Switching from active vitamin D and phosphate supplementation to burosumab significantly corrects lower limb malalignment in pediatric X-linked hypophosphatemia

低磷血症 磷酸盐 医学 内分泌学 内科学 维生素 下肢 化学 外科 生物化学
作者
Leanne M. Ward,Erik A. Imel,David B. Frumberg,Lisa Dilworth,Catherine Siener,Zunqiu Chen,Stan Krolczyk,Thomas O. Carpenter,XLH Disease Monitoring Program Investigators,Andrea Arcari,Ambika P. Ashraf,Richard Baquero-Rodríguez,Sanjukta Basak,Sasigarn A. Bowden,Oscar Brunetto,Thomas O. Carpenter,Janet Crane,Kathryn Dahir,Bradley P. Dixon,Walter Douthat
出处
期刊:Journal of Bone and Mineral Research [Oxford University Press]
卷期号:40 (12): 1332-1342 被引量:1
标识
DOI:10.1093/jbmr/zjaf079
摘要

X-linked hypophosphatemia (XLH) is a rare disorder of renal phosphate wasting and dysregulated active vitamin D metabolism, ultimately presenting as rickets and osteomalacia, among other manifestations. Lower extremity deformity (genu valgum and/or varum) is frequent in this pediatric population. Despite prompt active vitamin D and phosphate supplementation (active D/Pi), many patients require corrective surgery for lower limb malformation. Burosumab has demonstrated improvements in lower limb malalignment in children with XLH in several studies. We expand on those reports by assessing mechanical femoral tibial angle (mFTA) change in patients enrolled in the XLH Disease Monitoring Program (DMP), (NCT03651505) to determine the impact of initiating burosumab treatment after a history of active D/Pi. Included patients had either switched from active D/Pi to burosumab treatment at the discretion of their treating physician or as part of a burosumab clinical trial, or remained on active D/Pi through Year 3 of the DMP. Year 3 radiographs were compared with baseline to assess mFTA change and gauge improvement. Additional multivariate factor analysis examined 24 attributes to determine which had the greatest association with mFTA change. Change in mFTA was assessed for each limb independently. A greater proportion of limbs of patients switching from active D/Pi to burosumab had improved mFTA compared with those remaining on active D/Pi (p < .023). Odds ratios comparing limbs that improved to those that did not showed that switching to burosumab yields a significantly greater chance of improvement than continuing active D/Pi (OR [95% CI]: 4.38 [1.09-17.50]; p = .0469). Factor analysis identified younger age at burosumab initiation (p = .001) and lower baseline height Z-score (p = .006) as being significantly associated with greater change in mFTA Z-score. This study shows that switching to burosumab significantly improves lower limb malalignment in children with XLH over benefits conferred by active D/Pi, with early burosumab initiation providing the greatest benefit.
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