Biomechanical factors in atherosclerosis: mechanisms and clinical implications

Kwak, Brenda R.; Bäck, Magnus; Bochaton‐Piallat, Marie‐Luce; Caligiuri, Giuseppina; Daemen, Mat J.A.P.; Davies, Peter F.; Hoefer, Imo E.; Holvoet, Paul; Jo, Hanjoong; Krams, Rob; Lehoux, Stéphanie; Monaco, Claudia; Steffens, Sabine; Virmani, Renu; Weber, Christian; Wentzel, Jolanda J.; Evans, Paul C.

doi:10.1093/eurheartj/ehu353

Cited by 395 publications

(338 citation statements)

References 153 publications

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“…The underlying mechanism has remained elusive because ivabradine-targets have not been identified in vascular cells and ivabradine did not influence plasma lipid levels 11,13 . Given that ivabradine alters heart rate, stroke volume and coronary perfusion 22 , we tested the hypothesis that ivabradine may exert protective effects of arteries indirectly by altering hemodynamics which has been tightly linked to cardiovascular disease [15][16][17] . Our study demonstrated that ivabradine significantly altered flow in the murine aorta leading to enhanced WSS magnitude at both atheroprone and atheroprotected sites.…”

Section: Discussionmentioning

confidence: 99%

“…Indeed, although atherosclerosis is associated with systemic risk factors, such as hypercholesterolemia, it develops preferentially at branches and bends of the arterial tree that are exposed to complex patterns of blood flow 15 . Computational fluid dynamic (CFD) studies have demonstrated that the magnitude of WSS (time-averaged WSS (TAWSS) over the cardiac cycle) is lower at atherosclerosis-prone sites exposed to complex flow compared to regions that are protected 16,17 .…”

Section: Introductionmentioning

confidence: 99%

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Heart rate reduction with ivabradine promotes shear stress-dependent anti-inflammatory mechanisms in arteries

Luong¹,

Duckles²,

Schenkel³

et al. 2016

Thromb Haemost

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"Heart rate reduction with ivabradine promotes shear stress-dependent anti-inflammatory mechanisms in arteries", Thrombosis and Haemostasis, 2016: 116/1 (July) pp. [181][182][183][184][185][186][187][188][189][190]., is available online at: https://doi.org/10.1160/TH16-03-0214.eprints@whiterose.ac.uk https://eprints.whiterose.ac.uk/ Reuse Unless indicated otherwise, fulltext items are protected by copyright with all rights reserved. The copyright exception in section 29 of the Copyright, Designs and Patents Act 1988 allows the making of a single copy solely for the purpose of non-commercial research or private study within the limits of fair dealing. The publisher or other rights-holder may allow further reproduction and re-use of this version -refer to the White Rose Research Online record for this item. Where records identify the publisher as the copyright holder, users can verify any specific terms of use on the publisher's website. TakedownIf you consider content in White Rose Research Online to be in breach of UK law, please notify us by emailing eprints@whiterose.ac.uk including the URL of the record and the reason for the withdrawal request. 2 SUMMARY AimsBlood flow generates wall shear stress (WSS) which alters endothelial cell (EC) function. Low WSS promotes vascular inflammation and atherosclerosis whereas high uniform WSS is protective. Ivabradine decreases heart rate leading to altered hemodynamics. Besides its cardio-protective effects, ivabradine protects arteries from inflammation and atherosclerosis via unknown mechanisms. We hypothesised that ivabradine protects arteries by increasing WSS to reduce vascular inflammation. Methods and ResultsHypercholesterolemic mice were treated with ivabradine for 7 weeks in drinking water or remained untreated as a control. En face immunostaining demonstrated that treatment with ivabradine reduced the expression of pro-inflammatory VCAM-1 (p<0.01) and enhanced the expression of anti-inflammatory eNOS (p<0.01) at the inner curvature of the aorta. We concluded that ivabradine alters EC physiology indirectly via modulation of flow because treatment with ivabradine had no effect in ligated carotid arteries in vivo, and did not influence the basal or TNF -induced expression of inflammatory (VCAM-1, MCP-1) or protective (eNOS, HMOX1, KLF2, KLF4) genes in cultured EC. We therefore considered whether ivabradine can alter WSS which is a regulator of EC inflammatory activation. Computational fluid dynamics demonstrated that ivabradine treatment reduced heart rate by 20% and enhanced WSS in the aorta. ConclusionsIvabradine treatment altered hemodynamics in the murine aorta by increasing the magnitude of shear stress. This was accompanied by induction of eNOS and suppression of VCAM-1, whereas ivabradine did not alter EC that could not respond to flow. Thus ivabradine protects arteries by altering local mechanical conditions to trigger an anti-inflammatory response.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Heart rate reduction with ivabradine promotes shear stress-dependent anti-inflammatory mechanisms in arteries

Luong¹,

Duckles²,

Schenkel³

et al. 2016

Thromb Haemost

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“…22 This might be the consequence of local differences in the mechanical forces exerted to the artery wall and the endothelium of the coronary vascular bed, causing local differences in plaque initiation and progression. 33 In contrast to the coronary arteries, both carotid arteries are exposed to similar blood flow patterns and mechanical stress. This might result in the same pattern of plaque development and progression.…”

mentioning

confidence: 99%

18F-sodium fluoride positron emission tomography assessed microcalcifications in culprit and non-culprit human carotid plaques

