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首页> 外文期刊>International journal of rheumatology >IgG4-Related Fibrotic Diseases from an Immunological Perspective: Regulators out of Control?
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IgG4-Related Fibrotic Diseases from an Immunological Perspective: Regulators out of Control?

机译:从免疫学角度看与IgG4相关的纤维化疾病:调节剂失控了吗?

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Patients with autoimmune pancreatitis have a striking polyclonal elevation of total IgG4 in serum. This observation has been confirmed and extended to other fibrotic conditions (that are therefore called IgG4-related disease) but as yet remains unexplained. The affected tissue contains many IgG4-producing plasma cells embedded in a fibrotic matrix originating from activated mesenchymal (stellate) cells. We propose that the process results from an unusual interaction between two regulatory systems: the regulatory arm of the immune system (including Bregs) and the tissue repair regulatory components orchestrated by the activated stellate cell. This interaction results in ongoing mutual activation, generating TGFbeta, IL10, and vitamin D. This environment suppresses most immune reactions but stimulates the development of IgG4-producing plasma cells.
机译:自身免疫性胰腺炎患者的血清总IgG4明显升高。该观察已得到证实,并已扩展到其他纤维化疾病(因此被称为IgG4相关疾病),但仍无法解释。受影响的组织包含许多产自活化的间充质(星状)细胞的纤维化基质中嵌入的产生IgG4的浆细胞。我们认为该过程是由两个调节系统之间的异常相互作用导致的:免疫系统的调节臂(包括Bregs)和活化星状细胞精心组织的组织修复调节成分。这种相互作用导致持续的相互激活,生成TGFbeta,IL10和维生素D。这种环境抑制了大多数免疫反应,但刺激了产生IgG4的浆细胞的发育。

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