从阿加糖酶α转换为阿加糖酶β作为法布里病的酶替代疗法后血浆葡萄糖神经酰胺水平的降低。
Reduction of Plasma Globotriaosylsphingosine Levels After Switching from Agalsidase Alfa to Agalsidase Beta as Enzyme Replacement Therapy for Fabry Disease.
作者信息
Goker-Alpan Ozlem, Gambello Michael J, Maegawa Gustavo H B, Nedd Khan J, Gruskin Daniel J, Blankstein Larry, Weinreb Neal J
机构信息
Lysosomal Disorders Research and Treatment Unit, Center for Clinical Trials, 11212 Waples Mill Road, Fairfax, VA, 22030, USA.
Emory University School of Medicine, Atlanta, GA, USA.
出版信息
JIMD Rep. 2016;25:95-106. doi: 10.1007/8904_2015_483. Epub 2015 Aug 25.
INTRODUCTION
Agalsidase alfa and agalsidase beta, recombinant enzyme preparations for treatment of Fabry disease (FD), have different approved dosing schedules: 0.2 mg/kg and 1.0 mg/kg every other week (EOW), respectively.
METHODS
This open-label, multicenter, exploratory phase 4 study evaluated plasma globotriaosylsphingosine (lyso-GL-3) and plasma and urine globotriaosylceramide (GL-3) levels at baseline and 2, 4, and 6 months after the switch from agalsidase alfa (0.2 mg/kg EOW for ≥12 months) to agalsidase beta (1.0 mg/kg EOW) in 15 male patients with FD. Immunoglobulin (Ig)G antidrug antibody titers were assessed, and safety was monitored throughout the study.
RESULTS
Plasma lyso-GL-3 concentrations decreased significantly within 2 months after switch and reductions continued through month 6 (mean absolute changes, -12.8, -16.1, and -16.7 ng/mL at 2, 4, and 6 months, respectively; all P < 0.001). The mean percentage reduction from baseline was 39.5% (P < 0.001) at month 6. For plasma GL-3, the mean absolute change from baseline (-0.9 μg/mL) and percentage reduction (17.9%) at month 6 were both significant (P < 0.05). Urine GL-3 measurements showed intra-patient variability and changes from baseline were not significant. No clinical outcomes were assessed in this 6-month study, and, therefore, no conclusions can be drawn regarding the correlation of observed reductions in glycosphingolipid concentrations with clinically relevant outcomes. There were no differences in IgG antidrug antibody titers between the two enzymes. The switch from agalsidase alfa to agalsidase beta was well tolerated.
CONCLUSION
Plasma lyso-GL-3 and GL-3 levels reduced after switching from agalsidase alfa to agalsidase beta, indicating that agalsidase beta has a greater pharmacodynamic effect on these markers at the recommended dose. These data further support the use of agalsidase beta 1.0 mg/kg EOW as enzyme replacement therapy in FD.
引言
阿加糖酶α和阿加糖酶β是用于治疗法布里病(FD)的重组酶制剂,有不同的批准给药方案:分别为每两周一次(EOW),剂量为0.2mg/kg和1.0mg/kg。
方法
这项开放标签、多中心、探索性4期研究评估了15名男性FD患者从阿加糖酶α(0.2mg/kg EOW,持续≥12个月)转换为阿加糖酶β(1.0mg/kg EOW)后,在基线以及转换后2、4和6个月时血浆球三糖基鞘氨醇(溶酶体-GL-3)、血浆和尿液球三糖基神经酰胺(GL-3)的水平。评估了免疫球蛋白(Ig)G抗药物抗体滴度,并在整个研究过程中监测安全性。
结果
转换后2个月内血浆溶酶体-GL-3浓度显著下降,并持续至第6个月(2、4和6个月时的平均绝对变化分别为-12.8、-16.1和-16.7ng/mL;所有P<0.001)。在第6个月时,相对于基线的平均下降百分比为39.5%(P<0.001)。对于血浆GL-3,第6个月时相对于基线的平均绝对变化(-0.9μg/mL)和下降百分比(17.9%)均具有显著性(P<0.05)。尿液GL-3测量显示患者内存在变异性,相对于基线的变化不显著。在这项为期6个月的研究中未评估临床结局,因此,无法就观察到的糖鞘脂浓度降低与临床相关结局之间的相关性得出结论。两种酶之间的IgG抗药物抗体滴度没有差异。从阿加糖酶α转换为阿加糖酶β耐受性良好。
结论
从阿加糖酶α转换为阿加糖酶β后,血浆溶酶体-GL-3和GL-3水平降低,表明阿加糖酶β在推荐剂量下对这些标志物具有更大的药效学作用。这些数据进一步支持使用1.0mg/kg EOW的阿加糖酶β作为FD的酶替代疗法。
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