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9-顺式维甲酸α-生育酚酯(9-顺式维甲酸生育酚酯)诱导急性早幼粒细胞白血病细胞分化

Induction of differentiation in acute promyelocytic leukemia cells by 9-cis retinoic acid alpha-tocopherol ester (9-cis tretinoin tocoferil).

作者信息

Makishima M, Umesono K, Shudo K, Naoe T, Kishi K, Honma Y

机构信息

Department of Chemotherapy, Saitama Cancer Center Research Institute, Saitama, Japan.

出版信息

Blood. 1998 Jun 15;91(12):4715-26.

PMID:9616170
Abstract

Acute promyelocytic leukemia (APL) has a specific genetic rearrangement between the retinoic acid receptor (RAR)-alpha gene and the pml nuclear protein gene. All-trans retinoic acid (ATRA) induces granulocytic differentiation of APL-derived cells and is used to treat APL patients. However, ATRA interacts with normal cells with RAR throughout the entire body, and when used at high doses or over a long duration, it induces several adverse effects. The development of drugs that selectively act on APL cells may contribute to increasing the therapeutic efficacy of APL treatment as well as elucidating the mechanisms of response to ATRA. In this study, 9-cis retinoic acid alpha-tocopherol ester (9CTT) inhibited the proliferation of APL-derived NB4 and HT93 cells and induced differentiation markers, such as granulocytic maturation, nitroblue tetrazolium reduction, and CD11b expression, in these cells. The effects of 9CTT on non-APL cells, including HL-60 and U937 cells, were much weaker than those on APL cells, and tretinoin tocoferil (TT), which is an alpha-tocopherol ester of ATRA, did not induce the differentiation of APL cells as effectively as 9CTT. The differentiation-inducing effects of 9CTT were inhibited by RAR antagonists. 9CTT and TT similarly induced the transactivating activity of RARs, but were not effective on RXRs. 9CTT downregulated the expression of PML/RAR-alpha protein more effectively than TT, which suggests that it may be involved in the selectivity of 9CTT against APL cells. Interestingly, 9CTT enhanced the differentiation of APL cells induced by ATRA, 9-cis retinoic acid, and synthetic retinobenzoic acids. Combined with 1alpha,25-dihydroxyvitamin D3 (VD3), 9CTT also more than additively induced the differentiation of APL cells. Thus, 9CTT, alone or in combination with other retinoids or VD3, may be useful for the treatment of APL.

摘要

急性早幼粒细胞白血病(APL)在维甲酸受体(RAR)-α基因与早幼粒细胞白血病(PML)核蛋白基因之间存在特定的基因重排。全反式维甲酸(ATRA)可诱导APL来源细胞的粒细胞分化,并用于治疗APL患者。然而,ATRA会与全身表达RAR的正常细胞相互作用,当高剂量或长期使用时,会引发多种不良反应。开发选择性作用于APL细胞的药物可能有助于提高APL治疗的疗效,并阐明对ATRA的反应机制。在本研究中,9-顺式维甲酸α-生育酚酯(9CTT)抑制了APL来源的NB4和HT93细胞的增殖,并在这些细胞中诱导了分化标志物,如粒细胞成熟、硝基蓝四氮唑还原和CD11b表达。9CTT对包括HL-60和U937细胞在内的非APL细胞的作用比对APL细胞的作用弱得多,而维甲酸生育酚酯(TT),即ATRA的α-生育酚酯,诱导APL细胞分化的效果不如9CTT有效。9CTT的分化诱导作用被RAR拮抗剂抑制。9CTT和TT同样诱导了RAR的反式激活活性,但对维甲酸X受体(RXR)无效。9CTT比TT更有效地下调了PML/RAR-α蛋白的表达,这表明它可能与9CTT对APL细胞的选择性有关。有趣的是,9CTT增强了由ATRA、9-顺式维甲酸和合成视黄酸苯甲酸诱导的APL细胞的分化。与1α,25-二羟基维生素D3(VD3)联合使用时,9CTT还以超过相加的方式诱导APL细胞的分化。因此,9CTT单独或与其他类维生素A或VD3联合使用,可能对APL的治疗有用。

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