预防乳腺癌治疗心脏毒性的心脏保护策略系统综述

Sidhi Laksono, Nathania Purnomo, Hillary Kusharsamita
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引用次数: 0

摘要

背景:乳腺癌是全球妇女中发病率最高的恶性肿瘤,每年平均有 210 万人罹患乳腺癌。此外,多项研究表明,乳腺癌通常采用化疗药物和靶向疗法进行治疗,但据报道,这些治疗方法会对心血管系统产生副作用。这表明,有必要开发新的有效策略来预防相关副作用。因此,本系统综述旨在了解乳腺癌患者接受化疗或靶向治疗时预防心脏毒性的心脏保护策略。研究方法使用在线数据库 PubMed 进行数据收集,关键词为((心脏保护)和(乳腺癌治疗)和(心脏毒性)或(心脏功能障碍))。通过初步搜索,共获得 150 篇研究,不符合资格标准的文章被排除在外。此外,还对这些文章进行了全文阅读,最终有 19 篇文章被纳入本系统综述。结果共有 11 项研究评估了心脏保护药物对蒽环类药物(ANT)的影响,9 项研究评估了曲妥珠单抗。结果显示,8项研究使用了β-受体阻滞剂(BB)作为心脏保护策略,1项、1项、3项、2项、1项、1项和1项研究分别使用了血管紧张素受体阻滞剂(ARB)、ARB+β-受体阻滞剂、ACE-抑制剂(ACE-I)+β-受体阻滞剂、ACE-I/ARB/BB、螺内酯、他汀类药物和右雷佐生(DZR)。在大量报告中,联合使用 RAAS 抑制剂和 Beta 受体阻滞剂可降低 CTRCD 的风险。此外,在小型研究中,与对照组相比,螺内酯、他汀类药物和 DZR 可减轻 LVEF 的下降。结论:根据研究结果,化疗会降低左心室射血分数(LVEF)并诱发心力衰竭。此外,综述还显示,联合使用肾素血管紧张素-醛固酮系统(RAAS)抑制剂和贝塔受体阻滞剂可降低 CTRCD。今后还需要在更大的范围内进行研究,以调查他汀类药物、螺内酯、运动和 DZR 等其他策略的疗效。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A Systematic Review on Cardioprotection Strategies to Prevent Breast Cancer Therapy Cardiotoxicity
Background: Breast cancer is the most prevalent malignancy among women on a global scale, affecting an average of 2.1 million individuals annually. In addition, several studies have shown that it is often treated using chemotherapy drugs and targeted therapy, but these treatment methods have been reported to have side effects on the cardiovascular system. This indicates that there is a need to develop new and effective strategies to prevent the associated side effects. Therefore, this systematic review aims to obtain cardioprotection strategies to prevent cardiotoxicity in breast cancer patients receiving chemotherapy or targeted therapy. Methods: Data collection was carried out using the online database PubMed with keywords ((cardioprotection) AND (breast cancer therapy) AND (cardiotoxic) OR (Cardiac dysfunction.)) From the initial search, a total of 150 studies were obtained, while articles that did not meet the eligibility criteria were excluded. Furthermore, the articles were reviewed using full-text reading, leading to the inclusion of nineteen in this systematic review. Results: A total of eleven studies evaluated the effect of cardio-protective drugs on Anthracycline (ANT), and nine assessed Trastuzumab. The results showed that eight studies used Beta-blocker (BB) as cardio-protective strategies, while one, one, three, two, one, one, and one utilized Angiotensin receptor blockers (ARB), ARB + Beta-blocker, ACE-inhibitor (ACE-I) + Beta-blocker, ACE-I/ARB/BB, spironolactone, statin, and Dexrazoxane (DZR), respectively. In large reports, the risk of CTRCD was reduced by the use of a combination of RAAS inhibitors and Beta-blockers. Furthermore, spironolactone, statins, and DZR mitigated the decrease in LVEF compared to the control group in small studies. Conclusions: Based on the results, chemotherapy decreased left ventricular ejection fraction (LVEF) and induced heart failure. Furthermore, the review showed that a combination of reninangiotensin-aldosterone system (RAAS) inhibitors and Beta-blockers reduced CTRCD. Future studies in larger settings were needed to investigate the efficacy of other strategies, such as statins, Spironolactone, exercise, and DZR.
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