细胞遗传学缓解的慢性髓性白血病患者中BCR-ABL转录本变异的分子检测
Molecular measurement of BCR-ABL transcript variations in chronic myeloid leukemia patients in cytogenetic remission.
作者信息
Serpa Mariana, Sanabani Sabri S, Dorliac-Llacer Pedro Enrique, Conchon Monika, Pereira Thales Dalessandro Meneguin, Nardinelli Luciana, Costa Juliana Lima, Novaes Mafalda Megumi Yoshinaga, Ferreira Patricia de Barros, Bendit Israel
机构信息
Department of Hematology, Faculty of Medicine, University of São Paulo, São Paulo, Brazil.
出版信息
BMC Blood Disord. 2010 Nov 18;10:7. doi: 10.1186/1471-2326-10-7.
BACKGROUND
The monitoring of BCR-ABL transcript levels by real-time quantitative polymerase chain reaction (RT-qPCR) has become important to assess minimal residual disease (MRD) and standard of care in the treatment of chronic myeloid leukemia (CML). In this study, we performed a prospective, sequential analysis using RT-qPCR monitoring of BCR-ABL gene rearrangements in blood samples from 91 CML patients in chronic phase (CP) who achieved complete cytogenetic remission (CCyR) and major molecular remission (MMR) throughout imatinib treatment.
METHODS
The absolute level of BCR-ABL transcript from peripheral blood was serially measured every 4 to 12 weeks by RT-qPCR. Only level variations > 0.5%, according to the international scale, was considered positive. Sequential cytogenetic analysis was also performed in bone marrow samples from all patients using standard protocols.
RESULTS
Based on sequential analysis of BCR-ABL transcripts, the 91 patients were divided into three categories: (A) 57 (62.6%) had no variation on sequential analysis; (B) 30 (32.9%) had a single positive variation result obtained in a single sample; and (C) 4 (4.39%) had variations of BCR-ABL transcripts in at least two consecutive samples. Of the 34 patients who had elevated levels of transcripts (group B and C), 19 (55.8%) had a < 1% of BCR-ABL/BCR ratio, 13 (38.2%) patients had a 1% to 10% increase and 2 patients had a >10% increase of RT-qPCR. The last two patients had lost a CCyR, and none of them showed mutations in the ABL gene. Transient cytogenetic alterations in Ph-negative cells were observed in five (5.5%) patients, and none of whom lost CCyR.
CONCLUSIONS
Despite an increase levels of BCR-ABL/BCR ratio variations by RT-qPCR, the majority of CML patients with MMR remained in CCyR. Thus, such single variations should neither be considered predictive of subsequent failure and nor an indication for altering imatinib dose or switching to second generation therapy. Changing of imatinib on the basis of BCR-ABL/BCR% sustained increase and mutational studies is a prudent approach for preserving other therapeutic options in imatinib-resistant patients.
背景
通过实时定量聚合酶链反应(RT-qPCR)监测BCR-ABL转录水平对于评估慢性髓性白血病(CML)治疗中的微小残留病(MRD)和护理标准已变得至关重要。在本研究中,我们对91例慢性期(CP)CML患者在伊马替尼治疗期间实现完全细胞遗传学缓解(CCyR)和主要分子缓解(MMR)的血液样本进行了BCR-ABL基因重排的RT-qPCR监测的前瞻性序列分析。
方法
通过RT-qPCR每4至12周连续测量外周血中BCR-ABL转录本的绝对水平。根据国际标准,仅水平变化>0.5%被视为阳性。还使用标准方案对所有患者的骨髓样本进行了序列细胞遗传学分析。
结果
基于BCR-ABL转录本的序列分析,91例患者分为三类:(A)57例(62.6%)在序列分析中无变化;(B)30例(32.9%)在单个样本中获得单个阳性变化结果;(C)4例(4.39%)在至少两个连续样本中出现BCR-ABL转录本变化。在34例转录本水平升高的患者(B组和C组)中,19例(55.8%)的BCR-ABL/BCR比值<1%,13例(38.2%)患者升高1%至10%,2例患者的RT-qPCR升高>10%。最后两名患者失去了CCyR,且均未显示ABL基因突变。在5例(5.5%)患者中观察到Ph阴性细胞的短暂细胞遗传学改变,且均未失去CCyR。
结论
尽管RT-qPCR检测到BCR-ABL/BCR比值变化水平有所增加,但大多数达到MMR的CML患者仍保持CCyR。因此,这种单一变化既不应被视为随后失败的预测指标,也不应作为改变伊马替尼剂量或改用第二代疗法的指征。基于BCR-ABL/BCR%持续增加和突变研究来改变伊马替尼是一种谨慎的方法,可保留伊马替尼耐药患者的其他治疗选择。
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