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急性淋巴细胞白血病初始治疗期间或治疗后不久出现明显睾丸复发的男孩的治疗效果改善。一项儿科肿瘤学组研究。

Improved treatment results in boys with overt testicular relapse during or shortly after initial therapy for acute lymphoblastic leukemia. A Pediatric Oncology group study.

作者信息

Buchanan G R, Boyett J M, Pollock B H, Smith S D, Yanofsky R A, Ghim T, Wharam M D, Crist W M, Vietti T J, Johnson W

机构信息

University of Texas Southwestern Medical Center, Dallas.

出版信息

Cancer. 1991 Jul 1;68(1):48-55. doi: 10.1002/1097-0142(19910701)68:1<48::aid-cncr2820680110>3.0.co;2-x.

Abstract

Boys with acute lymphoblastic leukemia (ALL) who have overt testicular relapse (OTR) during initial continuation chemotherapy or within 6 months thereafter have poor outcomes, with long-term survival similar to patients with marrow relapse during treatment. In April 1983, the Pediatric Oncology Group (POG) adopted for these patients an intensive treatment protocol (POG 8303) consisting of a four-drug systemic reinduction (prednisone, vincristine, daunorubicin, and asparaginase), a brief intensive consolidation phase with teniposide and cytarabine, and a 2-year program of continuation chemotherapy with weekly rotating drug pairs (vincristine/cyclophosphamide and teniposide/cytarabine) with or without (by randomization) four-drug reinforcement pulses every 16 weeks. Bilateral testicular radiation (2600 cGy) was administered during reinduction, and intrathecal chemoprophylaxis was given every 4 to 6 weeks. Among 38 eligible study patients with OTR, 5 had prior or concominant extramedullary relapse in other sites. The median duration of complete remission before OTR was 27 months (range, 10 to 42 months). All 38 patients achieved clinical remission after reinduction. Three patients withdrew while in remission, 22 had another relapse (12 marrow, 5 central nervous system (CNS), 2 testicular, 1 retroperitoneal, 1 prostate, and 1 eye), and 13 (34%) remain in complete remission from 32+ to 74+ months after OTR (median, 53+ months). Eighteen patients had their therapy electively discontinued, and five relapses occurred thereafter. These results are superior to those observed in patients with first marrow relapse treated with the same protocol. Approximately one third of patients with OTR treated with POG protocol 8303 exhibit prolonged second remissions with the potential for cure.

摘要

在初始持续化疗期间或此后6个月内出现明显睾丸复发(OTR)的急性淋巴细胞白血病(ALL)男孩预后较差,其长期生存率与治疗期间出现骨髓复发的患者相似。1983年4月,儿科肿瘤学组(POG)为这些患者采用了一种强化治疗方案(POG 8303),该方案包括四药全身再诱导(泼尼松、长春新碱、柔红霉素和天冬酰胺酶)、用替尼泊苷和阿糖胞苷进行的短暂强化巩固阶段,以及为期2年的持续化疗方案,采用每周轮换药物组合(长春新碱/环磷酰胺和替尼泊苷/阿糖胞苷),随机分组决定是否每16周进行一次四药强化脉冲治疗。在再诱导期间给予双侧睾丸放疗(2600 cGy),每4至6周进行一次鞘内化学预防。在38例符合条件的OTR研究患者中,5例在其他部位有先前或同时发生的髓外复发。OTR前完全缓解的中位持续时间为27个月(范围10至42个月)。所有38例患者在再诱导后均实现临床缓解。3例患者在缓解期退出,22例出现再次复发(12例骨髓复发、5例中枢神经系统(CNS)复发、2例睾丸复发、1例腹膜后复发、1例前列腺复发和1例眼部复发),13例(34%)在OTR后32 +至74 +个月仍处于完全缓解状态(中位时间为53 +个月)。18例患者选择性停止治疗,此后发生5例复发。这些结果优于采用相同方案治疗的首次骨髓复发患者所观察到的结果。采用POG方案8303治疗的OTR患者中约三分之一表现出延长的第二次缓解期并有治愈的可能。

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