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双氢青蒿素对 NADH 依赖型谷氨酸合酶的影响:在疟疾管理中的意义。

Effect of Dihydroartemisinin on NADH-Dependent Glutamate Synthase: The Implication in Malaria Management.

机构信息

Research Center of Artemisinin, Institute of Chinese Materia Medica, China Academy of Chinese Medical Sciences, Beijing 100700, P. R. China.

Tang Center for Herbal Medicine Research, Institute of Chinese Materia Medica, China Academy of Chinese Medical Sciences, Beijing 100700, P. R. China.

出版信息

Am J Chin Med. 2019;47(6):1325-1343. doi: 10.1142/S0192415X1950068X. Epub 2019 Sep 5.

Abstract

Artemisinin and its analogues (ARTs) are currently the most effective anti-malarial drugs, but the precise mechanism of action is still highly controversial. Effects of ARTs on genes expression are studied in our Lab. The overexpression of an interesting amidotransferase, NADH-dependent glutamate synthase (NADH-GltS) was found in treated by dihydroartemisinin (DHA). The increased expression occurred not only from global transcriptomics analysis on the human malaria parasite () 3D7 and gene expression screening on all of iron-sulphur cluster proteins from . 3D7 but also from () ANKA in mice. Influence of DHA on NADH-GltS was specifically at trophozoite stage of and in a dose-dependent manner below the effective doses. L-glutamine (Gln) and L-glutamate (Glu) are the substrate and product of NADH-GltS respectively. Azaserine (Aza) is specific inhibitor for NADH-GltS. Experimental data showed that Glu levels were significantly decreasing with DHA dose increasing but NADH-GltS enzyme activities were still remained at higher levels in parasites, and appropriate amount of exogenous Glu could significantly reduce anti-malarial action of DHA but excessive amount lost the above effect. Aza alone could inhibit proliferation of and had an additive effect in combination with DHA. Those results could suggest that: Glutamate depletion is one of the anti-malarial actions of DHA; overexpression of NADH-GltS would be a feedback pattern of parasite itself due to glutamate depletion, but not a direct action of DHA; the "feedback pattern" is one of protective strategies of to interfere with the anti-malarial actions of DHA; and specific inhibitor for NADH-GltS as a new type of anti-malarial agents or new partner in ACT might provide a potential.

摘要

青蒿素及其类似物(ARTs)是目前最有效的抗疟药物,但确切的作用机制仍存在很大争议。我们实验室研究了 ARTs 对基因表达的影响。在二氢青蒿素(DHA)处理后,发现一种有趣的氨酰转移酶,即 NADH 依赖性谷氨酸合酶(NADH-GltS)过度表达。这种表达增加不仅来自于对人类疟原虫 3D7 的全转录组学分析和对 3D7 所有铁硫簇蛋白的基因表达筛选,还来自于小鼠中的 ANKA。DHA 对 NADH-GltS 的影响在 滋养体阶段是特异性的,并且在有效剂量以下呈剂量依赖性。L-谷氨酰胺(Gln)和 L-谷氨酸(Glu)分别是 NADH-GltS 的底物和产物。氮杂丝氨酸(Aza)是 NADH-GltS 的特异性抑制剂。实验数据表明,随着 DHA 剂量的增加,Glu 水平显著下降,但寄生虫中 NADH-GltS 酶活性仍保持在较高水平,适量外源性 Glu 可显著降低 DHA 的抗疟作用,但过量则失去上述作用。Aza 单独可以抑制 的增殖,与 DHA 联合使用具有相加作用。这些结果表明:谷氨酸耗竭是 DHA 的抗疟作用之一;由于谷氨酸耗竭,NADH-GltS 的过度表达可能是寄生虫自身的一种反馈模式,而不是 DHA 的直接作用;“反馈模式”是 干扰 DHA 抗疟作用的保护策略之一;NADH-GltS 的特异性抑制剂作为一种新型抗疟药物或 ACT 的新伙伴可能具有潜力。

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