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Developing Tadpole

机译:开发蝌蚪

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摘要

Mycobacterium abscessus (Mab) is an emerging, nontuberculosis mycobacterium (NTM) that infects humans. Mab has two morphotypes, smooth (S) and rough (R), related to the production of glycopeptidolipid (GPL), that differ in pathogenesis. To further understand the pathogenicity of these morphotypes in vivo, the amphibian Xenopus laevis was used as an alternative animal model. Mab infections have been previously modeled in zebrafish embryos and mice, but Mab are cleared early from immunocompetent mice, preventing the study of chronic infection, and the zebrafish model cannot be used to model a pulmonary infection and T cell involvement. Here, we show that X. laevis tadpoles, which have lungs and T cells, can be used as a complementary model for persistent Mab infection and pathogenesis. Intraperitoneal (IP) inoculation of S and R Mab morphotypes disseminated to tadpole tissues including liver and lungs, persisting for up to 40 days without significant mortality. Furthermore, the R morphotype was more persistent, maintaining a higher bacterial load at 40 days postinoculation. In contrast, the intracardiac (IC) inoculation with S Mab induced significantly greater mortality than inoculation with the R Mab form. These data suggest that X. laevis tadpoles can serve as a useful comparative experimental organism to investigate pathogenesis and host resistance to M. abscessus.
机译:分枝杆菌脓肿(MAB)是一种感染人类的​​新兴的Nontuberculosis(NTM)。 MAb有两种Morothy型,平滑(S)和粗糙(R),与糖肽脂脂(GPL)的产生有关,其在发病机制中不同。为了进一步了解这些Mor型型在体内这些Morothy型的致病性,Amphibian Xenopus Laevis被用作替代动物模型。 MAB感染先前已在斑马鱼胚胎和小鼠中进行建模,但是MAB从免疫活性小鼠早期清除,预防慢性感染的研究,并且斑马鱼模型不能用于模拟肺部感染和T细胞受累。在这里,我们表明,患有肺和T细胞的X. Laevis Tadpoles,可用作持久性mAb感染和发病机制的互补模型。腹膜内(IP)接种S和R MAB Morothy型散发到包括肝脏和肺的蝌蚪组织,持续最多40天,而不会显着死亡率。此外,r mor蝶型更持久,在发布后40天的40天保持更高的细菌负荷。相反,与S mAb接种的肠内腺(IC)接种的死亡率显着提高了与R mAb形式接种的死亡率。这些数据表明X. Laevis Tadpoles可以作为有用的比较实验器官来研究发病机制和宿主对M.脓肿的抗性。

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