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G. Schwartz, M. Szarek, Deepak L. Bhatt, V. Bittner, M. Bujas‐Bobanovic, R. Díaz, S. Fazio, Z. Fras, S. Goodman, R. Harrington, J. Jukema, G. Manvelian, R. Pordy, K. Ray, M. Scemama, H. White, P. Steg, Gregory G Gabriel Deepak L Vera A Rafael Shaun G Robert A Schwartz Steg Bhatt Bittner Diaz Goodman Harringto, G. Schwartz, G. Steg, Deepak L. Bhatt, V. Bittner, R. Diaz, S. Goodman, R. Harrington, J. Jukema, M. Szarek, H. White, A. Zeiher, P. Tricoci, M. Roe, K. Mahaffey, J. Edelberg, C. Hanotin, G. Lecorps, A. Moryusef, R. Pordy, W. Sasiela, J. Tamby, P. Aylward, H. Drexel, P. Sinnaeve, M. Dilić, R. Lopes, N. Gotcheva, Juan Carlos Prieto, Huo Yong, P. López-Jaramillo, I. Pećin, Željko Reiner, P. Ostadal, S. Poulsen, M. Viigimaa, M. Nieminen, N. Danchin, V. Chumburidze, Nikolaus Marx, E. Liberopoulos, P. Valdovinos, H. Tse, R. Kiss, D. Xavier, D. Zahger, M. Valgimigli, T. Kimura, H. Kim, Sang-Hyun Kim, A. Erglis, A. Laucevičius, S. Kedev, K. 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Lutchmedial, J. Rodés‐Cabau, Hussein Fadlallah, David J. Cleveland, T. Huynh, I. Bata, Adnan Hameed, Cristian Pincetti, S. Potthoff, Juan Carlos Prieto, M. Acevedo, Arnoldo Aguirre, M. Véjar, Mario Yañez, G. Araneda, M. Fernandez, Luis Perez, P. Varleta, F. Florenzano, Laura Huidobro, C. Raffo, C. Olivares, Leonardo Nahuelpan, H. Montecinos, Jiyan Chen, Yugang Dong, Weijian Huang, Jianzhong Wang, Shi'An Huang, Zhuhua Yao, Xiang Li, Lan Cui, Wenhua Lin, Yuemin Sun, Jingfeng Wang, Jian-ping Li, Xuelian Zhang, Hong Zhu, Dandan Chen, Lan Huang, Shaohong Dong, G. Su, Biao Xu, Xi Su, Xiaoshu Cheng, Jinxiu Lin, Wenxia Zong, Huanming Li, Yi Feng, Dingli Xu, Xinchun Yang, Yuannan Ke, X. Lin, Zheng Zhang, Zeqi Zheng, Zhurong Luo, Yundai Chen, Chunhua Ding, Yi Zhong, Yang Zheng, Xiaodong Li, Daoquan Peng, Shu-Lian Zhao, Y. Li, Xuebo Liu, Meng Wei, Shao-Kang Liu, Yihua Yu, B. Qu, Weihong Jiang, Yujie Zhou, Xingsheng Zhao, Zuyi Yuan, Ying Guo, Xiping Xu, Xubo Shi, J. Ge, G. Fu, F. Bai, Weiyi Fang, Xiling Shou, Xiangjun Yang, Jian'An Wang, Meixiang Xiang, Yingxian Sun, Q. Lu, Ruiyan Zhang, Jianhua Zhu, Yizhou Xu, Zhongcai Fan, Tianchang Li, Chun Wu, Nicolas Jaramillo, G. Vallejo, Diana C. Botía, R. Lopez, D. M. D. de Salazar, Alberto J Cadena Bonfanti, Carlos Cotes Aroca, Juan Diego Higuera, Marco Blanquicett, Sandra I Barrera Silva, H. G. Lozada, Julian A Coronel Arroyo, Jose L Accini Mendoza, Ricardo L Fernandez Ruiz, Alvaro M Quintero Ossa, Fernando G Manzur Jatin, Arístides Sotomayor Herazo, Jeffrey Castellanos Parada, Rafael Suarez Arambula, Miguel A Triana, Angela M Fernandez Trujillo, M. Strozzi, S. Car, M. Jerić, D. Miličić, M. L. Benčić, H. Pintarić, Đeiti Prvulović, J. Šikić, V. Peršić, D. Mileta, K. Štambuk, Z. Babić, Vjekoslav Tomulić, Josip Lukenda, Stanka Mejic-Krstulovic, B. Starčević, J. Špinar, D. Horák, Z. Velicka, J. Šťásek, David Alan, Vilma Machova, A. Linhart, V. Novotný, Vladimír Kaučák, R. Rokyta, R. Náplava, Z. Coufal, V. Adámková, I. Podpera, J. Žižka
10 5. 3. 2023.

Transiently achieved very low low-density lipoprotein cholesterol levels by statin and alirocumab after acute coronary syndrome are associated with cardiovascular risk reduction: the ODYSSEY OUTCOMES trial

Abstract Aims Long-term, placebo-controlled cholesterol-lowering trials have demonstrated legacy effects (clinical benefits that persist or emerge after trial end). It is unknown whether legacy effects follow a short period of very low low-density lipoprotein cholesterol (LDL-C) levels achieved with statin plus proprotein convertase subtilisin/kexin type 9 (PCSK9) inhibitor. Methods and results In 18 924 patients with recent acute coronary syndrome, the ODYSSEY OUTCOMES trial compared the PCSK9 inhibitor alirocumab with placebo, each added to high-intensity or maximum-tolerated statin therapy. Patients with two consecutive LDL-C levels <0.39 mmol/L (15 mg/dL) on alirocumab had blinded placebo substitution for the remainder of the trial with continued statin treatment. In post hoc analyses, major adverse cardiovascular events (MACE) in these patients were compared to MACE in propensity score–matched patients from the placebo group with similar baseline characteristics and study medication adherence. In the alirocumab group, 730 patients had blinded placebo substitution at a median of 8.3 months from randomization, after a median of 6.0 months with LDL-C <0.39 mmol/L. They were matched to 1460 placebo patients. Both groups had lower baseline LDL-C and lipoprotein(a) and better study medication adherence than those of the overall cohort. Over a median follow-up of 2.8 years, MACE occurred in 47 (6.4%) alirocumab patients with limited-duration, very low achieved LDL-C vs. 122 (8.4%) matched placebo patients (treatment hazard ratio 0.72; 95% confidence interval 0.51, 0.997; P = 0.047). Conclusion A short period of LDL-C levels <0.39 mmol/L achieved with statin and alirocumab, followed by statin monotherapy, was associated with a lower risk of MACE than statin monotherapy throughout the observation period. Clinical benefit persisted for several years. Trial registration ClinicalTrials.gov NCT01663402


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