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Species specialization in cytokine biology: Is interleukin-4 central to the T(H)1-T(H)2 paradigm in swine?

机译:专门从事细胞因子生物学研究的物种:白细胞介素4是猪T(H)1-T(H)2范例的核心吗?

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The T(H)1-T(H)2 paradigm provides an elegant model of directed response to infectious pathogens. Developed in the mouse, the model has provided a framework for systematic and mechanistic studies of immune regulation, protective immunity, and vaccine development in swine. Interleukin-4 (IL-4) plays a central role in the paradigm as a regulatory molecule directing development of the T(H)2 phenotype, as a developmental cytokine essential for antibody production, and as a soluble diagnostic marker of the T(H)2 cell type. In contrast, while characterizing the biological properties of porcine IL-4, we discovered that it was not a stimulatory factor for porcine B cells. Rather, it blocked antibody and IL-6 secretion and suppressed antigen-stimulated proliferation of B cells. Inhibition was not reversed by treatment with IL-2 and IL-6 treatment. IL-4 did not stimulate T lymphocyte proliferation, but induced cell growth in lymphoblasts in a dose-dependent fashion. These results suggest that IL-4 plays a different role in pigs than in mice and humans, in which it stimulates B cells and is essential for antibody production. Furthermore, the functions of IL-4 in swine cannot be inferred from results in model systems such as the mouse. General models of disease resistance show substantial variation between pigs and mice at the cellular and molecular level. Advances in somatic cell technologies and animal engineering to enable gene knockouts in pigs, in combination with a continuously expanding immunological toolkit, promise an exciting future for pig immunology, detailed mechanistic elucidation of the T(H)1-T(H)2 paradigm, and an improved understanding of the role of IL-4 in porcine immunity to infectious disease.
机译:T(H)1-T(H)2范式为传染病病原体的定向反应提供了一个优雅的模型。该模型是在小鼠体内开发的,为猪的免疫调节,保护性免疫和疫苗开发的系统和机制研究提供了框架。白介素-4(IL-4)在范式中起着核心作用,它是指导T(H)2表型发展的调节分子,抗体产生所必需的发育性细胞因子以及T(H)的可溶性诊断标记)2个单元格类型。相反,在表征猪IL-4的生物学特性时,我们发现它不是猪B细胞的刺激因子。相反,它阻断了抗体和IL-6的分泌,并抑制了抗原刺激的B细胞增殖。通过IL-2和IL-6处理不能抑制抑制作用。 IL-4不会刺激T淋巴细胞增殖,但会以剂量依赖的方式诱导淋巴母细胞中的细胞生长。这些结果表明,IL-4在猪中的作用与在小鼠和人类中的作用不同,在IL-4中,IL-4刺激B细胞,并且对于产生抗体至关重要。此外,不能从诸如小鼠的模型系统的结果中推断出猪中IL-4的功能。一般的抗病模型显示,猪和小鼠之间在细胞和分子水平上存在很大差异。体细胞技术和动物工程学的发展使猪能够进行基因敲除,再加上不断扩展的免疫学工具包,为猪的免疫学,T(H)1-T(H)2范式的详细机理阐明,前景光明,以及对IL-4在猪对传染病的免疫中的作用的进一步了解。

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