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全反式维甲酸增强巨核细胞集落形成:对急性早幼粒细胞白血病患者给药后的体内外效应

All-trans retinoic acid potentiates megakaryocyte colony formation: in vitro and in vivo effects after administration to acute promyelocytic leukemia patients.

作者信息

Visani G, Zauli G, Tosi P, Ottaviani E, Gibellini D, Manfroi S, Celeghini C, Pagliarini C, Bassini A, Tura S

机构信息

L.A. Seràgnoli Hematology Institute, University of Bologna, Italy.

出版信息

Leukemia. 1994 Dec;8(12):2183-7.

PMID:7528859
Abstract

In this study, we evaluated the in vitro growth of normal hematopoietic progenitors (CFU-GM, BFU-E, CFU-GEMM, CFU-meg) stimulated by optimal sources of colony stimulating activity in the absence or presence of 10(-6) M all-trans retinoic acid (ATRA). ATRA alone did not show any colony-stimulating ability when added in culture to partially purified bone marrow populations. On the other hand, it significantly increased the number of CFU-GM (p = 0.003) and both the number (p = 0.009) and size (p = 0.002) of CFU-meg in the presence of appropriate colony-stimulating activity. Since ATRA had only modest stimulatory effects on purified CD34+ cells, the megakaryocyte colony-stimulating activity of ATRA was mainly due to an increased production of endogenous cytokines by bone marrow accessory cells. In parallel experiments, the in vitro growth of the different hematopoietic progenitors was evaluated in 28 patients affected by acute non-lymphoid leukemia (ANLL), mainly acute promyelocytic leukemia (APL). Bone marrow cells were harvested after remission induction obtained: (i) in ten APL patients treated with ATRA followed by one chemotherapy cycle (CHT) (3/7: Daunorubicin+Ara-C): group A ('ATRA/CHT'); (ii) eight APL patients treated with one CHT cycle alone (3/7 as above): group B ('APL-CHT'); (iii) in ten ANLL-non-APL patients after one CHT cycle (3/7 as above): group C ('ANLL-CHT'). The number of the different hematopoietic progenitors, and in particular CFU-GM and CFU-meg, was significantly higher in APL patients treated with ATRA plus CHT (group A) compared to APL (group B) or ANLL-non-APL (group C) patients treated with CHT alone (CFU-GM: p = 0.01; CFU-meg: p = 0.03). Our data demonstrate that ATRA is able to potentiate both normal and APL megakaryocytopoiesis and suggest that the in vivo administration of ATRA could be beneficial in other pathological conditions, where the megakaryocyte progenitor cell compartment is impaired.

摘要

在本研究中,我们评估了在存在或不存在10⁻⁶ M全反式维甲酸(ATRA)的情况下,由集落刺激活性的最佳来源刺激的正常造血祖细胞(CFU - GM、BFU - E、CFU - GEMM、CFU - meg)的体外生长情况。当在培养中添加到部分纯化的骨髓群体时,单独的ATRA未显示出任何集落刺激能力。另一方面,在存在适当的集落刺激活性时,它显著增加了CFU - GM的数量(p = 0.003)以及CFU - meg的数量(p = 0.009)和大小(p = 0.002)。由于ATRA对纯化的CD34⁺细胞只有适度的刺激作用,ATRA的巨核细胞集落刺激活性主要归因于骨髓辅助细胞内源性细胞因子产生的增加。在平行实验中,评估了28例急性非淋巴细胞白血病(ANLL)患者,主要是急性早幼粒细胞白血病(APL)患者中不同造血祖细胞的体外生长情况。在诱导缓解后采集骨髓细胞,这些患者包括:(i)10例接受ATRA治疗随后进行一个化疗周期(CHT)(3/7:柔红霉素 + 阿糖胞苷)的APL患者:A组(“ATRA/CHT”);(ii)8例仅接受一个CHT周期治疗(3/7如上)的APL患者:B组(“APL - CHT”);(iii)10例在一个CHT周期后(3/7如上)的ANLL - 非APL患者:C组(“ANLL - CHT”)。与单独接受CHT治疗的APL(B组)或ANLL - 非APL(C组)患者相比,接受ATRA加CHT治疗的APL患者(A组)中不同造血祖细胞的数量,特别是CFU - GM和CFU - meg的数量显著更高(CFU - GM:p = 0.01;CFU - meg:p = 0.03)。我们的数据表明,ATRA能够增强正常和APL的巨核细胞生成,并表明在体内给予ATRA在其他巨核细胞祖细胞区室受损的病理状况下可能是有益的。

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