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首页> 外文期刊>European cytokine network >Spontaneous and cytokine-evoked production of matrix metalloproteinases by bone marrow and peripheral blood pre-B cells in childhood acute lymphoblastic leukaemia.
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Spontaneous and cytokine-evoked production of matrix metalloproteinases by bone marrow and peripheral blood pre-B cells in childhood acute lymphoblastic leukaemia.

机译:在儿童急性淋巴细胞白血病中,骨髓和外周血pre-B细胞自发和细胞因子诱发的基质金属蛋白酶产生。

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摘要

The present work focused on the study of the secretory activity of pre-B acute lymphoblastic leukaemia (ALL) cells harvested from bone marrow (BM) and peripheral blood (PB) in 16 children. The basal and cytokine (SDF-1, GM-CSF, bFGF, VEGF)-stimulated secretions of gelatinases 2 and 9 (MMPs-2 and -9) and expression of their genes were monitored by zymography and RT-PCR, respectively. A wide heterogeneity was found in the secretory capacities of these cells. The basal secretion of MMP-9 was more frequently observed than that of MMP-2 in both cell types. The cytokines VEGF and bFGF were found to induce predominant stimulatory effects on the MMP-2 secretion. In contrast, GM-CSF was shown to exert a more pronounced activation of the MMP-9 production. Experiments using inhibitors of metabolic pathways (U0126, LY294002 and SN50) revealed that the secretion of MMP-9 was mediated through PI3/MEK1 kinases. The MMP-2 secretion appeared to be however, stimulated through a different metabolic pathway. The microfluorimetric approach showed that the basal and stimulated secretions of MMPs-2 and -9 depended on the extracellular calcium pool. The cytokines VEGF and bFGF represent potent factors increasing the intracellular calcium concentration with similar kinetics. In contrast, GM-CSF was found to activate a verapamil-sensitive efflux of indo-1 from cytosol suggesting that this cytokine could be responsible for the activation of xenobiotic membrane transporters. Experiments using the trypan blue exclusion test demonstrated that bFGF, in contrast to VEGF and GM-CSF, markedly augmented pre-B ALL cell survival Further investigations into a possible correlation between the plasma concentrations of MMP-2 and -9, VEGF, bFGF and GM-CSF, and the poor evolution of pre-B ALL in children could have valuable diagnostic implications.
机译:目前的工作集中在研究从16名儿童的骨髓(BM)和外周血(PB)收集的B前急性淋巴细胞白血病(ALL)细胞的分泌活性。分别通过酶谱法和RT-PCR来监测基础和细胞因子(SDF-1,GM-CSF,bFGF,VEGF)刺激的明胶酶2和9(MMPs-2和-9)的分泌及其基因的表达。在这些细胞的分泌能力中发现了广泛的异质性。在两种细胞类型中,MMP-9的基础分泌都比MMP-2的分泌更为频繁。发现细胞因子VEGF和bFGF对MMP-2分泌具有主要的刺激作用。相反,显示出GM-CSF对MMP-9产生更明显的激活作用。使用代谢途径抑制剂(U0126,LY294002和SN50)进行的实验表明,MMP-9的分泌是通过PI3 / MEK1激酶介导的。然而,似乎通过不同的代谢途径刺激了MMP-2的分泌。微荧光法显示,MMPs-2和-9的基础分泌和刺激分泌取决于细胞外钙池。细胞因子VEGF和bFGF代表以相似的动力学增加细胞内钙浓度的有效因子。相比之下,发现GM-CSF激活了维拉帕米敏感的indo-1从胞质溶胶中流出,这表明该细胞因子可能是异种生物膜转运蛋白激活的原因。使用锥虫蓝排除试验的实验表明,与VEGF和GM-CSF相比,bFGF显着提高了前B ALL细胞的存活率。进一步研究了血浆MMP-2和-9,VEGF,bFGF和GM-CSF和儿童前B ALL的不良进展可能对诊断具有重要意义。

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