Do Patients With Arterial Occlusive Disease of Different Etiologies Benefit Equally From Cilostazol?

IF 0.8 4区 医学 Q4 CARDIAC & CARDIOVASCULAR SYSTEMS Texas Heart Institute journal Pub Date : 2023-01-01 DOI:10.14503/THIJ-21-7747
Burak Can Depboylu, Serkan Yazman, Bugra Harmandar, Muruvvet Funda Tetik, Hande Istar, Kadir Arslan, Gokhan Ilhan
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引用次数: 1

Abstract

Background: Cilostazol is a guideline-recommended drug that improves intermittent claudication and quality of life in patients with chronic atherosclerotic peripheral arterial disease. The drug is used for most etiologies of arterial occlusive diseases in clinical practice. This study aimed to evaluate whether patients benefit equally from cilostazol regardless of etiology.

Methods: Patients on cilostazol were divided into 4 groups according to arterial occlusive disease etiology: (1) atherosclerosis, (2) diabetic angiopathy, (3) embolism/thrombosis, and (4) Buerger disease. Patients' maximum walking distance, ankle-brachial index score and distal tissue oxygen saturation (Sto2), clinical improvement onset time, ability to reach maximum benefit time, vascular surgeries, and wounds were compared before they started cilostazol and after 12 months. Results were evaluated at a statistical significance of P < .05.

Results: In 194 patients, 307 target extremities were evaluated in the 4 disease groups. After cilostazol use, maximum walking distance, ankle-brachial index score, and distal Sto2 increased significantly in all groups (P < .001), but distal Sto2 in the diabetic angiopathy and Buerger disease groups was significantly lower than in the atherosclerosis group (P < .001). Ankle-brachial index and distal Sto2 differences in the Buerger disease group were significantly lower (both P < .001). The vascular surgery counts decreased significantly in the atherosclerosis and embolism/thrombosis groups (P = .019 and P = .004, respectively).

Conclusion: Patients with nonatherosclerotic arterial occlusive disease also benefit from cilostazol, but patients with Buerger disease or diabetic angiopathy seem to benefit less. Combining cilostazol with anticoagulant or antiaggregant agents and closer monitoring of these patients may produce better results.

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不同病因的动脉闭塞性疾病患者服用西洛他唑是否同样受益?
背景:西洛他唑是一种指南推荐的药物,可改善慢性动脉粥样硬化性外周动脉疾病患者的间歇性跛行和生活质量。在临床实践中,该药用于大多数动脉闭塞性疾病的病因。本研究旨在评估患者是否能从西洛他唑中获得相同的益处,而不考虑病因。方法:将西洛他唑患者根据动脉闭塞疾病病因分为4组:(1)动脉粥样硬化组,(2)糖尿病血管病变组,(3)栓塞/血栓形成组,(4)伯格病组。比较患者在使用西洛他唑前和12个月后的最大步行距离、踝-肱指数评分和远端组织氧饱和度(Sto2)、临床改善开始时间、达到最大受益时间的能力、血管手术和伤口。评价结果P < 0.05,差异有统计学意义。结果:194例患者共评价了4组患者307条靶肢。使用西洛他唑后,各组患者最大步行距离、踝肱指数评分、远端Sto2均显著升高(P < 0.001),但糖尿病血管病组和伯格病组远端Sto2显著低于动脉粥样硬化组(P < 0.001)。berger病组踝肱指数和远端Sto2差异均显著降低(P < 0.001)。动脉粥样硬化组和栓塞/血栓组血管手术计数明显下降(P = 0.019和P = 0.004)。结论:非动脉粥样硬化性动脉闭塞性疾病患者也受益于西洛他唑,但buberger病或糖尿病血管病变患者似乎获益较少。西洛他唑与抗凝或抗凝药物联合使用并密切监测这些患者可能会产生更好的结果。
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来源期刊
Texas Heart Institute journal
Texas Heart Institute journal 医学-心血管系统
CiteScore
1.10
自引率
11.10%
发文量
131
审稿时长
2 months
期刊介绍: For more than 45 years, the Texas Heart Institute Journal has been published by the Texas Heart Institute as part of its medical education program. Our bimonthly peer-reviewed journal enjoys a global audience of physicians, scientists, and healthcare professionals who are contributing to the prevention, diagnosis, and treatment of cardiovascular disease. The Journal was printed under the name of Cardiovascular Diseases from 1974 through 1981 (ISSN 0093-3546). The name was changed to Texas Heart Institute Journal in 1982 and was printed through 2013 (ISSN 0730-2347). In 2014, the Journal moved to online-only publication. It is indexed by Index Medicus/MEDLINE and by other indexing and abstracting services worldwide. Our full archive is available at PubMed Central. The Journal invites authors to submit these article types for review: -Clinical Investigations- Laboratory Investigations- Reviews- Techniques- Coronary Anomalies- History of Medicine- Case Reports/Case Series (Submission Fee: $70.00 USD)- Images in Cardiovascular Medicine (Submission Fee: $35.00 USD)- Guest Editorials- Peabody’s Corner- Letters to the Editor
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