巨细胞动脉炎的糖皮质激素相关毒性基线评分:GiACTA 试验的事后分析。

ACR Open Rheumatology Pub Date : 2023-01-01 Epub Date: 2023-01-05 DOI:10.1002/acr2.11520
Naomi J Patel, Xiaoqing Fu, Yuqing Zhang, John H Stone
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引用次数: 0

摘要

目的:巨细胞动脉炎(GCA)需要长期使用大剂量糖皮质激素(GCs)治疗。评估和量化患者基线糖皮质激素相关毒性的评分可能对开始使用免疫抑制剂的患者进行风险分层和治疗决策非常重要:我们分析了参加 "托西珠单抗治疗巨细胞动脉炎(GiACTA)"试验的GCA患者。根据基线用药、病史、生命体征和实验室值,从糖皮质激素毒性指数中得出12个领域的GC相关毒性基线评分。考察的 12 个领域包括体重指数、糖耐量、血压、脂质代谢、骨骼和/或肌腱、GC 肌病、皮肤毒性、神经精神影响、感染、眼部毒性、胃肠道损伤和肾上腺功能。潜在评分范围为 0 至 538 分。我们比较了基线时新确诊和复发疾病患者之间的差异:共纳入 250 名患者(75% 为女性,平均年龄 69 岁)。所有患者的基线 GC 相关毒性评分的平均值(± SD)为 111.3 ± 53.2。对总分影响最大的领域是血压(占总分的 24.0%),其次是糖耐量(22.6%)和神经精神影响(15.9%)。与新诊断疾病的患者相比,复发疾病患者的基线 GC 相关毒性评分更高(平均值为 122.5 分对 98.9 分;P 结论:GC 相关毒性的基线评分在新诊断疾病患者中更高:这种评估基线 GC 相关毒性的方法可将复发性 GCA 患者与新诊断疾病患者区分开来。基线 GC 相关毒性评分可能有助于开始接受免疫抑制治疗的患者做出治疗决策。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Baseline Glucocorticoid-Related Toxicity Scores in Giant Cell Arteritis: A Post Hoc Analysis of the GiACTA Trial.

Baseline Glucocorticoid-Related Toxicity Scores in Giant Cell Arteritis: A Post Hoc Analysis of the GiACTA Trial.

Objective: Giant cell arteritis (GCA) requires treatment with high-dose, long-term glucocorticoids (GCs). A score assessing and quantifying patients' baseline GC-related toxicity may be important to risk stratification and therapeutic decision-making in patients initiating immunosuppression.

Methods: We analyzed patients with GCA enrolled in the Tocilizumab in Giant Cell Arteritis (GiACTA) trial. Baseline GC-related toxicity scores for 12 domains were derived from the Glucocorticoid Toxicity Index using baseline medications, medical history, vital signs, and laboratory values. The 12 domains examined were body mass index, glucose tolerance, blood pressure, lipid metabolism, bone and/or tendon, GC myopathy, skin toxicity, neuropsychiatric effects, infection, ocular toxicity, gastrointestinal injury, and adrenal function. Potential scores ranged from 0 to 538. We compared differences between those with newly diagnosed versus relapsing disease at baseline.

Results: A total of 250 patients were included (75% female, mean age 69 years). The mean ± SD baseline GC-related toxicity score among all patients was 111.3 ± 53.2. The domains that contributed most to the overall scores were blood pressure (24.0% of the overall score), followed by glucose tolerance (22.6%) and neuropsychiatric effects (15.9%). Baseline GC-related toxicity scores were higher in patients with relapsing disease compared with those with newly diagnosed disease (mean of 122.5 vs. 98.9; P < 0.001). The body mass index and neuropsychiatric domain scores were significantly higher in patients with relapsing disease.

Conclusion: This approach to the assessment of baseline GC-related toxicity distinguished patients with relapsing GCA from those with newly diagnosed disease. Baseline GC-related toxicity scores may be useful in therapeutic decision-making for patients beginning immunosuppressive treatment.

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