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白细胞介素-6对粒细胞-巨噬细胞集落刺激因子(GM-CSF)依赖性人髓系白血病细胞系(AML-193)中GM-CSF受体的调节作用

Regulation of granulocyte-macrophage colony-stimulating factor (GM-CSF) receptors in a GM-CSF-dependent human myeloid leukemia cell line (AML-193) by interleukin-6.

作者信息

Li Y, Valeriote F, Chen B

机构信息

Division of Hematology/Oncology, Department of Internal Medicine, Wayne State University School of Medicine, Detroit, MI 48201, USA.

出版信息

Exp Hematol. 1996 Feb;24(2):94-100.

PMID:8641372
Abstract

AML-193 is a cytokine-dependent human leukemia cell line established from the bone marrow of an M5-type acute monocytic leukemia (AML) patient. The effect of recombinant human interleukin-6 (rhIL-6) on the proliferation of AML-193 cells was investigated. Both granulocyte-macrophage colony-stimulating factor (rhGM-CSF) and rhIL-3 promoted the DNA synthesis and growth of AML-193 cells in vitro. rhIL-6 alone did not support the growth of AML-193 cells, yet pretreatment of AML-193 cells with rhIL-6 markedly enhanced their proliferative response to subsequent rhGM-CSF or rhIL-3 stimulation. The growth-promoting effect induced by rhIL-6 was attributable in part to the upregulation of GM-CSF receptors on AML-193 cells; treatment of AML-193 cells with rhIL-6 for 24 to 48 hours greatly increased their GM-CSF binding activity, which occurred in a dose-dependent manner. Both the growth-promoting and receptor-upregulating effects induced by rhIL-6 could be blocked by treating AML-193 cells with neutralizing anti-gp130 antibodies (GPX7). Treatment of AML-193 cells with anti-gp130 antibodies alone also led to a notable decline in GM-CSF binding activity, suggesting a possible role of gpl30 in regulating the expression of GM-CSF receptors. When AML-193 cells were starved in cytokine-free medium and then restimulated with rhGM-CSF, a rapid increase (5 minutes) in lyn kinase activity was observed. A similar upregulation of lyn kinase activity by rhIL-6 treatment also was noted in AML-193 cells, but only after a prolonged incubation of the cells with rhIL-6 (>24 hours). These findings show that the growth-promoting effects of rhIL-6 are mediated through the upregulation of GM-CSF receptors on AML-193 cells by mechanisms that appear to involve the activation of both gp130 and lyn kinase.

摘要

AML-193是一种依赖细胞因子的人白血病细胞系,从一名M5型急性单核细胞白血病(AML)患者的骨髓中建立。研究了重组人白细胞介素-6(rhIL-6)对AML-193细胞增殖的影响。粒细胞-巨噬细胞集落刺激因子(rhGM-CSF)和rhIL-3均能促进AML-193细胞在体外的DNA合成和生长。单独的rhIL-6不能支持AML-193细胞的生长,但用rhIL-6预处理AML-193细胞可显著增强其对随后rhGM-CSF或rhIL-3刺激的增殖反应。rhIL-6诱导的生长促进作用部分归因于AML-193细胞上GM-CSF受体的上调;用rhIL-6处理AML-193细胞24至48小时可大大增加其GM-CSF结合活性,且呈剂量依赖性。rhIL-6诱导的生长促进和受体上调作用均可被用中和抗gp130抗体(GPX7)处理AML-193细胞所阻断。单独用抗gp130抗体处理AML-193细胞也导致GM-CSF结合活性显著下降,提示gpl30在调节GM-CSF受体表达中可能起作用。当AML-193细胞在无细胞因子的培养基中饥饿,然后用rhGM-CSF重新刺激时,观察到lyn激酶活性迅速增加(5分钟)。在AML-193细胞中也注意到rhIL-6处理导致lyn激酶活性有类似的上调,但只有在细胞与rhIL-6长时间孵育(>24小时)后才出现。这些发现表明,rhIL-6的生长促进作用是通过上调AML-193细胞上的GM-CSF受体介导的,其机制似乎涉及gp130和lyn激酶的激活。

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