The Antimalarial Natural Product Salinipostin A Identifies Essential α/β Serine Hydrolases Involved in Lipid Metabolism in <ce:italic>P.?falciparum</ce:italic> Parasites

Euna Yoo; Christopher J. Schulze; Barbara H. Stokes; Ouma Onguka; Tomas Yeo; Sachel Mok; Nina F. Gn?dig; Yani Zhou; Kenji Kurita; Ian T. Foe; Stephanie M. Terrell; Michael J. Boucher; Piotr Cieplak; Krittikorn Kumpornsin; Marcus C.S. Lee; Roger G. Linington; Jonathan Z. Long; Anne-Catrin Uhlemann; Eranthie Weerapana; David A. Fidock; Matthew Bogyo

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The Antimalarial Natural Product Salinipostin A Identifies Essential α/β Serine Hydrolases Involved in Lipid Metabolism in P.?falciparum Parasites

机译：抗疟天然产物Salinipostin A识别在 p.?falcarum 寄生虫中的脂质代谢中涉及脂质代谢的必要α/β丝氨酸水解酶。

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Salinipostin A (Sal A) is a potent antiplasmodial marine natural product with an undefined mechanism of action. Using a Sal A-derived activity-based probe, we identify its targets in thePlasmodium falciparumparasite. All of the identified proteins contain α/β serine hydrolase domains and several are essential for parasite growth. One of the essential targets displays a high degree of homology to human monoacylglycerol lipase (MAGL) and is able to process lipid esters including a MAGL acylglyceride substrate. This Sal A target is inhibited by the anti-obesity drug Orlistat, which disrupts lipid metabolism. Resistance selections yielded parasites that showed only minor reductions in sensitivity and that acquired mutations in a PRELI domain-containing protein linked to drug resistance inToxoplasma gondii. This inability to evolve efficient resistance mechanisms combined with the non-essentiality of human homologs makes the serine hydrolases identified here promising antimalarial targets.

机译：Salinipostin A（Sal A）是一种有效的抗疟原虫海洋天然产物，其作用机制尚不明确。使用Sal a衍生的活性探针，我们在恶性疟原虫寄生虫中确定了其靶点。所有已鉴定的蛋白质都含有α/β丝氨酸水解酶结构域，其中一些是寄生虫生长所必需的。其中一个重要靶点显示出与人类单酰甘油脂肪酶（MAGL）高度同源性，并且能够处理包括MAGL酰基甘油酯底物在内的脂酯。抗肥胖药物奥利司他（Orlistat）会破坏脂质代谢，从而抑制这一目标。耐药性选择产生的寄生虫仅显示出轻微的敏感性降低，并在含有PRELI结构域的蛋白质中获得了与弓形虫耐药相关的突变。由于无法进化出有效的抗药性机制，再加上人类同系物的非必要性，使得这里鉴定的丝氨酸水解酶成为有希望的抗疟靶点。

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来源
《Cell chemical biology》 |2020年第2期|共15页
作者
Euna Yoo; Christopher J. Schulze; Barbara H. Stokes; Ouma Onguka; Tomas Yeo; Sachel Mok; Nina F. Gn?dig; Yani Zhou; Kenji Kurita; Ian T. Foe; Stephanie M. Terrell; Michael J. Boucher; Piotr Cieplak; Krittikorn Kumpornsin; Marcus C.S. Lee; Roger G. Linington; Jonathan Z. Long; Anne-Catrin Uhlemann; Eranthie Weerapana; David A. Fidock; Matthew Bogyo;
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作者单位

Department of Pathology Stanford University School of Medicine;

Department of Pathology Stanford University School of Medicine;

Department of Microbiology and Immunology Columbia University Irving Medical Center;

Department of Pathology Stanford University School of Medicine;

Department of Microbiology and Immunology Columbia University Irving Medical Center;

Department of Microbiology and Immunology Columbia University Irving Medical Center;

Department of Microbiology and Immunology Columbia University Irving Medical Center;

Department of Chemistry Boston College;

Department of Chemistry Simon Fraser University;

Department of Pathology Stanford University School of Medicine;

Department of Pathology Stanford University School of Medicine;

Department of Microbiology and Immunology Stanford University School of Medicine;

Infectious &

Inflammatory Disease Center Sanford Burnham Prebys Medical Discovery Institute;

Wellcome Sanger Institute;

Wellcome Sanger Institute;

Department of Chemistry Simon Fraser University;

Department of Pathology Stanford University School of Medicine;

Division of Infectious Diseases Department of Medicine Columbia University Irving Medical Center;

Department of Chemistry Boston College;

Department of Microbiology and Immunology Columbia University Irving Medical Center;

Department of Pathology Stanford University School of Medicine;

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原文格式 PDF
正文语种 eng
中图分类普通生物学;生物化学;
关键词
malaria; natural products; Salinipostin A; serine hydrolases; lipid metabolism; Plasmodium falciparum; chemical proteomics; activity-based probes;

机译：疟疾;天然产品;Salinipostin A;丝氨酸水解酶;脂质代谢;疟原虫;化学蛋白质组学;基于活性的探针;

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外文文献

1. The Antimalarial Natural Product Salinipostin A Identifies Essential alpha/beta Serine Hydrolases Involved in Lipid Metabolism in P. falciparum Parasites [J] . Yoo Euna, Schulze Christopher J., Stokes Barbara H., Mathematical research letters: MRL . 2020,第2期

机译：抗疟天然产物Salinipostin A识别在P. falciparum寄生虫中涉及脂质代谢的基本α/β丝氨酸水解酶
2. A high yield optimized method for the production of acylated ACPs enabling the analysis of enzymes involved in P. falciparum fatty acid biosynthesis [J] . Leonardo Lauciello, Gabriela Lack, Leonardo Scapozza, Biochemistry and Biophysics Reports . 2016,第4期

机译：一种用于生产酰化ACP的高产率优化方法，能够分析与 P有关的酶。恶性疟原虫脂肪酸的生物合成
3. Thymus satureioides C. & B. and Origanum elongatum E. & M. ( Lamiaceae) essential oils against Varroa destructor Anderson & Trueman ( Acari: Varroidae)]]> [J] . Industrial Crops and Products . 2017,第期

机译：<！[CDATA [CDATA [CDATA [CE：斜体>斜胸腔SUPINICIOIDES C.＆amp; B.和 origanum elongatum E.＆amp; M.（ lamiaceae ）精油反对 varroa析构函数安德森＆amp; Trueman（ acari ： varroidae ）]]>
4. The Antimalarial Natural Product Salinipostin A Identifies Essential α/β Serine Hydrolases Involved in Lipid Metabolism in P. falciparum Parasites [O] . Euna Yoo, Christopher J. Schulze, Barbara H. Stokes, 2020

机译：抗疟天然产物Salinipostin A识别患有脂质代谢的必要α/β丝氨酸水解酶，所述脂质代谢寄生虫

The Antimalarial Natural Product Salinipostin A Identifies Essential α/β Serine Hydrolases Involved in Lipid Metabolism in P.?falciparum Parasites

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