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Review of a novel disease entity immunoglobulin G4-related disease

机译:审查新的疾病实体免疫球蛋白G4相关疾病

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摘要

Immunoglobulin G4 (IgG4)-related dacryoadenitis and sialoadenitis (IgG4-DS) are part of a multiorgan fibroinflammatory condition of unknown etiology termed IgG4-related disease (IgG4-RD), which has been recognized as a single diagnostic entity for less than 15 years. Histopathologic examination is critical for diagnosis of IgG4-RD. CD4+ T and B cells, including IgG4-expressing plasma cells, constitute the major inflammatory cell populations in IgG4-RD and are thought to cause organ damage and tissue fibrosis. Patients with IgG4-RD who have active, untreated disease exhibit significant increase of IgG4-secreting plasmablasts in the blood. Considerable insight into the immunologic mechanisms of IgG4-RD has been achieved in the last decade using novel molecular biology approaches, including next-generation and single-cell RNA sequencing. Exploring the interactions between CD4+ T cells and B lineage cells is critical for understanding the pathophysiology of IgG4-RD. Establishment of pathogenic T cell clones and identification of antigens specific to these clones constitutes the first steps in determining the pathogenesis of the disease. Herein, the clinical features and mechanistic insights regarding pathogenesis of IgG4-RD were reviewed.
机译:免疫球蛋白G4(IgG4)相关的泪腺炎和唾液腺炎(IgG4-DS)是病因不明的多器官纤维炎性疾病的一部分,被称为IgG4相关疾病(IgG4-RD),该疾病被认为是单一诊断实体不到15年。组织病理学检查对IgG4-RD的诊断至关重要。 CD4 + T和B细胞,包括表达IgG4的浆细胞,构成IgG4-RD中的主要炎症细胞群体,被认为会引起器官损伤和组织纤维化。患有未经治疗的活动性疾病的IgG4-RD患者的血液中分泌IgG4的浆母细胞显着增加。在最近十年中,使用新型分子生物学方法(包括下一代和单细胞RNA测序)对IgG4-RD的免疫学机制有了相当深入的了解。探索CD4 + T细胞和B谱系细胞之间的相互作用对于理解IgG4-RD的病理生理至关重要。病原性T细胞克隆的建立和对这些克隆特异的抗原的鉴定是确定疾病发病机理的第一步。在此,综述了有关IgG4-RD发病机理的临床特征和机理见解。

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