自体外周血细胞移植治疗晚期神经母细胞瘤。

A Di Caro, B Bostrom, T J Moss, J Neglia, N K Ramsay, J Smith, L C Sasky
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引用次数: 22

摘要

目的:我们回顾了明尼苏达大学自体外周血细胞移植(APBCT)治疗儿童神经母细胞瘤的经验。患者和方法:回顾了1987年9月至1989年12月期间9例晚期神经母细胞瘤患者(8例Evans期,1例III期)的外周血收集和使用情况,这些患者中位年龄为4岁(范围10个月-22岁),接受了大剂量化疗,无全身照射和APBCT治疗。结果:中位数为4.8 x 10(8)(范围3.3-8.9)单个核细胞每公斤体重通过中位数6(范围4 -8)收集获得。粒细胞-单核细胞集落形成细胞(CFU-GM)的体外测定显示,中位数为3.6 × 10(4)(范围0.7-7.8)CFU-GM/kg体重。APBCT后,粒细胞恢复(绝对中性粒细胞计数> 500 × 10(6)/L)的中位时间为28天(范围14-72),血小板恢复(> 150 × 10(9)/L)的中位时间为34天(范围19-202)。除了一名病情进展的患者外,所有患者都移植了残留病变。外周血干细胞采集的免疫细胞学分析显示,9例患者中有3例存在循环神经母细胞瘤细胞,所有患者活检均有最小的骨髓残留疾病。一名患者在5年后仍然活着,没有任何疾病迹象。其他患者在移植后平均14个月(范围3-29)死于复发性神经母细胞瘤。结论:APBCT在大剂量化疗后的造血重建中是安全有效的,当由于先前盆腔放疗或少量残留骨髓转移而无法进行骨髓采集时可能是有用的。应采用免疫细胞学方法确保产品无肿瘤污染。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Autologous peripheral blood cell transplantation in the treatment of advanced neuroblastoma.

Purpose: We review the experience with autologous peripheral blood cell transplantation (APBCT) in children with neuroblastoma at the University of Minnesota.

Patients and methods: Aspects of peripheral blood cell collection and use in nine patients who had advanced neuroblastoma (eight Evans stage IV, 1 stage III), who were median age 4 years (range 10 months-22 years) and who were treated with high-dose chemotherapy without total body irradiation and APBCT between September 1987 and December 1989 are reviewed.

Results: A median of 4.8 x 10(8) (range 3.3-8.9) mononuclear cells per kilogram of body weight were obtained by a median of six (range four-eight) collections. In vitro assay of granulocyte-monocyte colony-forming cells (CFU-GM) demonstrated a median of 3.6 x 10(4) (range 0.7-7.8) CFU-GM/kg of body weight. After APBCT, granulocyte recovery (absolute neutrophil count > 500 x 10(6)/L) occurred at a median of 28 days (range 14-72) and platelet recovery (> 150 x 10(9)/L) occurred at a median of 34 days (range 19-202). All patients but one, who had progressive disease, were transplanted with residual disease. Immunocytological analysis of peripheral blood stem cell harvest showed the presence of circulating neuroblastoma cells in three of nine patients, all of whom had minimal marrow residual disease by biopsy. One patient is still alive with no evidence of disease after 5 years. The others died of recurrent neuroblastoma a median of 14 months (range 3-29) after transplant.

Conclusion: APBCT is safe and effective for hematopoietic reconstitution after high-dose chemotherapy, and may be useful when a bone marrow harvest cannot be performed because of prior pelvic radiation or minimal residual bone marrow metastasis. Immunocytological methods to ensure that the product is free of tumor contamination should be performed.

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