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未来抗鞭虫疫苗的抗原选择:初次感染中细胞因子和抗体对幼虫及成虫抗原反应的比较

Antigen selection for future anti-Trichuris vaccines: a comparison of cytokine and antibody responses to larval and adult antigen in a primary infection.

作者信息

Dixon H, Johnston C E, Else K J

机构信息

Faculty of Life Sciences, Michael Smith Building, University of Manchester, Oxford Road, Manchester, UK.

出版信息

Parasite Immunol. 2008 Sep;30(9):454-61. doi: 10.1111/j.1365-3024.2008.01035.x. Epub 2008 Jun 17.

Abstract

Trichuriasis, caused by the whipworm Trichuris trichiura, is endemic in tropical and subtropical areas, affecting approximately 1 billion people. Child anthelminthic treatment programmes are being implemented but repeated treatments are costly, may prevent the development of acquired immunity and can lead to the development of drug resistant parasites. Thus, the development of a vaccine which would lead to the acquisition of immunity at an earlier age and reduce community faecal egg output would be beneficial. Development of subunit vaccines requires the identification of protective antigens and their formulation in a suitable adjuvant. Trichuris muris is an antigenically similar laboratory model for T. trichiura. Subcutaneous vaccination with adult excretory-secretory products (ES) protects susceptible mouse strains from T. muris. Larval stages may contain novel and more relevant antigens which when incorporated in a vaccine induce worm expulsion earlier in infection than the adult worm products. This study finds negligible difference in the cellular and humoral immune response to T. muris adult and third stage larva(e) (L3) ES during a primary T. muris infection, but identifies high molecular weight proteins in both adult and L3 ES as potential vaccine candidates.

摘要

鞭虫病由毛首鞭形线虫引起,在热带和亚热带地区流行,约有10亿人受其影响。目前正在实施儿童驱虫治疗项目,但反复治疗成本高昂,可能会阻碍获得性免疫的发展,并可能导致产生耐药性寄生虫。因此,开发一种能使人们在更早年龄获得免疫力并减少社区粪便虫卵排出量的疫苗将大有裨益。亚单位疫苗的开发需要鉴定保护性抗原并将其与合适的佐剂配制成型。鼠鞭虫是与毛首鞭形线虫抗原相似的实验模型。用成虫排泄分泌产物(ES)进行皮下接种可保护易感小鼠品系免受鼠鞭虫感染。幼虫阶段可能含有新的且更具相关性的抗原,将其用于疫苗中,与成虫产物相比,能在感染早期诱导排虫。本研究发现,在初次感染鼠鞭虫期间,对鼠鞭虫成虫和第三期幼虫(L3)ES的细胞免疫和体液免疫反应差异可忽略不计,但鉴定出成虫和L3 ES中的高分子量蛋白均为潜在的疫苗候选物。

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