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通过逆转录聚合酶链反应监测MLL-AF9阳性急性髓系白血病患者的微小残留白血病

Monitoring of minimal residual leukemia in patients with MLL-AF9 positive acute myeloid leukemia by RT-PCR.

作者信息

Mitterbauer G, Zimmer C, Fonatsch C, Haas O, Thalhammer-Scherrer R, Schwarzinger I, Kalhs P, Jaeger U, Lechner K, Mannhalter C

机构信息

Department of Laboratory Medicine, Division of Molecular Biology, Vienna, Austria.

出版信息

Leukemia. 1999 Oct;13(10):1519-24. doi: 10.1038/sj.leu.2401542.

Abstract

Twenty-seven patients with AML and MLL gene rearrangement were analyzed by a reverse transcriptase polymerase chain reaction (RT-PCR) for the MLL-AF9 translocation. The MLL-AF9 fusion transcript was detected in six patients. In five patients, the breakpoint of the AF9 gene was located within the recently described site A; in one patient, a novel breakpoint (AF9 site D) mapped to a position 377 bp 3' of site A. Five patients could be serially monitored for a period of 4-23 months. Two patients became two-step PCR negative in bone marrow and peripheral blood. Molecular remission was achieved rapidly after one cycle of induction chemotherapy. Both patients are in continuous complete remission (CR) at 22 and 15 months, respectively. Two patients who had achieved hematological CR did not become PCR negative and MLL-AF9 fusion transcripts were detectable in all samples after induction and consolidation chemotherapy. One patient relapsed 5 months after achieving CR. The other patient received allogeneic bone marrow transplantation from an HLA-identical sibling 2 months after achieving hematological CR and became PCR negative 4 weeks after transplantation. In the fifth patient, hematological CR could not be achieved with two cycles of intensive induction chemotherapy, and MLL-AF9 transcripts were present in all samples tested. Our data indicate that MLL-AF9 RT-PCR is specific for the t(9;11) translocation. PCR negativity can be achieved in responding patients already 1 month after induction chemotherapy. The fast reduction of MLL-AF9 positive blast cells below the detection limit of RT-PCR seems to be a prerequisite for long-term CR. The results of RT-PCR may be useful for treatment decisions (eg BMT).

摘要

采用逆转录聚合酶链反应(RT-PCR)对27例急性髓系白血病(AML)且伴有MLL基因重排的患者进行MLL-AF9易位分析。在6例患者中检测到MLL-AF9融合转录本。5例患者中,AF9基因的断点位于最近描述的A位点;1例患者中,一个新的断点(AF9位点D)定位于A位点下游377 bp处。5例患者可连续监测4 - 23个月。2例患者在骨髓和外周血中两步PCR转为阴性。诱导化疗一个周期后迅速实现分子缓解。这2例患者分别在22个月和15个月时持续完全缓解(CR)。2例达到血液学CR的患者未转为PCR阴性,诱导和巩固化疗后所有样本中均可检测到MLL-AF9融合转录本。1例患者在达到CR后5个月复发。另1例患者在达到血液学CR后2个月接受了来自HLA相同同胞的异基因骨髓移植,移植后4周转为PCR阴性。在第5例患者中,两个周期的强化诱导化疗未能实现血液学CR,所有检测样本中均存在MLL-AF9转录本。我们的数据表明,MLL-AF9 RT-PCR对t(9;11)易位具有特异性。诱导化疗后1个月,反应性患者即可实现PCR阴性。MLL-AF9阳性原始细胞快速减少至RT-PCR检测限以下似乎是长期CR的先决条件。RT-PCR结果可能有助于治疗决策(如骨髓移植)。

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