Disruption of circadian rhythm by alternating light-dark cycles aggravates atherosclerosis development in APOE*3-Leiden.CETP mice.

Maaike Schilperoort,Ko Willems Van Dijk,Esther Lutgens,Janine M Van Gils,Johanna H Meijer,Teun Guichelaar,Noortje A M Smits,Nienke R Biermasz,Tom Deboer,Margreet R De Vries,Rosa Van Den Berg,Lotte Koemans,Sander Kooijman,Debbie Van Baarle,Laura A Bosmans,Dianne Vreeken,Martijn E.t Dollé ,Jimmy F.p Berbée ,Patrick C.n Rensen ,Linda W M Van Kerkhof ,Bram Van Os

doi:10.1111/jpi.12614

Abstract

Disruption of circadian rhythm by means of shift work has been associated with cardiovascular disease in humans. However, causality and underlying mechanisms have not yet been established. In this study, we exposed hyperlipidemic APOE*3‐Leiden.CETP mice to either regular light‐dark cycles, weekly 6 hours phase advances or delays, or weekly alternating light‐dark cycles (12 hours shifts), as a well‐established model for shift work. We found that mice exposed to 15 weeks of alternating light‐dark cycles displayed a striking increase in atherosclerosis, with an approximately twofold increase in lesion size and severity, while mice exposed to phase advances and delays showed a milder circadian disruption and no significant effect on atherosclerosis development. We observed a higher lesion macrophage content in mice exposed to alternating light‐dark cycles without obvious changes in plasma lipids, suggesting involvement of the immune system. Moreover, while no changes in the number or activation status of circulating monocytes and other immune cells were observed, we identified increased markers for inflammation, oxidative stress, and chemoattraction in the vessel wall. Altogether, this is the first study to show that circadian disruption by shifting light‐dark cycles directly aggravates atherosclerosis development.

Highlights

Epidemiological studies have repeatedly shown associations between disturbance of biological clock function, responsible for generating circadian rhythms, and metabolic disorders such as obesity, type 2 diabetes, and cardiovascular disease (CVD).[1,2,3] Already in 1949, a Scandinavian observational study among factory workers reported an association between shift work and cardiovascular mortality[4] Longitudinal studies indicate that shift work is a risk factor for cardiovascular events, including hard end‐points like ischemic stroke and myocardial infarction[5,6] the underlying mechanisms remained elusive
We aimed to investigate whether mistimed light exposure has an effect on atherosclerosis development
A complete reversal of the light and dark cycle (12 hours shifts) resulted in the strongest lesion progression, with an approximately twofold increase in atherosclerotic lesion size and severity. This demonstrates a causal relationship between mistimed light exposure and atherosclerosis

Summary

Funding information

Rijksinstituut voor Volksgezondheid en Milieu, Grant/Award Number: S/133800/01; Netherlands Ministry of Social Affairs and Employment, Grant/Award Number: KV 110016; Nederlandse Organisatie voor Wetenschappelijk Onderzoek, Grant/Award Number: 016.136.125 ; Hartstichting, Grant/Award Number: 2013T127 and

| INTRODUCTION

| MATERIALS AND METHODS

| RESULTS

| DISCUSSION

Findings

CONFLICT OF INTEREST