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利用结核病患者血清分析结核分枝杆菌基因组DNA表达文库:宿主免疫反应调节的证据

Analysis of a genomic DNA expression library of Mycobacterium tuberculosis using tuberculosis patient sera: evidence for modulation of host immune response.

作者信息

Amara R R, Satchidanandam V

机构信息

Centre for Genetic Engineering, Indian Institute of Science, Bangalore, India.

出版信息

Infect Immun. 1996 Sep;64(9):3765-71. doi: 10.1128/iai.64.9.3765-3771.1996.

Abstract

DNA obtained from a human sputum isolate of Mycobacterium tuberculosis, NTI-64719, which showed extensive dissemination in the guinea pig model resulting in a high score for virulence was used to construct an expression library in the lambda ZAP vector. The size of DNA inserts in the library ranged from 1 to 3 kb, and recombinants represented 60% of the total plaques obtained. When probed with pooled serum from chronically infected tuberculosis patients, the library yielded 176 recombinants with a range of signal intensities. Among these, 93 recombinants were classified into 12 groups on the basis of DNA hybridization experiments. The polypeptides synthesized by the recombinants were predominantly LacZ fusion proteins. Serum obtained from patients who were clinically diagnosed to be in the early phase of M. tuberculosis infection was used to probe the 176 recombinants obtained. Interestingly, some recombinants that gave very strong signals in the original screen did not react with early-phase serum; conversely, other whose signals were extremely weak in the original screen gave very intense signals with serum from recently infected patients. This indicates the differential nature of either the expression of these antigens or the immune response elicited by them as a function of disease progression.

摘要

从人痰液分离的结核分枝杆菌NTI - 64719中提取的DNA,该菌株在豚鼠模型中显示出广泛传播,毒力得分很高,用其构建了λZAP载体表达文库。文库中DNA插入片段大小在1至3 kb之间,重组体占所获总噬菌斑的60%。用慢性感染结核病患者的混合血清进行探测时,该文库产生了176个信号强度各异的重组体。其中,93个重组体根据DNA杂交实验被分为12组。重组体合成的多肽主要是LacZ融合蛋白。用临床诊断为处于结核分枝杆菌感染早期阶段的患者的血清探测所获的176个重组体。有趣的是,一些在最初筛选中信号很强的重组体与早期血清不发生反应;相反,其他在最初筛选中信号极弱的重组体与近期感染患者的血清反应时产生很强的信号。这表明这些抗原的表达或它们引发的免疫反应随疾病进展具有差异特性。

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