高剂量他汀类药物对多发性硬化免疫细胞干扰素- β反应的抑制作用

Xuan Feng, Diana Han, Bharat K Kilaru, Beverly S Franek, Timothy B Niewold, Anthony T Reder
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引用次数: 31

摘要

目的:确定他汀类药物是否影响复发-缓解型多发性硬化症(RRMS)患者的1型干扰素应答。设计:在体外研究阿托伐他汀对Jurkat细胞、未接受治疗的RRMS患者的单核细胞(MNCs)和接受干扰素治疗的RRMS患者的单核细胞(MNCs)在4种情况下的1型干扰素应答的影响:无药物、单用他汀类药物、单用干扰素和在干扰素治疗的基础上加用他汀类药物。患者:该研究检查了临床稳定的RRMS患者:21名未接受治疗的患者和14名接受干扰素- β和他汀类药物治疗的患者。干预措施:他汀类药物对体外和体内干扰素β诱导的STAT1转录因子激活、干扰素刺激蛋白在跨国公司的表达和血清1型干扰素活性的影响。结果:在体外,阿托伐他汀剂量依赖性地抑制干扰素刺激的P- y- stat1表达44% (P < .001),干扰素调节因子1蛋白表达30% (P=.006),黏液病毒耐药1蛋白表达32% (P=.004)。在体内,接受高剂量他汀类药物(80 mg)治疗的10名患者中有9名患者的血清干扰素-α/β活性显著降低,而接受中剂量他汀类药物(40 mg)治疗的4名患者中只有2名患者的血清干扰素-α/β活性降低。高剂量的他汀类药物治疗可显著阻断干扰素- β功能,减少P-Y-STAT1转录因子的激活,减少黏液病毒抗性1蛋白和蝰蛇蛋白的产生。中等剂量的他汀类药物没有改变STAT1的激活。结论:大剂量他汀类药物治疗可显著降低RRMS患者的干扰素- β功能和1型干扰素反应。这些数据为他汀类药物如何抵消干扰素- β的有益作用并使疾病恶化提供了一个假定的机制。
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Inhibition of interferon-beta responses in multiple sclerosis immune cells associated with high-dose statins.

Objective: To determine whether statins affect type 1 interferon responses in relapsing-remitting multiple sclerosis (RRMS).

Design: Study effects of atorvastatin on type 1 interferon responses in Jurkat cells, mononuclear cells (MNCs) from therapy-naive patients with RRMS in vitro, and MNCs from interferon-treated RRMS patients in vivo in 4 conditions: no drug, statin only, interferon-beta only, and statin added on to interferon-beta therapy.

Patients: The study examined clinically stable patients with RRMS: 21 therapy-naive patients and 14 patients receiving interferon-beta with a statin.

Interventions: Statin effects on in vitro and in vivo interferon-beta-induced STAT1 transcription factor activation, expression of interferon-stimulated proteins in MNCs, and serum type 1 interferon activity.

Results: In vitro, atorvastatin dose dependently inhibited expression of interferon-stimulated P-Y-STAT1 by 44% (P < .001), interferon regulatory factor 1 protein by 30% (P=.006), and myxovirus resistance 1 protein by 32% (P=.004) compared with no-statin control in MNCs from therapy-naive RRMS patients. In vivo, 9 of 10 patients who received high-dose statins (80 mg) had a significant reduction in interferon-beta therapy-induced serum interferon-α/β activity, whereas only 2 of 4 patients who received medium- dose statins (40 mg) had reductions. High-dose add-on statin therapy significantly blocked interferon-beta function, with less P-Y-STAT1 transcription factor activation, and reduced myxovirus resistance 1 protein and viperin protein production. Medium doses of statins did not change STAT1 activation.

Conclusions: High-dose add-on statin therapy significantly reduces interferon-beta function and type 1 interferon responses in RRMS patients. These data provide a putative mechanism for how statins could counteract the beneficial effects of interferon-beta and worsen disease.

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Archives of neurology
Archives of neurology 医学-临床神经学
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