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Growth factors can enhance lymphocyte survival without committing the cell to undergo cell division.

机译:生长因子可以增强淋巴细胞存活,而不会使细胞发生细胞分裂。

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摘要

Growth factors have been defined by their ability to promote the proliferative expansion of receptor-bearing cells. For example, antigen-activated T cells expressing the alpha beta gamma form of the interleukin 2 (IL-2) receptor will proliferate in response to IL-2. In contrast, resting T cells, which express the IL-2 receptor beta and gamma chains, do not proliferate in response to IL-2. We demonstrate that the survival of resting T cells following gamma irradiation is greatly enhanced by pretreatment with IL-2. The radioprotective effect of IL-2 is dose dependent, does not result from the induction of cell proliferation, and does not require expression of the IL-2 receptor alpha chain. Thus, the beta gamma IL-2 receptor expressed on resting T cells can transduce signals that promote cell survival without committing the T cell to undergo cell division. IL-4 and IL-7, but not IL-1, IL-3, or IL-6, were also found to enhance the survival of quiescent T cells following gamma irradiation. Thus, certain growth factor-receptor interactions can serve to maintain cell viability in a manner that is independent of their ability to initiate or maintain cell proliferation. These data may have important implications for the use of growth factors in patients being treated with radiation and/or chemotherapy.
机译:生长因子已经通过它们促进带有受体的细胞的增殖扩展的能力来定义。例如,表达白介素2(IL-2)受体的αβγ形式的抗原激活的T细胞将响应IL-2增殖。相反,表达IL-2受体β和γ链的静止T细胞不响应IL-2而增殖。我们证明,用IL-2预处理可大大提高γ射线照射后静息T细胞的存活。 IL-2的辐射防护作用是剂量依赖性的,不是由细胞增殖诱导引起的,并且不需要表达IL-2受体α链。因此,在静止的T细胞上表达的βγIL-2受体可以转导促进细胞存活的信号,而不会使T细胞经历细胞分裂。还发现IL-4和IL-7,但不是IL-1,IL-3或IL-6,可以增强γ射线照射后静态T细胞的存活。因此,某些生长因子-受体相互作用可以以不依赖于它们启动或维持细胞增殖能力的方式来维持细胞活力。这些数据可能对在接受放射和/或化学疗法治疗的患者中生长因子的使用具有重要意义。

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