冠心病患者肌肉组织和血浆中的阿托伐他汀代谢物模式与他汀类药物的肌肉副作用有关;一项探索性病例对照研究

IF 1.4 Q3 PERIPHERAL VASCULAR DISEASE
Trine Lauritzen , John Munkhaugen , Stein Bergan , Kari Peersen , Anja Camilla Svarstad , Anders M. Andersen , Jens Pahnke , Einar Husebye , Nils Tore Vethe
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引用次数: 0

摘要

背景和目的他汀相关肌肉症状(SAMS)是他汀类药物停用的一个普遍原因。对于临床医生来说,评估症状是否由他汀引起既具有挑战性又耗费时间,因此需要诊断性生物标志物。阿托伐他汀代谢物与 SAMS 相关。我们的目的是比较冠心病(CHD)患者中存在和不存在他汀类药物临床不耐受和他汀依赖性肌肉组织病理改变的阿托伐他汀药代动力学。其次,我们还旨在评估与观察到的药代动力学变量相关的基因变异。方法2020 年,28 名患有冠心病和主观 SAMS 的患者被纳入探索性 MUSE 生物标记物研究。参与者连续七周每天服用阿托伐他汀 40 毫克,之后八周不再服用他汀类药物。每个阶段结束时收集肌肉活检和血液。结果我们发现,他汀类药物不耐受者肌肉和血浆中的阿托伐他汀酸水平明显较低,内酯/酸比率较高。在最佳截断条件下,2-OH-阿托伐他汀酸和2-OH-阿托伐他汀内酯/酸比值的灵敏度、特异性和预测值均为100%。UGT1A1和UGT1A3变异的患者肌肉和血浆中的内酯代谢物水平均高于野生型患者。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

The atorvastatin metabolite pattern in muscle tissue and blood plasma is associated with statin muscle side effects in patients with coronary heart disease; An exploratory case-control study

The atorvastatin metabolite pattern in muscle tissue and blood plasma is associated with statin muscle side effects in patients with coronary heart disease; An exploratory case-control study

Background and aims

Statin-associated muscle symptoms (SAMS) is a prevalent cause of statin discontinuation. It is challenging and time-consuming for clinicians to assess whether symptoms are caused by the statin or not, and diagnostic biomarkers are requested. Atorvastatin metabolites have been associated with SAMS. We aimed to compare atorvastatin pharmacokinetics between coronary heart disease (CHD) patients with and without clinically statin intolerance and statin-dependent histopathological alterations in muscle tissue. Secondarily we aimed to assess genetic variants relevant for the observed pharmacokinetic variables.

Methods

Twenty-eight patients with CHD and subjective SAMS were included in the exploratory MUSE biomarker study in 2020. Participants received atorvastatin 40 mg/day for seven weeks followed by no statins for eight weeks. Muscle biopsies and blood were collected at the end of each period. Four patients were categorized as clinically intolerant to ≥3 statins prior to study start whereas four patients had signs of muscle cell damage during treatment.

Results

We found significantly lower levels of atorvastatin acids, and higher lactone/acid ratios in the statin intolerant, both in muscle and plasma. With optimal cut-off, the combination of 2-OH-atorvastatin acid and the 2-OH-atorvastatin lactone/acid ratio provided sensitivity, specificity, and predictive values of 100 %. Patients with variants in UGT1A1 and UGT1A3 had higher lactone metabolite levels than those with wild type, both in muscle and plasma.

Conclusion

Atorvastatin metabolites appear promising as biomarkers for the identification of clinical statin intolerance in patients with self-perceived SAMS, but the findings have to be confirmed in larger studies.

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来源期刊
Atherosclerosis plus
Atherosclerosis plus Cardiology and Cardiovascular Medicine
CiteScore
2.60
自引率
0.00%
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审稿时长
66 days
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