The gut microbiota posttranslationally modifies IgA1 in autoimmune glomerulonephritis,Science Translational Medicine

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The gut microbiota posttranslationally modifies IgA1 in autoimmune glomerulonephritis
Science Translational Medicine ( IF 17.1 ) Pub Date : 2024-03-27 , DOI: 10.1126/scitranslmed.adl6149
Patrick J. Gleeson _{1,

2,

3} , Nicolas Benech _{4,

5,

6} , Jonathan Chemouny _{1,

7} , Eleftheria Metallinou ₁ , Laureline Berthelot ₁ , Jennifer da Silva ₁ , Julie Bex-Coudrat ₁ , Erwan Boedec ₁ , Fanny Canesi ₁ , Carine Bounaix ₁ , Willy Morelle ₈ , Maryse Moya-Nilges ₉ , John Kenny _{10,

11} , Liam O’Mahony ₂ , Loredana Saveanu ₁ , Bertrand Arnulf ₁₂ , Aurélie Sannier ₁₃ , Eric Daugas _{1,

3} , François Vrtovsnik _{1,

3} , Patricia Lepage ₇ , Harry Sokol _{4,

5,

7} , Renato C. Monteiro _{1,

14}

Affiliation

Université Paris Cité, INSERM UMR1149 and CNRS EMR8252, Centre de Recherche sur l’Inflammation, Inflamex Laboratory of Excellence, Paris 75018, France.
Department of Medicine, School of Microbiology, APC Microbiome Ireland, University College Cork, Cork T12 Y337 Ireland.
AP-HP, Nord/université de Paris, hôpital Bichat-Claude Bernard, Service de Néphrologie, Paris 75018, France.
Sorbonne Université, INSERM, Centre de Recherche Saint-Antoine, CRSA, AP-HP, Saint Antoine Hospital, Gastroenterology Department, Paris 75012, France.
Paris Center for Microbiome Medicine (PaCeMM) FHU, Paris 75012, France.
Hospices Civils de Lyon, Claude Bernard Lyon 1 University, CRCL, 69003 Lyon, France.
Université Paris-Saclay, INRAE, AgroParisTech, Micalis Institute, 78350 Jouy-en-Josas, France.
Université Lille, Centre National de la Recherche Française, UMR 8576-Unité de Glycobiologie Structurale et Fonctionnelle-Unité de Glycobiologie Structurale et Fonctionnelle, F-59000 Lille, France.
Unité Technologie et Service Bioimagerie Ultrastructurale (UTechS UBI), Institut Pasteur, 28 Rue Du Docteur Roux, 75015 Paris, France.
Teagasc Food Research Centre, Moorepark, Fermoy, Co. Cork P61 C996 Ireland.
APC Microbiome Ireland, University College Cork, College Road, Cork, T12 YT20 Ireland.
AP-HP, Nord/université de Paris, hôpital Saint Louis, Service d'Immuno-Hématologie, Myosotis 4, 75010 Paris, France.
AP-HP, Nord/université de Paris, hôpital Bichat-Claude Bernard, Service d'Anatomie-Pathologique, 75018 Paris, France.
AP-HP, Nord/université de Paris, hôpital Bichat-Claude Bernard, Service d’Immunologie, 75018 Paris, France.

Mechanisms underlying the disruption of self-tolerance in acquired autoimmunity remain unclear. Immunoglobulin A (IgA) nephropathy is an acquired autoimmune disease where deglycosylated IgA1 (IgA subclass 1) auto-antigens are recognized by IgG auto-antibodies, forming immune complexes that are deposited in the kidneys, leading to glomerulonephritis. In the intestinal microbiota of patients with IgA nephropathy, there was increased relative abundance of mucin-degrading bacteria, including Akkermansia muciniphila . IgA1 was deglycosylated by A. muciniphila both in vitro and in the intestinal lumen of mice. This generated neo-epitopes that were recognized by autoreactive IgG from the sera of patients with IgA nephropathy. Mice expressing human IgA1 and the human Fc α receptor I (α1 KI -CD89 tg ) that underwent intestinal colonization by A. muciniphila developed an aggravated IgA nephropathy phenotype. After deglycosylation of IgA1 by A. muciniphila in the mouse gut lumen, IgA1 crossed the intestinal epithelium into the circulation by retrotranscytosis and became deposited in the glomeruli of mouse kidneys. Human α-defensins—a risk locus for IgA nephropathy—inhibited growth of A. muciniphila in vitro. A negative correlation observed between stool concentration of α-defensin 6 and quantity of A. muciniphila in the guts of control participants was lost in patients with IgA nephropathy. This study demonstrates that gut microbiota dysbiosis contributes to generation of auto-antigens in patients with IgA nephropathy and in a mouse model of this disease.

中文翻译：

肠道微生物群翻译后修饰自身免疫性肾小球肾炎中的 IgA1

获得性自身免疫中自我耐受破坏的机制仍不清楚。免疫球蛋白 A (IgA) 肾病是一种获得性自身免疫性疾病，其中去糖基化的 IgA1（IgA 亚类 1）自身抗原被 IgG 自身抗体识别，形成免疫复合物沉积在肾脏中，导致肾小球肾炎。在 IgA 肾病患者的肠道微生物群中，粘蛋白降解细菌的相对丰度增加，包括嗜粘液阿克曼氏菌。 IgA1 被去糖基化嗜粘液酸杆菌在体外和小鼠的肠腔中。这产生了新表位，可以被 IgA 肾病患者血清中的自身反应性 IgG 识别。表达人 IgA1 和人 Fc α 受体 I (α1KI-CD89TG）经历了肠道定植嗜粘液酸杆菌出现加重的 IgA 肾病表型。 IgA1 去糖基化后嗜粘液酸杆菌在小鼠肠腔中，IgA1 通过逆转录转胞吞作用穿过肠上皮进入循环系统，并沉积在小鼠肾脏的肾小球中。人类 α-防御素（IgA 肾病的风险位点）抑制生长A. muciniphila 中体外。粪便中α-防御素6浓度与α-防御素6数量呈负相关嗜粘液酸杆菌在 IgA 肾病患者的对照参与者的肠道中丢失了。这项研究表明，肠道微生物群失调会导致 IgA 肾病患者和该疾病的小鼠模型中自身抗原的产生。

更新日期：2024-03-27

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