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存在于人体滑膜中的肺炎衣原体具有活性且代谢活跃。

Chlamydia pneumoniae present in the human synovium are viable and metabolically active.

作者信息

Gérard H C, Schumacher H R, El-Gabalawy H, Goldbach-Mansky R, Hudson A P

机构信息

Department of Immunology and Microbiology, Wayne State University School of Medicine, Detroit, MI 48201, USA.

出版信息

Microb Pathog. 2000 Jul;29(1):17-24. doi: 10.1006/mpat.2000.0360.

Abstract

We demonstrated that chromosomal DNA from Chlamydia pneumoniae is present in synovial tissue in at least some patients with reactive arthritis/Reiter's syndrome and other arthritides. Here, we provide initial molecular evidence that the bacterium is viable and metabolically active when present in the synovium. We used reverse transcription-polymerase chain reaction (RT-PCR) assays targeting primary transcripts from the chlamydial rRNA operons, and mRNA from several C. pneumoniae genes (hsp60, ompA, KDO transferase, Mr=76000 protein), to analyse RNA preparations from synovial tissue of 10 patients with various forms of arthritis; each patient was known to be PCR-positive for C. pneumoniae DNA in synovium prior to RT-PCR assays. Two PCR-negative patients served as controls for RT-PCR assays. In the 10 patients PCR-positive for C. pneumoniae DNA, RT-PCR assays targeting primary transcripts from the rRNA operons of the organism showed that these molecules were present in each sample, as were transcripts from the bacterial hsp60 gene. Assays targeting mRNAs from the Mr=76000 protein and the KDO transferase genes of C. pneumoniae gave positive results for 6/10 preparations. We were unable to identify mRNA from the chlamydial major outer membrane protein gene (ompA) in any preparation. RNA preparations from the two control patients were negative in all RT-PCR assays targeting C. pneumoniae transcripts. These results indicate that in patients infected with the organism, synovial C. pneumoniae are viable and metabolically active, as are C. trachomatis cells in the same context. Such viability is consistent with a role in long-term contribution to pathogenesis in joint disease.

摘要

我们证明,在至少部分反应性关节炎/赖特综合征及其他关节炎患者的滑膜组织中存在肺炎衣原体的染色体DNA。在此,我们提供了初步的分子证据,表明该细菌存在于滑膜中时具有活性且代谢活跃。我们使用逆转录聚合酶链反应(RT-PCR)分析方法,针对衣原体rRNA操纵子的初级转录本以及几个肺炎衣原体基因(hsp60、ompA、KDO转移酶、分子量76000的蛋白质)的mRNA,来分析10例患有各种形式关节炎患者的滑膜组织RNA样本;在进行RT-PCR分析之前,已知每例患者滑膜中的肺炎衣原体DNA经PCR检测呈阳性。两名PCR检测阴性的患者作为RT-PCR分析的对照。在10例肺炎衣原体DNA PCR检测呈阳性的患者中,针对该生物体rRNA操纵子初级转录本的RT-PCR分析表明,这些分子存在于每个样本中,细菌hsp60基因的转录本也同样存在。针对肺炎衣原体分子量76000的蛋白质和KDO转移酶基因的mRNA的分析,在10个样本中有6个得到阳性结果。我们在任何样本中均未鉴定出衣原体主要外膜蛋白基因(ompA)的mRNA。来自两名对照患者的RNA样本在所有针对肺炎衣原体转录本的RT-PCR分析中均为阴性。这些结果表明,在感染该生物体的患者中,滑膜中的肺炎衣原体具有活性且代谢活跃,沙眼衣原体在相同情况下也是如此。这种活性与在关节疾病发病机制中的长期作用相符。

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