Departamento de Ciencias Biomédicas (INTOXCAL), Universidad de León, , Campus de Vegazana s/n, León, Spain.
Proc Biol Sci. 2010 Jun 22;277(1689):1777-87. doi: 10.1098/rspb.2009.2176. Epub 2010 Mar 3.
The phylum Apicomplexa includes a large group of protozoan parasites responsible for a wide range of animal and human diseases. Destructive pathogens, such as Plasmodium falciparum and Plasmodium vivax, causative agents of human malaria, Cryptosporidium parvum, responsible of childhood diarrhoea, and Toxoplasma gondii, responsible for miscarriages and abortions in humans, are frequently associated with HIV immunosuppression in AIDS patients. The lack of effective vaccines, along with years of increasing pressure to eradicate outbreaks with the use of drugs, has favoured the formation of multi-drug resistant strains in endemic areas. Almost all apicomplexan of medical interest contain two endosymbiotic organelles that contain their own mitochondrial and apicoplast DNA. Apicoplast is an attractive target for drug testing because in addition to harbouring singular metabolic pathways absent in the host, it also has its own transcription and translation machinery of bacterial origin. Accordingly, apicomplexan protozoa contain an interesting mixture of enzymes to unwind DNA from eukaryotic and prokaryotic origins. On the one hand, the main mechanism of DNA unwinding includes the scission of one-type I-or both DNA strands-type II eukaryotic topoisomerases, establishing transient covalent bonds with the scissile end. These enzymes are targeted by camptothecin and etoposide, respectively, two natural drugs whose semisynthetic derivatives are currently used in cancer chemotherapy. On the other hand, DNA gyrase is a bacterial-borne type II DNA topoisomerase that operates within the apicoplast and is effectively targeted by bacterial antibiotics like fluoroquinolones and aminocoumarins. The present review is an update on the new findings concerning topoisomerases in apicomplexan parasites and the role of these enzymes as targets for therapeutic agents.
门孢子虫门包括一大组原生动物寄生虫,这些寄生虫可导致广泛的动物和人类疾病。疟原虫属(Plasmodium falciparum 和 Plasmodium vivax)等破坏性病原体、导致儿童腹泻的微小隐孢子虫(Cryptosporidium parvum)和导致人类流产和堕胎的刚地弓形虫(Toxoplasma gondii),经常与艾滋病患者的 HIV 免疫抑制有关。缺乏有效的疫苗,再加上多年来为了使用药物根除疫情而不断施加的压力,导致在流行地区形成了多种耐药菌株。几乎所有具有医学意义的顶复门生物都含有两个共生细胞器,这些细胞器含有自己的线粒体和质体 DNA。质体是药物测试的一个有吸引力的目标,因为除了含有宿主中不存在的独特代谢途径外,它还有自己的细菌起源转录和翻译机制。因此,顶复门原生动物包含了有趣的混合酶,可从真核生物和原核生物中解开 DNA。一方面,DNA 解旋的主要机制包括一种类型 I 或两种 DNA 链类型 II 真核拓扑异构酶的断裂,与切割末端建立短暂的共价键。这些酶分别是喜树碱和依托泊苷的靶标,这两种天然药物的半合成衍生物目前用于癌症化疗。另一方面,DNA 回旋酶是一种源自细菌的 II 型 DNA 拓扑异构酶,在质体中发挥作用,可被氟喹诺酮类和氨基香豆素类等细菌抗生素有效地靶向。本文综述了关于顶复门寄生虫中的拓扑异构酶的新发现,以及这些酶作为治疗剂靶标的作用。