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心血管疾病与胰腺炎防治中的高甘油三酯血症的临床管理。

Clinical Management of Hypertriglyceridemia in the Prevention of Cardiovascular Disease and Pancreatitis.

机构信息

Perelman School of Medicine, University of Pennsylvania, Philadelphia, PA, USA.

Diabetes & Endocrine Associates of Hunterdon, Flemington, NJ, USA.

出版信息

Curr Atheroscler Rep. 2021 Sep 13;23(11):72. doi: 10.1007/s11883-021-00962-z.

Abstract

PURPOSE OF REVIEW

Hypertriglyceridemia (HTG) is common and is a significant contributor to atherosclerosis and pancreatitis risk. Specific HTG treatments have had variable success in reducing atherosclerosis risk. Novel therapies for severe HTG treatment and pancreatitis risk reduction are likely to be available soon. These novel therapies are expected to have broader applications for more moderate HTG and atherosclerosis risk reduction as well.

RECENT FINDINGS

NHANES 2012 data has confirmed a reduction in average triglyceride (TG) levels in the US population. Dietary modification and weight reduction when needed remain the core treatment elements for all individuals with HTG, while statin therapy is a foundational pharmacologic care for atherosclerotic cardiovascular disease (ASCVD) event risk reduction. In addition, the REDUCE-IT study provides evidence for additional benefit from the use of high-dose icosapent ethyl (IPE) on top of background medical therapy in adults with moderate HTG and ASCVD or type 2 diabetes mellitus (T2D) and additional ASCVD risk factors. However, treatment with eicosapentaenoic acid (EPA) combined with docosahexanoic acid (DHA) did not reduce ASCVD in a similar population studied in the STRENGTH trial. Furthermore, novel therapeutics targeting PPAR-ɑ, as well as ApoC-III and AngPTL3, effectively lower TG levels in individuals with moderate and severe HTG, respectively. These treatments may have applicability for reducing risk from ASCVD among individuals with chylomicronemia; in addition, ApoC-III and AngPTL3 treatments may have a role in treating individuals with the rare monogenic familial chylomicronemia syndrome (FCS) at risk for acute pancreatitis (AP). Residual ASCVD risk in individuals treated with contemporary care may be due in part to non-LDL lipid abnormalities including HTG. The findings from REDUCE-IT, but not STRENGTH, confirm that consumption of high-dose EPA may reduce ASCVD risk, while combination therapy of EPA plus DHA does not reduce ASCVD in a similar population. TG lowering likely reduces ASCVD risk in individuals with HTG, but ASCVD risk is multifactorial; the added benefit of IPE to contemporary preventive therapy is the consequence of differential non-TG biologic properties between the two fatty acids. Acute pancreatitis is more difficult to study prospectively since it is less common; however, TG lowering is likely critical for the care of at-risk individuals. Additional benefit from novel therapy that has an impact on this otherwise refractory condition is anticipated.

摘要

目的综述

高甘油三酯血症(HTG)很常见,是动脉粥样硬化和胰腺炎风险的重要因素。特定的 HTG 治疗方法在降低动脉粥样硬化风险方面取得了不同程度的成功。用于严重 HTG 治疗和降低胰腺炎风险的新型疗法可能很快就会问世。这些新型疗法预计也将更广泛地应用于更中度的 HTG 和降低动脉粥样硬化风险。

最近的发现

NHANES 2012 数据证实美国人群的平均甘油三酯(TG)水平有所降低。饮食调整和需要时的体重减轻仍然是所有 HTG 患者的核心治疗要素,而他汀类药物治疗是降低动脉粥样硬化性心血管疾病(ASCVD)事件风险的基础药物治疗。此外,REDUCE-IT 研究为在中度 HTG 且有 ASCVD 或 2 型糖尿病(T2D)和其他 ASCVD 危险因素的成年人中,在基础医学治疗的基础上使用高剂量icosapent ethyl(IPE)带来的额外获益提供了证据。然而,在 STRENGTH 试验中研究的类似人群中,EPA 与 DHA 联合治疗并未降低 ASCVD 风险。此外,针对 PPAR-ɑ 以及 ApoC-III 和 AngPTL3 的新型治疗方法可分别有效降低中度和重度 HTG 个体的 TG 水平。这些治疗方法可能适用于降低乳糜微粒血症个体的 ASCVD 风险;此外,ApoC-III 和 AngPTL3 治疗方法可能在治疗有急性胰腺炎(AP)风险的罕见单基因家族性乳糜微粒血症综合征(FCS)个体方面发挥作用。接受当代治疗的个体仍存在 ASCVD 残留风险,部分原因是非 LDL 脂质异常包括 HTG。REDUCE-IT 的研究结果,但 STRENGTH 研究结果没有,证实高剂量 EPA 的摄入可能降低 ASCVD 风险,而 EPA 加 DHA 的联合治疗并不能降低类似人群的 ASCVD 风险。降低 TG 可能会降低 HTG 个体的 ASCVD 风险,但 ASCVD 风险是多因素的;IPE 对当代预防治疗的额外获益是两种脂肪酸在非 TG 生物学特性上的差异所致。由于胰腺炎不太常见,前瞻性研究更具挑战性;然而,降低 TG 对于高危人群的护理可能至关重要。预计会有新型疗法对这种难治性疾病产生额外的获益。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9534/8436578/a8080bf6730d/11883_2021_962_Fig1_HTML.jpg

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