不同血液病移植患者化学状态的长期随访。

Sbornik lekarsky Pub Date : 2003-01-01
R Dvoráková, H Ríhová, S Zilovcová, L Krsková, R Formánková, Z Sieglová, R Brdicka
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引用次数: 0

摘要

对接受BMT或PBSCT治疗的患者外周细胞嵌合的长期随访显示,他们在分子水平上进行持续监测是有用的。我们的结果是基于对120名患者的监测,他们被随访了至少24个月。慢性髓性白血病(CML)、急性髓细胞白血病(AML)、急性淋巴细胞白血病(ALL)、骨髓增生异常综合征(MDS)和再生障碍性贫血(AA)患者的比较显示,混合嵌合现象在MDS患者中几乎不存在,而在ALL和AA患者中相对持续时间较长(无论移植后治疗方式有多大差异)。在持续数年的缓解期后,通过混合外周嵌合的分子检查也观察到第一次疾病复发。分子观察使我们能够在一开始就发现复发,而这些复发对于不那么敏感的方法来说是无法发现的。我们认为,所有的移植患者应该监测残余疾病,即细胞嵌合,使用分子方法,没有时间限制。另一方面,低水平的混合细胞嵌合并不一定是疾病进展的标志,可以在很长一段时间内保持“现状”不变。
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Long-term follow-up of chimerical state of the patients transplanted for different haematologic diseases.

Long-term follow-up of peripheral cellular chimerism in patients treated with BMT or PBSCT revealed the usefulness of their continuous monitoring at molecular level. Our results are based on monitoring of 120 patients, who were followed for at least 24 months. Comparison of the patients treated for chronic myelogenous leukemia (CML), acute myelocytic leukemia (AML), acute lymphocytic leukemia (ALL), myelodysplastic syndromes (MDS) and aplastic anaemia (AA) revealed that mixed chimerism was practically absent in MDS and relatively long-lasting in ALL and AA (regardless to substantially different post-transplantation treatment). The first disease relapses signalized by molecular checking of mixed peripheral chimerism were observed also after a period of remission lasting for several years. Molecular watching enables us to detect relapses at their very beginning that would remain hidden to less sensitive methods. We believe that all of the transplanted patients ought to be monitored for residual disease i.e. cellular chimerism using molecular methods without time limits. On the other hand low level of mixed cellular chimerism is not necessarily a sign of disease progression and can remain unchanged as "status quo" for a very long period.

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