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在接受高辐射剂量照射后不久,抗凋亡细胞因子与聚乙二醇化重组人粒细胞刺激因子联合使用可减轻非人灵长类动物的骨髓抑制。

Antiapoptotic cytokines in combination with pegfilgrastim soon after irradiation mitigates myelosuppression in nonhuman primates exposed to high irradiation dose.

作者信息

Hérodin Francis, Roy Laurence, Grenier Nancy, Delaunay Christophe, Baugé Stéphane, Vaurijoux Aurélie, Grégoire Eric, Martin Cécile, Alonso Antonia, Mayol Jean-François, Drouet Michel

机构信息

Centre de Recherches du Service de Santé des Armées, la Tronche, France.

出版信息

Exp Hematol. 2007 Aug;35(8):1172-81. doi: 10.1016/j.exphem.2007.04.017. Epub 2007 Jun 8.

Abstract

OBJECTIVE

Preservation of hematopoietic stem and progenitor cells from early radiation-induced apoptosis is the rationale for emergency antiapoptotic cytokine therapy (EACK) after radiation accidents. This strategy is based on the combination of stem cell factor + Flt3-ligand + thrombopoietin + interleukin 3 (SFT3). The long-term safety and efficacy of EACK in managing severe radiation exposure were evaluated.

MATERIAL AND METHODS

Early administration of SFT3 + pegfilgrastim was assessed in 7-Gy gamma total body-irradiated (TBI) monkeys. Efficiency of delayed administration was also addressed after 5-Gy TBI.

RESULTS

Here we showed that a single, intravenous injection of SFT3 2 hours after 7-Gy TBI reduced the period of thrombocytopenia (platelet count <20 x 10(9)/L: 0.8 +/- 1.5 day vs 23.8 +/- 15.9 days in controls; p < 0.05) and blood transfusion needs. Moreover, addition of pegfilgrastim to SFT3 treatment shortened the period of neutropenia compared with SFT3 and control groups (neutrophil count <0.5 x 10(9)/L: 7 +/- 1.4 days vs 13 +/- 3.2 days and 15.2 +/- 1.5 days; p < 0.05). In both SFT3 groups, bone marrow activity recovered earlier and, in contrast with controls, platelet count returned to baseline values from 250 days after irradiation. Furthermore, delayed (48 hours) single SFT3 administration in 5-Gy irradiated monkeys significantly reduced thrombocytopenia compared to controls. Finally, SFT3 did not increase frequency of total chromosome translocations observed in the blood lymphocytes of controls 1 year after 5 Gy TBI.

CONCLUSION

These results suggest the safety and efficacy of EACK in managing severe radiation exposure.

摘要

目的

保护造血干细胞和祖细胞免受早期辐射诱导的凋亡是辐射事故后进行紧急抗凋亡细胞因子治疗(EACK)的理论依据。该策略基于干细胞因子+Flt3配体+血小板生成素+白细胞介素3(SFT3)的联合应用。评估了EACK在处理严重辐射暴露方面的长期安全性和有效性。

材料与方法

在接受7 Gy全身γ射线照射(TBI)的猴子中评估早期给予SFT3+聚乙二醇化重组人粒细胞刺激因子(pegfilgrastim)的效果。还研究了在5 Gy TBI后延迟给药的效果。

结果

我们发现,在7 Gy TBI后2小时单次静脉注射SFT3可缩短血小板减少期(血小板计数<20×10⁹/L:0.8±1.5天,而对照组为23.8±15.9天;p<0.05)以及减少输血需求。此外,与SFT3组和对照组相比,在SFT3治疗中添加pegfilgrastim可缩短中性粒细胞减少期(中性粒细胞计数<0.5×10⁹/L:7±1.4天,而SFT3组为13±3.2天,对照组为15.2±1.5天;p<0.05)。在两个SFT3组中,骨髓活性恢复较早,与对照组不同的是,血小板计数在照射后250天恢复到基线值。此外,在接受5 Gy照射的猴子中延迟(48小时)单次给予SFT3与对照组相比显著减轻了血小板减少。最后,SFT3并未增加5 Gy TBI后1年在对照组血液淋巴细胞中观察到的总染色体易位频率。

结论

这些结果表明EACK在处理严重辐射暴露方面具有安全性和有效性。

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