Literature DB >> 32276965

Gut-resident CX3CR1hi macrophages induce tertiary lymphoid structures and IgA response in situ.

Balázs Koscsó1, Sravya Kurapati1,2, Richard R Rodrigues3, Jelena Nedjic4, Kavitha Gowda5, Changsik Shin5, Chetna Soni5, Azree Zaffran Ashraf1, Indira Purushothaman6, Maryknoll Palisoc7, Sulei Xu8, Haoyu Sun8, Sathi Babu Chodisetti5, Eugene Lin1, Matthias Mack9, Yuka Imamura Kawasawa10, Pingnian He8, Ziaur S M Rahman5, Iannis Aifantis4, Natalia Shulzhenko11, Andrey Morgun3, Milena Bogunovic12,5,13.   

Abstract

Intestinal mononuclear phagocytes (MPs) are composed of heterogeneous dendritic cell (DC) and macrophage subsets necessary for the initiation of immune response and control of inflammation. Although MPs in the normal intestine have been extensively studied, the heterogeneity and function of inflammatory MPs remain poorly defined. We performed phenotypical, transcriptional, and functional analyses of inflammatory MPs in infectious Salmonella colitis and identified CX3CR1+ MPs as the most prevalent inflammatory cell type. CX3CR1+ MPs were further divided into three distinct populations, namely, Nos2 +CX3CR1lo, Ccr7 +CX3CR1int (lymph migratory), and Cxcl13 +CX3CR1hi (mucosa resident), all of which were transcriptionally aligned with macrophages and derived from monocytes. In follow-up experiments in vivo, intestinal CX3CR1+ macrophages were superior to conventional DC1 (cDC1) and cDC2 in inducing Salmonella-specific mucosal IgA. We next examined spatial organization of the immune response induced by CX3CR1+ macrophage subsets and identified mucosa-resident Cxcl13 +CX3CR1hi macrophages as the antigen-presenting cells responsible for recruitment and activation of CD4+ T and B cells to the sites of Salmonella invasion, followed by tertiary lymphoid structure formation and the local pathogen-specific IgA response. Using mice we developed with a floxed Ccr7 allele, we showed that this local IgA response developed independently of migration of the Ccr7 +CX3CR1int population to the mesenteric lymph nodes and contributed to the total mucosal IgA response to infection. The differential activity of intestinal macrophage subsets in promoting mucosal IgA responses should be considered in the development of vaccines to prevent Salmonella infection and in the design of anti-inflammatory therapies aimed at modulating macrophage function in inflammatory bowel disease.
Copyright © 2020 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works.

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Year:  2020        PMID: 32276965      PMCID: PMC7296464          DOI: 10.1126/sciimmunol.aax0062

Source DB:  PubMed          Journal:  Sci Immunol        ISSN: 2470-9468


  104 in total

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Authors:  Casandra Panea; Adam M Farkas; Yoshiyuki Goto; Shahla Abdollahi-Roodsaz; Carolyn Lee; Balázs Koscsó; Kavitha Gowda; Tobias M Hohl; Milena Bogunovic; Ivaylo I Ivanov
Journal:  Cell Rep       Date:  2015-08-13       Impact factor: 9.423

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Journal:  Sci Immunol       Date:  2019-06-14

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6.  Monocyte-like and mature macrophages produce CXCL13 (B cell-attracting chemokine 1) in inflammatory lesions with lymphoid neogenesis.

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Authors:  Naresh S Redhu; Vasudevan Bakthavatchalu; Evan A Conaway; Dror S Shouval; Amy Tsou; Jeremy A Goettel; Amlan Biswas; Chuanwu Wang; Michael Field; Werner Muller; Andre Bleich; Ning Li; Georg K Gerber; Lynn Bry; James G Fox; Scott B Snapper; Bruce H Horwitz
Journal:  Elife       Date:  2017-07-05       Impact factor: 8.140

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2.  A RORγt+ cell instructs gut microbiota-specific Treg cell differentiation.

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Review 7.  Neurodegenerative disorders and gut-brain interactions.

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Review 8.  B cell class switching in intestinal immunity in health and disease.

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Review 9.  T Cell Responses to the Microbiota.

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Review 10.  Know your enemy or find your friend?-Induction of IgA at mucosal surfaces.

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