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Current treatment of dyslipidaemia: PCSK9 inhibitors and statin intolerance.

机译:目前血脂异常的治疗:PCSK9抑制剂和他汀类药物不耐受。

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摘要

Statins are the cornerstone of the management of dyslipidaemias and prevention of cardiovascular disease. Although statins are, overall, safe and well tolerated, adverse events can occur and constitute an important barrier to maintaining long-term adherence to statin treatment. In patients who cannot tolerate statins, alternative treatments include switch to another statin, intermittent-dosage regimens and non-statin lipid-lowering medications. Nonetheless, a high proportion of statin-intolerant patients are unable to achieve recommended low-density lipoprotein (LDL) cholesterol goals, thereby resulting in substantial residual cardiovascular risk. Proprotein convertase subtilisin/kexin type 9 (PCSK9) is a protease implicated in LDL receptor degradation and plays a central role in cholesterol metabolism. In recent studies, PCSK9 inhibition by means of monoclonal antibodies achieved LDL cholesterol reductions of 50% to 70% across various patient populations and background lipid-lowering therapies, while maintaining a favourable safety profile. The efficacy and safety of the monoclonal antibodies alirocumab and evolocumab were confirmed in statin-intolerant patients, indicating that PCSK9 inhibitors represent an attractive treatment option in this challenging clinical setting. PCSK9 inhibitors recently received regulatory approval for clinical use and may be considered in properly selected patients according to current consensus documents, including patients with statin intolerance. In this review we summarise current evidence regarding diagnostic evaluation of statin-related adverse events, particularly statin-associated muscle symptoms, and we discuss current recommendations on the management of statin-intolerant patients. In view of emerging evidence of the efficacy and safety of PCSK9 inhibitors, we further discuss the role of monoclonal PCSK9 antibodies in the management of statin-intolerant hypercholesterolaemic patients.
机译:他汀类药物是控制血脂异常和预防心血管疾病的基石。尽管他汀类药物总体上是安全且耐受性良好的,但不良事件仍可能发生,并构成维持长期坚持他汀类药物治疗的重要障碍。对于不能耐受他汀类药物的患者,替代疗法包括改用另一种他汀类药物,间歇给药方案和非他汀类降脂药物。尽管如此,仍有大量不能接受他汀类药物治疗的患者无法达到推荐的低密度脂蛋白(LDL)胆固醇目标,从而导致大量残留的心血管风险。前蛋白转化酶枯草杆菌蛋白酶/ kexin 9型(PCSK9)是一种与LDL受体降解有关的蛋白酶,在胆固醇代谢中起着核心作用。在最近的研究中,通过单克隆抗体的PCSK9抑制在各种患者人群和背景降脂疗法中实现了LDL胆固醇降低50%至70%,同时保持了良好的安全性。在他汀类药物不耐受的患者中证实了单克隆抗体alirocumab和evolocumab的有效性和安全性,表明PCSK9抑制剂在这种具有挑战性的临床环境中代表了有吸引力的治疗选择。 PCSK9抑制剂最近获得了临床使用的监管批准,根据当前的共识文件,包括他汀类药物不耐受的患者,可以在适当选择的患者中考虑PCSK9抑制剂。在这篇综述中,我们总结了有关他汀类药物相关不良事件(尤其是他汀类药物相关的肌肉症状)的诊断评估的当前证据,并且我们讨论了他汀类药物耐受患者的治疗建议。鉴于PCSK9抑制剂功效和安全性的新兴证据,我们进一步讨论了单克隆PCSK9抗体在他汀类药物耐受性高胆固醇血症患者的治疗中的作用。

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