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近期长春新碱对中枢神经系统肿瘤患儿人类造血祖细胞采集的影响。

The impact of recent vincristine on human hematopoietic progenitor cell collection in pediatric patients with central nervous system tumors.

作者信息

Cooling Laura, Bombery Melissa, Hoffmann Sandra, Davenport Robertson, Robertson Patricia, Levine John E

机构信息

Department of Pathology, University of Michigan, Ann Arbor, Michigan.

出版信息

Transfusion. 2014 Aug;54(8):2004-14. doi: 10.1111/trf.12574. Epub 2014 Feb 17.

Abstract

BACKGROUND

Central nervous system (CNS) malignancies represent 20% of all childhood cancers. To improve outcomes in infants and children with high-risk disease, treatment can include adjuvant chemotherapy and early autologous peripheral blood human progenitor cell collection (AHPCC), followed by high-dose chemotherapy and stem cell rescue. In many protocols, postoperative chemotherapy includes the administration of weekly vincristine (VCR) between induction chemotherapy cycles, regardless of scheduled AHPCC. We observed anecdotal AHPCC failures in children receiving midcycle VCR (MC-VCR).

STUDY DESIGN AND METHODS

The study was an 8-year retrospective chart review of all children with a CNS malignancy and who underwent AHPCC. Information included patient demographic and clinical data, mobilization regimen, VCR administration, product yields, infusion toxicity, and patient charges. Data were analyzed relative to MC-VCR administration. Graphics and statistical analysis (t-test, chi-square, linear regression) were performed with commercial software.

RESULTS

Twenty-four patients and 47 AHPCCs were available for analysis. Nine patients (37%) received MC-VCR within 7 days of scheduled AHPCC. MC-VCR was associated with delayed marrow recovery (17.9 days vs. 14.9 days, p=0.0012), decreased median peripheral CD34 counts (75 × 10(6) CD34/L vs. 352 × 10(6) CD34/L, p=0.03), decreased median CD34 yields (2.4 × 10(6) CD34/L vs. 17.8 × 10(6) CD34/kg, p=0.08), more AHPCCs per mobilization (2.9 vs. 1.1, p=0.01), and an increased rate of remobilization (33% vs. 6%). Mean patient charges were 2.5× higher in patients receiving MC-VCR than controls (p=0.01).

CONCLUSION

MC-VCR should be withheld before scheduled AHPCC to optimize CD34 collection.

摘要

背景

中枢神经系统(CNS)恶性肿瘤占儿童所有癌症的20%。为改善高危疾病婴幼儿和儿童的治疗效果,治疗可包括辅助化疗和早期自体外周血人类祖细胞采集(AHPCC),随后进行大剂量化疗和干细胞救援。在许多方案中,术后化疗包括在诱导化疗周期之间每周给予长春新碱(VCR),无论是否安排了AHPCC。我们观察到接受周期中VCR(MC-VCR)治疗的儿童出现了AHPCC失败的个案。

研究设计与方法

该研究是对所有患有CNS恶性肿瘤且接受AHPCC的儿童进行的为期8年的回顾性病历审查。信息包括患者人口统计学和临床数据、动员方案、VCR给药、产品产量、输注毒性和患者费用。相对于MC-VCR给药对数据进行了分析。使用商业软件进行图形绘制和统计分析(t检验、卡方检验、线性回归)。

结果

24例患者和47次AHPCC可用于分析。9例患者(37%)在预定AHPCC的7天内接受了MC-VCR。MC-VCR与骨髓恢复延迟(17.9天对14.9天,p = 0.0012)、外周血CD34计数中位数降低(75×10⁶ CD34/L对352×10⁶ CD34/L,p = 0.03)、CD34产量中位数降低(2.4×10⁶ CD34/L对17.8×10⁶ CD34/kg,p = 0.08)、每次动员的AHPCC次数更多(2.9次对1.1次,p = 0.01)以及再次动员率增加(33%对6%)相关。接受MC-VCR的患者平均费用比对照组高2.5倍(p = 0.01)。

结论

在预定AHPCC之前应停用MC-VCR,以优化CD34采集。

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