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疟疾蛋白酶与宿主细胞逸出:一个“新兴”的级联反应

Malarial proteases and host cell egress: an 'emerging' cascade.

作者信息

Blackman Michael J

机构信息

Division of Parasitology, National Institute for Medical Research, Mill Hill, London NW7 1AA, UK.

出版信息

Cell Microbiol. 2008 Oct;10(10):1925-34. doi: 10.1111/j.1462-5822.2008.01176.x. Epub 2008 Jun 28.

Abstract

Malaria is a scourge of large swathes of the globe, stressing the need for a continuing effort to better understand the biology of its aetiological agent. Like all pathogens of the phylum Apicomplexa, the malaria parasite spends part of its life inside a host cell or cyst. It eventually needs to escape (egress) from this protective environment to progress through its life cycle. Egress of Plasmodium blood-stage merozoites, liver-stage merozoites and mosquito midgut sporozoites relies on protease activity, so the enzymes involved have potential as antimalarial drug targets. This review examines the role of parasite proteases in egress, in the light of current knowledge of the mechanics of the process. Proteases implicated in egress include the cytoskeleton-degrading malarial proteases falcipain-2 and plasmepsin II, plus a family of putative papain-like proteases called SERA. Recent revelations have shown that activation of the SERA proteases may be triggered by regulated secretion of a subtilisin-like serine protease called SUB1. These findings are discussed in the context of the potential for development of new chemotherapeutics targeting this stage in the parasite's life cycle.

摘要

疟疾是全球大片地区的一大灾祸,这凸显了持续努力以更好地了解其病原体生物学特性的必要性。与顶复门的所有病原体一样,疟原虫的部分生命周期是在宿主细胞或包囊内度过的。它最终需要从这个保护环境中逸出(出芽),以完成其生命周期。疟原虫血液期裂殖子、肝期裂殖子和蚊子中肠子孢子的出芽依赖于蛋白酶活性,因此所涉及的酶有作为抗疟药物靶点的潜力。本综述根据目前对该过程机制的了解,探讨了寄生虫蛋白酶在出芽中的作用。与出芽有关的蛋白酶包括降解细胞骨架的疟原虫蛋白酶恶性疟原虫蛋白酶2和天冬氨酸蛋白酶II,以及一类名为SERA的假定木瓜蛋白酶样蛋白酶。最近的研究表明,SERA蛋白酶的激活可能由一种名为SUB1的枯草杆菌蛋白酶样丝氨酸蛋白酶的调节分泌触发。本文结合针对寄生虫生命周期这一阶段开发新化疗药物的潜力对这些发现进行了讨论。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/947d/2610400/5ead91a5ae81/cmi0010-1925-f1.jpg

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