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禽痘病毒-粒细胞巨噬细胞集落刺激因子(Avipox-GM-CSF)与重组GM-CSF蛋白作为不同疫苗平台免疫佐剂的比较研究。

Comparative studies of Avipox-GM-CSF versus recombinant GM-CSF protein as immune adjuvants with different vaccine platforms.

作者信息

Reali E, Canter D, Zeytin H, Schlom J, Greiner J W

机构信息

Laboratory of Tumor Immunology and Biology, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Vaccine. 2005 Apr 22;23(22):2909-21. doi: 10.1016/j.vaccine.2004.11.060.

Abstract

Granulocyte-macrophage colony-stimulating factor (GM-CSF) is a potent immune stimulant when administered with different vaccines. Optimal use of GM-CSF resides in its ability to act locally to stimulate the proliferation and maturation of professional antigen-presenting cells (APCs) (i.e., Langerhans' cells) at the injection site. GM-CSF was engineered into a replication-incompetent recombinant avian (fowlpox) virus (rF-GM-CSF) and a single subcutaneous injection resulted in a sustained enrichment of activated dendritic cells within the regional draining lymph nodes. Those changes were attributed to local GM-CSF production at the injection site by rF-GM-CSF-infected cells. Studies were carried out in which mice were administered different types of beta-galactosidase (beta-gal)-based vaccines--whole protein, peptide, recombinant poxviruses--and GM-CSF was administered either as a single injection of rF-GM-CSF or four daily bolus injections of the recombinant protein. The use of rF-GM-CSF either improved the immune adjuvant effect, as observed for poxvirus-based vaccines, or was equivalent to rGM-CSF, as observed with the beta-gal protein vaccine. It is important to note that with either the replication-competent (vaccinia) or replication-incompetent (fowlpox) vaccines expressing LacZ, strong CTL responses directed against beta-gal were induced only when rF-GM-CSF was used as the immune adjuvant. Engineering GM-CSF into a recombinant fowlpox virus offers an excellent vehicle for the delivery of this cytokine as an immune adjuvant with specific vaccine platforms. In particular, delivery of GM-CSF via the rF-GM-CSF construct would be preferred over bolus injections of rGM-CSF when used as an immune adjuvant with whole protein or recombinant poxvirus-based vaccines. The study underscores the importance of defining the appropriate delivery form of an immune adjuvant, such as GM-CSF, relative to the immunization strategy to maximize the host immune responses against a specific antigen.

摘要

粒细胞巨噬细胞集落刺激因子(GM-CSF)与不同疫苗联合使用时是一种有效的免疫刺激剂。GM-CSF的最佳应用在于其能够在局部发挥作用,刺激注射部位专业抗原呈递细胞(APC,即朗格汉斯细胞)的增殖和成熟。GM-CSF被构建到一种无复制能力的重组禽痘病毒(rF-GM-CSF)中,单次皮下注射可导致区域引流淋巴结内活化树突状细胞持续富集。这些变化归因于rF-GM-CSF感染的细胞在注射部位产生局部GM-CSF。开展了多项研究,给小鼠接种不同类型的基于β-半乳糖苷酶(β-gal)的疫苗——全蛋白、肽、重组痘病毒——GM-CSF要么以单次注射rF-GM-CSF的形式给药,要么以重组蛋白每日四次推注的形式给药。使用rF-GM-CSF要么改善了免疫佐剂效果(如基于痘病毒的疫苗所见),要么与重组GM-CSF相当(如β-gal蛋白疫苗所见)。需要注意的是,对于表达LacZ的有复制能力(痘苗病毒)或无复制能力(禽痘病毒)的疫苗,仅当使用rF-GM-CSF作为免疫佐剂时,才会诱导针对β-gal的强烈CTL反应。将GM-CSF构建到重组禽痘病毒中为作为免疫佐剂与特定疫苗平台一起递送这种细胞因子提供了一种极佳的载体。特别是,当与全蛋白或基于重组痘病毒的疫苗一起用作免疫佐剂时,通过rF-GM-CSF构建体递送GM-CSF比推注rGM-CSF更可取。该研究强调了确定免疫佐剂(如GM-CSF)相对于免疫策略的合适递送形式以最大化宿主针对特定抗原的免疫反应的重要性。

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