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Transient presence of clonal chromosomal aberrations in Ph-negative cells in patients with chronic myeloid leukemia remaining in deep molecular response on tyrosine kinase inhibitor treatment

机译:慢性髓细胞性白血病患者在Ph阴性细胞中克隆染色体畸变的瞬时存在仍在酪氨酸激酶抑制剂治疗的深层分子反应中

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Advancements in treatment of chronic myeloid leukemia (CML) turned this formerly fatal neoplasm into a manageable chronic condition. Therapy with tyrosine kinase inhibitors (TKIs) often leads to significant reduction of disease burden, known as the deep molecular response (DMR). Herein, we decided to analyze the cohort of CML patients treated in our center with TKIs, who obtain and retain DMR for a period longer than 24 months. The aim of the study was to evaluate the frequency of clonal cytogenetic aberrations in Philadelphia-negative (Ph-) cells in patients with DMR during TKI treatment. The analyzed data was obtained during routine molecular and cytogenetic treatment monitoring, using G-banded trypsin and Giemsa stain (GTG) karyotyping and reverse transcription quantitative PCR. We noticed that approximately 50% of patients (28 of 55) in DMR had, at some follow-up point, transient changes in the karyotype of their Ph- bone marrow cells. In 9.1% of cases (5 of 55), the presence of the same aberrations was observed at different time points. The most frequently appearing aberrations were monosomies of chromosomes 19, 20, 21, and Y. Statistical analysis suggests that the occurrence of such abnormalities in CML patients correlates with the TKI treatment time.
机译:慢性粒细胞白血病(CML)的治疗进展使这种以前致命的肿瘤变成了可控制的慢性病。酪氨酸激酶抑制剂(TKIs)的治疗通常可以显着减少疾病负担,称为深度分子反应(DMR)。在此,我们决定分析在我们中心接受TKI治疗的CML患者队列,这些患者获得并保留DMR的时间超过24个月。这项研究的目的是评估TKI治疗期间DMR患者的费城阴性(Ph-)细胞中克隆细胞遗传异常的频率。分析的数据是在常规的分子和细胞遗传学治疗监测过程中获得的,使用的是G型胰蛋白酶和Giemsa染色(GTG)核型和逆转录定量PCR。我们注意到,大约有50%的DMR患者(55名患者中的28名)在某些随访点上具有其Ph骨髓细胞核型的短暂变化。在9.1%的情况下(55中的5),在不同的时间点观察到相同的像差。最常出现的像差是19、20、21和Y染色体的单体性。统计分析表明,CML患者中此类异常的发生与TKI治疗时间相关。

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