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Dr. Ahmed Mahmoud Bendary :: Publications:

Title:
Egyptian Association of Vascular Biology and Atherosclerosis (EAVA) consensus on the usage of proprotein convertase subtilisin/kexin type 9 (PCSK9) inhibitors
Authors: Ashraf Reda, Ahmed Shawky Elserafy, Elsayed Farag, Tamer Mostafa, Nabil Farag, Atef Elbahry, Osama Sanad, Ahmed Bendary, Ahmed Elkersh, Mohammed Selim, Morad Beshay & Hazem Khamis
Year: 2020
Keywords: Egypt, Dyslipidemia, PCSK-9
Journal: The Egyptian Heart Journal
Volume: 72
Issue: Not Available
Pages: Not Available
Publisher: Springer Nature
Local/International: International
Paper Link:
Full paper Ahmed Mahmoud Bendary_TEHJ.pdf
Supplementary materials Not Available
Abstract:

Background The current expert view of the PCSK9 inhibitors’ use in Egypt is still ambiguous. Main body Hyperlipidemia is an important, if not the most important, risk factor for the occurrence of atherosclerosis worldwide. Egypt is the most populous country in the Middle East and North Africa and has > 15% of the cardiovascular deaths in the region. The burden of dyslipidemia as seen in the recently published CardioRisk project conducted throughout Egypt shows a high prevalence of dyslipidemia as a risk factor that is still reaching up to 71% in female participants. Reaching the targets for LDL lowering, and thus control of hyperlipidemia, is quite often very difficult especially with the update of the last ESC guidelines. With the advent of PCSK9 inhibitors, the control rate of patients, reduction of cardiac major adverse events, and mortality have been improved. However, Egypt is not considered a rich country on the grounds of annual income, and this raises a concern on which patients would benefit from these expensive medications. Revising the randomized control trials, we analyzed the data that would enable us to control LDL in those patients, at risk, to obtain simple clear indications for the use of these rather expensive medications. Conclusion We recommend the use of PCSK9 inhibitors in addition to statins ± ezetimibe in patients with ASCVD, by definition at very high risk; patients with ASCVD at very high risk who do not tolerate appropriate doses of at least three statins; and familial hypercholesterolaemia patients with clinically diagnosed ASCVD, at very high cardiovascular risk.

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