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Minimal residual disease levels in bone marrow and peripheral blood are comparable in children with T cell acute lymphoblastic leukemia (ALL), but not in precursor-B-ALL

机译:在患有T细胞急性淋巴细胞白血病(ALL)的儿童中,骨髓和外周血中的最小残留疾病水平相当,但在前体B-ALL中则没有

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摘要

Sensitive and quantitative detection of minimal residual disease (MRD) in bone marrow (BM) samples of children with acute lymphoblastic leukemia (ALL) is essential for evaluation of early treatment response. In this study, we evaluated whether the traumatic BM samplings can be replaced by peripheral blood (1313) samplings. MRD levels were analyzed in follow-up samples of 62 children with precursor-B-ALL (532 paired BM-PB samples) and 22 children with T-ALL (149 paired BM-PB samples) using real-time quantitative PCR (RQ-PCR) analysis of immunoglobulin and T cell receptor gene rearrangements with sensitivities of 10(-3) to 10(-5) (one ALL cell in 103 to 105 normal cells). In 14 of the 22 T-ALL patients, detectable MRD levels were found in 67 paired BM-PB samples: in 47 pairs MRD was detected both in BM and 1313, whereas in the remaining pairs very low MRD levels were detected in BM (n = 11) or PB (n = 9) only. The MRD levels in the paired BM-PB samples were very comparable and strongly correlated (r(s) = 0.849). Comparable results were obtained earlier by immunophenotyping in 26 T-ALL patients (321 paired BM-PB samples), which also showed a strong correlation between MRD levels in paired BM and PB samples (r(s) = 0.822). In 39 of the 62 precursor-B-ALL patients, MRD was detected in 107 BM-PB pairs: in 48 pairs MRD was detected in both BM and PB, in 47 pairs MRD was solely detected in BM (at variable levels), and in 12 pairs only the 1313 sample was MRD-positive at very low levels (less than or equal to10(-4)). Furthermore, in the 48 double-positive pairs, MRD levels in BM and PB varied enormously with MRD levels in BM being up to 1000 times higher than in the corresponding PB samples. Consequently, BM samples cannot easily be replaced by PB sampling for MRD analysis in childhood precursor-B-ALL, in line with their BM origin. In T-ALL, which are of thymic origin, BM sampling might be replaced by PB sampling, because the dissemination of T-ALL cells to BM and PB appears to be comparable.
机译:敏感和定量检测急性淋巴细胞性白血病(ALL)儿童骨髓(BM)样本中的最小残留疾病(MRD)对于评估早期治疗反应至关重要。在这项研究中,我们评估了是否可以用外周血(1313)代替创伤性BM采样。使用实时定量PCR(RQ-R)对62例前体B-ALL患儿(532对BM-PB样本)和22例T-ALL患儿(149对BM-PB样本)的随访样本中的MRD水平进行了分析。 PCR)对免疫球蛋白和T细胞受体基因重排的敏感性为10(-3)至10(-5)的分析(103至105个正常细胞中有1个ALL细胞)。在22例T-ALL患者中的14例中,在67对BM-PB样本中发现了可检测到的MRD水平:在47对BM和1313对中均检测到MRD,而在其余对中,在BM中检测到极低的MRD水平(n = 11)或PB(n = 9)。配对的BM-PB样品中的MRD水平非常可比且相关性极强(r(s)= 0.849)。通过免疫分型在26例T-ALL患者(321对BM-PB样本)中获得了可比的结果,这也表明成对的BM和PB样本中的MRD水平之间具有很强的相关性(r = 0.822)。在62例B-ALL前体患者中,有39例在BM-PB对中检出了MRD:在48对BM和PB中均检出了MRD,在47对BRD中仅在BM中检出了MRD(变化水平),并且在12对中,只有1313个样品的MRD阳性水平非常低(小于或等于10(-4))。此外,在48个双阳性对中,BM和PB中的MRD水平差异很大,而BM中的MRD水平则比相应的PB样品高1000倍。因此,根据其BM来源,在儿童前体B-ALL中不能轻易用PB样品代替BM样品进行MRD分析。在胸腺起源的T-ALL中,BM采样可能被PB采样代替,因为T-ALL细胞向BM和PB的传播似乎是可比的。

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