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Is Tolerance Broken in Autoimmunity?

机译:耐受性在自身免疫中被破坏了吗?

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Autoimmune diseases are classified into about 80 different types based on their specificity related to system, organ and/or tissue. About 5% of the western population is affected by this anomaly, but its worldwide incidence is unknown. Autoimmune diseases are heterogeneous in nature and clinical manifestations range from benign disorders to life-threatening conditions. Autoimmunity strikes at any stage of life, but age and/or gender also play role in onset of some of these anomalies. The autoimmune pathogenesis is initiated by the origination of autoantigens, which leads to the development of autoantibodies followed by auto-immunogenicity and the ultimate onset of autoimmunity. There is a lack of suitable therapies to treat autoimmune diseases, because mechanisms involved in the onset of these anomalies were poorly understood. Present therapies are limited to symptomatic treatment and come with severe side effects. Here, I described the molecular mechanisms and cellular events involved in the initiation of autoimmunity and proposed better strategies to modulate such molecular and cellular anomalies, which will help in preventing and/or controlling autoimmune pathogenesis and ultimately aid in enhancing the quality of life.
机译:根据自身免疫性疾病与系统,器官和/或组织有关的特异性,其可分为约80种不同类型。大约5%的西方人口受此异常影响,但其全球发病率尚不清楚。自身免疫性疾病本质上是异质的,临床表现范围从良性疾病到危及生命的状况。自身免疫在生命的任何阶段都会发作,但是年龄和/或性别在某些此类异常的发作中也起作用。自身免疫的发病机制是由自身抗原的起源引发的,这导致自身抗体的发展,继之以自身免疫原性和自身免疫的最终发作。缺乏合适的疗法来治疗自身免疫性疾病,因为人们对这些异常发作的机制知之甚少。目前的疗法仅限于对症治疗,并伴有严重的副作用。在这里,我描述了涉及自身免疫的分子机制和细胞事件,并提出了更好的策略来调节此类分子和细胞异常,这将有助于预防和/或控制自身免疫病的发病机制,并最终有助于提高生活质量。

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