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人淋巴细胞上H-铁蛋白的特异性结合位点:细胞增殖过程中的调节及其对细胞生长控制的潜在影响

Specific binding sites for H-ferritin on human lymphocytes: modulation during cellular proliferation and potential implication in cell growth control.

作者信息

Fargion S, Fracanzani A L, Brando B, Arosio P, Levi S, Fiorelli G

机构信息

Institute of Internal Medicine, Milan, Italy.

出版信息

Blood. 1991 Aug 15;78(4):1056-61.

PMID:1831058
Abstract

Interactions between human recombinant H- and L-ferritins and human lymphocytes were studied in vitro by direct binding assays and by flow cytometry. L-ferritin did not cause detectable specific binding, whereas H-ferritin showed a specific and saturable binding that increased markedly in phytohemagglutinin (PHA)-stimulated cells. This ferritin bound up to 30% of CD4+ and CD8+ T-lymphocytes and most B cells, indicating that expression of ferritin binding sites is not related to cell lineage or function. Dual-color flow cytometry experiments showed that ferritin binding sites were present on cells expressing the proliferation markers HLA-DR, MLR3, interleukin 2 (IL-2), and transferrin receptors (Tf-R). In addition, after PHA induction, the time course of the expression of H-ferritin binding sites was similar to those of the above proliferation markers. Ferritin binding sites were observed in lymphocytes at all cell cycle phases, including the early S-phase. H-Ferritin at nanomolar and picomolar concentrations had an inhibitory effect on PHA-induced blastogenesis. We propose that H-ferritin binding sites behave like proliferation markers, with the unusual function of downregulating proliferation.

摘要

通过直接结合试验和流式细胞术在体外研究了人重组H-和L-铁蛋白与人淋巴细胞之间的相互作用。L-铁蛋白未引起可检测到的特异性结合,而H-铁蛋白显示出特异性和饱和性结合,在植物血凝素(PHA)刺激的细胞中显著增加。这种铁蛋白可结合高达30%的CD4+和CD8+ T淋巴细胞以及大多数B细胞,表明铁蛋白结合位点的表达与细胞谱系或功能无关。双色流式细胞术实验表明,铁蛋白结合位点存在于表达增殖标志物HLA-DR、MLR3、白细胞介素2(IL-2)和转铁蛋白受体(Tf-R)的细胞上。此外,PHA诱导后,H-铁蛋白结合位点表达的时间进程与上述增殖标志物相似。在包括早期S期在内的所有细胞周期阶段的淋巴细胞中均观察到铁蛋白结合位点。纳摩尔和皮摩尔浓度的H-铁蛋白对PHA诱导的细胞增殖有抑制作用。我们提出,H-铁蛋白结合位点的行为类似于增殖标志物,具有下调增殖的异常功能。

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