Laboratory of Biological and Medical Chemistry, Faculté de Phamacie, Université Libre de Bruxelles (ULB), Brussels, Belgium.
Service of Clinical Chemistry, Laboratoire Hospitalier Universitaire de Bruxelles (LHUB-ULB), Brussels, Belgium.
Pediatr Blood Cancer. 2018 Jul;65(7):e27022. doi: 10.1002/pbc.27022. Epub 2018 Mar 7.
Hydroxyurea (HU) reduces the severity of sickle cell disease (SCD) in children; nevertheless, its long-term safety is an important concern. This paper evaluates HU genotoxicity at dose ≤ 30 mg/kg/day after over 2 years of treatment.
The study included 76 children: 32 SCD patients treated with HU, 27 SCD patients not treated with HU, and 17 unaffected children. HU patients were classified as good or poor responders according to their clinical response. Comet assay allows the comparison of DNA damage between both groups of patients and unaffected children. Maximal concentration (C ) of HU in plasma was determined after drug administration.
Mean values of DNA in the comet tail were 5.13 ± 6.84 for unaffected children, 5.80 ± 7.78 for patients with SCD treated with HU, and 5.61 ± 6.91 for patients with SCD not treated with HU. Significant differences were observed between unaffected children and children with SCD. No difference was evident between comets from SCD patients treated and not treated with HU. In the case of HU, mean DNA in the comet tail was significantly lower in good responders than in poor responders: 5.54 ± 7.77 and 6.69 ± 8.43, respectively. Mean C value on plasma was 39.08 ± 15.65 mg/l; N = 31.
SCD increases, slightly but significantly, DNA damage in lymphocytes from patients with SCD. Patients with SCD treated with HU do not present more nucleoid damage than patients with SCD not treated with HU. Good responders to the HU treatment have significantly less nucleoid damage than poor responders. HU treatment at ≤30 mg/kg/day does not expose patients to a genotoxic plasma concentration.
羟基脲(HU)可降低儿童镰状细胞病(SCD)的严重程度;然而,其长期安全性是一个重要的关注点。本研究评估了 HU 在剂量≤30mg/kg/天治疗 2 年以上的情况下的遗传毒性。
该研究纳入了 76 名儿童:32 名接受 HU 治疗的 SCD 患者,27 名未接受 HU 治疗的 SCD 患者,以及 17 名未受影响的儿童。根据临床反应,HU 患者被分为良好或不良反应者。彗星试验可比较两组患者和未受影响儿童之间的 DNA 损伤。测定给药后 HU 血浆的最大浓度(C)。
未受影响儿童的彗星尾 DNA 平均浓度为 5.13±6.84,接受 HU 治疗的 SCD 患者为 5.80±7.78,未接受 HU 治疗的 SCD 患者为 5.61±6.91。未受影响儿童与 SCD 患者之间存在显著差异。接受 HU 治疗的 SCD 患者和未接受 HU 治疗的 SCD 患者之间的彗星没有差异。在 HU 组中,良好反应者的彗星尾 DNA 明显低于不良反应者:5.54±7.77 和 6.69±8.43。HU 在血浆中的平均 C 值为 39.08±15.65mg/L;N=31。
SCD 略微但显著增加了 SCD 患者淋巴细胞的 DNA 损伤。接受 HU 治疗的 SCD 患者的核小体损伤并不比未接受 HU 治疗的 SCD 患者多。HU 治疗的良好反应者的核小体损伤明显低于不良反应者。HU 治疗剂量≤30mg/kg/天不会使患者暴露于遗传毒性的血浆浓度下。
