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用查巴迪疟原虫多价DNA疫苗对A/J小鼠进行接种,可使其对查巴迪疟原虫DK株和强毒查巴迪疟原虫AS株的攻击产生交叉保护。

Vaccination with a Plasmodium chabaudi adami multivalent DNA vaccine cross-protects A/J mice against challenge with P. c. adami DK and virulent Plasmodium chabaudi chabaudi AS parasites.

作者信息

Scorza T, Grubb K, Cambos M, Santamaria C, Tshikudi Malu D, Spithill T W

机构信息

Department of Biological Sciences, Université du Québec à Montréal, Case postale 8888, Succursale Centre-Ville, Montréal, Quebec, Canada.

出版信息

Int J Parasitol. 2008 Jun;38(7):819-27. doi: 10.1016/j.ijpara.2007.10.009. Epub 2007 Nov 20.

Abstract

A current goal of malaria vaccine research is the development of vaccines that will cross-protect against multiple strains of malaria. In the present study, the breadth of cross-reactivity induced by a 30K multivalent DNA vaccine has been evaluated in susceptible A/J mice (H-2a) against infection with the Plasmodium chabaudi adami DK strain and a virulent parasite subspecies, Plasmodium chabaudi chabaudi AS. Immunized A/J mice were significantly protected against infection with both P. c. adami DK (31-40% reduction in cumulative parasitemia) and P. c. chabaudi AS parasites, where a 30-39% reduction in cumulative parasitemia as well as enhanced survival was observed. The 30K vaccine-induced specific IFN-gamma production by splenocytes in response to native antigens from both P. c. chabaudi AS and P. c. adami DK. Specific antibodies reacting with surface antigens expressed on P. c. adami DS and P. c. chabaudi AS infected red blood cells, and with opsonizing properties, were detected. These results suggest that multivalent vaccines encoding conserved antigens can feasibly induce immune cross-reactivity that span Plasmodium strains and subspecies and can protect hosts of distinct major histocompatibility complex haplotypes.

摘要

疟疾疫苗研究的当前目标是开发能够对多种疟疾菌株产生交叉保护作用的疫苗。在本研究中,已在易感的A/J小鼠(H-2a)中评估了一种30K多价DNA疫苗诱导的交叉反应广度,以抵抗恰氏疟原虫DK株和一种毒性寄生虫亚种——恰氏疟原虫AS的感染。免疫的A/J小鼠对恰氏疟原虫DK(累积虫血症降低31%-40%)和恰氏疟原虫AS寄生虫感染均有显著保护作用,累积虫血症降低30%-39%,同时观察到存活率提高。30K疫苗可诱导脾细胞针对来自恰氏疟原虫AS和恰氏疟原虫DK的天然抗原产生特异性干扰素-γ。检测到与恰氏疟原虫DS和恰氏疟原虫AS感染的红细胞表面表达的表面抗原发生反应且具有调理特性的特异性抗体。这些结果表明,编码保守抗原的多价疫苗能够切实诱导跨越疟原虫菌株和亚种的免疫交叉反应,并能保护具有不同主要组织相容性复合体单倍型的宿主。

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