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通过RNA干扰长期抑制组织蛋白酶B水平可延缓血吸虫的生长。

Long-term suppression of cathepsin B levels by RNA interference retards schistosome growth.

作者信息

Correnti Jason M, Brindley Paul J, Pearce Edward J

机构信息

Department of Pathobiology, University of Pennsylvania, School of Veterinary Medicine, Philadelphia, PA 19104-6008, USA.

出版信息

Mol Biochem Parasitol. 2005 Oct;143(2):209-15. doi: 10.1016/j.molbiopara.2005.06.007.

Abstract

Schistosoma mansoni is an important flatworm parasite of man that has remained intractable to experimental analyses of gene function. We have developed an approach for using dsRNA to target schistosome transcripts for RNA interference, and used it to address the role of cathepsin B (SmCB1), a cysteine protease that has been proposed to play a central role in hemoglobin digestion in the schistosome gut. Electroporation of 3 h old larval schistosomes with SmCB1-specific dsRNA (SmCB1-dsRNA) resulted in a greater than 10-fold reduction in SmCB1 transcript levels that persisted for >20 days. RNAi mediated reductions in transcript levels led to associated reductions in SmCB1 enzyme activity. Schistosomes treated with SmCB1-dsRNA were viable and developed intestinal heme pigmentation indicative of hemoglobin digestion, but showed significant growth retardation when compared to control parasites, indicating that SmCB1 function is not essential for hemoglobin digestion but is necessary for normal parasite growth. This effect on growth was apparent when parasites were maintained in culture or introduced into mammalian hosts. The report sheds new light on the role of SmCB1 and provides a template for using RNAi to examine gene function in the mammal-parasitic stages of schistosomes during early development in vitro and in vivo.

摘要

曼氏血吸虫是一种重要的人体扁形寄生虫,其基因功能的实验分析一直难以进行。我们开发了一种利用双链RNA靶向血吸虫转录本进行RNA干扰的方法,并将其用于研究组织蛋白酶B(SmCB1)的作用,组织蛋白酶B是一种半胱氨酸蛋白酶,有人认为它在血吸虫肠道血红蛋白消化中起核心作用。用SmCB1特异性双链RNA(SmCB1-dsRNA)对3小时龄的血吸虫幼虫进行电穿孔处理,导致SmCB1转录水平降低了10倍以上,并持续超过20天。RNA干扰介导的转录水平降低导致SmCB1酶活性相应降低。用SmCB1-dsRNA处理的血吸虫是活的,并且出现了肠道血红素色素沉着,这表明血红蛋白发生了消化,但与对照寄生虫相比,其生长明显迟缓,这表明SmCB1功能对于血红蛋白消化并非必不可少,但对于寄生虫的正常生长是必需的。当寄生虫在培养物中维持或引入哺乳动物宿主时,这种对生长的影响很明显。该报告为SmCB1的作用提供了新的见解,并为利用RNA干扰研究血吸虫在体外和体内早期发育过程中哺乳动物寄生阶段的基因功能提供了一个模板。

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