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疟疾中的氧化应激;对预防和治疗的意义。

Oxidative stress in malaria; implications for prevention and therapy.

作者信息

Postma N S, Mommers E C, Eling W M, Zuidema J

机构信息

Department of Pharmaceutics, University of Utrechi, The Netherlands.

出版信息

Pharm World Sci. 1996 Aug;18(4):121-9. doi: 10.1007/BF00717727.

Abstract

Malaria affects world-wide more than 200 million people, of which 1-2 million die every year. New drugs and treatment strategies are needed to face the rapidly increasing problems of drug resistance. During a malaria infection, both host and parasite are under oxidative stress. Increased production levels of reactive oxygen species (ROS, e.g superoxide anion and the hydroxyl radical) are produced by activated neutrophils in the host and during degradation of haemoglobin in the parasite. The effects of ROS in malaria can be both beneficial and pathological, depending on the amount and place of production. Enhanced ROS production after the administration of pro-oxidants, which is directed against the intra-erythrocytic parasite, inhibits the infection both in vitro and in vivo. However, ROS are also involved in pathological changes in host tissue like damage of the vascular endothelial lining during a malaria infection (cerebral malaria). Pro-oxidants support the host defense against the parasite when working in or near the infected cell but potentially cause vascular damage when working on or near the vascular lining. Examples of pro-oxidants are found among xenobiotics and food components. Important new drugs belonging to the class of pro-oxidants are artemisinin and its derivatives. Anti-oxidants potentially counteract these agents. Treatment with anti-oxidants or chelators of metals to prevent their catalytic function in the generation of ROS may prevent vascular pathology. In addition, the iron chelator desferrioxamine, exhibits an antiparasitic activity, because iron is also essential for the proliferation of the parasite. Cytokines play an important role in ROS-related pathology of malaria, though their mechanism of action is not completely elucidated. This field might bring up new treatment concepts and drugs. Drugs which prevent host pathology, such as the cerebral complications might be life saving.

摘要

疟疾在全球影响着超过2亿人,其中每年有100万至200万人死亡。需要新的药物和治疗策略来应对耐药性迅速增加的问题。在疟疾感染期间,宿主和寄生虫都处于氧化应激状态。活性氧(ROS,如超氧阴离子和羟基自由基)的产生水平在宿主中由活化的中性粒细胞增加,以及在寄生虫中血红蛋白降解期间增加。ROS在疟疾中的作用可能是有益的,也可能是病理性的,这取决于产生的量和位置。给予促氧化剂后增强的ROS产生,其针对红细胞内寄生虫,在体外和体内均抑制感染。然而,ROS也参与宿主组织的病理变化,如疟疾感染(脑型疟疾)期间血管内皮衬里的损伤。促氧化剂在感染细胞内或附近起作用时支持宿主对寄生虫的防御,但在血管衬里上或附近起作用时可能导致血管损伤。促氧化剂的例子存在于外源性物质和食物成分中。属于促氧化剂类别的重要新药是青蒿素及其衍生物。抗氧化剂可能会抵消这些药物的作用。用抗氧化剂或金属螯合剂进行治疗以防止它们在ROS产生中的催化功能,可能会预防血管病变。此外,铁螯合剂去铁胺具有抗寄生虫活性,因为铁对于寄生虫的增殖也是必不可少的。细胞因子在疟疾的ROS相关病理中起重要作用,尽管它们的作用机制尚未完全阐明。该领域可能会带来新的治疗概念和药物。预防宿主病理的药物,如脑部并发症,可能会挽救生命。

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