Pediatric and Adolescent Endocrinology, Division of Pediatrics, Department of Obstetrics, Gynecology and Pediatrics, University Hospital, Pisa, Italy.
Department of Woman, Child and General and Specialized Surgery, University of Campania "Luigi Vanvitelli", Naples, Italy.
Eur J Med Genet. 2024 Aug;70:104958. doi: 10.1016/j.ejmg.2024.104958. Epub 2024 Jun 29.
X-linked hypophosphatemic rickets (XLH) is due to loss-of-function mutations in the phosphate-regulating endopeptidase homologue on the X chromosome (PHEX) that lead to increased fibroblast growth factor 23 (FGF23) production. FGF23 excess causes renal phosphate wasting and insufficient 1,25-dihydroxyvitamin D (1,25(OH)D) synthesis with reduced intestinal phosphate absorption, ultimately resulting in chronic hypophosphatemia. Children with XLH show typical skeletal lesions of rickets, deformities of the lower limbs, stunted growth with disproportionate short stature, bone pain, and physical dysfunctions. Burosumab, a fully human IgG1 monoclonal antibody that binds to FGF23 to inhibit its activity, is more effective to improve the biochemical and clinical signs of XLH than conventional treatment with phosphate supplements and vitamin D active metabolites. Data on adolescents with XLH during the transition period to young adulthood are few. In this prospective case series, we aimed to assess safety and efficacy of burosumab in adolescents with XLH who discontinued long-term conventional therapy.
Five Caucasian adolescents (4 males, 1 female; mean age 15.4 ± 1.5 years) with XLH were recruited and switched from conventional treatment to burosumab (0.8-1.2 mg/kg, s. c. QW2). Burosumab was continued for 12-48 months and, once discontinued, patients were followed-up for 6-12 months. In all patients, serum calcium, phosphate, alkaline phosphatase (ALP), parathyroid hormone (PTH), and 1,25(OH)D levels, and renal tubular reabsorption of phosphate (TmP/GFR) values were assessed at entry and during burosumab. Intact FGF23 plasma levels were measured at entry. Patient-reported outcomes (PROs) were assessed at entry and every 3-6 months to evaluate the impact of low extremity pain, stiffness, and difficulties performing daily activities.
At entry, all patients showed hypophosphatemia, increased intact FGF23 levels, reduced TmP/GFR, insufficient 1,25(OH)D levels, and in four out of five increased ALP levels. Two patients had radiological signs of rickets. During burosumab, all patients showed a significant increase in serum phosphate and 1,25(OH)D levels, and in TmP/GFR values (P < 0.05 - P < 0.0001). Serum ALP levels significantly declined (P < 0.05) to normal values. No changes of serum calcium and PTH levels (PNS) were found during burosumab. PROs significantly improved (P < 0.02 - P < 0.0001) in all patients. Four patients discontinued burosumab when they turned 18 or 19, whereas one continued the treatment since he was still younger than 18 during the study period. Four patients who suspended burosumab showed a rapid decline in serum phosphate and 1,25(OH)D levels and in TmP/GFR values; serum ALP levels increased, and PROs progressively worsened with a significant reduction in quality of life. These consequences were not observed in the patient who continued burosumab treatment.
Our data showed that conventional treatment improved only in part the signs and symptoms of XLH. Burosumab was well tolerated and was effective in improving phosphate metabolism, bone health, and PROs. All the benefits of burosumab were lost after its discontinuation. These results suggested that continuing burosumab is required to achieve and maintain the clinical benefits of the treatment during the transition to young adulthood in patients with XLH.
X 连锁低磷血症性佝偻病(XLH)是由于 X 染色体上磷调节内肽酶同源物(PHEX)的功能丧失突变导致成纤维细胞生长因子 23(FGF23)产生增加引起的。FGF23 过多导致肾脏磷酸盐丢失和 1,25-二羟维生素 D(1,25(OH)D)合成不足,肠道磷酸盐吸收减少,最终导致慢性低磷血症。患有 XLH 的儿童表现出典型的佝偻病骨骼病变、下肢畸形、生长受限和不成比例的身材矮小、骨痛和身体功能障碍。Burosumab 是一种完全人源 IgG1 单克隆抗体,可与 FGF23 结合以抑制其活性,与磷酸盐补充剂和维生素 D 活性代谢物的常规治疗相比,更有效地改善 XLH 的生化和临床体征。关于青少年 XLH 在向青年期过渡期间的数据很少。在这项前瞻性病例系列研究中,我们旨在评估 Burosumab 在停止长期常规治疗的 XLH 青少年中的安全性和有效性。
招募了 5 名白种人青少年(4 名男性,1 名女性;平均年龄 15.4±1.5 岁)患有 XLH,并从常规治疗转换为 Burosumab(0.8-1.2mg/kg,皮下 QW2)。Burosumab 持续使用 12-48 个月,一旦停药,患者将继续随访 6-12 个月。所有患者在入组时和 Burosumab 期间评估血清钙、磷、碱性磷酸酶(ALP)、甲状旁腺激素(PTH)和 1,25(OH)D 水平,以及肾小管重吸收磷酸盐(TmP/GFR)值。在入组时测量完整的 FGF23 血浆水平。在入组时和每 3-6 个月评估患者报告的结局(PROs),以评估下肢疼痛、僵硬和日常活动困难的影响。
在入组时,所有患者均表现出低磷血症、升高的完整 FGF23 水平、降低的 TmP/GFR、不足的 1,25(OH)D 水平,以及五名患者中有四名升高的 ALP 水平。两名患者有佝偻病的放射学迹象。在 Burosumab 期间,所有患者均表现出血清磷酸盐和 1,25(OH)D 水平以及 TmP/GFR 值显著增加(P<0.05-P<0.0001)。血清 ALP 水平显著下降(P<0.05)至正常水平。血清钙和 PTH 水平(PNS)在 Burosumab 期间没有变化。所有患者的 PROs 均显著改善(P<0.02-P<0.0001)。当他们年满 18 或 19 岁时,四名患者停止使用 Burosumab,而一名患者由于在研究期间仍未满 18 岁而继续使用该药物。四名停止使用 Burosumab 的患者血清磷酸盐和 1,25(OH)D 水平以及 TmP/GFR 值迅速下降;血清 ALP 水平升高,PROs 逐渐恶化,生活质量显著降低。这些后果在继续接受 Burosumab 治疗的患者中未观察到。
我们的数据表明,常规治疗仅部分改善了 XLH 的体征和症状。Burosumab 耐受性良好,有效改善了磷酸盐代谢、骨骼健康和 PROs。停止使用 Burosumab 后,所有 Burosumab 的益处均丧失。这些结果表明,在 XLH 患者向青年期过渡期间,需要继续使用 Burosumab 以实现并维持治疗的临床益处。
