首页> 美国卫生研究院文献>Journal of Visualized Experiments : JoVE >Application of Long-term cultured Interferon-γ Enzyme-linked Immunospot Assay for Assessing Effector and Memory T Cell Responses in Cattle
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Application of Long-term cultured Interferon-γ Enzyme-linked Immunospot Assay for Assessing Effector and Memory T Cell Responses in Cattle

机译:长期培养的干扰素-γ酶联免疫斑点法在牛效应和记忆T细胞反应评估中的应用

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摘要

Effector and memory T cells are generated through developmental programing of naïve cells following antigen recognition. If the infection is controlled up to 95 % of the T cells generated during the expansion phase are eliminated (i.e., contraction phase) and memory T cells remain, sometimes for a lifetime. In humans, two functionally distinct subsets of memory T cells have been described based on the expression of lymph node homing receptors. Central memory T cells express C-C chemokine receptor 7 and CD45RO and are mainly located in T-cell areas of secondary lymphoid organs. Effector memory T cells express CD45RO, lack CCR7 and display receptors associated with lymphocyte homing to peripheral or inflamed tissues. Effector T cells do not express either CCR7 or CD45RO but upon encounter with antigen produce effector cytokines, such as interferon-γ. Interferon-γ release assays are used for the diagnosis of bovine and human tuberculosis and detect primarily effector and effector memory T cell responses. Central memory T cell responses by CD4+ T cells to vaccination, on the other hand, may be used to predict vaccine efficacy, as demonstrated with simian immunodeficiency virus infection of non-human primates, tuberculosis in mice, and malaria in humans. Several studies with mice and humans as well as unpublished data on cattle, have demonstrated that interferon-γ ELISPOT assays measure central memory T cell responses. With this assay, peripheral blood mononuclear cells are cultured in decreasing concentration of antigen for 10 to 14 days (long-term culture), allowing effector responses to peak and wane; facilitating central memory T cells to differentiate and expand within the culture.
机译:效应和记忆T细胞是通过抗原识别后的幼稚细胞的发育程序产生的。如果控制感染,则在扩张阶段(即收缩阶段)产生的T细胞的高达95%被消除,并且记忆T细胞得以保留,有时是一生的。在人类中,已经根据淋巴结归巢受体的表达描述了记忆T细胞的两个功能上不同的子集。中枢记忆T细胞表达C-C趋化因子受体7和CD45RO,主要位于次要淋巴器官的T细胞区域。效应记忆T细胞表达CD45RO,缺乏CCR7,并显示与淋巴细胞归巢至周围或发炎组织相关的受体。效应T细胞既不表达CCR7也不表达CD45RO,但是在遇到抗原时会产生效应细胞因子,例如干扰素-γ。 γ-干扰素释放测定法用于牛和人结核病的诊断,主要检测效应子和效应记忆T细胞反应。另一方面,CD4 + T细胞对疫苗的中央记忆T细胞反应可用于预测疫苗效力,如猿猴免疫缺陷病毒感染非人类灵长类动物,小鼠结核病所证明的那样,和人类的疟疾。几项关于小鼠和人类的研究以及未发表的关于牛的数据表明,干扰素-γELISPOT分析可测量中枢记忆T细胞反应。通过这种测定,外周血单核细胞以递减的抗原浓度培养10到14天(长期培养),从而使效应子对峰和峰减弱。促进中央记忆T细胞在培养物中分化和扩增。

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