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. 2021 Feb 2;33(2):300-318.e12.
doi: 10.1016/j.cmet.2020.12.016. Epub 2021 Jan 8.

Caloric Restriction Promotes Immunometabolic Reprogramming Leading to Protection from Tuberculosis

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Caloric Restriction Promotes Immunometabolic Reprogramming Leading to Protection from Tuberculosis

Carla Palma et al. Cell Metab. .

Abstract

There is a strong relationship between metabolic state and susceptibility to Mycobacterium tuberculosis (MTB) infection, with energy metabolism setting the basis for an exaggerated immuno-inflammatory response, which concurs with MTB pathogenesis. Herein, we show that controlled caloric restriction (CR), not leading to malnutrition, protects susceptible DBA/2 mice against pulmonary MTB infection by reducing bacterial load, lung immunopathology, and generation of foam cells, an MTB reservoir in lung granulomas. Mechanistically, CR induced a metabolic shift toward glycolysis, and decreased both fatty acid oxidation and mTOR activity associated with induction of autophagy in immune cells. An integrated multi-omics approach revealed a specific CR-induced metabolomic, transcriptomic, and proteomic signature leading to reduced lung damage and protective remodeling of lung interstitial tightness able to limit MTB spreading. Our data propose CR as a feasible immunometabolic manipulation to control MTB infection, and this approach offers an unexpected strategy to boost immunity against MTB.

Keywords: T cells; adipose tissue; body weight; caloric restriction; immune response; immunometabolism; infection; tuberculosis.

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Declaration of Interests Authors declare no competing interests.

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