首页> 外文期刊>International journal of infectious diseases: IJID : official publication of the International Society for Infectious Diseases >Prophylactic effect of the anti-inflammatory drug diclofenac in experimental schistosomiasis mansoni.
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Prophylactic effect of the anti-inflammatory drug diclofenac in experimental schistosomiasis mansoni.

机译:抗炎药双氯芬酸对曼氏血吸虫病的预防作用。

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OBJECTIVES: This study was a trial to demonstrate the prophylactic effect of diclofenac, a widely used anti-inflammatory drug (diclofenac potassium, CAS-15307-81-0, Ciba Geigy, 334.2) in experimental schistosomiasis mansoni. Two different dose regimens were used to explore the effects upon worm load, tissue egg load, and hepatic granuloma size. METHODS: In this study, a group of 50 Swiss albino mice was used. This group was divided into five subgroups: subgroup I constituted infected untreated control mice; subgroup II, infected mice given 0.5mg diclofenac orally 24h post infection, then sacrificed three weeks later; subgroup III, infected mice given 0.5mg diclofenac orally six weeks post infection and sacrificed one week later; subgroup IV, infected mice administered 1mg diclofenac orally 24h post infection and sacrificed three weeks later; and subgroup V, infected mice given 1mg of the drug orally six weeks post infection and sacrificed one week later. RESULTS: Mice given the high dose regimen (1mg orally/mouse) 24h post infection, then sacrificed three weeks later, demonstrated a significant reduction in the immature worms recovered, compared to the untreated controls. Animals receiving the high dose of the drug six weeks post infection, then sacrificed one week later, revealed a drop in the number of mature worms and in the tissue egg load (hepatic and intestinal), and the smallest hepatic granuloma measurement compared to the untreated controls. These findings were less conspicuous in animals given the low dose regimen. CONCLUSION: Diclofenac could be used successfully as a preventive agent against schistosomiasis mansoni infection in endemic areas.
机译:目的:该研究旨在证明双氯芬酸(一种广泛使用的抗炎药(双氯芬酸钾,CAS-15307-81-0,Ciba Geigy,334.2)在曼氏血吸虫病中的预防作用。两种不同的剂量方案用于探讨对蠕虫负荷,组织卵负荷和肝肉芽肿大小的影响。方法:在这项研究中,使用了50只瑞士白化病小鼠。该组分为五个亚组:第一亚组构成感染的未经治疗的对照小鼠;第二亚组,感染后24小时口服0.5mg双氯芬酸的感染小鼠,三周后处死。第三亚组,感染的小鼠在感染后六周口服0.5mg双氯芬酸并在一周后处死。 IV亚组,感染后24小时口服给予1mg双氯芬酸的感染小鼠,三周后处死。在感染后6周内,给受感染的小鼠口服1mg的药物,并在1周后处死。结果:小鼠在感染后24小时接受了高剂量方案(口服/小鼠1mg口服),然后在三周后处死,与未处理的对照组相比,表明回收的未成熟蠕虫显着减少。感染后六周接受高剂量药物的动物,然后在一周后处死,动物的蠕虫数量和组织卵负荷(肝和肠)均下降,与未治疗相比,肝肉芽肿的测量最小控件。在给予低剂量方案的动物中,这些发现不太明显。结论:双氯芬酸可以成功地作为流行区的曼氏血吸虫感染的预防剂。

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