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寄生虫质体的研究进展。

Progress with parasite plastids.

作者信息

Wilson R J M Iain

机构信息

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

出版信息

J Mol Biol. 2002 May 31;319(2):257-74. doi: 10.1016/S0022-2836(02)00303-0.

DOI:10.1016/S0022-2836(02)00303-0
PMID:12051904
Abstract

This review offers a snapshot of our current understanding of the origin, biology, and metabolic significance of the non-photosynthetic plastid organelle found in apicomplexan parasites. These protists are of considerable medical and veterinary importance world-wide, Plasmodium spp., the causative agent of malaria being foremost in terms of human disease. It has been estimated that approximately 8% of the genes currently recognized by the malarial genome sequencing project (now nearing completion) are of bacterial/plastid origin. The bipartite presequences directing the products of these genes back to the plastid have provided fresh evidence that secondary endosymbiosis accounts for this organelle's presence in these parasites. Mounting phylogenetic evidence has strengthened the likelihood that the plastid originated from a red algal cell. Most importantly, we now have a broad understanding of several bacterial metabolic systems confined within the boundaries of the parasite plastid. The primary ones are type II fatty acid biosynthesis and isoprenoid biosynthesis. Some aspects of heme biosynthesis also might take place there. Retention of the plastid's relict genome and its still ill-defined capacity to participate in protein synthesis might be linked to an important house-keeping process, i.e. guarding the type II fatty acid biosynthetic pathway from oxidative damage. Fascinating observations have shown the parasite plastid does not divide by constriction as in typical plants, and that plastid-less parasites fail to thrive after invading a new cell. The modes of plastid DNA replication within the phylum also have provided surprises. Besides indicating the potential of the parasite plastid for therapeutic intervention, this review exposes many gaps remaining in our knowledge of this intriguing organelle. The rapid progress being made shows no sign of slackening.

摘要

本综述概述了我们目前对顶复门寄生虫中非光合质体细胞器的起源、生物学特性及代谢意义的理解。这些原生生物在全球范围内具有相当重要的医学和兽医学意义,疟原虫属(Plasmodium spp.)作为疟疾的病原体,在人类疾病方面最为突出。据估计,目前疟疾基因组测序项目(现已接近完成)所识别的基因中,约8%起源于细菌/质体。将这些基因产物导向质体的双元前导序列提供了新的证据,表明次生内共生导致了这种细胞器在这些寄生虫中的存在。越来越多的系统发育证据增强了质体起源于红藻细胞的可能性。最重要的是,我们现在对局限于寄生虫质体内的几种细菌代谢系统有了广泛的了解。主要的系统是II型脂肪酸生物合成和类异戊二烯生物合成。血红素生物合成的某些方面可能也在那里进行。质体残余基因组的保留及其参与蛋白质合成的仍不明确的能力可能与一个重要的管家过程有关,即保护II型脂肪酸生物合成途径免受氧化损伤。有趣的观察表明,寄生虫质体不像典型植物那样通过缢缩进行分裂,而且没有质体的寄生虫在侵入新细胞后无法茁壮成长。该门内质体DNA复制的模式也带来了惊喜。除了表明寄生虫质体在治疗干预方面的潜力外,本综述还揭示了我们对这个有趣细胞器的认识中仍存在的许多空白。正在取得的快速进展没有放缓的迹象。

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