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Immunity and autoimmunity to dsDNA and chromatin the role of immunogenic DNA-binding proteins and nuclease deficiencies

机译:对dsDNA和染色质的免疫和自身免疫免疫原性DNA结合蛋白和核酸酶缺陷的作用

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Loss of immunological tolerance results in autoimmunity and may finally end in autoimmune disorders. For an autoimmune response against chromatin, autologous chromatin (nucleosomes) is assumed to activate both chromatin-specific B and T cells with a resulting anti-chromatin antibody response. As only fragmental elements of this process have been described, we do not have the full insight to justify this model in vivo. Early experimental immunization with methylated bovine serum albumin-DNA complexes elicited antibodies to various forms of synthetic ssDNA/dsDNA, but notably not to mammalian dsDNA. Thus, for a long time with intense research, the general result was that all forms of ssDNA and dsDNA, but mammalian B helical DNA, had an immunogenic potential. Summarizing these results, a preliminary conclusion was settled, saying that mammalian dsDNA was not immunogenic while other forms of DNA were really immunogenic in the situation where they were in complex with proteins. Recent studies have focused on nuclease deficiencies as a condition where chromatin may be presented to the immune system in an immunogenic form. However, although such deficiencies may provide information as to how chromatin may be exposed and targeted by relevant antibodies, data demonstrate that nuclease deficiencies is not in general correlated with autoimmunity to components of chromatin. This review discusses these topics, and provides information that may explain processes that account for anti-dsDNA antibody responses in vivo.
机译:免疫耐受性的丧失导致自身免疫,并最终可能导致自身免疫疾病。对于针对染色质的自身免疫反应,假定自身染色质(核小体)激活染色质特异性B细胞和T细胞,并产生抗染色质抗体反应。由于仅描述了该过程的片段性元素,因此我们没有充分的见识来证明该模型在体内的合理性。甲基化牛血清白蛋白-DNA复合物的早期实验免疫引发了针对各种形式的合成ssDNA / dsDNA的抗体,但对哺乳动物dsDNA的抗体却没有。因此,经过长时间的深入研究,总的结果是所有形式的ssDNA和dsDNA,但哺乳动物的B螺旋DNA具有免疫原性。总结这些结果,得出初步结论,说哺乳动物dsDNA不具有免疫原性,而其他形式的DNA在与蛋白质复合的情况下确实具有免疫原性。最近的研究集中于核酸酶缺乏症,即染色质可能以免疫原性形式呈递给免疫系统。但是,尽管此类缺陷可能提供有关染色质如何被相关抗体暴露和靶向的信息,但数据表明核酸酶缺陷通常与对染色质成分的自身免疫性无关。这篇综述讨论了这些主题,并提供了可以解释体内抗dsDNA抗体应答的过程的信息。

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