Department of Oncology, St Jude Children's Research Hospital, Memphis, TN 38105, USA.
Blood. 2010 Jun 10;115(23):4657-63. doi: 10.1182/blood-2009-11-253435. Epub 2010 Mar 19.
Minimal residual disease (MRD) at the end of remission-induction therapy predicts relapse in acute lymphoblastic leukemia (ALL). We examined the clinical significance of levels below the usual threshold value for MRD positivity (0.01%) in 455 children with B-lineage ALL, using polymerase chain reaction amplification of antigen-receptor genes capable of detecting at least 1 leukemic cell per 100 000 normal mononucleated cells (0.001%). Of the 455 clinical samples studied on day 46 of therapy, 139 (30.5%) had MRD 0.001% or more with 63 of these (45.3%) showing levels of 0.001% to less than 0.01%, whereas 316 (69.5%) had levels that were either less than 0.001% or undetectable. MRD measurements of 0.001% to less than 0.01% were not significantly related to presenting characteristics but were associated with a poorer leukemia cell clearance on day 19 of remission induction therapy. Patients with this low level of MRD had a 12.7% (+/- 5.1%; SE) cumulative risk of relapse at 5 years, compared with 5.0% (+/- 1.5%) for those with lower or undetectable MRD (P < .047). Thus, low levels of MRD (0.001%-< 0.01%) at the end of remission induction therapy have prognostic significance in childhood ALL, suggesting that patients with this finding should be monitored closely for adverse events.
缓解诱导治疗结束时的微小残留病(MRD)可预测急性淋巴细胞白血病(ALL)的复发。我们使用能够检测至少每 100000 个正常单核细胞中有 1 个白血病细胞的抗原受体基因的聚合酶链反应扩增,检测了 455 例 B 系 ALL 患儿缓解诱导治疗结束时低于通常 MRD 阳性阈值(0.01%)的水平的临床意义。在治疗第 46 天研究的 455 例临床样本中,139 例(30.5%)MRD 为 0.001%或更高,其中 63 例(45.3%)水平为 0.001%至<0.01%,而 316 例(69.5%)水平低于 0.001%或无法检测。0.001%至<0.01%的 MRD 测量值与临床表现无显著相关性,但与缓解诱导治疗第 19 天的白血病细胞清除率较差相关。该低水平 MRD 的患者在 5 年内的累积复发风险为 12.7%(+/-5.1%;SE),而 MRD 水平较低或无法检测的患者为 5.0%(+/-1.5%)(P<.047)。因此,缓解诱导治疗结束时的低水平 MRD(0.001%-<0.01%)在儿童 ALL 中有预后意义,提示具有该发现的患者应密切监测不良事件。
