Cellular senescence mediates doxorubicin chemotherapy-induced vascular endothelial dysfunction: translational evidence of prevention with senolytic treatment

Oct 27, 2025American journal of physiology. Heart and circulatory physiology

Cell aging causes blood vessel damage from doxorubicin chemotherapy and may be prevented by drugs that remove aged cells

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Abstract

Doxorubicin (Doxo) treatment reduced peak endothelial-dependent dilation (EDD) to 75 ± 3% compared to control at 93 ± 1%.

Cellular senescence is associated with doxorubicin-induced vascular endothelial dysfunction.
Senolytic therapy using Ganciclovir (GCV) or ABT263 prevented the reduction in endothelial function following Doxo treatment.
Preserved nitric oxide availability and reduced mitochondrial oxidative stress were linked to the protective effects of senolytic therapy.
Ex vivo exposure to Doxo impaired peak EDD in human arterioles, which was improved by concurrent ABT263 treatment.

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Mechanisms underlying doxorubicin (Doxo) chemotherapy-induced vascular endothelial dysfunction are incompletely understood. This study aimed to determine the role of cellular senescence in mediating Doxo-induced vascular endothelial dysfunction and the influence of senolytic therapy as a therapeutic strategy to mitigate endothelial dysfunction with Doxo. Endothelial function [carotid artery endothelium-dependent dilation (EDD) to increasing concentrations of acetylcholine] and associated mechanisms were assessed in young adult p16-3MR mice [which allow for genetic-based clearance of senescent cells with ganciclovir (GCV)] injected with Doxo and subsequently treated with GCV or ABT263 (senolytic). We also assessed the influence of Doxo and ABT263 ex vivo on EDD to increase flow in human arterioles. Lower peak EDD with Doxo (75 ± 3% vs. control, 93 ± 1%;< 0.05) was prevented with GCV (94 ± 1%;< 0.05) and ABT263 (95 ± 2%;< 0.05) treatment, which was mediated by preserved nitric oxide bioavailability and prevention of excess mitochondrial oxidative stress. In human arterioles, ex vivo Doxo exposure impaired peak EDD (Doxo, 32 ± 10% vs. Control, 94 ± 2%;< 0.05), which was prevented with concomitant incubation of Doxo with ABT263 (82 ± 7%;< 0.05 vs. Doxo alone;= 0.63 vs. Control). We provide translational evidence that cellular senescence contributes to Doxo-induced vascular endothelial dysfunction and that senolytics hold promise for preserving vascular endothelial function following Doxo exposure.We demonstrate that cellular senescence contributes to doxorubicin-related vascular endothelial dysfunction and establishes efficacy for the use of senolytic therapy to improve vascular function following doxorubicin administration. Mechanistically, we found that cellular senescence reduced NO bioavailability and promoted excessive production of vascular mitochondrial superoxide-related oxidative stress, both of which were prevented with senolytic therapy. We translated these findings to humans and showed that ex vivo exposure to doxorubicin impaired arteriole endothelial function, which was prevented with senolytic exposure. P P P P P P NEW & NOTEWORTHY

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Cellular senescence mediates doxorubicin chemotherapy-induced vascular endothelial dysfunction: translational evidence of prevention with senolytic treatment

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