Intestinal inflammation alters the antigen-specific immune response to a skin commensal

肠道炎症会改变针对皮肤共生菌的抗原特异性免疫反应

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作者:Geil R Merana ,Laura R Dwyer ,Miqdad O Dhariwala ,Antonin Weckel ,Jeanmarie R Gonzalez ,Joy N Okoro ,Jarish N Cohen ,Courtney M Tamaki ,Jungmin Han ,Preston Tasoff ,Yasmin Palacios-Calderon ,Connie W Y Ha ,Susan V Lynch ,Julia A Segre ,Heidi H Kong ,Michael G Kattah ,Averil Ma ,Tiffany C Scharschmidt

Abstract

Resident microbes in skin and gut predominantly impact local immune cell function during homeostasis. However, colitis-associated neutrophilic skin disorders suggest possible breakdown of this compartmentalization with disease. Using a model wherein neonatal skin colonization by Staphylococcus epidermidis facilitates generation of commensal-specific tolerance and CD4+ regulatory T cells (Tregs), we ask whether this response is perturbed by gut inflammation. Chemically induced colitis is accompanied by intestinal expansion of S. epidermidis and reduces gut-draining lymph node (dLN) commensal-specific Tregs. It also results in reduced commensal-specific Tregs in skin and skin-dLNs and increased skin neutrophils. Increased CD4+ circulation between gut and skin dLN suggests that the altered cutaneous response is initiated in the colon, and resistance to colitis-induced effects in Cd4creIl1r1fl/fl mice implicate interleukin (IL)-1 in mediating the altered commensal-specific response. These findings provide mechanistic insight into observed connections between inflammatory skin and intestinal diseases.

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