首页> 外文期刊>Leukemia Research: A Forum for Studies on Leukemia and Normal Hemopoiesis >Estimations of BCR-ABL/ABL transcripts by quantitative PCR in chronic myeloid leukaemia after allogeneic bone marrow transplantation and donor lymphocyte infusion.
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Estimations of BCR-ABL/ABL transcripts by quantitative PCR in chronic myeloid leukaemia after allogeneic bone marrow transplantation and donor lymphocyte infusion.

机译:定量PCR评估异基因骨髓移植和供体淋巴细胞输注后慢性髓样白血病中BCR-ABL / ABL转录本。

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Serial assays of qualitative (multiplex and nested) and quantitative PCR were carried out for detecting and estimating the level of BCR-ABL transcripts in 39 CML patients following bone marrow transplantation. Seven of these patients, who received donor lymphocyte infusions (DLIs) following to relapse, were also monitored. Quantitative estimates of BCR-ABL transcripts were obtained by co-amplification with a competitor sequence. Estimates of ABL transcripts were used, an internal control and the ratio BCR-ABL/ABL was thus estimated for evaluating the kinetics of residual clones. Twenty four patients were followed shortly after BMT; two of these patients were in cytogenetic relapse coexisting with very high BCR-ABL levels while other 22 were in clinical, haematologic and cytogenetic remission 2-42 months after BMT. In this latter group, seven patients showed a favourable clinical-haematological progression in association with molecular remission while in 14 patients quantitative PCR assays indicated molecular relapse that was not associated with an early cytogenetic-haematologic relapse. BCR-ABL/ABL levels could not be correlated with presence of GVHD in 24 patients after BMT. In all seven patients treated with DLI, high levels of transcripts were detected at least 4 months before the appearance of clinical haematological relapse. Following DLI, five of these patients showed decreasing transcript levels from 2 to 5 logs between 4 and 12 months. In eight other patients studied long after BMT, five showed molecular relapse up to 117 months post-BMT and only one showed cytogenetic relapse. Our findings indicated that quantitative estimates of BCR-ABL transcripts were valuable for monitoring minimal residual disease in each patient.
机译:进行了定性(多重和巢式)和定量PCR的系列检测,以检测和评估39名CML患者骨髓移植后BCR-ABL转录本的水平。这些患者中有7例在复发后接受了供体淋巴细胞输注(DLI)。通过与竞争者序列的共扩增获得BCR-ABL转录本的定量估计。使用ABL转录物的估计,内部对照,并且因此估计比率BCR-ABL / ABL用于评估残留克隆的动力学。 BMT后不久随访了24例患者。这些患者中有两个患者的细胞遗传学复发与BCR-ABL水平很高并存,而其他22例患者则在BMT后2至42个月出现临床,血液学和细胞遗传学缓解。在后一组中,有7例患者表现出与分子缓解相关的良好的临床血液学进展,而在14例患者中,定量PCR分析表明分子复发与早期细胞遗传学和血液学复发无关。 BMT后24例患者中,BCR-ABL / ABL水平与GVHD的存在无关。在全部7例接受DLI治疗的患者中,至少在临床血液学复发出现前4个月检测到高水平的转录本。 DLI后,这些患者中有5例在4到12个月之间显示从2到5个对数的转录水平下降。在其他八名接受BMT后不久进行研究的患者中,有五名在BMT后117个月内显示出分子复发,只有一例显示出细胞遗传学复发。我们的研究结果表明,对BCR-ABL转录本的定量估计对于监测每位患者的最小残留疾病非常有价值。

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