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首页> 外文期刊>Journal of Translational Medicine >Circulating microRNAs as minimal residual disease biomarkers in childhood acute lymphoblastic leukemia
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Circulating microRNAs as minimal residual disease biomarkers in childhood acute lymphoblastic leukemia

机译:作为儿童急性淋巴细胞白血病的循环微小RNA作为急性残留疾病生物标志物

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BACKGROUND:Treatment stratification based on bone marrow minimal residual disease (MRD) at set time points has resulted in considerably improved survival in pediatric acute lymphoblastic leukemia (ALL). Treatment response is assessed using bone marrow samples. MicroRNAs (miRs) easily traffic among fluid spaces and are more stable than most other RNA classes. We examined the role of circulating miRs as putative less invasive MRD biomarkers.METHODS:In an exploratory experiment, expression of 46 preselected miRs was studied in platelet-free blood plasma samples of 15 de novo, 5 relapsed ALL patients and 10 controls by Custom TaqMan Array Advanced MicroRNA Card. Based on their high expression in ALL compared to controls, and on the reduction observed along the induction therapy, four miRs were selected for further analyses: miR-128-3p, -181a-5p, -181b-5p and 222-3p. Their expression was measured by qPCR at 4 time points in 27 de novo ALL patients treated in the ALL IC-BFM 2009 study.RESULTS:The expression of all 4 miRs significantly decreased over the first week of therapy (miR-128-3p: log2 fold change -?2.86; adjusted p 3.6?×?10-7; miR-181b-5p: log2 fold change -?1.75; adjusted p 1.48?×?10-2; miR-181a-5p: log2 fold change -1.33; adjusted p 3.12?×?10-2; miR-222-3p: log2 fold change -?1.25; adjusted p 1.66?×?10-2). However, no significant further reduction in miR expression was found after the 8th day of therapy. Measured drop in expression of 2 miRs at day 8 strongly correlated with day 15 bone marrow flow cytometry MRD results (miR-128-3p: Pearson's r?=?0.88, adjusted p?=?2.71?×?10-4; miR-222-3p: r?=?0.81, adjusted p?=?2.99?×?10-3).CONCLUSION:In conclusion, these circulating miRs might act as biomarkers of residual leukemia. MiR-128-3p and miR-222-3p in blood predict day 15 flow cytometry MRD results 7?days earlier. Although, their sensitivity falls behind that of bone marrow flow cytometry MRD at day 15.
机译:背景技术基于骨髓最小残留疾病(MRD)在设定时间点的治疗分层导致小儿急性淋巴细胞白血病(全部)的存在显着提高的存活。使用骨髓样品评估治疗响应。 MicroRNA(MIRS)在流体空间之间容易交通,比大多数其他RNA类更稳定。我们检查了循环mirs作为推定较少的侵入式德尔德生物标志物的作用。方法:在探索性实验中,在46个预选的mirs的表达在15 de Novo的血小板血浆样本中研究了所有患者和10个患者的托塔克曼阵列高级MicroRNA卡。基于它们的高表达与对照组相比,并在沿着感应疗法观察到的还原,选择了四种MIR,用于进一步分析:miR-128-3p,-181a-5p,-181b-5p和222-3p。通过QPCR在27 de Novo中的QPCR测量它们的表达,所有在所有IC-BFM 2009研究中均治疗的所有患者均可治疗。结果:在治疗的第一周(miR-128-3p:log2折叠变化 - ?2.86;调整后的p 3.6?×10-7; mir-181b-5p:log2折变化 - ?1.75;调整的p 1.48?×10-2; mir-181a-5p:log2折叠变化-1.33 ;调整的P 3.12?×10-2; miR-222-3p:log2折变化 - ?1.25;调整的p 1.66?×10-2)。然而,在治疗第8天后没有发现miR表达的显着进一步降低。在第8天表达2 mirs的测量表达强烈相关,与第15天骨髓流式细胞术MRD结果(MiR-128-3P:Pearson's R?=?0.88,调整为P?=?2.71?×10-4; mir- 222-3p:r?=?0.81,调整p?=?2.99?×10-3)。结论:总而言之,这些循环mir可能担任残留白血病的生物标志物。 MiR-128-3P和MiR-222-3P在血液中预测第15天流式细胞术MRD结果7?天前。虽然,它们的敏感性在第15天骨髓流式细胞术MRD落后于此。

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