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Genomic Appraisal of the Multifactorial Basis for In Vitro Acquisition of Miltefosine Resistance in Leishmania donovani

机译:利什曼原虫多抗性米特磷碱抗性体外获得的多因素基础的基因组评估。

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摘要

Protozoan parasites of the Leishmania donovani complex are the causative agents of visceral leishmaniasis (VL), the most severe form of leishmaniasis, with high rates of mortality if left untreated. Leishmania parasites are transmitted to humans through the bite of infected female sandflies (Diptera: Phlebotominae), and approximately 500,000 new cases of VL are reported each year. In the absence of a safe human vaccine, chemotherapy, along with vector control, is the sole tool with which to fight the disease. Miltefosine (hexadecylphosphatidylcholine [HePC]), an antitumoral drug, is the only successful oral treatment for VL. In the current study, we describe the phenotypic traits of L. donovani clonal lines that have acquired resistance to HePC. We performed whole-genome and RNA sequencing of these resistant lines to provide an inclusive overview of the multifactorial acquisition of experimental HePC resistance, circumventing the challenge of identifying changes in membrane-bound proteins faced by proteomics. This analysis was complemented by assessment of the in vitro infectivity of HePC-resistant parasites. Our work underscores the importance of complementary "omics" to acquire the most comprehensive insight for multifaceted processes, such as HePC resistance.
机译:Leishmania donovani复合体的原生动物寄生虫是内脏利什曼病(VL)的病原体,内脏利什曼病是最严重的利什曼病形式,如果不加以治疗,死亡率很高。利什曼原虫的寄生虫通过被感染的雌性沙蝇叮咬而传播给人类(双翅目:Phlebotominae),每年报告约500,000例新的VL病例。在没有安全的人类疫苗的情况下,化学疗法以及媒介控制是对抗这种疾病的唯一工具。 Miltefosine(十六烷基磷脂酰胆碱[HePC])是一种抗肿瘤药物,是唯一成功的VL口服治疗药物。在当前的研究中,我们描述了已经获得了对HePC的抗性的L. donovani克隆系的表型性状。我们对这些抗性品系进行了全基因组和RNA测序,以提供关于实验性HePC抗性的多因素采集的全面概述,从而规避了鉴定蛋白质组学所面临的膜结合蛋白变化的挑战。该分析通过评估HePC耐药性寄生虫的体外感染性得到补充。我们的工作强调了补充“组学”对于获取多方面过程(例如,抗HePC耐药性)的最全面见解的重要性。

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