Hop

Boer

Reijrink

et al. 2019

Journal of Nuclear Cardiology

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Background 18 F-NaF positron emission tomography (PET) targets microcalcifications. We compared in vitro microPET assessed 18 F-NaF uptake between culprit and non-culprit human carotid plaques. Furthermore, we compared 18 F-NaF uptake with calcification visualized on microcomputed tomography (microCT). Methods Carotid plaques from stroke patients undergoing surgery were incubated in 18 F-NaF and scanned using a microPET and a microCT scan. The average PET assessed 18 F-NaF uptake was expressed as percentage of the incubation dose per gram (%Inc/g). 18 F-NaF PET volume of interest (VOI) was compared with CT calcification VOI. Results 23 carotid plaques (17 culprit, 6 non-culprit) were included. The average 18 F-NaF uptake in culprit carotid plaques was comparable with the uptake in non-culprit carotid plaques (median 2.32 %Inc/g [IQR 1.98 to 2.81] vs. median 2.35 %Inc/g [IQR 1.77 to 3.00], P = 0.916). Only a median of 10% (IQR 4 to 25) of CT calcification VOI showed increased 18 F-NaF uptake, while merely a median of 35% (IQR 6 to 42) of 18 F-NaF PET VOI showed calcification on CT. Conclusions 18 F-NaF PET represents a different stage in the calcification process than CT. We observed a similar PET assessed 18 F-NaF uptake and pattern in culprit and non-culprit plaques of high-risk patients, indicating that this method may be of more value in early atherosclerotic stenosis development. Electronic supplementary material The online version of this article (10.1007/s12350-018-1325-5) contains supplementary material, which is available to authorized users.

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“…4 Suggested mechanisms include an increase in the magnitude and frequency of the mechanical stress imposed on the arterial wall, shortening of the atheroprotective diastolic period, and prolongation of endothelial exposure to atherogenic local hemodynamic factors. 5,6 The atherogenic microenvironment modulated by increased HR, in conjunction with the effect of systemic risk factors, promotes plaque formation and progression in atherosclerosis-prone regions.7 Reducing HR could potentially restrain the process of atherosclerosis which clearly relates to ischemia and, thus, angina.8 Ivabradine is a selective, pure HR-lowering agent that inhibits the If current in the sinoatrial node.9 Several studies have shown ivabradine to be noninferior to first-line antianginal agents, such as beta-blockers and calcium channel blockers, and superior to placebo.10-13 Ivabradine has a class IIa (level of evidence B) indication for the symptomatic treatment of chronic stable angina in patients intolerant to or inadequately controlled by beta-blockers. …”

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confidence: 99%

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confidence: 99%

Lowering Heart Rate Post Revascularization

2016

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Coronary artery disease (CAD) is responsible for 38% of cardiovascular (CV) deaths in women and 46% in men.1 Stable angina pectoris, the principle manifestation of CAD, affects close to 15% of the population aged 65 to 84 years. 2 The chronicity and the frequency of symptoms have a direct effect on quality of life (QOL); realization of subpar health conditions promotes a vicious circle of stressful stimuli that, in turn, can promote angina attacks.3 Given our aging population and the increasingly good prognosis of patients with stable CAD, this group of patients is growing.Elevated heart rate (HR) may be implicated in coronary atherosclerosis and subsequently to myocardial ischemia and angina in an independent manner. 4 Suggested mechanisms include an increase in the magnitude and frequency of the mechanical stress imposed on the arterial wall, shortening of the atheroprotective diastolic period, and prolongation of endothelial exposure to atherogenic local hemodynamic factors. 5,6 The atherogenic microenvironment modulated by increased HR, in conjunction with the effect of systemic risk factors, promotes plaque formation and progression in atherosclerosis-prone regions.7 Reducing HR could potentially restrain the process of atherosclerosis which clearly relates to ischemia and, thus, angina.8 Ivabradine is a selective, pure HR-lowering agent that inhibits the If current in the sinoatrial node.9 Several studies have shown ivabradine to be noninferior to first-line antianginal agents, such as beta-blockers and calcium channel blockers, and superior to placebo.10-13 Ivabradine has a class IIa (level of evidence B) indication for the symptomatic treatment of chronic stable angina in patients intolerant to or inadequately controlled by beta-blockers. 2In this issue of Angiology, Zarifis et al 14 evaluated the potential antianginal effect of ivabradine when coadministered with beta-blockers in 926 patients with chronic stable angina and history of coronary revascularization (coronary artery bypass graft or percutaneous coronary intervention) in a time period of 4 months. Evaluation was performed via 1 objective marker (resting HR at baseline and at 3 follow-up time points) and 2 subjective, patient-dependent markers, namely, the Canadian Cardiology Society (CCS) angina classification and QOL in means of the EuroQol-5 Dimension (EQ-5D) questionnaire. 15 The authors 14 showed that blocking the If channels and reducing HR, with the addition of ivabradine to beta-blockers therapy, decreased the number of angina events, from 2.2 + to 83.1%, P < .001). There was an overall improvement of QOL in the magnitude of previously reported larger scale ivabradine studies. 16 Another key point of the study is the high compliance with ivabradine treatment, in a noninstitutional environment, thus reflecting routine clinical practice. This could explain the efficacy in reducing angina attacks.The antianginal effects of ivabradine are dose dependent. 17Notably, in the current study, 14 only *50% of the patients received the recommended ...

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Biomechanical factors in atherosclerosis: mechanisms and clinical implications

Cited by 395 publications

References 153 publications

Heart rate reduction with ivabradine promotes shear stress-dependent anti-inflammatory mechanisms in arteries

Heart rate reduction with ivabradine promotes shear stress-dependent anti-inflammatory mechanisms in arteries

18F-sodium fluoride positron emission tomography assessed microcalcifications in culprit and non-culprit human carotid plaques

Lowering Heart Rate Post Revascularization

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