Author:
Wehbi Batoul,Oblet Christelle,Boyer François,Huard Arnaud,Druilhe Anne,Paraf François,Cogné Etienne,Moreau Jeanne,El Makhour Yolla,Badran Bassam,Van Egmond Marjolein,Cogné Michel,Aldigier Jean-Claude
Abstract
BackgroundIgA nephropathy (IgAN) often follows infections and features IgA mesangial deposition. Polymeric IgA deposits in the mesangium seem to have varied pathogenic potential, but understanding their pathogenicity remains a challenge. Most mesangial IgA1 in human IgAN has a hypogalactosylated hinge region, but it is unclear whether this is required for IgA deposition. Another important question is the role of adaptive IgA responses and high-affinity mature IgA antibodies and whether low-affinity IgA produced by innate-like B cells might also yield mesangial deposits.MethodsTo explore the effects of specific qualitative variations in IgA and whether altered affinity maturation can influence IgA mesangial deposition and activate complement, we used several transgenic human IgA1-producing models with IgA deposition, including one lacking the DNA-editing enzyme activation-induced cytidine deaminase (AID), which is required in affinity maturation. Also, to explore the potential role of the IgA receptor CD89 in glomerular inflammation, we used a model that expresses CD89 in a pattern observed in humans.ResultsWe found that human IgA induced glomerular damage independent of CD89. When comparing mice able to produce high-affinity IgA antibodies with mice lacking AID-enabled Ig affinity maturation, we found that IgA deposition and complement activation significantly increased and led to IgAN pathogenesis, although without significant proteinuria or hematuria. We also observed that hinge hypoglycosylation was not mandatory for IgA deposition.ConclusionsIn a mouse model of IgAN, compared with high-affinity IgA, low-affinity innate-like IgA, formed in the absence of normal antigen-driven maturation, was more readily involved in IgA glomerular deposition with pathogenic effects.
Funder
Région Nouvelle-Aquitaine
Chaire d’Immuno-pathologie des Maladies Rénales, Limoges University
Association Limousine pour l’Utilisation du Rein Artificiel à Domicile
Lebanese University and Lebanese National Council for Scientific Research
Publisher
American Society of Nephrology (ASN)
Subject
Nephrology,General Medicine
Cited by
9 articles.
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