首页> 外文期刊>The Lancet >Persistence of DNA from Mycobacterium tuberculosis in superficially normal lung tissue during latent infection.
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Persistence of DNA from Mycobacterium tuberculosis in superficially normal lung tissue during latent infection.

机译:在潜伏感染期间,结核分枝杆菌的DNA在表面正常肺组织中的持久性。

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BACKGROUND: A third of the world's population has latent infection with Mycobacterium tuberculosis, and in areas of low endemicity, most cases of active tuberculosis arise as a result of reactivation of latent bacilli. We sought to establish the cellular location of these latent organisms to facilitate their elimination. METHODS: We applied in-situ PCR to sections of macroscopically normal lung tissue from 13 individuals from Ethiopia and 34 from Mexico who had died from causes other than tuberculosis. Sections of lung tissue from six Norwegian individuals (ie, individuals from a non-endemic population) acted as negative controls, and six Ethiopian tuberculosis cases acted as positive controls. FINDINGS: Control necropsy samples from the Norwegian individuals were all negative by in-situ PCR and conventional PCR, whereas all samples from known Ethiopian tuberculosis cases were positive by both methods. However, in macroscopically normal lung tissue from Ethiopian and Mexican individuals without tuberculous lesions, the in-situ PCR revealed five of 13 and ten of 34 positive individuals, respectively. These results were confirmed by conventional PCR with extracted DNA. Positive cells included alveolar and interstitial macrophages, type II pneumocytes, endothelial cells, and fibroblasts. INTERPRETATION: M. tuberculosis can persist intracellularly in lung tissue without histological evidence of tuberculous lesions. M. tuberculosis DNA is situated not only in macrophages but also in other non-professional phagocytic cells. These findings contradict the dominant view that latent organisms exist in old classic tuberculous lesions, and have important implications for strategies aimed at the elimination of latent and persistent bacilli.
机译:背景:世界三分之一的人口患有结核分枝杆菌潜伏感染,在低流行地区,大多数活动性结核病例是由于潜伏细菌的重新激活而引起的。我们试图建立这些潜在生物的细胞位置,以促进其消除。方法:我们对来自埃塞俄比亚的13位个体和墨西哥的34位因肺结核以外其他原因死亡的宏观正常肺组织切片进行了原位PCR。来自六个挪威个体(即来自非流行人群的个体)的肺组织切片充当阴性对照,六个埃塞俄比亚结核病例充当阳性对照。结果:通过原位PCR和常规PCR,来自挪威个体的对照尸检样品均为阴性,而两种方法均来自已知埃塞俄比亚结核病病例的所有样品均为阳性。然而,在没有结核病灶的埃塞俄比亚和墨西哥个体的宏观正常肺组织中,原位PCR分别显示13个阳性个体中的5个和34个阳性个体中的10个。用提取的DNA进行常规PCR证实了这些结果。阳性细胞包括肺泡和间质巨噬细胞,II型肺细胞,内皮细胞和成纤维细胞。解释:结核分枝杆菌可在肺组织内持续存在于细胞内,而无组织学证据表明结核病灶。结核分枝杆菌DNA不仅位于巨噬细胞中,而且位于其他非专业吞噬细胞中。这些发现与主流观点认为潜伏性细菌存在于古老的经典结核病灶中,并且对旨在消除潜伏性细菌和持久性细菌的策略具有重要意义。

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