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白细胞介素-12可刺激抗病毒的1型细胞因子反应,但在干扰素-γ受体缺陷小鼠中缺乏佐剂活性。

IL-12 stimulates an antiviral type 1 cytokine response but lacks adjuvant activity in IFN-gamma-receptor-deficient mice.

作者信息

Schijns V E, Haagmans B L, Horzinek M C

机构信息

Department of Infectious Diseases and Immunology, Veterinary Faculty, Ultrecht University, The Netherlands.

出版信息

J Immunol. 1995 Sep 1;155(5):2525-32.

PMID:7650382
Abstract

Cytokines can be used as adjuvants to enhance and direct protective immune responses induced by vaccines. IL-12, a cytokine that favors the maturation of Th1-type cells and stimulates associated cell-mediated responses was evaluated as immunologic adjuvant for a viral vaccine in a mouse challenge model. When it was administered together with inactivated pseudorabies virus, a herpes simplex virus related alpha-herpesvirus, increased production of IFN-gamma by ex vivo-stimulated splenocytes was observed as well as augmented production of antiviral serum lgG2a. This was associated with increased protection against a lethal challenge infection. Infection of IfN-gamma-neutralizing Ab reduced the increased antiviral resistance in IL-12-treated mice. Also, in mice bearing an inactivated IFN-gamma-receptor gene IL-12 failed to stimulate protection against challenge and the synthesis of antiviral lgG2a. However, in these IFN-gamma-receptor knockout mice, increased antiviral lgG2b levels and enhanced IFN-gamma-secretion, with minimal IL-4 production, by ex vivo-stimulated splenocytes was observed. In wild-type mice administration of recombinant IFN-gamma but not IL-2 mimicked the immune-stimulating activity of IL-12; it is therefore likely that the IL-12 adjuvant activity is largely mediated by physiologic IFN-gamma.

摘要

细胞因子可作为佐剂,增强并引导疫苗诱导的保护性免疫反应。白细胞介素-12(IL-12)是一种有助于Th1型细胞成熟并刺激相关细胞介导反应的细胞因子,在小鼠攻毒模型中被评估作为一种病毒疫苗的免疫佐剂。当它与灭活的伪狂犬病病毒(一种与单纯疱疹病毒相关的甲型疱疹病毒)一起给药时,观察到体外刺激的脾细胞产生的γ干扰素增加,以及抗病毒血清IgG2a的产生增加。这与对致死性攻毒感染的保护作用增强有关。γ干扰素中和抗体的感染降低了IL-12处理小鼠中增加的抗病毒抵抗力。此外,在携带灭活的γ干扰素受体基因的小鼠中,IL-12未能刺激对攻毒的保护作用以及抗病毒IgG2a的合成。然而,在这些γ干扰素受体敲除小鼠中,观察到体外刺激的脾细胞产生的抗病毒IgG2b水平增加,γ干扰素分泌增强,而白细胞介素-4产生极少。在野生型小鼠中,重组γ干扰素而非白细胞介素-2的给药模拟了IL-12的免疫刺激活性;因此,IL-12的佐剂活性很可能主要由生理性γ干扰素介导。

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