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靶向亮氨酸氨肽酶的RNA干扰可阻断曼氏血吸虫卵的孵化。

RNA interference targeting leucine aminopeptidase blocks hatching of Schistosoma mansoni eggs.

作者信息

Rinaldi Gabriel, Morales Maria E, Alrefaei Yousef N, Cancela Martín, Castillo Estela, Dalton John P, Tort José F, Brindley Paul J

机构信息

Department of Microbiology, Immunology & Tropical Medicine, George Washington University Medical Center, Washington, DC 20037, USA.

出版信息

Mol Biochem Parasitol. 2009 Oct;167(2):118-26. doi: 10.1016/j.molbiopara.2009.05.002. Epub 2009 May 20.

Abstract

Schistosoma mansoni leucine aminopeptidase (LAP) is thought to play a central role in hatching of the miracidium from the schistosome egg. We identified two discrete LAPs genes in the S. mansoni genome, and their orthologs in S. japonicum. The similarities in sequence and exon/intron structure of the two genes, LAP1 and LAP2, suggest that they arose by gene duplication and that this occurred before separation of the mansoni and japonicum lineages. The SmLAP1 and SmLAP2 genes have different expression patterns in diverse stages of the cycle; whereas both are equally expressed in the blood dwelling stages (schistosomules and adult), SmLAP2 expression was higher in free living larval (miracidia) and in parasitic intra-snail (sporocysts) stages. We investigated the role of each enzyme in hatching of schistosome eggs and the early stages of schistosome development by RNA interference (RNAi). Using RNAi, we observed marked and specific reduction of mRNAs, along with a loss of exopeptidase activity in soluble parasite extracts against the diagnostic substrate l-leucine-7-amido-4-methylcoumarin hydroxide. Strikingly, knockdown of either SmLAP1 or SmLAP2, or both together, was accompanied by >or=80% inhibition of hatching of schistosome eggs showing that both enzymes are important to the escape of miracidia from the egg. The methods employed here refine the utility of RNAi for functional genomics studies in helminth parasites and confirm these can be used to identify potential drug targets, in this case schistosome aminopeptidases.

摘要

曼氏血吸虫亮氨酸氨肽酶(LAP)被认为在血吸虫虫卵中毛蚴的孵化过程中起关键作用。我们在曼氏血吸虫基因组中鉴定出两个不同的LAP基因,以及它们在日本血吸虫中的直系同源基因。LAP1和LAP2这两个基因在序列和外显子/内含子结构上的相似性表明,它们是通过基因复制产生的,且这种复制发生在曼氏血吸虫和日本血吸虫谱系分离之前。SmLAP1和SmLAP2基因在生命周期的不同阶段具有不同的表达模式;虽然它们在血居阶段(童虫和成虫)表达水平相当,但SmLAP2在自由生活的幼虫(毛蚴)和寄生在螺内的阶段(胞蚴)表达较高。我们通过RNA干扰(RNAi)研究了每种酶在血吸虫虫卵孵化和血吸虫发育早期阶段中的作用。使用RNAi,我们观察到mRNA显著且特异性地减少,同时可溶性寄生虫提取物中针对诊断底物L-亮氨酸-7-氨基-4-甲基香豆素羟基化物的外肽酶活性丧失。引人注目的是,单独敲低SmLAP1或SmLAP2,或两者同时敲低,都伴随着血吸虫虫卵孵化受到≥80%的抑制,这表明这两种酶对于毛蚴从虫卵中逸出都很重要。这里采用的方法改进了RNAi在蠕虫寄生虫功能基因组学研究中的效用,并证实其可用于识别潜在的药物靶点,在这种情况下是血吸虫氨肽酶。

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