Carotenuto P, Pontesilli O, Cambier J C, Hayward A R
J Immunol. 1986 Apr 1;136(7):2342-7.
Thymidine uptake by PHA-stimulated human lymphocytes is reduced in the presence of 100 microM or greater concentrations of the iron-chelating agent desferoxamine (DF). We assessed expression of IL 2 receptor, 4F2 and Ia antigens, IL 2 production, and cell cycle progression by blood mononuclear cells (MNC) stimulated by PHA in the presence or absence of DF to determine whether the lack of T cell proliferation was a manifestation of inhibition of an earlier activation event. Tac antigen expression on PHA-stimulated MNC was inhibited by DF throughout 8 days of culture, and those cells which were positive had a low density of Tac antigen as compared with controls without DF. Expression of other activation antigens, 4F2 and Ia, was not impaired by DF. The supernatants of the DF-containing and control cultures contained equivalent IL 2 activity, as measured on the HT-2 cell line. Cell cycle analysis of these cultures shows that the addition of DF at the beginning of culture blocks most cells from undergoing G0 to G1 transition, whereas later addition of DF arrests the progression of the T cell blasts through the cell cycle. Separation of cells cultured with PHA and DF into Tac+ and Tac- subsets showed that progression from G0 to G1 was restricted to the former subset. These results suggest that interference with IL 2 receptor expression might contribute to the block in mitogen-induced proliferation caused by DF.
在存在100微摩尔或更高浓度的铁螯合剂去铁胺(DF)的情况下,PHA刺激的人淋巴细胞对胸苷的摄取减少。我们评估了在有或没有DF的情况下,PHA刺激的血液单核细胞(MNC)中IL-2受体、4F2和Ia抗原的表达、IL-2的产生以及细胞周期进程,以确定T细胞增殖的缺乏是否是早期激活事件受到抑制的表现。在整个8天的培养过程中,DF抑制了PHA刺激的MNC上Tac抗原的表达,与没有DF的对照组相比,那些呈阳性的细胞Tac抗原密度较低。DF并未损害其他激活抗原4F2和Ia的表达。如在HT-2细胞系上所测,含DF培养物和对照培养物的上清液含有等量的IL-2活性。对这些培养物的细胞周期分析表明,在培养开始时添加DF会阻止大多数细胞从G0期向G1期转变,而在后期添加DF会使T细胞母细胞在细胞周期中的进程停滞。将用PHA和DF培养的细胞分离为Tac+和Tac-亚群表明,从G0期到G1期的进程仅限于前一个亚群。这些结果表明,对IL-2受体表达的干扰可能是DF导致有丝分裂原诱导的增殖受阻的原因。
