Department of Pediatric Kidney, Liver and Metabolic Diseases, Hannover Medical School, Hannover 30625, Germany.
Department of Pediatrics, Faculty of Medicine and University Hospital Cologne, University of Cologne, Cologne 50937, Germany.
J Clin Endocrinol Metab. 2023 Sep 18;108(10):e998-e1006. doi: 10.1210/clinem/dgad223.
Burosumab has been approved for the treatment of children and adults with X-linked hypophosphatemia (XLH). Real-world data and evidence for its efficacy in adolescents are lacking.
To assess the effects of 12 months of burosumab treatment on mineral metabolism in children (aged <12 years) and adolescents (aged 12-18 years) with XLH.
Prospective national registry.
Hospital clinics.
A total of 93 patients with XLH (65 children, 28 adolescents).
Z scores for serum phosphate, alkaline phosphatase (ALP), and renal tubular reabsorption of phosphate per glomerular filtration rate (TmP/GFR) at 12 months.
At baseline, patients showed hypophosphatemia (-4.4 SD), reduced TmP/GFR (-6.5 SD), and elevated ALP (2.7 SD, each P < .001 vs healthy children) irrespective of age, suggesting active rickets despite prior therapy with oral phosphate and active vitamin D in 88% of patients. Burosumab treatment resulted in comparable increases in serum phosphate and TmP/GFR in children and adolescents with XLH and a steady decline in serum ALP (each P < .001 vs baseline). At 12 months, serum phosphate, TmP/GFR, and ALP levels were within the age-related normal range in approximately 42%, 27%, and 80% of patients in both groups, respectively, with a lower, weight-based final burosumab dose in adolescents compared with children (0.72 vs 1.06 mg/kg, P < .01).
In this real-world setting, 12 months of burosumab treatment was equally effective in normalizing serum ALP in adolescents and children, despite persistent mild hypophosphatemia in one-half of patients, suggesting that complete normalization of serum phosphate is not mandatory for substantial improvement of rickets in these patients. Adolescents appear to require lower weight-based burosumab dosage than children.
布罗索尤单抗已被批准用于治疗 X 连锁低磷血症(XLH)的儿童和成人。目前缺乏其在青少年中疗效的真实世界数据和证据。
评估布罗索尤单抗治疗 12 个月对 XLH 儿童(<12 岁)和青少年(12-18 岁)矿物质代谢的影响。
前瞻性国家注册研究。
医院诊所。
共 93 例 XLH 患者(65 例儿童,28 例青少年)。
12 个月时血清磷酸盐、碱性磷酸酶(ALP)和肾小球滤过率肾小管磷重吸收率(TmP/GFR)的 Z 评分。
基线时,所有患者均表现为低磷血症(-4.4 SD)、TmP/GFR 降低(-6.5 SD)和 ALP 升高(2.7 SD,均 P <.001 与健康儿童相比),提示尽管 88%的患者接受了口服磷酸盐和活性维生素 D 治疗,但仍存在活跃性佝偻病。布罗索尤单抗治疗可使 XLH 儿童和青少年的血清磷酸盐和 TmP/GFR 均显著增加,且血清 ALP 持续下降(均 P <.001 与基线相比)。治疗 12 个月时,两组约 42%、27%和 80%的患者血清磷酸盐、TmP/GFR 和 ALP 水平分别恢复至年龄相关的正常范围,两组青少年患者的最终布罗索尤单抗剂量(0.72 与 1.06 mg/kg,P <.01)较儿童组低,与体重相关。
在本真实世界环境中,布罗索尤单抗治疗 12 个月可同样有效地使青少年和儿童的血清 ALP 恢复正常,尽管半数患者仍持续存在轻度低磷血症,但这表明这些患者佝偻病的显著改善并不一定需要血清磷酸盐完全正常化。青少年似乎需要比儿童更低的基于体重的布罗索尤单抗剂量。
