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Braking the system: the aryl hydrocarbon receptor controls monocytes in homeostasis
Jessica E. Kenison, Francisco J. Quintana
Jessica E. Kenison, Francisco J. Quintana
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Commentary

Braking the system: the aryl hydrocarbon receptor controls monocytes in homeostasis

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Abstract

The aryl hydrocarbon receptor (AhR) is increasingly recognized as a physiologic modulator of the immune response, a function that extends beyond its established role as a sensor for environmental xenobiotics. In a recent report published in the JCI, Cros et al. demonstrate that the AhR restrains tonic, microbiota-driven inflammatory cytokine production in monocytes. Through the combined use of murine models, human ex vivo systems, and the analysis of patient-derived data, Cros and coworkers established that the AhR limits stimulator of IFN gene–induced (STING-induced) proinflammatory signals. These findings define cell type–specific physiologic roles for the AhR in the regulation of innate immunity and underscore its potential as a therapeutic target for the treatment of inflammatory and autoimmune diseases.

Authors

Jessica E. Kenison, Francisco J. Quintana

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Figure 1

The AhR functions as a homeostatic brake on monocyte responses to microbiota.

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The AhR functions as a homeostatic brake on monocyte responses to microb...
(A) The AhR restrains proinflammatory cytokine output by suppressing STING signaling, a function that maintains systemic immune balance. (B) Cros et al. reported that AhR deficiency in monocytes produced a proinflammatory response to tonic sensing of microbiota-derived signals (5).

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ISSN: 0021-9738 (print), 1558-8238 (online)

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