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首页> 外文期刊>Leukemia >Relapse of acute promyelocytic leukemia with PML-RAR|[alpha]| mutant subclones independent of proximate all-trans retinoic acid selection pressure
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Relapse of acute promyelocytic leukemia with PML-RAR|[alpha]| mutant subclones independent of proximate all-trans retinoic acid selection pressure

机译:PML-RAR |α|引起的急性早幼粒细胞白血病的复发不依赖于全反式维甲酸选择压力的突变亚克隆

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Relapse of acute promyelocytic leukemia (APL) following all-trans retinoic acid (ATRA) therapy has been associated with the acquisition of mutations in the high-affinity ATRA binding site in PML-RAR, but little information is available about the selection dynamics of the mutation-harboring subclones. In this study, 6/18 patients treated with sequential ATRA and chemotherapy on protocol INT0129 relapsed with complete replacement of the nonmutant pretreatment APL cell population by a PML-RAR mutant subclone. Two patients relapsed in proximity of ATRA treatment; however, in four patients there was a 6–48 month hiatus between the last ATRA treatment and relapse. The mutant subclones were not detectable in samples tested 3 months before relapse at 1 in 102 (10-2) sensitivity. In one patient, a functionally weak mutation was detected at 10-4 sensitivity before therapy but only limited pre-relapse enrichment of the mutant subclone was observed on subsequent ATRA therapy. These results indicate that proximate ATRA selection pressure is frequently not the main determinant for the emergence of strongly dominant PML-RAR mutant subclones and suggest that APL subclones harboring PML-RAR mutations are predisposed to the acquisition of secondary genetic/epigenetic alterations that result in a growth/survival advantage.
机译:全反式视黄酸(ATRA)治疗后急性早幼粒细胞白血病(APL)的复发与PML-RAR中高亲和力ATRA结合位点的突变获得有关,但关于其选择动态的信息很少。突变突变亚克隆。在这项研究中,按协议INT0129接受序贯ATRA和化学疗法治疗的6/18患者复发,并用PML-RAR突变体亚克隆完全替代了非突变型预处理APL细胞。 2例患者在ATRA治疗附近复发;但是,在四名患者中,最后一次ATRA治疗与复发之间有6-48个月的中断。在复发前3个月测试的样品中,检测不到突变亚克隆,灵敏度为102(10-2)的1分。一名患者在治疗前以10-4灵敏度检测到功能弱的突变,但是在随后的ATRA治疗中仅观察到有限的复发前富集的突变亚克隆。这些结果表明,接近ATRA的选择压力通常不是决定性强PML-RAR突变亚克隆出现的主要决定因素,并且表明具有PML-RAR突变的APL亚克隆容易导致获得继发性遗传/表观遗传变异,增长/生存优势。

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