Dokhélar M C, Garson D, Testa U, Tursz T
Eur J Immunol. 1984 Apr;14(4):340-4. doi: 10.1002/eji.1830140412.
The transferrin receptor (TfR) was recently proposed as putative natural killer (NK) cell target structure. Here data are presented against this hypothesis and it is shown that low TfR expression and high NK sensitivity can occur concommitantly . K562 cells were studied at various stages of cell proliferation. No change in NK sensitivity could be observed between exponential growth and the plateau phase, whereas TfR expression completely disappeared during the latter. Protein synthesis inhibitors such as cycloheximide (1 microgram/ml, 48 h) and actinomycin D (50 micrograms/ml, 48 h), that abolished the TfR expression at the K562 cell surface, had no effect on NK sensitivity. Similarly, hemin induction (0.1 mM, 5 days) did not change NK susceptibility of K562 cells but considerably diminished TfR expression. Moreover, attempts to block NK sensitivity with anti-TfR monoclonal antibodies were unsuccessful, even when the 42.6 antibody, which is known to bind to the active site of TfR, was used. Finally, no blocking of NK sensitivity could be achieved when K562 cells were preincubated with saturating concentrations of transferrin or when transferrin was added during the NK assay. It therefore seems doubtful that TfR is the unique target structure for NK cells. It remains possible that TfR and NK target structures are often coexpressed on actively dividing cells.
转铁蛋白受体(TfR)最近被认为是天然杀伤(NK)细胞的假定靶结构。本文提供的数据反对这一假说,并表明低TfR表达和高NK敏感性可同时出现。对处于细胞增殖不同阶段的K562细胞进行了研究。在指数生长期和平稳期之间未观察到NK敏感性的变化,而在后一阶段TfR表达完全消失。蛋白质合成抑制剂如环己酰亚胺(1微克/毫升,48小时)和放线菌素D(50微克/毫升,48小时)可消除K562细胞表面的TfR表达,但对NK敏感性没有影响。同样,血红素诱导(0.1毫摩尔,5天)不会改变K562细胞的NK易感性,但会显著降低TfR表达。此外,用抗TfR单克隆抗体阻断NK敏感性的尝试未成功,即使使用已知能结合TfR活性位点的42.6抗体也是如此。最后,当K562细胞用饱和浓度的转铁蛋白预孵育或在NK检测期间加入转铁蛋白时,均无法实现对NK敏感性的阻断。因此,TfR是否是NK细胞的唯一靶结构值得怀疑。TfR和NK靶结构经常在活跃分裂的细胞上共同表达仍是有可能的。
