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首页> 外文期刊>Leukemia Research: A Forum for Studies on Leukemia and Normal Hemopoiesis >Protein kinase C isoforms in normal and leukemic neutrophils: altered levels in leukemic neutrophils and changes during myeloid maturation in chronic myeloid leukemia.
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Protein kinase C isoforms in normal and leukemic neutrophils: altered levels in leukemic neutrophils and changes during myeloid maturation in chronic myeloid leukemia.

机译:正常和白血病中性粒细胞中的蛋白激酶C亚型:慢性粒细胞白血病中性粒细胞水平的改变和在髓样成熟过程中的变化。

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摘要

Protein kinase C (PKC) is reported to play a role in maturation of the myeloid cell and functions of the mature neutrophil. The neutrophils in chronic myeloid leukemia (CML) exhibit defects in several functions. As a step towards understanding the role of PKC in the defects in function of the leukemic cells, this study investigates the expression of PKC isoforms, their subcellular distribution, levels and kinase activity in the normal and leukemic neutrophils. It also investigates changes in representative PKC isoforms during myeloid maturation. This study confirms the presence of PKC alpha, beta and delta and shows, for the first time, the presence of non conventional PKC isoform theta, atypical PKC isoform lambda/iota and PKC isoform mu in normal human neutrophils. In unstimulated cells all the detected PKC isoforms showed a predominantly cytosolic localisation in normal and CML neutrophils. Cytosol-membrane distribution of PKC alpha and delta were significantly altered in leukemic neutrophils as compared to normal cells. Cytosolic levels of all PKC isoforms were reduced in CML neutrophils with PKC alpha, beta, iota, theta, and mu showing a significant decrease. Cytosolic levels of PKC delta contrary to the trend observed for other PKC isoforms showed a slight increase in CML cells, while its membrane levels were significantly reduced in CML neutrophils. Total PKC kinase activity in CML neutrophil cytosol was significantly reduced, while specific kinase activity of two representative isoforms, PKC alpha and delta, from normal and CML neutrophils were similar, thereby increasing the significance of the altered levels of PKC isoforms in CML, and highlighting their role in the defects in function exhibited by the leukemic neutrophils. The levels of PKC delta and iota increased and decreased respectively as the leukemic myeloid cell matured from the blast to the neutrophil, while the levels of PKC alpha and beta were not altered. This suggests a role for PKC delta and iota in the maturation of the leukemic myeloid cell.
机译:据报道,蛋白激酶C(PKC)在髓样细胞的成熟和中性粒细胞的功能中发挥作用。慢性粒细胞白血病(CML)中的中性粒细胞在某些功能上表现出缺陷。为了进一步了解PKC在白血病细胞功能缺陷中的作用,本研究调查了正常和白血病中性粒细胞中PKC亚型的表达,亚细胞分布,水平和激酶活性。它还研究了髓样成熟过程中代表性PKC同工型的变化。这项研究证实了PKCα,β和δ的存在,并首次显示了正常人中性粒细胞中非常规PKC亚型θ,非典型PKC亚型λ/ iota和PKC亚型mu的存在。在未刺激的细胞中,所有检测到的PKC亚型在正常和CML中性粒细胞中均显示出胞浆定位。与正常细胞相比,白血病中性粒细胞的PKCα和δ的细胞膜分布明显改变。在CML中性粒细胞中,所有PKC亚型的胞浆水平均降低,其中PKCα,β,iota,θ和mu显着降低。与其他PKC亚型观察到的趋势相反,PKCδ的胞质水平显示CML细胞略有增加,而其膜水平在CML中性粒细胞中则明显降低。 CML中性粒细胞胞浆中的总PKC激酶活性显着降低,而来自正常和CML中性粒细胞的两种代表性同工型PKCα和δ的特异性激酶活性相似,从而增加了CML中PKC同工型水平改变的重要性,并强调它们在白血病中性粒细胞所表现出的功能缺陷中的作用。随着白血病髓样细胞从胚泡成熟到中性粒细胞的成熟,PKCδ和iota的水平分别增加和减少,而PKCα和β的水平没有改变。这表明PKCδ和iota在白血病髓样细胞成熟中起作用。

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