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DPP4 Inhibition Impairs Senohemostasis to Improve Plaque Stability in Atherosclerotic Mice

Overview

Overview

Journal J Clin Invest

Specialty General Medicine

Date 2023 Apr 25

PMID 37097759

Authors

Authors

Allison B Herman

Dimitrios Tsitsipatis

Carlos Anerillas

Krystyna Mazan-Mamczarz

Angelica E Carr

Jordan M Gregg

Mingyi Wang

Jing Zhang

Marc Michel

Charnae A Henry-Smith

Sophia C Harris

Rachel Munk

Jennifer L Martindale

Yulan Piao

Jinshui Fan

Julie A Mattison

Supriyo De

Kotb Abdelmohsen

Robert W Maul

Toshiko Tanaka

Ann Zenobia Moore

Megan E DeMouth

Simone Sidoli

Luigi Ferrucci

Yie Liu

Rafael de Cabo

Edward G Lakatta

Myriam Gorospe

Affiliations

Affiliations

Soon will be listed here.

Abstract

Senescent vascular smooth muscle cells (VSMCs) accumulate in the vasculature with age and tissue damage and secrete factors that promote atherosclerotic plaque vulnerability and disease. Here, we report increased levels and activity of dipeptidyl peptidase 4 (DPP4), a serine protease, in senescent VSMCs. Analysis of the conditioned media from senescent VSMCs revealed a unique senescence-associated secretory phenotype (SASP) signature comprising many complement and coagulation factors; silencing or inhibiting DPP4 reduced these factors and increased cell death. Serum samples from persons with high risk for cardiovascular disease contained high levels of DPP4-regulated complement and coagulation factors. Importantly, DPP4 inhibition reduced senescent cell burden and coagulation and improved plaque stability, while single-cell resolution of senescent VSMCs reflected the senomorphic and senolytic effects of DPP4 inhibition in murine atherosclerosis. We propose that DPP4-regulated factors could be exploited therapeutically to reduce senescent cell function, reverse senohemostasis, and improve vascular disease.

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