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用于同时诱导体液免疫和细胞介导免疫的新型蛋白质和基于痘病毒的疫苗组合。

Novel protein and poxvirus-based vaccine combinations for simultaneous induction of humoral and cell-mediated immunity.

作者信息

Hutchings Claire L, Gilbert Sarah C, Hill Adrian V S, Moore Anne C

机构信息

Wellcome Trust Centre for Human Genetics, University of Oxford, Oxford, United Kingdom.

出版信息

J Immunol. 2005 Jul 1;175(1):599-606. doi: 10.4049/jimmunol.175.1.599.

Abstract

The presence of both cell-mediated and humoral immunity is important in protection from and clearance of a number of infectious pathogens. We describe novel vaccine regimens using combinations of plasmid DNA, poxvirus and protein to induce strong Ag-specific T cell and Ab responses simultaneously in a murine model. Intramuscular (i.m.) immunization with plasmid DNA encoding the middle Ag of hepatitis B (DNA) concurrently with a commercial hepatitis B virus (HBV) vaccine (Engerix-B) followed by boosting immunizations with both modified vaccinia virus Ankara (MVA) encoding the middle Ag of HBV and Engerix-B induced high levels of CD4(+) and CD8(+) T cells and high titer Ab responses to hepatitis B surface Ag (HbsAg). Substitution of Engerix-B with adjuvant-free rHBsAg induced similar T cell responses and greatly enhanced Ab levels. Repeated immunizations with recombinant or nonrecombinant MVA mixed with Ag induced higher titers of Abs compared with immunization with either Ag or Engerix-B further demonstrating this novel adjuvant effect of MVA. The poxviruses NYVAC, fowlpox (FP9) and ALVAC, and to a lesser extent, adenovirus, also displayed similar adjuvant properties when used in combination with rHBsAg. The use of poxviruses as an adjuvant for protein to concurrently induce Ag-specific T cells and Abs could be applied to the development of vaccines for many diseases, including HIV and malaria, where both cell mediated and humoral immunity may be important for protection.

摘要

细胞介导免疫和体液免疫的存在对于抵御多种感染性病原体并将其清除至关重要。我们描述了在小鼠模型中使用质粒DNA、痘病毒和蛋白质的组合来诱导强烈的抗原特异性T细胞和抗体反应的新型疫苗方案。用编码乙肝病毒核心抗原的质粒DNA进行肌肉注射免疫(i.m.),同时接种市售乙肝疫苗(安在时),随后用编码乙肝病毒核心抗原的改良安卡拉痘苗病毒(MVA)和安在时进行加强免疫,可诱导产生高水平的CD4(+)和CD8(+) T细胞以及对乙肝表面抗原(HbsAg)的高滴度抗体反应。用无佐剂的重组乙肝表面抗原(rHBsAg)替代安在时可诱导相似的T细胞反应,并显著提高抗体水平。与单独使用抗原或安在时免疫相比,用重组或非重组MVA与抗原混合进行重复免疫可诱导产生更高滴度的抗体,这进一步证明了MVA的这种新型佐剂作用。痘病毒NYVAC、鸡痘(FP9)和ALVAC,以及程度较轻的腺病毒,与rHBsAg联合使用时也表现出类似的佐剂特性。将痘病毒用作蛋白质佐剂以同时诱导抗原特异性T细胞和抗体,可应用于包括HIV和疟疾在内的许多疾病的疫苗开发,在这些疾病中,细胞介导免疫和体液免疫对于保护机体可能都很重要。

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