Commensal bacteria–derived signals regulate basophil hematopoiesis and allergic inflammation

Hill, David R.C.; Siracusa, Mark C.; Abt, Michael C.; Kim, Brian; Kobuley, Dmytro; Kubo, Masato; Kambayashi, Taku; LaRosa, David F.; Renner, Ellen D.; Orange, Jordan S.; Bushman, Frederic D.; Artis, David

doi:10.1038/nm.2657

Cited by 401 publications

(348 citation statements)

References 57 publications

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“…As expected for GF conditions (16,17), serum IgE was elevated in GF-WT mice compared with CNV.WT mice, and 53BP1 deficiency suppressed this elevation (Fig. S6), consistent with the absence of cCSR in 53BP1-deficient mice.…”

Section: Significancesupporting

confidence: 84%

IgD class switching is initiated by microbiota and limited to mucosa-associated lymphoid tissue in mice

Choi

Wang

Zhang

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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Class-switch recombination (CSR) alters the Ig isotype to diversify antibody effector functions. IgD CSR is a rare event, and its regulation is poorly understood. We report that deficiency of 53BP1, a DNA damage-response protein, caused age-dependent overproduction of secreted IgD resulting from increased IgD CSR exclusively within B cells of mucosa-associated lymphoid tissues. IgD overproduction was dependent on activation-induced cytidine deaminase, hematopoietic MyD88 expression, and an intact microbiome, against which circulating IgD, but not IgM, was reactive. IgD CSR occurred via both alternative nonhomologous end-joining and homologous recombination pathways. Microbiota-dependent IgD CSR also was detected in nasal-associated lymphoid tissue of WT mice. These results identify a pathway, present in WT mice and hyperactivated in 53BP1-deficient mice, by which microbiota signal via Toll-like receptors to elicit IgD CSR.

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Section: Significancesupporting

confidence: 84%

IgD class switching is initiated by microbiota and limited to mucosa-associated lymphoid tissue in mice

Choi

Wang

Zhang

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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“…In a murine model of allergic airway disease, germ-free mice exhibit more severe disease than conventionally housed controls, an effect that could be ameliorated by recolonization with conventional microbiota (57). Similar results were found when disturbance of the gut microbiome was induced by administration of antibiotics in drinking water or by an antibiotic-fungal microbiota combination (42,58). Microbial colonization early in life regulates mucosal invariant natural killer T-cell tolerance and can impact immune responses at mucosal sites later in adulthood (59).…”

Section: State Of the Art S24mentioning

confidence: 57%

A Brave New World: The Lung Microbiota in an Era of Change

Segal

Blaser

2014

Annals ATS

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“…One protocol using a cocktail of 4 antibiotics for 4-5 weeks has been exceptionally popular among investigators and allowed to demonstrate the involvement of microbiota in host functions and disease pathogenesis in a variety of models. [29][30][31][32] Furthermore, a few studies compared both germfree and antibiotic-treated animals and detected concordant results. 31,33 However, concordant results are not always observed between these 2 models.…”

Section: Introductionmentioning

confidence: 84%

“…[29][30][31][32] Furthermore, a few studies compared both germfree and antibiotic-treated animals and detected concordant results. 31,33 However, concordant results are not always observed between these 2 models. For example, in an animal model of common variable immunodeficiency (CVID) associated enteropathy (in B lymphocyte deficient mice), we found that derivation of B cell knockout (BcKO) and control mice as germfree abolished differences in the host phenotype between the 2 genotypes observed in conventional mice ( Fig.…”

Section: Introductionmentioning

confidence: 84%

Investigating a holobiont: Microbiota perturbations and transkingdom networks

et al. 2016

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The scientific community has recently come to appreciate that, rather than existing as independent organisms, multicellular hosts and their microbiota comprise a complex evolving superorganism or metaorganism, termed a holobiont. This point of view leads to a re-evaluation of our understanding of different physiological processes and diseases. In this paper we focus on experimental and computational approaches which, when combined in one study, allowed us to dissect mechanisms (traditionally named host-microbiota interactions) regulating holobiont physiology. Specifically, we discuss several approaches for microbiota perturbation, such as use of antibiotics and germ-free animals, including advantages and potential caveats of their usage. We briefly review computational approaches to characterize the microbiota and, more importantly, methods to infer specific components of microbiota (such as microbes or their genes) affecting host functions. One such approach called transkingdom network analysis has been recently developed and applied in our study. 1 Finally, we also discuss common methods used to validate the computational predictions of host-microbiota interactions using in vitro and in vivo experimental systems.

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Commensal bacteria–derived signals regulate basophil hematopoiesis and allergic inflammation

Cited by 401 publications

References 57 publications

IgD class switching is initiated by microbiota and limited to mucosa-associated lymphoid tissue in mice

IgD class switching is initiated by microbiota and limited to mucosa-associated lymphoid tissue in mice

A Brave New World: The Lung Microbiota in an Era of Change

Investigating a holobiont: Microbiota perturbations and transkingdom networks

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