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酸性和碱性异铁蛋白对人粒细胞-单核细胞祖细胞体外生长的影响。

Effect of acidic and basic isoferritins on in vitro growth of human granulocyte-monocyte progenitors.

作者信息

Dezza L, Cazzola M, Piacibello W, Arosio P, Levi S, Aglietta M

出版信息

Blood. 1986 Mar;67(3):789-95.

PMID:3947747
Abstract

Acidic isoferritins have been previously found to be highly potent inhibitors of hematopoietic progenitors at concentrations of 10(-16) to 10(-18) mol/L, and it has been suggested that acidic isoferritin inhibitory activity plays a role in the regulation of normal hematopoiesis and also in the pathogenesis of leukemia. To characterize the ferritin species that affect the in vitro growth of human colony-forming unit-granulocyte-macrophage (CFU-GM), we tested different preparations of basic (L-subunit-rich) and acidic (H-subunit-rich) isoferritins. Three preparations of human liver (basic) ferritin did not show any effects on CFU-GM growth at concentrations up to 10(-9) mol/L, irrespective of the degree of glycosylation. Acidic isoferritins were purified both from HeLa cells and human heart. HeLa cell ferritin did not affect in vitro colony formation. One of two preparations of human heart ferritin, containing 5% glycosylated ferritin, showed a mean inhibition of 26% +/- 8% of the control at 10(-9) mol/L (P less than .02), whereas the other preparation, which contained no glycosylated ferritin, did not show any effect of CFU-GM growth. A preparation enriched for glycosylated acidic isoferritins from human heart was found to produce a mean inhibition of 32% +/- 11% of the control at 10(-9) mol/L (P less than .01), whereas another one was ineffective. A significant part of the inhibitory activity was removed by preincubation with the monoclonal antibody 2A4 directed against human heart ferritin. The present findings indicate that basic isoferritins, ie, the predominant ferritin type in human blood, have no effect on the growth of human CFU-GM, and this is in keeping with indirect clinical evidence. Inhibition of colony formation may be obtained by some preparations of acidic isoferritins that are rich in H subunits and bind to concanavalin A. The mechanism(s) responsible for this are not clear, but the effective concentrations are higher than those found in human blood both under normal conditions and in leukemia. At present, the physiologic significance of the observed inhibitory activity is uncertain.

摘要

此前已发现,酸性异铁蛋白在浓度为10^(-16)至10^(-18)摩尔/升时是造血祖细胞的高效抑制剂,有人提出酸性异铁蛋白抑制活性在正常造血调节以及白血病发病机制中起作用。为了鉴定影响人粒细胞-巨噬细胞集落形成单位(CFU-GM)体外生长的铁蛋白种类,我们测试了不同的碱性(富含L亚基)和酸性(富含H亚基)异铁蛋白制剂。三种人肝(碱性)铁蛋白制剂在浓度高达10^(-9)摩尔/升时,无论糖基化程度如何,对CFU-GM生长均无任何影响。酸性异铁蛋白从HeLa细胞和人心脏中均有纯化。HeLa细胞铁蛋白不影响体外集落形成。两种人心脏铁蛋白制剂中的一种,含有5%糖基化铁蛋白,在10^(-9)摩尔/升时对对照的平均抑制率为26%±8%(P<0.02),而另一种不含糖基化铁蛋白的制剂对CFU-GM生长无任何影响。从人心脏中富集糖基化酸性异铁蛋白的一种制剂在10^(-9)摩尔/升时对对照的平均抑制率为32%±11%(P<0.01),而另一种则无效。通过与针对人心脏铁蛋白的单克隆抗体2A4预孵育,可去除大部分抑制活性。目前的研究结果表明,碱性异铁蛋白,即人血液中主要的铁蛋白类型,对人CFU-GM的生长无影响,这与间接临床证据一致。某些富含H亚基并与伴刀豆球蛋白A结合的酸性异铁蛋白制剂可抑制集落形成。其作用机制尚不清楚,但有效浓度高于正常条件下和白血病患者血液中的浓度。目前,所观察到的抑制活性的生理意义尚不确定。

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