Aging Is Associated With Organ-Specific Alterations in the Level and Expression Pattern of von Willebrand Factor

Parnian Alavi; Radya Yousef Abdualla; Douglas Brown; Anahita Mojiri; Jayan Nagendran; John Lewis; Stephane L Bourque; Nadia Jahroudi

doi:10.1161/ATVBAHA.123.319255

Aging Is Associated With Organ-Specific Alterations in the Level and Expression Pattern of von Willebrand Factor

Arterioscler Thromb Vasc Biol. 2023 Nov;43(11):2183-2196. doi: 10.1161/ATVBAHA.123.319255. Epub 2023 Sep 21.

Authors

Parnian Alavi¹, Radya Yousef Abdualla¹, Douglas Brown², Anahita Mojiri^{1

3}, Jayan Nagendran⁴, John Lewis², Stephane L Bourque⁵, Nadia Jahroudi¹

Affiliations

¹ Departments of Medicine (P.A., R.Y.A., A.M., N.J.), University of Alberta, Edmonton, Canada.
² Oncology (D.B., J.L.), University of Alberta, Edmonton, Canada.
³ Now with Department of Cardiovascular Sciences, Houston Methodist Research Institute, TX (A.M.).
⁴ Surgery (J.N.), University of Alberta, Edmonton, Canada.
⁵ Anesthesiology and Pain Medicine (S.L.B.), University of Alberta, Edmonton, Canada.

PMID: 37732483
DOI: 10.1161/ATVBAHA.123.319255

Abstract

Background: VWF (von Willebrand factor) is an endothelial-specific procoagulant protein with a major role in thrombosis. Aging is associated with increased circulating levels of VWF, which presents a risk factor for thrombus formation.

Methods: Circulating plasma, cellular protein, and mRNA levels of VWF were determined and compared in young and aged mice. Major organs were subjected to immunofluorescence analyses to determine the vascular pattern of VWF expression and the presence of platelet aggregates. An in vitro model of aging, using extended culture time of endothelial cells, was used to explore the mechanism of age-associated increased VWF levels.

Results: Increased circulating plasma levels of VWF with elevated levels of larger multimers, indicative of VWF functional activity, were observed in aged mice. VWF mRNA and cellular protein levels were significantly increased in the brains, lungs, and livers but not in the kidneys and hearts of aged mice. Higher proportion of small vessels in brains, lungs, and livers of aged mice exhibited VWF expression compared with young, and this was concomitant with increased platelet aggregate formation. Prolonged culture of endothelial cells resulted in increased cell senescence that correlated with increased VWF expression; VWF expression was specifically detected in senescent cultured endothelial cells and abolished in response to p53 knockdown. A significantly higher proportion of VWF expressing endothelial cells in vivo exhibited senescence markers SA-β-Gal (senescence-associated β-galactosidase) and p53 in aged mouse brains compared with that of the young.

Conclusions: Aging elicits a heterogenic response in endothelial cells with regard to VWF expression, leading to organ-specific increase in VWF levels and alterations in vascular tree pattern of expression. This is concomitant with increased platelet aggregate formation. The age-associated increase in VWF expression may be modulated through the process of cell senescence, and p53 transcription factor contributes to its regulation.

Keywords: aging; endothelial cells; gene expression; platelet aggregation; risk factors; von Willebrand factor.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Aging / genetics
Animals
Endothelial Cells / metabolism
Mice
RNA, Messenger / metabolism
Thrombosis* / genetics
Thrombosis* / metabolism
Tumor Suppressor Protein p53 / metabolism
von Willebrand Diseases*
von Willebrand Factor / genetics
von Willebrand Factor / metabolism

Substances

von Willebrand Factor
Tumor Suppressor Protein p53
RNA, Messenger