Bührer C, Hartmann R, Fengler R, Rath B, Schrappe M, Janka-Schaub G, Henze G
Department of Pediatric Hematology/Oncology, Children's Hospital, Virchow Medical Center, Humboldt University, Berlin, Germany.
J Clin Oncol. 1996 Oct;14(10):2812-7. doi: 10.1200/JCO.1996.14.10.2812.
In newly diagnosed childhood acute lymphoblastic leukemia (ALL), a high tumor burden indicates a poor prognosis, while no such link has been established yet after relapse. The impact of the absolute peripheral blast count (PBC) at the time of relapse on the response to salvage chemotherapy after a late isolated bone marrow (BM) relapse is the subject of this prospective analysis.
Since 1983, 260 children with a first isolated BM relapse of ALL that occurred 6 months or later after elective cessation of front-line therapy were enrolled onto four consecutive multicenter trials of the Berlin-Frankfurt-Münster (BFM) Relapse Study Group. All patients received intensive multiagent induction and consolidation chemotherapy for 6 months, followed by maintenance therapy with methotrexate (MTX) and thioguanine for 2 years. Treatment of subclinical meningeal leukemia consisted of high-dose intravenous MTX and intrathecally administered cytostatic drugs, which was augmented by cranial irradiation since 1988.
At the time relapse was diagnosed, PBC varied considerably among patients (median, 1,060/microL; range, 0 to 106,800/microL). Achievement of a second complete remission (CR) was not significantly different in children without detectable circulating blasts at relapse (37 of 38) and those with moderate (1 to 9,999/microL) PBC (165 of 171). In contrast, only 42 of 51 children with high PBC (> or = 10,000/microL) achieved a second CR (P = .0015). At a median follow-up time of 40 months, the 10-year event-free survival (EFS) probability was significantly (P = .0001) higher in children without circulating blasts (.64) than in children with moderate PBC (.32) or high PBC (.10). There was a preponderance of boys in the group without detectable circulating blasts, while the three PBC-defined groups did not differ with respect to frontline treatment, age at initial diagnosis, age at relapse, time off therapy, or salvage treatment protocol. On sequential univariate and multivariate analysis, only duration of first remission > or = 48 months was an additional independent indicator of adverse prognosis, while preventive cranial irradiation improved outcome independently of PBC.
The absence of blasts on peripheral-blood smears at the time of a first late isolated BM relapse of childhood ALL is associated with a favorable response and prognosis in chemotherapy-treated children, who should be regarded as ineligible for bone marrow transplantation (BMT) unless a second round of chemotherapy has failed to produce a response.
在新诊断的儿童急性淋巴细胞白血病(ALL)中,高肿瘤负荷预示着预后不良,而复发后尚未确立此类关联。本次前瞻性分析的主题是复发时的外周原始细胞绝对计数(PBC)对晚期孤立骨髓(BM)复发后挽救化疗反应的影响。
自1983年以来,260例一线治疗选择性停止6个月或更久后首次出现孤立BM复发的ALL患儿被纳入柏林 - 法兰克福 - 明斯特(BFM)复发研究组的四项连续多中心试验。所有患者接受为期6个月的强化多药诱导和巩固化疗,随后用甲氨蝶呤(MTX)和硫鸟嘌呤进行2年维持治疗。亚临床脑膜白血病的治疗包括大剂量静脉注射MTX和鞘内注射细胞毒性药物,自1988年起增加了颅脑照射。
在诊断复发时,患者的PBC差异很大(中位数为1,060/μL;范围为0至106,800/μL)。复发时外周血未检测到原始细胞的儿童(38例中的37例)和PBC中等(1至9,999/μL)的儿童(171例中的165例)达到第二次完全缓解(CR)的情况无显著差异。相比之下,PBC高(≥10,000/μL)的51例儿童中只有42例达到第二次CR(P = 0.0015)。在中位随访时间40个月时,外周血无原始细胞的儿童10年无事件生存(EFS)概率(0.64)显著高于PBC中等的儿童(0.32)或PBC高的儿童(0.10)(P = 0.0001)。外周血未检测到原始细胞的组中男孩居多,而根据PBC定义的三组在一线治疗、初始诊断年龄、复发年龄、停止治疗时间或挽救治疗方案方面无差异。在单因素和多因素序贯分析中,只有首次缓解持续时间≥48个月是不良预后的另一个独立指标,而预防性颅脑照射独立于PBC改善了预后。
儿童ALL首次晚期孤立BM复发时外周血涂片无原始细胞与化疗治疗儿童的良好反应和预后相关,除非第二轮化疗未能产生反应,否则这些儿童不应被视为适合进行骨髓移植(BMT)。
