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人髓细胞对两种功能不同类型的粒细胞-巨噬细胞集落刺激因子受体的分化相关表达。

Differentiation-associated expression of two functionally distinct classes of granulocyte-macrophage colony-stimulating factor receptors by human myeloid cells.

作者信息

Cannistra S A, Koenigsmann M, DiCarlo J, Groshek P, Griffin J D

机构信息

Division of Tumor Immunology, Dana-Farber Cancer Institute, Harvard Medical School, Boston, Massachusetts 02115.

出版信息

J Biol Chem. 1990 Jul 25;265(21):12656-63.

PMID:2165070
Abstract

Granulocyte-macrophage colony-stimulating factor (GM-CSF) activates a broad range of myeloid cells through binding to high affinity surface membrane receptors. The effects of this hematopoietin are dependent upon the differentiation status of the myeloid cell and range from proliferation of early myeloid progenitor cells to activation of neutrophil and monocyte function. In addition, many of the biological effects of GM-CSF are shared with interleukin-3 (IL-3), a distantly related lymphokine. In this study, we have characterized the GM-CSF receptor of myeloid cells at various stages of differentiation by comparing the binding characteristics and surface regulation of this receptor in early versus late myeloid cells. Scatchard analysis revealed a single class of high affinity receptors on normal neutrophils, monocytes, and myeloblasts from patients with acute myeloid leukemia. Neutrophils expressed significantly higher numbers of receptors, with an approximately 2-fold lower affinity, when compared with other myeloid cells. Two different patterns of GM-CSF receptor regulation and binding were observed. In the first pattern, the GM-CSF receptor of neutrophils was rapidly down-regulated by GM-CSF itself, by phorbol myristate acetate (PMA), and by the calcium ionophore A23187, and it was not competed for by IL-3 (class I receptor). In contrast to the neutrophil receptor, the GM-CSF receptor of the myeloblast demonstrated resistance to the down-regulatory effects of GM-CSF itself, PMA, and A23187, and it was completely competed for by IL-3 (class II receptor). In some cases of acute myeloid leukemia and monocytes, a mixed pattern of partial PMA responsiveness and partial competition by unlabeled IL-3 was observed, suggesting the coexpression of both class I and II receptors in these cells. In these cells, after down-regulation of the class I receptor by PMA, the remaining receptors were shown to be completely cross-competed for by IL-3, further supporting the hypothesis that these cells have a mixture of class I and II receptors. Chemical cross-linking of radiolabeled GM-CSF to myeloid cells revealed the labeling of three proteins (156, 126, and 82 kDa) which were identical in cells expressing either class I or II binding sites. These data show that there are differentiation-associated differences in the regulation of the GM-CSF receptor which may have important physiological consequences.

摘要

粒细胞-巨噬细胞集落刺激因子(GM-CSF)通过与高亲和力的表面膜受体结合来激活多种髓系细胞。这种造血生长因子的作用取决于髓系细胞的分化状态,范围从早期髓系祖细胞的增殖到中性粒细胞和单核细胞功能的激活。此外,GM-CSF的许多生物学效应与白细胞介素-3(IL-3)相同,IL-3是一种关系较远的淋巴因子。在本研究中,我们通过比较早期和晚期髓系细胞中GM-CSF受体的结合特性和表面调节,对不同分化阶段的髓系细胞的GM-CSF受体进行了表征。Scatchard分析显示,正常中性粒细胞、单核细胞以及急性髓系白血病患者的成髓细胞上存在一类高亲和力受体。与其他髓系细胞相比,中性粒细胞表达的受体数量显著更多,但亲和力约低2倍。观察到两种不同的GM-CSF受体调节和结合模式。在第一种模式中,中性粒细胞的GM-CSF受体被GM-CSF自身、佛波醇肉豆蔻酸酯乙酸酯(PMA)和钙离子载体A23187迅速下调,并且不受IL-3的竞争(I类受体)。与中性粒细胞受体相反,成髓细胞的GM-CSF受体对GM-CSF自身、PMA和A23187的下调作用具有抗性,并且完全受IL-3竞争(II类受体)。在某些急性髓系白血病病例和单核细胞中,观察到部分PMA反应性和未标记IL-3部分竞争的混合模式,表明这些细胞中I类和II类受体共表达。在这些细胞中,PMA下调I类受体后,剩余的受体显示完全受IL-3交叉竞争,进一步支持了这些细胞具有I类和II类受体混合物的假设。将放射性标记的GM-CSF与髓系细胞进行化学交联,显示出三种蛋白质(156、126和82 kDa)被标记,在表达I类或II类结合位点的细胞中这些蛋白质是相同的。这些数据表明,GM-CSF受体的调节存在与分化相关的差异,这可能具有重要的生理意义。

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