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使用从曼氏血吸虫克隆的重组谷胱甘肽S-转移酶对实验感染埃及血吸虫的派塔斯猴进行疫苗接种。

Vaccination of patas monkeys experimentally infected with Schistosoma haematobium using a recombinant glutathione S-transferase cloned from S. mansoni.

作者信息

Boulanger D, Warter A, Trottein F, Mauny F, Brémond P, Audibert F, Couret D, Kadri S, Godin C, Sellin E

机构信息

Centre de Recherche sur les Méningites et les Schistosomiases (CERMES/OCCGE/ORSTOM), Niamey, Niger.

出版信息

Parasite Immunol. 1995 Jul;17(7):361-9. doi: 10.1111/j.1365-3024.1995.tb00903.x.

DOI:10.1111/j.1365-3024.1995.tb00903.x
PMID:8552409
Abstract

The capacity of a recombinant glutathione S-transferase from Schistosoma mansoni (rSm28GST) to vaccinate primates (Erythrocebus patas) against a heterologous infection with Schistosoma haematobium has been tested. Two injections of the purified molecule with Muramyl-Di-Peptide (MDP) as adjuvant resulted in a high level antibody response in the five immunized animals and in a significant reduction in worm fecundity compared to the controls which received adjuvant alone. Mean levels of daily egg excretion in urine an faeces were reduced by respectively 55% and 74% although perfusion revealed that worm burdens were similar in both groups. The protective effect was long lasting since it was maintained up to the end of the experiment, 42 weeks after infection. Hatching rates and the numbers of intra-uterine eggs were also significantly affected by the vaccination. Tissue eggs were also drastically diminished in the urogenital system (-80%) but the reduction was not statistically significant. One animal was not protected by the immunization. There was a good correlation between parasitological data and the intensity of bladder lesions assessed by microscopic examination. Polypoid formations together with an intense exudation of the lamina propria were frequently seen in the controls but rarely in the vaccinated group where formation of scar tissue was predominant. These results underline the vaccine potential of the recombinant Sm28GST as a possible valuable prophylactic tool for the control of egg-induced pathology and transmission of African schistosomes.

摘要

已经对来自曼氏血吸虫的重组谷胱甘肽S-转移酶(rSm28GST)针对灵长类动物(赤猴)预防埃及血吸虫异源感染的能力进行了测试。用胞壁酰二肽(MDP)作为佐剂对纯化分子进行两次注射,导致五只免疫动物产生高水平抗体反应,与仅接受佐剂的对照组相比,虫体繁殖力显著降低。尿液和粪便中每日排虫卵量的平均水平分别降低了55%和74%,尽管灌注显示两组的虫负荷相似。保护作用持续时间长,因为在感染后42周的实验结束时仍保持这种作用。孵化率和子宫内虫卵数量也受到疫苗接种的显著影响。泌尿生殖系统中的组织虫卵也大幅减少(-80%),但减少不具有统计学显著性。有一只动物未受到免疫保护。寄生虫学数据与通过显微镜检查评估的膀胱病变强度之间存在良好的相关性。对照组中经常可见息肉样形成以及固有层的强烈渗出,而在接种疫苗组中很少见,接种疫苗组中主要是瘢痕组织形成。这些结果强调了重组Sm28GST作为控制非洲血吸虫卵诱导的病理和传播的一种可能有价值的预防工具的疫苗潜力。

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