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Methylprednisolone induces preferential and rapid differentiation of CD34+ cord blood precursors toward NK cells

机译:甲基强的松龙可诱导CD34 + 脐带血前体优先快速分化为NK细胞

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Previous studies showed that methylprednisolone (MePDN) down-regulates the surface expression of activating NK receptors and sharply inhibits the NK cytotoxicity both in vitro and in vivo. Since MePDN is administered to patients undergoing hemopoietic stem cell transplant to treat acute graft versus host disease (GvHD), we analyzed whether it could also inhibit the NK cell differentiation from CD34+ hemopoietic cell precursors, thus interfering with the development of effector cells with anti-leukemic potential. We show that MePDN promotes the in vitro differentiation of CD161+CD56+/− immature NK cells by inducing a rapid expression of NKp46, NKG2D, DNAX-accessory molecule 1 (DNAM-1), leukocyte function-associated antigen-1 and NKG2A and an efficient cytolytic activity. This phenotypic and functional NK cell maturation occurred more rapidly than in parallel control cultures performed in the absence of MePDN. In addition, MePDN induced CD33+CD161−CD56− myeloid precursors to switch toward NK cells. It is also of note that immature NK cells when cultured in the absence (but not in the presence) of MePDN produced high amounts of IL-8. These data indicate that MePDN can accelerate the in vitro NK cell differentiation, thus revealing a dichotomous effect on immature versus mature NK cells; in addition, interference with the in vitro development of myeloid cells occurred. These effects should be further investigated in hemopoietic stem cell transplanted patients receiving steroids to treat GvHD.
机译:先前的研究表明,甲基强的松龙(MePDN)在体内外均可下调激活性NK受体的表面表达,并显着抑制NK细胞的毒性。由于将MePDN应用于造血干细胞移植的患者以治疗急性移植物抗宿主病(GvHD),因此我们分析了它是否还可以抑制NK细胞从CD34 + 造血细胞前体分化,从而干扰具有抗白血病潜能的效应细胞的发展。我们显示,MePDN通过诱导NKp46,NKG2D,DNAX辅助分子1(DNAM)的快速表达,促进CD161 + CD56 +/- 未成熟NK细胞的体外分化。 -1),白细胞功能相关抗原-1和NKG2A以及有效的细胞溶解活性。这种表型和功能性NK细胞成熟的发生比没有MePDN的平行对照培养更快。另外,MePDN诱导CD33 + CD161 - CD56 -髓样前体转变为NK细胞。还要注意的是,在不存在(但不存在)MePDN的条件下培养未成熟的NK细胞会产生大量的IL-8。这些数据表明,MePDN可以加速体外NK细胞的分化,从而揭示了未成熟与成熟NK细胞的二分作用。另外,干扰了骨髓细胞的体外发育。这些作用应在接受类固醇治疗GvHD的造血干细胞移植患者中进一步研究。

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