抗氧化剂可预防伯氏疟原虫感染小鼠的脑型疟疾。

C M Thumwood, N H Hunt, W B Cowden, I A Clark
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引用次数: 0

摘要

A/J和CBA/H小鼠感染伯氏疟原虫ANKA(脑型疟疾小鼠模型),观察抗氧化剂是否影响这种疾病的结果。未经治疗的感染小鼠在感染后7至9天死亡,通常伴有脑部症状。中枢神经系统(CNS)有出血、单核浸润和水肿。饲粮中添加0.75% (w/w)的丁基羟基茴味醚(BHA)可显著改变该病的病程。死亡被推迟了2周,并且小鼠在寄生虫病中看起来很健康,如果它们在传统饮食中会引起大脑症状和死亡。bha喂养的小鼠在对照组小鼠明显受到影响的同时几乎没有或没有表现出大脑症状,并且在检查中枢神经系统时大大减少了出血、单核细胞浸润和水肿。类似的,但更一致的是,通过重复注射或渗透泵给予BHA后,可以看到保护作用。当静脉注射超氧化物歧化酶和过氧化氢酶与聚乙二醇结合时,也可以保护小鼠免受脑并发症的死亡。使用125i标记的牛血清白蛋白、51cr标记的红细胞和埃文斯蓝染料监测血脑屏障的通透性,这些物质通常被排除在中枢神经系统之外。对照组感染小鼠的埃文斯蓝染色增加,中枢神经系统组织本身的125I和51Cr保留量增加。饲粮中添加丁基羟基茴香醚降低了这些增加的血脑屏障通透性指标。鉴于BHA在许多其他系统中具有强大的自由基清除活性,这可能是它在这里的主要作用,但尚未得到证实。超氧化物歧化酶和过氧化氢酶的保护作用支持了活性氧参与实验性脑疟疾病理的观点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Antioxidants can prevent cerebral malaria in Plasmodium berghei-infected mice.

A/J and CBA/H mice infected with Plasmodium berghei ANKA, a murine model of cerebral malaria, were used to see whether antioxidants influenced the outcome of this disease. Untreated, infected mice died 7 to 9 days after infection, often with cerebral symptoms. Haemorrhages, mononuclear infiltration and oedema were present in the central nervous system (CNS). Feeding a diet containing 0.75% (w/w) butylated hydroxyanisole (BHA) greatly altered the course of this disease. Death was delayed by up to 2 weeks and mice appeared healthy at parasitaemias that would have caused cerebral symptoms and death had they been on a conventional diet. BHA-fed mice showed few or no cerebral symptoms at a time at which control mice were clearly affected, and greatly reduced haemorrhages, mononuclear infiltration and oedema when the CNS was examined. Similar, but more consistent, protective effects were seen after administration of BHA by repeated injections or in osmotic pumps. The combination of superoxide dismutase and catalase, coupled to polyethylene glycol, when administered intravenously also protected mice against death from cerebral complications. Permeability of the blood-brain barrier was monitored by the use of 125I-labelled bovine serum albumin, 51Cr-labelled erythrocytes and the dye Evans blue, all of which are normally excluded from the CNS. Infected mice on control diet showed an increase in Evans blue staining and 125I and 51Cr retention in the CNS tissue itself. Feeding the diet containing BHA reduced these indices of increased blood-brain barrier permeability. In view of the potent radical scavenging activity of BHA in many other systems it is likely, but unproven, that this is its main role here. The protective effect of superoxide dismutase and catalase lends support to the idea that reactive oxygen species are involved in the pathology of experimental cerebral malaria.

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