterium tuberculosis: practical considerations for clinical trials

Chetan Seshadri; Jo Anne L. Flynn; Pauline Maiello; Dirk Schnappinger; Robert J. Wilkinson; Stephen B. Gordon; Henry C. Mwandumba; Kondwani C. Jambo; Daniel F. Hoft; Eric J. Rubin; Euzebiusz Jamrozik; Sarah M. Fortune; James G. Kublin

doi:10.1016/j.lanmic.2025.101278

Controlled human infection with Mycobacterium tuberculosis: practical considerations for clinical trials

Chetan Seshadri
, Jo Anne L. Flynn
, Pauline Maiello
, Dirk Schnappinger
, Robert J. Wilkinson
, Stephen B. Gordon
, Henry C. Mwandumba
, Kondwani C. Jambo
, Daniel F. Hoft
, Eric J. Rubin
, Euzebiusz Jamrozik
, Sarah M. Fortune
, James G. Kublin

Clinical Sciences

University of Washington
Seattle Tuberculosis Research Advancement Center
University of Pittsburgh
Cornell University
University of Cape Town
Imperial College London
Mill Hill Laboratory
University of Edinburgh
Kamuzu University of Health Sciences
Saint Louis University
Harvard University
Department of Infectious Diseases
University of Oxford
Fred Hutchinson Cancer Research Center

Research output: Contribution to journal › Article › peer-review

1 Citation (Scopus)

Abstract

Controlled human infection models (CHIMs) can accelerate vaccine development for infectious diseases. Mycobacterium tuberculosis is a human-adapted pathogen that is the leading infectious cause of death worldwide. M tuberculosis infection results in a spectrum of clinical outcomes that are incompletely modelled in animals. To date, the risks of infection, prolonged treatment, and sequelae related to CHIMs with M tuberculosis have been considered ethically unacceptable. However, recent advances in bacterial engineering have resulted in safe strains that could permit M tuberculosis CHIM studies with reduced risks. In this Personal View, we address the practical considerations for conducting a pulmonary M tuberculosis CHIM study. We summarise the ethical issues of M tuberculosis CHIM studies in tuberculosis-endemic and non-endemic settings; describe safety considerations, such as optimising the challenge dose and minimising risks to third parties; and outline and prioritise clinical, microbiological, immunological, and radiological endpoints that would render such a model useful for vaccine development.

Original language	English
Article number	101278
Journal	The Lancet Microbe
Volume	7
Issue number	3
DOIs	https://doi.org/10.1016/j.lanmic.2025.101278
Publication status	Published - 23 Jan 2026

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SDG 3 Good Health and Well-being

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1-s2.0-S266652472500206X-mainFinal published version, 1.83 MBLicence: CC BY-NC-ND

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Seshadri, C., Flynn, J. A. L., Maiello, P., Schnappinger, D., Wilkinson, R. J., Gordon, S. B., Mwandumba, H. C., Jambo, K. C., Hoft, D. F., Rubin, E. J., Jamrozik, E., Fortune, S. M., & Kublin, J. G. (2026). Controlled human infection with Mycobacterium tuberculosis: practical considerations for clinical trials. The Lancet Microbe, 7(3), Article 101278. https://doi.org/10.1016/j.lanmic.2025.101278

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abstract = "Controlled human infection models (CHIMs) can accelerate vaccine development for infectious diseases. Mycobacterium tuberculosis is a human-adapted pathogen that is the leading infectious cause of death worldwide. M tuberculosis infection results in a spectrum of clinical outcomes that are incompletely modelled in animals. To date, the risks of infection, prolonged treatment, and sequelae related to CHIMs with M tuberculosis have been considered ethically unacceptable. However, recent advances in bacterial engineering have resulted in safe strains that could permit M tuberculosis CHIM studies with reduced risks. In this Personal View, we address the practical considerations for conducting a pulmonary M tuberculosis CHIM study. We summarise the ethical issues of M tuberculosis CHIM studies in tuberculosis-endemic and non-endemic settings; describe safety considerations, such as optimising the challenge dose and minimising risks to third parties; and outline and prioritise clinical, microbiological, immunological, and radiological endpoints that would render such a model useful for vaccine development.",

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AU - Gordon, Stephen B.

AU - Mwandumba, Henry C.

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AU - Hoft, Daniel F.

AU - Rubin, Eric J.

AU - Jamrozik, Euzebiusz

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AB - Controlled human infection models (CHIMs) can accelerate vaccine development for infectious diseases. Mycobacterium tuberculosis is a human-adapted pathogen that is the leading infectious cause of death worldwide. M tuberculosis infection results in a spectrum of clinical outcomes that are incompletely modelled in animals. To date, the risks of infection, prolonged treatment, and sequelae related to CHIMs with M tuberculosis have been considered ethically unacceptable. However, recent advances in bacterial engineering have resulted in safe strains that could permit M tuberculosis CHIM studies with reduced risks. In this Personal View, we address the practical considerations for conducting a pulmonary M tuberculosis CHIM study. We summarise the ethical issues of M tuberculosis CHIM studies in tuberculosis-endemic and non-endemic settings; describe safety considerations, such as optimising the challenge dose and minimising risks to third parties; and outline and prioritise clinical, microbiological, immunological, and radiological endpoints that would render such a model useful for vaccine development.

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Controlled human infection with Mycobacterium tuberculosis: practical considerations for clinical trials

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