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非转铁蛋白结合铁对小鼠T淋巴细胞亚群的影响:克隆技术分析

The effect of non-transferrin-bound iron on murine T lymphocyte subsets: analysis by clonal techniques.

作者信息

Good M F, Powell L W, Halliday J W

机构信息

Department of Medicine, University of Queensland, royal Brisbane Hospital, Australia.

出版信息

Clin Exp Immunol. 1987 Oct;70(1):164-72.

Abstract

A number of different immunological properties have been attributed to iron (Fe3+ and Fe2+) and iron-binding proteins. However, in many previous studies, high concentrations of iron were used and cell-cell interactions were not excluded as a possible cause of the observed immunomodulatory effects. In this study, clonal techniques have been used to examine the effect of non-transferrin-bound iron (Fe3+) on the T lymphocyte subsets required for the generation of cytotoxic T lymphocytes (CTL). Concentrations of non-transferrin-bound Fe3+ of 10 microM or greater were shown to inhibit the generation of C57, BALB/c and CBA allo-specific CTL in bulk culture. Limit-dilution analysis revealed that: (i) Fe3+ reduced the cloning efficiency of CTL-precursors (CTL-P) by up to 96% without affecting the rate of clone growth; (ii) Fe3+ did not affect the cloning efficiency of allo-stimulated Ly-2-ve T cell precursors but reduced the rate of clone growth of these cells; (iii) Fe3+ enhanced, by more than 13-fold, the function of clones of Concanavalin A (Con A)-induced suppressor T lymphocytes (STL) which suppressed in vitro the development of CTL from their precursor cells. The data provide further evidence that low concentrations of non-transferrin-bound Fe3+, of the same order as those reported to be present in the serum of patients with iron-overload, have significant immunoregulatory properties.

摘要

许多不同的免疫特性已被归因于铁(Fe3+和Fe2+)及铁结合蛋白。然而,在许多先前的研究中,使用的是高浓度的铁,并且未排除细胞间相互作用作为观察到的免疫调节作用的可能原因。在本研究中,已使用克隆技术来检测非转铁蛋白结合铁(Fe3+)对细胞毒性T淋巴细胞(CTL)产生所需的T淋巴细胞亚群的影响。结果显示,在批量培养中,10 microM或更高浓度的非转铁蛋白结合Fe3+可抑制C57、BALB/c和CBA同种异体特异性CTL的产生。极限稀释分析表明:(i)Fe3+可使CTL前体细胞(CTL-P)的克隆效率降低多达96%,而不影响克隆生长速率;(ii)Fe3+不影响同种异体刺激的Ly-2阴性T细胞前体细胞的克隆效率,但降低了这些细胞的克隆生长速率;(iii)Fe3+使伴刀豆球蛋白A(Con A)诱导的抑制性T淋巴细胞(STL)克隆的功能增强了13倍以上,这些克隆在体外抑制了CTL从前体细胞的发育。这些数据进一步证明,与铁过载患者血清中报道的浓度处于同一水平的低浓度非转铁蛋白结合Fe3+具有显著的免疫调节特性。

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