Study Design and Protocol for a Randomized Controlled Trial to Assess Long-Term Efficacy and Safety of a Triple Combination of Ezetimibe, Fenofibrate, and Moderate-Intensity Statin in Patients with Type 2 Diabetes and Modifiable Cardiovascular Risk...

Overview

Journal Endocrinol Metab (Seoul)

Specialty Endocrinology

Date 2024 Aug 22

PMID 39174014

Authors

Nam Hoon Kim

Juneyoung Lee

Suk Chon

Jae Myung Yu

In-Kyung Jeong

Soo Lim

Won Jun Kim

Keeho Song

Ho Chan Cho

Hea Min Yu

Kyoung-Ah Kim

Sang Soo Kim

Soon Hee Lee

Chong Hwa Kim

Soo Heon Kwak

Yong-Ho Lee

Choon Hee Chung

Sihoon Lee

Heung Yong Jin

Jae Hyuk Lee

Gwanpyo Koh

Sang-Yong Kim

Jaetaek Kim

Ju Hee Lee

Tae Nyun Kim

Hyun Jeong Jeon

Ji Hyun Lee

Jae-Han Jeon

Hye Jin Yoo

Hee Kyung Kim

Hyeong-Kyu Park

Il Seong Nam-Goong

Seongbin Hong

Chul Woo Ahn

Ji Hee Yu

Jong Heon Park

Keun-Gyu Park

Chan Ho Park

Kyong Hye Joung

Ohk-Hyun Ryu

Keun Yong Park

Eun-Gyoung Hong

Bong-Soo Cha

Kyu Chang Won

Yoon-Sok Chung

Sin Gon Kim

Affiliations

Soon will be listed here.

Abstract

Backgruound: Atherogenic dyslipidemia, which is frequently associated with type 2 diabetes (T2D) and insulin resistance, contributes to the development of vascular complications. Statin therapy is the primary approach to dyslipidemia management in T2D, however, the role of non-statin therapy remains unclear. Ezetimibe reduces cholesterol burden by inhibiting intestinal cholesterol absorption. Fibrates lower triglyceride levels and increase high-density lipoprotein cholesterol (HDL-C) levels via peroxisome proliferator- activated receptor alpha agonism. Therefore, when combined, these drugs effectively lower non-HDL-C levels. Despite this, few clinical trials have specifically targeted non-HDL-C, and the efficacy of triple combination therapies, including statins, ezetimibe, and fibrates, has yet to be determined.

Methods: This is a multicenter, prospective, randomized, open-label, active-comparator controlled trial involving 3,958 eligible participants with T2D, cardiovascular risk factors, and elevated non-HDL-C (≥100 mg/dL). Participants, already on moderate-intensity statins, will be randomly assigned to either Ezefeno (ezetimibe/fenofibrate) addition or statin dose-escalation. The primary end point is the development of a composite of major adverse cardiovascular and diabetic microvascular events over 48 months.

Conclusion: This trial aims to assess whether combining statins, ezetimibe, and fenofibrate is as effective as, or possibly superior to, statin monotherapy intensification in lowering cardiovascular and microvascular disease risk for patients with T2D. This could propose a novel therapeutic approach for managing dyslipidemia in T2D.

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