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脂蛋白(a)、心血管疾病和当代管理。

Lipoprotein(a), cardiovascular disease, and contemporary management.

机构信息

Office of Health Promotion and Disease Prevention, Department of Medicine, Emory University School of Medicine, Atlanta, GA.

出版信息

Mayo Clin Proc. 2013 Nov;88(11):1294-311. doi: 10.1016/j.mayocp.2013.09.003.

DOI:10.1016/j.mayocp.2013.09.003
PMID:24182706
Abstract

Elevated lipoprotein(a) (Lp[a]) is a causal genetic risk factor for cardiovascular disease. To determine if current evidence supports both screening and treatment for elevated Lp(a) in high-risk patients, an English-language search of PubMed and MEDLINE was conducted. In population studies, there is a continuous association between Lp(a) concentrations and cardiovascular risk, with synergistic effects when low-density lipoprotein (LDL) is also elevated. Candidates for Lp(a) screening include patients with a personal or family history of premature cardiovascular disease, familial hypercholesterolemia, recurrent cardiovascular events, or inadequate LDL cholesterol (LDL-C) responses to statins. Given the comparative strength of clinical evidence, reducing LDL-C to the lowest attainable value with a high-potency statin should be the primary focus of lipid-modifying therapies. If the Lp(a) level is 30 mg/dL or higher in a patient who has the aforementioned characteristics plus residual LDL-C elevations (≥70-100 mg/dL) despite maximum-potency statins or combination statin therapy, the clinician may consider adding niacin (up to 2 g/d). If, after these interventions, the patient has progressive coronary heart disease (CHD) or LDL-C levels of 160-200 mg/dL or higher, LDL apheresis should be contemplated. Although Lp(a) is a major causal risk factor for CHD, no currently available controlled studies have suggested that lowering it through either pharmacotherapy or LDL apheresis specifically and significantly reduces coronary risk. Further research is needed to (1) optimize management in order to reduce CHD risk associated with elevated Lp(a) and (2) determine what other intermediate- or high-risk groups might benefit from Lp(a) screening.

摘要

脂蛋白(a)(Lp[a])升高是心血管疾病的一个因果遗传风险因素。为了确定目前的证据是否支持对高危患者进行升高的 Lp(a)的筛查和治疗,对 PubMed 和 MEDLINE 进行了英语搜索。在人群研究中,Lp(a)浓度与心血管风险之间存在连续关联,当低密度脂蛋白(LDL)也升高时,存在协同作用。Lp(a)筛查的候选者包括有早发性心血管疾病、家族性高胆固醇血症、复发性心血管事件或他汀类药物治疗后 LDL 胆固醇(LDL-C)反应不足的个人或家族史的患者。鉴于临床证据的相对强度,用高效他汀类药物将 LDL-C 降低到可达到的最低水平应是脂质调节治疗的主要重点。如果在具有上述特征的患者中 Lp(a)水平为 30mg/dL 或更高,并且尽管使用最大剂量的他汀类药物或联合他汀类药物治疗后 LDL-C 仍升高(≥70-100mg/dL),临床医生可以考虑添加烟酸(高达 2g/d)。如果在这些干预措施之后,患者有进行性冠心病(CHD)或 LDL-C 水平为 160-200mg/dL 或更高,则应考虑 LDL 血浆置换。尽管 Lp(a)是 CHD 的主要因果风险因素,但目前尚无对照研究表明通过药物治疗或 LDL 血浆置换降低其水平可特异性和显著降低冠心病风险。需要进一步研究(1)优化管理以降低与升高的 Lp(a)相关的 CHD 风险,以及(2)确定其他中危或高危人群是否可能受益于 Lp(a)筛查。

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