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白细胞介素-2和催乳素对T细胞和NK细胞来源的淋巴因子激活的杀伤细胞(LAK)效应细胞发育的独立及协同作用。

Independent and synergistic effect of interleukin-2 and prolactin on development of T- and NK-derived LAK effectors.

作者信息

Cesano A, Oberholtzer E, Contarini M, Geuna M, Bellone G, Matera L

机构信息

Istituto di Medicina Interna, Università di Torino, Italy.

出版信息

Immunopharmacology. 1994 Jul-Aug;28(1):67-75. doi: 10.1016/0162-3109(94)90040-x.

DOI:10.1016/0162-3109(94)90040-x
PMID:7928303
Abstract

We have studied the effect of recombinant (r)-Prl on the in vitro-induced MHC-unrestricted cytotoxicity of NK and T cells. A 4-day treatment with r-Prl in serum-free medium enhanced the cytotoxicity of NK cells to the NK-susceptible cell lines K562 and U937, but did not induce de novo NK cytotoxicity in T lymphocytes. By contrast, development of cytotoxicity against the LAK-susceptible cell lines HL60, Jurkat, Daudi and Supt-1 occurred in both NK and T cells. The effect of r-Prl on NK cells was bi-phasic with peaks at 25 ng/ml (1.2 nM), the upper physiological level, and 200 ng/ml (9.6 nM). By contrast, LAK activation of T cells only occurred at the highest r-Prl concentration. In addition to its intrinsic stimulatory activity, r-Prl was also capable of modulating in a dose-dependent manner distinct stages of the IL2-driven LAK/T differentiation pathway. Physiological concentrations of r-Prl interacted with low doses r-IL2 to significantly enhance generation of NK- and T-LAK activities. By contrast, pathological concentrations had opposite effects on generation of optimal LAK response, depending on the kind of LAK progenitor. The T-derived LAK activity was reversibly inhibited at the effector level, while the mature NK-LAK cells were stimulated. These data confirm our previous findings of a co-operative effect of Prl and IL2 on NK cell proliferation and reinforce the view that the signals conveyed by the two factors may be functionally related.

摘要

我们研究了重组(r)-催乳素对体外诱导的自然杀伤细胞(NK)和T细胞的MHC非限制性细胞毒性的影响。在无血清培养基中用r-催乳素处理4天可增强NK细胞对NK敏感细胞系K562和U937的细胞毒性,但不会在T淋巴细胞中诱导新的NK细胞毒性。相比之下,NK细胞和T细胞均出现了对LAK敏感细胞系HL60、Jurkat、Daudi和Supt-1的细胞毒性。r-催乳素对NK细胞的作用呈双相性,在25 ng/ml(1.2 nM)(生理上限水平)和200 ng/ml(9.6 nM)处出现峰值。相比之下,T细胞的LAK激活仅在最高r-催乳素浓度下发生。除了其内在的刺激活性外,r-催乳素还能够以剂量依赖的方式调节IL2驱动的LAK/T分化途径的不同阶段。r-催乳素的生理浓度与低剂量r-IL2相互作用,可显著增强NK和T-LAK活性的产生。相比之下,病理浓度根据LAK祖细胞的类型对最佳LAK反应的产生有相反的影响。T衍生的LAK活性在效应水平上被可逆抑制,而成熟的NK-LAK细胞则受到刺激。这些数据证实了我们之前关于催乳素和IL2对NK细胞增殖有协同作用的发现,并强化了这两种因子传递的信号可能在功能上相关的观点。

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Independent and synergistic effect of interleukin-2 and prolactin on development of T- and NK-derived LAK effectors.白细胞介素-2和催乳素对T细胞和NK细胞来源的淋巴因子激活的杀伤细胞(LAK)效应细胞发育的独立及协同作用。
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