Ito Y, Wasserman R, Galili N, Reichard B A, Shane S, Lange B, Rovera G
Wistar Institute, Philadelphia, PA 19104.
J Clin Oncol. 1993 Mar;11(3):546-53. doi: 10.1200/JCO.1993.11.3.546.
We have investigated whether the extent of residual leukemia in the marrows obtained at the completion of chemotherapy can predict subsequent relapse in children with B-lineage acute lymphoblastic leukemia (ALL).
Marrow samples of 24 patients were examined for residual disease at the end of treatment using a quantitative method based on the polymerase chain reaction (PCR) amplification of the complementarity determining region-3 of the immunoglobulin heavy chain.
Of the 15 patients who remain in continuous bone marrow remission (range, 41 to 98 months), 14 had no detectable leukemic cells; one patient had a very low level (one in approximately 335,000 marrow cells) of residual leukemic cells that underwent clonal evolution. Among the nine patients who had a marrow relapse after the completion of treatment, eight patients whose relapses occurred 4 to 54 months from the end of therapy had no detectable leukemic cells, whereas only the one patient who relapsed 2 months after the completion of therapy had detectable residual disease.
These observations indicate that the absence of detectable residual leukemia by PCR at the end of chemotherapy is not sufficient to assure that the patient is cured and suggest that frequent serial monitoring is required for the early prediction of relapse off therapy.
我们研究了化疗结束时所获骨髓中残留白血病的程度是否可预测B系急性淋巴细胞白血病(ALL)患儿随后的复发情况。
采用基于免疫球蛋白重链互补决定区-3聚合酶链反应(PCR)扩增的定量方法,对24例患者治疗结束时的骨髓样本进行残留疾病检测。
在15例持续处于骨髓缓解状态(时间范围为41至98个月)的患者中,14例未检测到白血病细胞;1例患者残留白血病细胞水平极低(约335,000个骨髓细胞中有1个),且该残留白血病细胞发生了克隆演变。在9例治疗结束后出现骨髓复发的患者中,8例在治疗结束后4至54个月复发的患者未检测到白血病细胞,而仅1例在治疗结束后2个月复发的患者检测到了残留疾病。
这些观察结果表明,化疗结束时通过PCR未检测到残留白血病并不足以确保患者已治愈,并提示需要进行频繁的系列监测以早期预测治疗后复发。
