首页> 外文期刊>American Journal of Pathology: Official Publication of the American Association of Pathologists >Bone Marrow Mesenchymal Stem Cells Provide an Antibiotic-Protective Niche for Persistent Viable Mycobacterium tuberculosis that Survive Antibiotic Treatment
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Bone Marrow Mesenchymal Stem Cells Provide an Antibiotic-Protective Niche for Persistent Viable Mycobacterium tuberculosis that Survive Antibiotic Treatment

机译:骨髓间充质干细胞为持续生存的结核分枝杆菌提供了一种抗生素保护性的小生境,可以生存于抗生素治疗中

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摘要

During tuberculosis (TB), some Mycobacterium tuberculosis bacilli persist in the presence of an active immunity and antibiotics that are used to treat the disease. Herein, by using the Cornell model of TB persistence, we further explored our recent finding that suggested that M. tuberculosis can escape therapy by residing in the bone marrow (BM) mesenchymal stem cells. We initially showed that M. tuberculosis rapidly disseminates to the mouse BM after aerosol exposure and maintained a stable burden for at least 220 days. In contrast, in the Lungs, the M. tuberculosis burden peaked at 28 days and subsequently declined approximately 10-fold. More important, treatment of the mice with the antibiotics rifampicin and isoniazid, as expected, resulted in effective clearance of M. tuberculosis from the lungs and spleen. In contrast, M. tuberculosis persisted, albeit at low numbers, in the BM of antibiotic-treated mice. Moreover, most viable M. tuberculosis was recovered from the bone marrow CD271(+)CD45(-)-enriched cell fraction, and only few viable bacteria could be isolated from the CD271(-)CD45(+) cell fraction. These results clearly show that BM mesenchymal stem cells provide an antibiotic-protective niche for M. tuberculosis and suggest that unraveling the mechanisms underlying this phenomenon will enhance our understanding of M. tuberculosis persistence in treated TB patients.
机译:在结核病(TB)期间,某些结核分枝杆菌杆菌会在存在主动免疫力和用于治疗该疾病的抗生素的情况下持续存在。在这里,通过使用结核病持久性的康奈尔模型,我们进一步探索了我们最近的发现,表明结核分枝杆菌可以通过驻留在骨髓(BM)间充质干细胞中而逃脱治疗。我们最初显示,气溶胶暴露后结核分枝杆菌迅速传播给小鼠BM,并保持稳定的负担至少220天。相反,在肺中,结核分枝杆菌的负担在28天达到峰值,随后下降了大约10倍。更重要的是,按预期使用抗生素利福平和异烟肼治疗小鼠,可有效清除肺结核和脾脏中的结核分枝杆菌。相反,在经抗生素治疗的小鼠的BM中,结核分枝杆菌持续存在,尽管数量很少。此外,大多数存活的结核分枝杆菌是从富含CD271(+)CD45(-)的骨髓细胞部分中回收的,只有很少的存活细菌可以从CD271(-)CD45(+)细胞部分中分离出来。这些结果清楚地表明,BM间充质干细胞为结核分枝杆菌提供了一种抗生素保护位,并表明揭示这种现象的潜在机制将增进我们对已治疗结核病患者持久性结核分枝杆菌的了解。

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