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重组钩虫疫苗研发的实验方法。

Experimental approaches to the development of a recombinant hookworm vaccine.

作者信息

Hotez P J, Ghosh K, Hawdon J M, Narasimhan S, Jones B, Shuhua X, Sen L, Bin Z, Haechou X, Hainan R, Heng W, Koski R A

机构信息

Department of Epidemiology & Public Health, Yale University School of Medicine, New Haven, Connecticut 06520, USA.

出版信息

Immunol Rev. 1999 Oct;171:163-71. doi: 10.1111/j.1600-065x.1999.tb01347.x.

Abstract

Hookworm infection is a major parasitic cause of morbidity in the developing nations of the tropics. Development of a genetically engineered vaccine would be a useful tool in the control of this infection in highly endemic areas. Recombinant polypeptides belonging to the Ancylostoma secreted protein (ASP)-1 family have shown promise for reducing hookworm burdens after larval challenge infections in mice. Typically, these polypeptides are expressed in Escherichia coli and administered as an alum precipitate. Vaccine protection is antibody dependent. It is anticipated that a cocktail of different recombinant hookworm antigens may be required in order to effectively prevent heavy hookworm infections and disease. The progress of this work has been hampered by the absence of both a convenient laboratory animal with which to study hookworm infections resembling human infection, as well as the lack of easy availability of native hookworm antigens. In addition, useful human serologic correlates of antihookworm immunity are still poorly defined.

摘要

钩虫感染是热带地区发展中国家发病的主要寄生虫病因。开发基因工程疫苗将是在高度流行地区控制这种感染的有用工具。属于钩口线虫分泌蛋白(ASP)-1家族的重组多肽在小鼠幼虫攻击感染后显示出减轻钩虫负担的前景。通常,这些多肽在大肠杆菌中表达,并作为明矾沉淀物给药。疫苗保护依赖于抗体。预计可能需要不同重组钩虫抗原的混合物,以有效预防严重的钩虫感染和疾病。这项工作的进展受到阻碍,既缺乏便于研究类似人类感染的钩虫感染的实验动物,也缺乏天然钩虫抗原的容易获取途径。此外,抗钩虫免疫的有用人类血清学关联仍未明确界定。

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