Cohen B H, Zeltzer P M, Boyett J M, Geyer J R, Allen J C, Finlay J L, McGuire-Cullen P, Milstein J M, Rorke L B, Stanley P
Cleveland Clinic Foundation, OH, USA.
J Clin Oncol. 1995 Jul;13(7):1687-96. doi: 10.1200/JCO.1995.13.7.1687.
To determine clinical characteristics and response to treatment for children with supratentorial primitive neuroectodermal tumors (S-PNETs).
After surgery and staging, 55 patients aged 1.5 to 19.3 years with S-PNETs were randomized to receive craniospinal radiotherapy (RT) followed by eight cycles of 1-(2-chloro-ethyl)-3-cyclohexylnitrosourea (CCNU), vincristine (VCR), and prednisone (standard treatment) or two cycles of 8-in-1 chemotherapy followed by RT and then eight additional cycles of 8-in-1.
Three-year Kaplan-Meier estimates (estimate +/- SE) of survival and progression-free survival (PFS) rates for patients with confirmed diagnoses of S-PNET were 57% +/- 8% and 45% +/- 8%, respectively; survival and PFS rates for children with PNETs located in the pineal region were 73% +/- 12% and 61% +/- 13%, respectively, and were significantly different from the other S-PNETs (P < .03). The 8-in-1 arm had greater toxicity than the standard-treatment arm. Distributions of PFS between the two treatment groups were not significantly different (P > .5). Other univariate prognostic factors that influenced PFS included metastasis (M) stage (P < .03: M0 50% +/- 9% v M1-4 0%) and age (P < .02: 1.5 to 2 years 25% +/- 13% v > or = 3 years 53% +/- 9%).
In this first randomized treatment trial for S-PNETs in children, no significant differences were detected between the two treatment groups. M0 and pineal site of involvement were independent predictors of a better outcome. However, survival was better than previously reported.
确定幕上原始神经外胚层肿瘤(S-PNETs)患儿的临床特征及对治疗的反应。
55例年龄在1.5至19.3岁的S-PNETs患儿在手术及分期后,被随机分为两组,一组接受全脑全脊髓放疗(RT),随后进行8个周期的1-(2-氯乙基)-3-环己基硝脲(CCNU)、长春新碱(VCR)及泼尼松治疗(标准治疗);另一组先接受2个周期的8合1化疗,接着进行放疗,然后再进行8个周期的8合1化疗。
确诊为S-PNET的患者3年的Kaplan-Meier生存估计值(估计值±标准误)和无进展生存(PFS)率分别为57%±8%和45%±8%;松果体区PNETs患儿的生存和PFS率分别为73%±12%和61%±13%,与其他S-PNETs有显著差异(P<.03)。8合1治疗组的毒性比标准治疗组更大。两个治疗组之间的PFS分布无显著差异(P>.5)。其他影响PFS的单因素预后因素包括转移(M)分期(P<.03:M0为50%±9%,M1 - 4为0%)和年龄(P<.02:1.5至2岁为25%±13%,≥3岁为53%±9%)。
在这项针对儿童S-PNETs的首次随机治疗试验中,两个治疗组之间未检测到显著差异。M0和松果体受累部位是预后较好的独立预测因素。然而,生存率高于先前报道。
