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IgM Antibodies Targeting Malondialdehyde Promote Complement-Mediated Liver Injury in Alcohol-Related Liver Disease

IF 5.2 2区医学 Q1 GASTROENTEROLOGY & HEPATOLOGY

Liver International Pub Date : 2025-09-17 DOI:10.1111/liv.70356

Dragana Rajcic, Beatriz Pereira da Silva, Taras Baranovskyi, Benedikt Simbrunner, Benedikt S. Hofer, Constanze Hoebinger, Tereza Duckova, Nikolina Papac-Milicevic, Stephan Listabarth, Sabine Weber, Benjamin Vyssoki, Daniel König, Katharina Burger, Ina Bergheim, Christoph J. Binder, Mattias Mandorfer, Thomas Reiberger, Tim Hendrikx

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Abstract

Background and Aims

Alcohol-related liver disease (ALD) is associated with elevated blood immunoglobulin-type M (IgM) levels and hepatic lipid peroxidation. Nevertheless, the functional relevance of systemic IgM targeting lipid peroxidation products during ALD is incompletely understood.

Methods

Levels of IgM and IgG recognising malondialdehyde–acetaldehyde (MAA), as a hallmark epitope of lipid peroxidation, as well as complement factors were assessed in the serum of patients with ALD. The influence of alcohol abstinence on anti-MAA IgM and IgG levels was determined in AUD patients. A chronic-binge ethanol diet was given to mice deficient in sialic acid-binding immunoglobulin-like lectin G (Siglec-G^−/−), with specifically increased systemic IgM, and mice lacking soluble IgM (sIgM^−/−), and their corresponding littermates. Furthermore, wildtype mice were injected with MAA-binding IgM antibodies (LR04) or isotype control IgM during chronic-binge ethanol feeding. Siglec-G^−/− bone marrow transplantation into wildtype or complement C3 deficient mice (C3^−/−) was performed to investigate the involvement of complement activation by elevated IgM in ALD.

Results

Serum levels of anti-MAA IgM positively correlated with ALD severity in humans. While mice lacking soluble IgM had less pronounced liver injury, increased circulating anti-MAA IgM titers in Siglec-G^−/− mice associated with more hepatocellular damage after ethanol feeding than wildtypes. Similarly, mice receiving LR04 displayed elevated liver injury compared to control-injected mice. Moreover, besides less hepatic neutrophil and macrophage content, and stellate cell activation than wildtypes, ethanol-fed Siglec-G^−/− and LR04-treated mice had increased hepatic C3b deposition. Mice deficient in C3 displayed ameliorated ethanol-induced liver injury compared with controls, despite similarly high anti-MAA IgM levels after Siglec-G^−/− bone marrow transplantation, suggesting complement-dependent liver injury upon high anti-MAA IgM. In line, levels of MAA-binding IgM inversely correlated with C3c and C4 in serum of patients with ALD.

Conclusion

Elevated systemic IgM titres that recognise MDA facilitate complement recruitment, which enhances hepatocyte injury, thereby promoting alcohol-associated liver disease.

Abstract Image

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针对丙二醛的IgM抗体促进酒精相关性肝病补体介导的肝损伤

背景和目的：酒精相关性肝病（ALD）与血液免疫球蛋白型M （IgM）水平升高和肝脂质过氧化有关。然而，ALD期间针对脂质过氧化产物的系统性IgM的功能相关性尚不完全清楚。方法：评估ALD患者血清中识别丙二醛乙醛（MAA）的IgM和IgG水平以及补体因子。MAA是脂质过氧化的标志表位。测定戒酒对AUD患者抗maa IgM和IgG水平的影响。研究人员给缺乏唾液酸结合免疫球蛋白样凝集素G （Siglec-G-/-）的小鼠和缺乏可溶性IgM （sIgM-/-）的小鼠及其相应的窝鼠喂食慢性暴饮乙醇。此外，野生型小鼠在慢性酒精暴食期间注射maa结合IgM抗体（LR04）或同型对照IgM。将siglece - g -/-骨髓移植到野生型或补体C3缺陷小鼠（C3-/-）中，研究IgM升高激活补体在ALD中的作用。结果：人血清抗maa IgM水平与ALD严重程度呈正相关。虽然缺乏可溶性IgM的小鼠的肝损伤不那么明显，但与野生型相比，乙醇喂养后siglece - g -/-小鼠的循环抗maa IgM滴度增加与肝细胞损伤更多相关。同样，与注射对照组小鼠相比，接受LR04的小鼠表现出更高的肝损伤。此外，与野生型相比，siglece - g -/-和lr04处理的小鼠，除了肝脏中性粒细胞和巨噬细胞含量和星状细胞活化较少外，肝脏C3b沉积增加。尽管siglece - g -/-骨髓移植后抗maa IgM水平相似，但与对照组相比，C3缺乏小鼠显示乙醇诱导的肝损伤有所改善，这表明补体依赖性肝损伤是由高抗maa IgM引起的。与此同时，ALD患者血清中maa结合IgM水平与C3c和C4呈负相关。结论：识别MDA的全身IgM滴度升高促进补体募集，从而增强肝细胞损伤，从而促进酒精相关肝病。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Liver International

Liver International 医学-胃肠肝病学

CiteScore

13.90

自引率

4.50%

发文量

348

审稿时长

2 months

期刊介绍： Liver International promotes all aspects of the science of hepatology from basic research to applied clinical studies. Providing an international forum for the publication of high-quality original research in hepatology, it is an essential resource for everyone working on normal and abnormal structure and function in the liver and its constituent cells, including clinicians and basic scientists involved in the multi-disciplinary field of hepatology. The journal welcomes articles from all fields of hepatology, which may be published as original articles, brief definitive reports, reviews, mini-reviews, images in hepatology and letters to the Editor.

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