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系统评价:评估降脂治疗对脂蛋白和血脂值的影响。

Systematic review: Evaluating the effect of lipid-lowering therapy on lipoprotein and lipid values.

机构信息

Icahn School of Medicine at Mount Sinai, New York, NY, 10029, USA,

出版信息

Cardiovasc Drugs Ther. 2013 Oct;27(5):465-79. doi: 10.1007/s10557-013-6477-6.

Abstract

PURPOSE

This systematic review was performed to summarize published experience using low density lipoprotein particle number (LDL-P) to monitor the efficacy of lipid-lowering pharmacotherapies.

METHODS

Studies were identified from a literature search of MEDLINE (January 1, 2000 - June 30, 2012); and abstract searches of select conferences. All accepted studies reported mean (or median) nuclear magnetic resonance (NMR)-based LDL-P values for at least 10 subjects receiving lipid lowering pharmacotherapy.

RESULTS

Searches revealed 36 studies (with 61 treatment arms) in which LDL-P measurements were reported pre- and post-treatment. Most studies also reported changes in low-density lipoprotein cholesterol (LDL-C), but fewer studies reported changes in apolipoprotein B (apoB)(n = 20) and non-HDL-C (n = 28). Treatments included statins (22 arms/15 studies), fibrates (7 arms/7 studies), niacin (7 arms/6 studies), bile acid sequestrants (5 arms/2 studies), an anti-apoB oligonucleotide (2 arms/2 studies), combination therapies (8 arms/6 studies), anti-diabetics (5 arms/4 studies), and, other treatments (5 arms/2 studies). Lipid-lowering pharmacotherapy resulted in reductions in mean LDL-P in all but two studies. In several statin studies, the percent reductions in LDL-P were smaller than reductions in LDL-C, comparable changes were reported when LDL-P and apoB, were reported.

CONCLUSIONS

Study-level data from this systemic review establish that different lipid lowering agents can lead to discordance between LDL-P and LDL-C, therefore, basing LDL-lowering therapy only on the achievement of cholesterol goals may result in a treatment gap. Therefore, the use of LDL-P for monitoring lipid-lowering therapy, particularly for statins, can provide a more accurate assessment of residual cardiovascular risk.

摘要

目的

本系统评价旨在总结使用低密度脂蛋白颗粒数(LDL-P)监测降脂药物疗效的已发表经验。

方法

通过对 MEDLINE(2000 年 1 月 1 日至 2012 年 6 月 30 日)的文献检索和对选定会议的摘要搜索,确定了研究。所有接受的研究均报告了至少 10 名接受降脂药物治疗的患者的核磁共振(NMR)基于 LDL-P 的平均(或中位数)值。

结果

检索结果显示 36 项研究(61 个治疗组)报告了治疗前后的 LDL-P 测量值。大多数研究还报告了低密度脂蛋白胆固醇(LDL-C)的变化,但较少的研究报告了载脂蛋白 B(apoB)(n=20)和非高密度脂蛋白胆固醇(非 HDL-C)(n=28)的变化。治疗包括他汀类药物(22 个臂/15 个研究)、贝特类药物(7 个臂/7 个研究)、烟酸(7 个臂/6 个研究)、胆汁酸螯合剂(5 个臂/2 个研究)、抗 apoB 寡核苷酸(2 个臂/2 个研究)、联合治疗(8 个臂/6 个研究)、抗糖尿病药物(5 个臂/4 个研究)和其他治疗(5 个臂/2 个研究)。降脂药物治疗后,除两项研究外,所有研究的平均 LDL-P 均降低。在一些他汀类药物研究中,LDL-P 的降低百分比小于 LDL-C 的降低百分比,当报告 LDL-P 和 apoB 时,报告了可比的变化。

结论

本系统评价的研究水平数据表明,不同的降脂药物可能导致 LDL-P 和 LDL-C 之间的不一致,因此,仅根据胆固醇目标的实现来确定 LDL 降低治疗可能会导致治疗差距。因此,使用 LDL-P 监测降脂治疗,特别是他汀类药物,可以更准确地评估残余心血管风险。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ab03/3777154/ce4921b9656c/10557_2013_6477_Fig1_HTML.jpg

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