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线粒体精脒合酶对疟原虫的血期生长至关重要。

Mitochondrial Spermidine Synthase is Essential for Blood-stage growth of the Malaria Parasite.

机构信息

Aly Lab, Beykoz Institute of Life Sciences and Biotechnology, Bezmialem Vakif University, Istanbul 34820, Turkey.

Aly Lab, Beykoz Institute of Life Sciences and Biotechnology, Bezmialem Vakif University, Istanbul 34820, Turkey; Department of Biotechnology, Institute of Health Sciences, Bezmialem Vakif University, Istanbul, Turkey.

出版信息

Microbiol Res. 2022 Dec;265:127181. doi: 10.1016/j.micres.2022.127181. Epub 2022 Sep 9.

Abstract

Positively-charged polyamines are essential molecules for the replication of eukaryotic cells and are particularly important for the rapid proliferation of parasitic protozoa and cancer cells. Unlike in Trypanosoma brucei, the inhibition of the synthesis of intermediate polyamine Putrescine caused only partial defect in malaria parasite blood-stage growth. In contrast, reducing the intracellular concentrations of Spermidine and Spermine by polyamine analogs caused significant defects in blood-stage growth in Plasmodium yoelii and P. falciparum. However, little is known about the synthesizing enzyme of Spermidine and Spermine in the malaria parasite. Herein, malaria parasite conserved Spermidine Synthase (SpdS) gene was targeted for deletion/complementation analyses by knockout/knock-in constructs in P. yoelii. SpdS was found to be essential for blood-stage growth. Live fluorescence imaging in blood-stages and sporozoites confirmed a specific mitochondrial localization, which is not known for any polyamine-synthesizing enzyme so far. This study identifies SpdS as an excellent drug targeting candidate against the malaria parasite, which is localized to the parasite mitochondrion.

摘要

正电多胺是真核细胞复制的必需分子,对寄生原生动物和癌细胞的快速增殖尤其重要。与在布氏锥虫不同,中间多胺腐胺合成的抑制仅导致疟原虫血期生长的部分缺陷。相比之下,通过多胺类似物降低精脒和精胺的细胞内浓度会导致约氏疟原虫和恶性疟原虫血期生长显著缺陷。然而,关于疟原虫中精脒和精胺的合成酶知之甚少。在此,通过在约氏疟原虫中构建敲除/敲入构建体,针对疟原虫保守的精脒合酶(SpdS)基因进行了缺失/互补分析。发现 SpdS 对血期生长至关重要。在血期和子孢子中的活荧光成像证实了特定的线粒体定位,迄今为止尚未发现任何多胺合成酶具有这种定位。这项研究确定 SpdS 是一种针对疟原虫的优秀药物靶向候选物,它定位于寄生虫线粒体。

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