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Treatment of advanced atherosclerotic mice with ABT-263 reduced indices of plaque stability and increased mortality
Santosh Karnewar, … , Laura S. Shankman, Gary K. Owens
Santosh Karnewar, … , Laura S. Shankman, Gary K. Owens
Published January 23, 2024
Citation Information: JCI Insight. 2024;9(2):e173863. https://doi.org/10.1172/jci.insight.173863.
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Research Article Vascular biology Article has an altmetric score of 3

Treatment of advanced atherosclerotic mice with ABT-263 reduced indices of plaque stability and increased mortality

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Abstract

The use of senolytic agents to remove senescent cells from atherosclerotic lesions is controversial. A common limitation of previous studies is the failure to rigorously define the effects of senolytic agent ABT-263 (Navitoclax) on smooth muscle cells (SMC) despite studies claiming that these cells are the major source of senescent cells. Moreover, there are no studies on the effect of ABT-263 on endothelial cells (EC), which — along with SMC — comprise 90% of α-smooth muscle actin+ (α-SMA+) myofibroblast-like cells in the protective fibrous cap. Here we tested the hypothesis that treatment of advanced atherosclerotic mice with ABT-263 will reduce lesion size and increase plaque stability. SMC (Myh11-CreERT2-eYFP) and EC (Cdh5-CreERT2-eYFP) lineage tracing Apoe–/– mice were fed a western diet (WD) for 18 weeks, followed by ABT-263 at 100 mg/kg/bw for 6 weeks or 50 mg/kg/bw for 9 weeks. ABT-263 treatment did not change lesion size or lumen area of the brachiocephalic artery (BCA). However, ABT-263 treatment reduced SMC by 90% and increased EC contributions to lesions via EC-to-mesenchymal transition (EndoMT) by 60%. ABT-263 treatment also reduced α-SMA+ fibrous cap thickness by 60% and was associated with a > 50% mortality rate. Taken together, ABT-263 treatment of WD-fed Apoe–/– mice with advanced lesions resulted in multiple detrimental changes, including reduced indices of stability and increased mortality.

Authors

Santosh Karnewar, Vaishnavi Karnewar, Laura S. Shankman, Gary K. Owens

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