Circadian misalignment disrupts biomarkers of cardiovascular disease risk and promotes a hypercoagulable state

Author:

McHill Andrew W.12,Melanson Edward L.34,Wright Kenneth P.35,Depner Christopher M.6ORCID

Affiliation:

1. Sleep, Chronobiology, and Health Laboratory, School of Nursing Oregon Health & Science University Portland Oregon USA

2. Oregon Institute of Occupational Health Sciences Oregon Health & Science University Portland Oregon USA

3. Division of Endocrinology, Metabolism, and Diabetes University of Colorado Anschutz Medical Campus Aurora Colorado USA

4. Division of Geriatric Medicine University of Colorado Anschutz Medical Campus Aurora Colorado USA

5. Sleep and Chronobiology Laboratory, Department of Integrative Physiology University of Colorado Boulder Boulder Colorado USA

6. Department of Health and Kinesiology University of Utah Salt Lake City Utah USA

Abstract

AbstractThe circadian system regulates 24‐h time‐of‐day patterns of cardiovascular physiology, with circadian misalignment resulting in adverse cardiovascular risk. Although many proteins in the coagulation‐fibrinolysis axis show 24‐h time‐of‐day patterns, it is not understood if these temporal patterns are regulated by circadian or behavioral (e.g., sleep and food intake) cycles, or how circadian misalignment influences these patterns. Thus, we utilized a night shiftwork protocol to analyze circadian versus behavioral cycle regulation of 238 plasma proteins linked to cardiovascular physiology. Six healthy men aged 26.2 ± 5.6 years (mean ± SD) completed the protocol involving two baseline days with 8‐h nighttime sleep opportunities (circadian alignment), a transition to shiftwork day, followed by 2 days of simulated night shiftwork with 8‐h daytime sleep opportunities (circadian misalignment). Plasma was collected for proteomics every 4 h across 24 h during baseline and during daytime sleep and the second night shift. Cosinor analyses identified proteins with circadian or behavioral cycle‐regulated 24‐h time‐of‐day patterns. Five proteins were circadian regulated (plasminogen activator inhibitor‐1, angiopoietin‐2, insulin‐like growth factor binding protein‐4, follistatin‐related protein‐3, and endoplasmic reticulum resident protein‐29). No cardiovascular‐related proteins showed regulation by behavioral cycles. Within the coagulation pathway, circadian misalignment decreased tissue factor pathway inhibitor, increased tissue factor, and induced a 24‐h time‐of‐day pattern in coagulation factor VII (all FDR < 0.10). Such changes in protein abundance are consistent with changes observed in hypercoagulable states. Our analyses identify circadian regulation of proteins involved in cardiovascular physiology and indicate that acute circadian misalignment could promote a hypercoagulable state, possibly contributing to elevated cardiovascular disease risk among shift workers.

Funder

Sleep Research Society Foundation

National Institutes of Health

Publisher

Wiley

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