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日本血吸虫肌球蛋白:曼氏血吸虫肌球蛋白片段IrV-5同源物的克隆、表达及疫苗接种研究

Schistosoma japonicum myosin: cloning, expression and vaccination studies with the homologue of the S. mansoni myosin fragment IrV-5.

作者信息

Zhang Y, Taylor M G, Bickle Q D

机构信息

Department of Infectious and Tropical Diseases, London School of Hygiene and Tropical Medicine, UK.

出版信息

Parasite Immunol. 1998 Dec;20(12):583-94. doi: 10.1046/j.1365-3024.1998.00189.x.

Abstract

The Schistosoma japonicum homologue of the 62 kDa fragment of S. mansoni myosin (SmIrV-5), which has proved highly protective against S. mansoni infection in mice and rats, has been cloned and expressed as the full length 62 kDa equivalent, Sj62, and a truncated 44 kDa version, Sj44. DNA sequencing showed the Sj62 sequence to be 88.4% identical at the nucleic acid level and 96% identical in deduced amino acid sequence to that of SmIrV-5. The recombinant proteins (rSj44 and rSj62) were strongly recognized in Western blotting by sera from mice multiply vaccinated with UV-irradiated S. japonicum cercariae and weakly recognized by S. japonicum chronic infection mouse sera. Unlike SmIrV-5, mouse antisera against the recombinant S. japonicum proteins did not give positive recognition in immunofluorescence assay with the surface of newly transformed schistosomula of the homologous species, S. japonicum, nor did they react with S. mansoni schistosomula. However, the anti-rSj62 sera clearly localized the native antigen to the subtegumental muscle layers in male adult worm sections by immunoelectron microscopy. Vaccination of several groups of mice and/or rats with rSj44 and rSj62 incorporated into different adjuvants induced high titres of specific IgG but in only one experimental group was there a significant reduction in worm burden (27%, P < 0.05). The possible reasons for the disparity between the vaccination results presented here and those demonstrated in experiments using rSm62 (IrV-5) are discussed.

摘要

曼氏血吸虫肌球蛋白62 kDa片段(SmIrV-5)的日本血吸虫同源物已被克隆并表达为全长62 kDa的等效物Sj62和截短的44 kDa版本Sj44,该同源物已被证明对小鼠和大鼠的曼氏血吸虫感染具有高度保护作用。DNA测序显示,Sj62序列在核酸水平上与SmIrV-5的序列有88.4%的同一性,在推导的氨基酸序列上有96%的同一性。重组蛋白(rSj44和rSj62)在蛋白质免疫印迹中被多次接种紫外线照射的日本血吸虫尾蚴的小鼠血清强烈识别,而被日本血吸虫慢性感染小鼠血清弱识别。与SmIrV-5不同,针对重组日本血吸虫蛋白的小鼠抗血清在对同源物种日本血吸虫新转化的童虫表面进行免疫荧光测定时未给出阳性识别,也不与曼氏血吸虫童虫反应。然而,抗rSj62血清通过免疫电子显微镜清楚地将天然抗原定位在雄性成虫切片的皮下肌层。用掺入不同佐剂的rSj44和rSj62对几组小鼠和/或大鼠进行疫苗接种诱导了高滴度的特异性IgG,但只有一个实验组的虫负荷有显著降低(27%,P<0.05)。本文讨论了此处呈现的疫苗接种结果与使用rSm62(IrV-5)的实验结果之间差异可能的原因。

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