首页> 外文期刊>Immunology and Cell Biology >Automatic generation of lymphocyte heterogeneity: Division-dependent changes in the expression of CD27, CCR7 and CD45 by activated human naive CD4+ T cells are independently regulated.
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Automatic generation of lymphocyte heterogeneity: Division-dependent changes in the expression of CD27, CCR7 and CD45 by activated human naive CD4+ T cells are independently regulated.

机译:淋巴细胞异质性的自动产生:激活的人类幼稚CD4 + T细胞对CD27,CCR7和CD45表达的分区依赖性变化是独立调节的。

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摘要

Lymphocyte differentiation is a complex process regulated by the integration of signals received through a variety of cell surface receptors that results in populations of differentiated cells that have acquired novel characteristics and effector functions. Differentiation of T and B lymphocytes into effector cells, such as cytokine-secreting CD4+ T cells, cytotoxic CD8+ T cells and Ig-secreting B cells, as well as alterations in cell surface phenotype, have been reported to be associated with cell division. Nevertheless, the genesis of heterogeneity in effector cell type is unknown. A strictly deterministic view holds that heterogeneity arises from distinct signalling histories for each functionally or phenotypically different cell type. In contrast, a probabilistic interpretation proposes that internal stochastic regulation of gene expression gives rise to lymphocytes of mixed phenotypes. To help distinguish between these explanations, we examined the expression of CD27, CCR7, CD45RA and CD45RO by human naive CD4+ T cells in the context of the division history of the lymphocyte. Our results show that each marker independently changes with progressive divisions, strongly supporting the proposal that phenotypic heterogeneity in lymphocytes can arise as the result of independent stochastic processes controlling the expression of individual molecules.
机译:淋巴细胞分化是一个复杂的过程,受各种细胞表面受体接收到的信号整合的调节,从而导致分化细胞群体获得新特性和效应子功能。 T和B淋巴细胞分化为效应细胞,例如分泌细胞因子的CD4 + T细胞,细胞毒性CD8 + T细胞和分泌Ig的B细胞,以及细胞表面表型的改变,都与细胞分裂有关。然而,效应细胞类型异质性的起源尚不清楚。严格的确定性观点认为,异质性源于每种功能或表型不同细胞类型的不同信号传导历史。相反,概率解释表明基因表达的内部随机调节产生混合表型的淋巴细胞。为帮助区分这些解释,我们在淋巴细胞分裂史的背景下检查了人类幼稚CD4 + T细胞对CD27,CCR7,CD45RA和CD45RO的表达。我们的结果表明,每个标记物都随着进行性分裂而独立变化,这强烈支持了淋巴细胞表型异质性可能是由于控制单个分子表达的独立随机过程的结果而引起的提议。

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