医学
流行病学
疾病
脂蛋白(a)
风险因素
人口
狭窄
内科学
脂蛋白
重症监护医学
生物信息学
心脏病学
胆固醇
环境卫生
生物
作者
Zeeshan Afzal,Huili Cao,M.A. Chaudhary,Himaja Dutt Chigurupati,Sivaram Neppala,Waleed Alruwaili,Maan Awad,Darshan Sandesara,Muzammil Siddique,Ali Farman,Fnu Zafrullah,Karthik Gonuguntla,Yasar Sattar
标识
DOI:10.1016/j.cpcardiol.2024.102586
摘要
Cardiovascular disease (CVD) remains a significant global health challenge despite advancements in prevention and treatment. Elevated Lipoprotein(a) [Lp(a)] levels have emerged as a crucial risk factor for CVD and aortic stenosis, affecting approximately 20% of the global population. Research over the last decade has established Lp(a) as an independent genetic contributor to CVD and aortic stenosis, beginning with Kare Berg's discovery in 1963. This has led to extensive exploration of its molecular structure and pathogenic roles. Despite the unknown physiological function of Lp(a), studies have shed light on its metabolism, genetics, and involvement in atherosclerosis, inflammation, and thrombosis. Epidemiological evidence highlights the link between high Lp(a) levels and increased cardiovascular morbidity and mortality. Newly emerging therapies, including pelacarsen, zerlasiran, olpasiran, muvalaplin, and lepodisiran, show promise in significantly lowering Lp(a) levels, potentially transforming the management of cardiovascular disease. However, further research is essential to assess these novel therapies' long-term efficacy and safety, heralding a new era in cardiovascular disease prevention and treatment and providing hope for at-risk patients.
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