评估羟基脲治疗镰状细胞贫血儿童的遗传毒性。
Assessment of genotoxicity associated with hydroxyurea therapy in children with sickle cell anemia.
机构信息
Department of Hematology, St. Jude Children's Research Hospital, Memphis, TN 38105, USA.
出版信息
Mutat Res. 2010 Apr 30;698(1-2):38-42. doi: 10.1016/j.mrgentox.2010.03.001. Epub 2010 Mar 15.
Hydroxyurea induces fetal hemoglobin, improves laboratory parameters, and ameliorates clinical complications of sickle cell anemia (SCA), but its long-term efficacy and safety in this patient population remain incompletely defined. Although generally considered non-DNA reactive, an important safety concern is that hydroxyurea may indirectly cause genotoxic damage. To better address this safety issue of hydroxyurea in patients with SCA, we measured the production of micronuclei (MN) in red blood cells (RBCs) as a marker of genotoxicity. Blood samples were collected from children with SCA enrolled in the Hydroxyurea Study of Long-term Effects (ClinicalTrials.gov NCT00305175). Flow cytometry quantified circulating MN-containing erythrocyte sub-populations before and during hydroxyurea exposure. The frequency of micronucleated reticulocytes (MN-CD71(+)) and micronucleated mature erythrocytes (MN-RBC) was then tested for associations with laboratory and clinical data. In cross-sectional analysis of 293 blood samples from 105 children with SCA and a median of 2 years of hydroxyurea therapy, exposure to hydroxyurea was associated with significantly increased frequencies of MN-CD71(+) and MN-RBC compared to baseline. The increases were evident by 3 months of therapy, and did not escalate further with up to 12 years of continuous drug exposure. In prospective longitudinal analysis, substantial inter-individual variation in the effect of hydroxyurea on %MN-CD71(+) was observed that was associated with the expected laboratory effects of hydroxyurea. In conclusion, clinically relevant exposure to hydroxyurea is associated with increased MN production consistent with erythroblast genotoxicity but with substantial inter-patient variability. Associations between increased %MN-CD71(+) and laboratory benefits suggest that hydroxyurea effects on MN production may be related to individual patient sensitivity to hydroxyurea within the bone marrow.
羟脲诱导胎儿血红蛋白,改善实验室参数,并改善镰状细胞贫血(SCA)的临床并发症,但在该患者人群中其长期疗效和安全性仍不完全明确。尽管羟脲通常被认为是非 DNA 反应性的,但一个重要的安全问题是,羟脲可能间接引起遗传毒性损伤。为了更好地解决 SCA 患者羟脲的安全性问题,我们测量了红细胞(RBC)中的微核(MN)产生作为遗传毒性的标志物。从参加羟脲长期疗效研究(ClinicalTrials.gov NCT00305175)的 SCA 儿童中采集血液样本。在羟脲暴露之前和期间,通过流式细胞术定量循环中含有 MN 的红细胞亚群。然后测试微核网织红细胞(MN-CD71(+))和微核成熟红细胞(MN-RBC)的频率与实验室和临床数据的相关性。在对 105 例 SCA 儿童的 293 份血液样本的横断面分析中,中位羟脲治疗时间为 2 年,与基线相比,羟脲暴露与 MN-CD71(+)和 MN-RBC 的频率显著增加相关。在 3 个月的治疗中就可以观察到这种增加,并且在长达 12 年的持续药物暴露中不会进一步增加。在前瞻性纵向分析中,观察到羟脲对%MN-CD71(+)的影响存在个体间的显著差异,这与羟脲的预期实验室效应相关。总之,临床相关的羟脲暴露与 MN 产生增加相关,这与红系母细胞的遗传毒性一致,但存在很大的个体间变异性。%MN-CD71(+)增加与实验室益处之间的关联表明,羟脲对 MN 产生的影响可能与骨髓中个体对羟脲的敏感性有关。
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