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自身免疫性疾病的患病率、谱和病例定义的最新评估。

Updated assessment of the prevalence, spectrum and case definition of autoimmune disease.

机构信息

ANU Medical School, Frank Fenner Building 42, The Australian National University, Canberra, ACT, 0200, Australia.

出版信息

Autoimmun Rev. 2012 Aug;11(10):754-65. doi: 10.1016/j.autrev.2012.02.001. Epub 2012 Feb 23.

Abstract

Autoimmune diseases are heterogeneous with regard to prevalence, manifestations, and pathogenesis. The classification of autoimmune diseases has varied over time. Here, we have compiled a comprehensive up-to-date list of the autoimmune diseases, and have reviewed published literature to estimate their prevalence. We identified 81 autoimmune diseases. The overall estimated prevalence is 4.5%, with 2.7% for males and 6.4% for females. For specific diseases, prevalence ranges from 1% to <1/10(6). Considering all diseases in the class, the most common mean age-of-onset was 40-50 years. This list of autoimmune diseases has also yielded information about autoantigens. Forty-five autoimmune diseases have been associated with well-defined autoantigens. Of the diseases with known autoantigens, 33.3% had highly repetitive sequences, 35.6% had coiled-coil arrangements and 57.8% were associated with cellular membranes, which means that based on these structural motifs alone, autoantigens do not appear to be a random sample of the human proteome. Finally, we identified 19 autoimmune diseases that phenocopy diseases arising from germline mutations in the corresponding autoantigen. Collectively, our findings lead to a tentative proposal for criteria for assigning autoimmune pathogenesis to a particular disease.

摘要

自身免疫性疾病在患病率、表现和发病机制方面存在异质性。自身免疫性疾病的分类随时间而变化。在这里,我们汇编了一份全面的最新自身免疫性疾病清单,并回顾了已发表的文献,以估计其患病率。我们确定了 81 种自身免疫性疾病。总体估计患病率为 4.5%,男性为 2.7%,女性为 6.4%。对于特定疾病,患病率范围为 1%至 <1/10(6)。考虑到该类别中的所有疾病,最常见的平均发病年龄为 40-50 岁。这份自身免疫性疾病清单还提供了有关自身抗原的信息。45 种自身免疫性疾病与明确的自身抗原有关。在已知自身抗原的疾病中,33.3%具有高度重复序列,35.6%具有螺旋排列,57.8%与细胞膜有关,这意味着仅基于这些结构模体,自身抗原似乎不是人类蛋白质组的随机样本。最后,我们确定了 19 种自身免疫性疾病,其表型类似于相应自身抗原中胚系突变引起的疾病。总的来说,我们的发现导致了一个暂定的建议,即根据特定疾病分配自身免疫发病机制的标准。

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