Publication date: Available online 23 March 2017
Source:Cell Host & Microbe
Author(s): Tiffany C. Scharschmidt, Kimberly S. Vasquez, Mariela L. Pauli, Elizabeth G. Leitner, Kevin Chu, Hong-An Truong, Margaret M. Lowe, Robert Sanchez Rodriguez, Niwa Ali, Zoltan G. Laszik, Justin L. Sonnenburg, Sarah E. Millar, Michael D. Rosenblum
Regulatory T cells (Tregs) are required to establish immune tolerance to commensal microbes. Tregs accumulate abruptly in the skin during a defined window of postnatal tissue development. However, the mechanisms mediating Treg migration to neonatal skin are unknown. Here we show that hair follicle (HF) development facilitates the accumulation of Tregs in neonatal skin and that upon skin entry these cells localize to HFs, a primary reservoir for skin commensals. Further, germ-free neonates had reduced skin Tregs indicating that commensal microbes augment Treg accumulation. We identified Ccl20 as a HF-derived, microbiota-dependent chemokine and found its receptor, Ccr6, to be preferentially expressed by Tregs in neonatal skin. The Ccl20-Ccr6 pathway mediated Treg migration in vitro and in vivo. Thus, HF morphogenesis, commensal microbe colonization, and local chemokine production work in concert to recruit Tregs into neonatal skin, thereby establishing this tissue Treg niche early in life.
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Teaser
Regulatory T cells (Tregs) accumulate in the skin during a defined window of postnatal development, but the underlying mechanisms are unclear. Scharschmidt et al. demonstrate that microbial colonization of developing hair follicles is required for Treg migration and homing into neonatal skin and is mediated by the Ccl20-Ccr6 pathway.http://ift.tt/2nOUTHq
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