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Leishmania infantum Asparagine Synthetase A Is Dispensable for Parasites Survival and Infectivity

机译:婴儿利什曼原虫天冬酰胺合成酶A对寄生虫的存活和传染性至关重要

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摘要

A growing interest in asparagine (Asn) metabolism has currently been observed in cancer and infection fields. Asparagine synthetase (AS) is responsible for the conversion of aspartate into Asn in an ATP-dependent manner, using ammonia or glutamine as a nitrogen source. There are two structurally distinct AS: the strictly ammonia dependent, type A, and the type B, which preferably uses glutamine. Absent in humans and present in trypanosomatids, AS-A was worthy of exploring as a potential drug target candidate. Appealingly, it was reported that AS-A was essential in Leishmania donovani, making it a promising drug target. In the work herein we demonstrate that Leishmania infantum AS-A, similarly to Trypanosoma spp. and L. donovani, is able to use both ammonia and glutamine as nitrogen donors. Moreover, we have successfully generated LiASA null mutants by targeted gene replacement in L. infantum, and these parasites do not display any significant growth or infectivity defect. Indeed, a severe impairment of in vitro growth was only observed when null mutants were cultured in asparagine limiting conditions. Altogether our results demonstrate that despite being important under asparagine limitation, LiAS-A is not essential for parasite survival, growth or infectivity in normal in vitro and in vivo conditions. Therefore we exclude AS-A as a suitable drug target against L. infantum parasites.
机译:目前,在癌症和感染领域中,人们对天冬酰胺(Asn)代谢的兴趣日益浓厚。天冬酰胺合成酶(AS)负责使用氨或谷氨酰胺作为氮源,以ATP依赖性方式将天冬氨酸转化为Asn。在结构上有两种不同的AS:严格依赖氨的A型和B型,最好使用谷氨酰胺。 AS-A在人类中不存在且在锥虫中存在,值得探索作为潜在的药物靶标候选物。有吸引力的是,据报道AS-A在多形利什曼原虫中是必不可少的,使其成为有希望的药物靶标。在本文的工作中,我们证明了婴儿利什曼原虫AS-A与锥虫属相似。 L. donovani和L. donovani能够同时使用氨和谷氨酰胺作为氮供体。此外,我们已经通过在婴儿乳杆菌中的靶向基因置换成功地产生了LiASA null突变体,并且这些寄生虫没有显示任何明显的生长或感染性缺陷。实际上,仅当在天冬酰胺限制条件下培养无效突变体时才观察到严重的体外生长损伤。总的来说,我们的结果表明,尽管在天冬酰胺限制下很重要,但LiAS-A对于正常的体外和体内条件下的寄生虫存活,生长或感染性并不是必需的。因此,我们将AS-A排除为对抗婴儿乳杆菌寄生虫的合适药物靶标。

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