Synergistic convergence of microbiota-specific systemic IgG and secretory IgA

Fadlallah, Jehane; Sterlin, Delphine; Fieschi, Claire; Parizot, Christophe; Dorgham, Karim; Kafsi, Hela El; Autaa, Gaëlle; Ghillani‐Dalbin, Pascale; Juste, Catherine; Lepage, Patricia; Malphettes, Marion; Galicier, Lionel; Boutboul, David; Clément, Karine; André, Sébastien; Marquet, Florian; Trésallet, Christophe; Mathian, Alexis; Miyara, Makoto; Oksenhendler, Éric; Amoura, Zahir; Yssel, Hans; Larsen, Martin; Gorochov, Guy

doi:10.1016/j.jaci.2018.09.036

Cited by 79 publications

(95 citation statements)

References 39 publications

(46 reference statements)

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“…In the lamina propria, B cells may also switch into IgA in a T cell-independent way (21). The T cell-independent generation of SIgA by B cells may represent a mechanism to generate IgA expressing a wide repertoire of Ig genes, useful to face the thousands of different bacterial species of the microbiota (23,24,42), and to control host-microbiota mutualism, reducing the risk of bacterial translocation and immune activation (43)(44)(45). IgM memory B cells have been shown to home to the gut and to locally switch to IgA (21,46).…”

Section: Discussionmentioning

confidence: 99%

Lack of Gut Secretory Immunoglobulin A in Memory B-Cell Dysfunction-Associated Disorders: A Possible Gut-Spleen Axis

et al. 2020

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Background: B-1a B cells and gut secretory IgA (SIgA) are absent in asplenic mice. Human immunoglobulin M (IgM) memory B cells, which are functionally equivalent to mouse B-1a B cells, are reduced after splenectomy. Objective: To demonstrate whether IgM memory B cells are necessary for generating IgA-secreting plasma cells in the human gut. Methods: We studied intestinal SIgA in two disorders sharing the IgM memory B cell defect, namely asplenia, and common variable immune deficiency (CVID). Results: Splenectomy was associated with reduced circulating IgM memory B cells and disappearance of intestinal IgA-secreting plasma cells. CVID patients with reduced circulating IgM memory B cells had a reduced frequency of gut IgA + plasma cells and a disrupted film of SIgA on epithelial cells. Toll-like receptor 9 (TLR9) and transmembrane activator and calcium-modulator and cyclophilin ligand interactor (TACI) induced IgM memory B cell differentiation into IgA + plasma cells in vitro. In the human gut, TACI-expressing IgM memory B cells were localized under the epithelial cell layer where the TACI ligand a proliferation inducing ligand (APRIL) was extremely abundant. Conclusions: Circulating IgM memory B cell depletion was associated with a defect of intestinal IgA-secreting plasma cells in asplenia and CVID. The observation that IgM memory B cells have a distinctive role in mucosal protection suggests the existence of a functional gut-spleen axis.

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Section: Discussionmentioning

confidence: 99%

Lack of Gut Secretory Immunoglobulin A in Memory B-Cell Dysfunction-Associated Disorders: A Possible Gut-Spleen Axis

et al. 2020

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“…As is well-known, some patients with selective IgA deficiency show clinically asymptomatic or mild infections but have a higher risk of allergy and autoimmunity [61]. Researches show that both secretory IgM and systemic IgG can replace part of sIgA and establish the second defense line [62,63]. Is sIgA a redundant component in the immune system?…”

Section: Siga and Commensal Organismsmentioning

confidence: 99%

The Effects of Secretory IgA in the Mucosal Immune System

Jin

Chen

2020

BioMed Research International

145

117

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Immunoglobulin A (IgA) is the most abundant antibody isotype in the mucosal immune system. Structurally, IgA in the mucosal surface is a polymeric structure, while serum IgA is monomeric. Secretory IgA (sIgA) is one of the polymeric IgAs composed of dimeric IgA, J chain, and secretory component (SC). Most of sIgAs were generated by gut and have effects in situ. Besides the function of “immune exclusion,” a nonspecific immune role, recent studies found it also played an important role in the specific immunity and immunoregulation. Thanks to the critical role of sIgA during the mucosal immune system homeostasis between commensal microorganisms and pathogens; it has been an important field exploring the relationship between sIgA and commensal microorganisms.

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“…The disruption of this feedback loop by low IgA levels and an unhealthy microbiome leads to reduction in T R cells and subsequent immune dysregulation. Importantly, systemic IgG responses may be significant in preventing inflammation in those with IgA deficiency as a consequence of microbial dysbiosis (107). Such protective IgG responses may be significantly impaired in some CVID patients, thus predisposing to inflammation and, potentially, autoimmune disease.…”

Section: Microbiome In Cvid and Autoimmunitymentioning

confidence: 99%

Current Understanding and Recent Developments in Common Variable Immunodeficiency Associated Autoimmunity

Gereige

Maglione

2019

Front. Immunol.

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Common variable immunodeficiency (CVID) is the most prevalent symptomatic primary immunodeficiency and comprises a group of disorders with similar antibody deficiency but a myriad of different etiologies, most of which remain undefined. The variable aspect of CVID refers to the approximately half of patients who develop non-infectious complications in addition to heightened susceptibility to infection. The pathogenesis of these complications is poorly understood and somewhat counterintuitive because these patients that are defined by their immune futility simultaneously have elevated propensity for autoimmune disease. There are numerous aspects of immune dysregulation associated with autoimmunity in CVID that have only begun to be studied. These findings include elevations of T helper type 1 and follicular helper T cells and B cells expressing low levels of CD21 as well as reciprocal decreases in regulatory T cells and isotype-switched memory B cells. Recently, advances in genomics have furthered our understanding of the fundamental biology underlying autoimmunity in CVID and led to precision therapeutic approaches. However, these genetic etiologies are also associated with clinical heterogeneity and incomplete penetrance, highlighting the fact that continued research efforts remain necessary to optimize treatment. Additional factors, such as commensal microbial dysbiosis, remain to be better elucidated. Thus, while recent advances in our understanding of CVID-associated autoimmunity have been exciting and substantial, these current scientific advances must now serve as building blocks for the next stages of discovery.

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Synergistic convergence of microbiota-specific systemic IgG and secretory IgA

Cited by 79 publications

References 39 publications

Lack of Gut Secretory Immunoglobulin A in Memory B-Cell Dysfunction-Associated Disorders: A Possible Gut-Spleen Axis

Lack of Gut Secretory Immunoglobulin A in Memory B-Cell Dysfunction-Associated Disorders: A Possible Gut-Spleen Axis

The Effects of Secretory IgA in the Mucosal Immune System

Current Understanding and Recent Developments in Common Variable Immunodeficiency Associated Autoimmunity

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