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对来自多发性硬化症病灶的一个测序cDNA文库的分析。

Analysis of a sequenced cDNA library from multiple sclerosis lesions.

作者信息

Becker K G, Mattson D H, Powers J M, Gado A M, Biddison W E

机构信息

Molecular Immunology Section, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda MD, USA.

出版信息

J Neuroimmunol. 1997 Jul;77(1):27-38. doi: 10.1016/s0165-5728(97)00045-3.

Abstract

To identify genes that are expressed in MS pathogenesis, we have analyzed a normalized cDNA library made from mRNA obtained from CNS lesions of a patient with primary progressive MS. Complementary DNA clones obtained from this library were subjected to automated DNA sequencing to generate expressed sequence tags. Analysis of this MS cDNA library revealed the presence of 54 cDNAs that were associated with immune activation and indicated the presence of an ongoing inflammatory response with evidence of both cell-mediated and humoral immune responses. The surprising finding was that 16 of the cDNAs encoded autoantigens associated with seven other autoimmune disorders, while only three of these 16 autoantigen cDNAs were present in a similarly constructed adult brain library. Such aberrant autoantigen expression could provide a source of secondary autoimmune stimulation that could contribute to the ongoing inflammatory response in MS. In addition, two cDNAs were found that mapped to a known MS susceptibility locus (5p14-p12): one encoded an excitatory amino acid transporter and the other a human homologue of the Drosophila disabled gene. This approach to the molecular biology of MS pathogenesis may help to illuminate previously unappreciated aspects of this disease.

摘要

为了鉴定在多发性硬化症(MS)发病机制中表达的基因,我们分析了一个标准化的cDNA文库,该文库由取自一名原发性进行性MS患者中枢神经系统(CNS)病变的mRNA构建而成。从该文库获得的互补DNA克隆进行了自动化DNA测序以生成表达序列标签。对这个MS cDNA文库的分析揭示了54个与免疫激活相关的cDNA的存在,并表明存在持续的炎症反应,有细胞介导和体液免疫反应的证据。令人惊讶的发现是,其中16个cDNA编码与其他七种自身免疫性疾病相关的自身抗原,而在一个类似构建的成人大脑文库中仅存在这16个自身抗原cDNA中的三个。这种异常的自身抗原表达可能提供继发性自身免疫刺激的来源,这可能导致MS中持续的炎症反应。此外,发现两个cDNA定位于一个已知的MS易感位点(5p14 - p12):一个编码兴奋性氨基酸转运体,另一个编码果蝇失活基因的人类同源物。这种研究MS发病机制分子生物学的方法可能有助于阐明该疾病以前未被认识的方面。

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