Bell Eric B, Westermann Jürgen
Faculty of Life Sciences, Immunology Section, University of Manchester, Manchester M13 9PT, UK.
Trends Immunol. 2008 Sep;29(9):405-11. doi: 10.1016/j.it.2008.06.002. Epub 2008 Jul 31.
Immunological memory crucially depends on CD4 T cells. In contrast with B cells, we find no decisive evidence that CD4 T cells are permanently altered by antigen stimulation. We propose that the memory response is derived from an increase in frequency of resting naïve-like CD4 T cells with a half-life of years (or months in rodents), rather than the currently proposed specialized T-cell types that have a known lifespan of days. In addition, residual antigen will significantly influence the longevity of a memory response. Our model offers a new insight into immunological memory that could assist the development of CD4 T cell-based vaccines.
免疫记忆至关重要地依赖于CD4 T细胞。与B细胞不同,我们没有发现决定性证据表明CD4 T细胞会因抗原刺激而发生永久性改变。我们提出,记忆反应源自半衰期长达数年(在啮齿动物中为数月)的静息幼稚样CD4 T细胞频率的增加,而不是目前所提出的寿命已知为数天的特殊T细胞类型。此外,残留抗原将显著影响记忆反应的持久性。我们的模型为免疫记忆提供了新的见解,这可能有助于基于CD4 T细胞的疫苗的开发。
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