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Serum lipid profile changes predict neurodegeneration in interferon-β1a-treated multiple sclerosis patients

机译:血清脂质谱变化预测干扰素-β1a治疗的多发性硬化症患者的神经变性

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The purpose of this work was to determine whether changes in cholesterol profiles after interferon-{beta} (IFN-{beta})1a treatment initiation following the first demyelinating event suggestive of multiple sclerosis are associated with clinical and MRI outcomes over 4 years. A group of 131 patients (age: 27.9 {+/-} 7.8 years, 63% female) with serial 3-monthly clinical and 12-monthly MRI follow-ups over 4 years were investigated. Serum cholesterol profiles, including total cholesterol (TC), HDL cholesterol (HDL-C), and LDL cholesterol (LDL-C) were obtained at baseline, 1 month, 3 months, and every 6 months thereafter. IFN-{beta}1a initiation caused rapid decreases in serum HDL-C, LDL-C, and TC within 1 month of IFN-{beta}1a initiation (all P 0.001) that returned slowly toward baseline. In predictive mixed model analyses, greater percent decreases in HDL-C after 3 months of IFN-{beta}1a treatment initiation were associated with less brain atrophy over the 4 year time course, as assessed by percent brain volume change (P 0.001), percent gray matter volume change (P 0.001), and percent lateral ventricle volume change (P = 0.005). Decreases in cholesterol biomarkers following IFN-{beta}1a treatment are associated with brain atrophy outcomes over 4 years. Pharmacological interventions targeting lipid homeostasis may be clinically beneficial for disrupting neurodegenerative processes.
机译:这项工作的目的是确定在提示多发性硬化的首例脱髓鞘事件后,干扰素-β(IFN-β)1a治疗开始后胆固醇谱的变化是否与4年内的临床和MRI结果相关。对一组131例患者(年龄:27.9 {+/-} 7.8岁,女性63%)进行了为期4年的连续3个月临床和12个月MRI随访研究。在基线,1个月,3个月以及此后每6个月获得血清胆固醇概况,包括总胆固醇(TC),高密度脂蛋白胆固醇(HDL-C)和低密度脂蛋白胆固醇(LDL-C)。 IFN-β1a的启动会导致IFN-β1a的启动后1个月内血清HDL-C,LDL-C和TC迅速降低(所有P <0.001),并缓慢返回基线。在预测性混合模型分析中,通过脑容量变化百分比评估,在IFN-β1aa治疗开始3个月后,HDL-C降低的百分比更大,与脑萎缩较少相关(P <0.001) ,灰质体积变化百分比(P <0.001)和侧脑室体积变化百分比(P = 0.005)。 IFN-β1a治疗后胆固醇生物标志物的减少与4年后脑萎缩的结果相关。针对脂质稳态的药理干预措施可能在临床上有利于破坏神经退行性过程。

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