美泊利珠单抗通过糖皮质激素毒性指数降低糖皮质激素毒性。
Glucocorticoid toxicity reduction with mepolizumab using the Glucocorticoid Toxicity Index.
机构信息
Wellcome-Wolfson Centre for Experimental Medicine, School of Medicine, Dentistry, and Biological Sciences, Queen's University Belfast, Belfast, UK.
Division of Rheumatology, Allergy, and Clinical Immunology, Massachusetts General Hospital, Harvard Medical School, Boston, MA, USA.
出版信息
Eur Respir J. 2022 Jan 20;59(1). doi: 10.1183/13993003.00160-2021. Print 2022 Jan.
BACKGROUND
Reduction in glucocorticoid exposure is the primary benefit of new biologic treatments in severe asthma, but there is currently no evidence that reduction in glucocorticoid exposure corresponds to a proportionate reduction in associated toxicity.
OBJECTIVES
To use the validated Glucocorticoid Toxicity Index (GTI) to assess change in glucocorticoid toxicity after 12 months treatment with mepolizumab, and compare toxicity change to glucocorticoid reduction and change in patient-reported outcome measures (PROMs).
METHODS
A longitudinal, real-world prospective cohort of 101 consecutive patients with severe asthma commenced on mepolizumab in a specialist UK regional severe asthma clinic. GTI toxicity assessment, cumulative glucocorticoid exposure and PROMs were recorded on commencing mepolizumab (V1), and after 12 months treatment (V2).
RESULTS
There was significant reduction in oral glucocorticoid exposure (V1 median 4280 mg prednisolone per year (interquartile range 3083-5475 mg) V2 2450 mg prednisolone per year (1243-3360 mg), p<0.001). Substantial improvements in individual toxicities were observed, but did not correlate with oral glucocorticoid reduction. Mean±sd GTI aggregate improvement score (AIS) was -35.7±57.8 with a wide range in toxicity change at individual patient level (AIS range -165 to +130); 70% (71 out of 101) had a reduction in toxicity (AIS <0); 3% (three out of 101) had no change (AIS=0); and 27% (27 out of 101) an increase in overall toxicity. 62% (62 out of 101) of patients met the AIS minimally clinically important difference of ≤-10, but AIS did not correlate with glucocorticoid reduction or change in PROMs.
CONCLUSION
Mepolizumab resulted in substantial oral glucocorticoid reduction, but this did not correlate with reduction in oral glucocorticoid toxicity, which varies widely at the individual patient level. Oral glucocorticoid reduction is not a comprehensive measure of response to mepolizumab.
背景
新型生物制剂治疗严重哮喘的主要益处是减少糖皮质激素暴露,但目前尚无证据表明糖皮质激素暴露的减少与相关毒性的成比例减少相对应。
目的
使用经过验证的糖皮质激素毒性指数(GTI)评估美泊利珠单抗治疗 12 个月后糖皮质激素毒性的变化,并将毒性变化与糖皮质激素减少和患者报告的结果测量(PROM)变化进行比较。
方法
一项在英国一个专门的严重哮喘诊所进行的 101 例连续严重哮喘患者的纵向、真实世界前瞻性队列研究,这些患者开始接受美泊利珠单抗治疗。在开始美泊利珠单抗治疗时(V1)和治疗 12 个月后(V2)记录 GTI 毒性评估、累积糖皮质激素暴露和 PROM。
结果
口服糖皮质激素暴露显著减少(V1 中位数为 4280mg 泼尼松龙/年(四分位距 3083-5475mg),V2 为 2450mg 泼尼松龙/年(1243-3360mg),p<0.001)。观察到个别毒性的显著改善,但与口服糖皮质激素减少无关。平均±标准差 GTI 综合改善评分(AIS)为-35.7±57.8,个体患者毒性变化范围很宽(AIS 范围-165 至+130);70%(71/101)的毒性降低(AIS<0);3%(3/101)无变化(AIS=0);27%(27/101)的毒性增加。62%(62/101)的患者符合 AIS 最小临床重要差异≤-10,但 AIS 与糖皮质激素减少或 PROM 变化无关。
结论
美泊利珠单抗导致口服糖皮质激素大量减少,但这与口服糖皮质激素毒性的减少无关,后者在个体患者水平上差异很大。口服糖皮质激素减少不是美泊利珠单抗治疗反应的综合衡量标准。
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