Cholesteryl Hemiazelate Present in Cardiovascular Disease Patients Causes Lysosome Dysfunction in Murine Fibroblasts.
Elizeth LopesGisela Machado-OliveiraCatarina Guerreiro SimõesInês S FerreiraCristiano RamosJosé S RamalhoMaria I L SoaresTeresa M V D Pinho E MeloRosa PuertollanoAndré R A MarquesOtília V VieiraPublished in: Cells (2023)
There is growing evidence supporting the role of fibroblasts in all stages of atherosclerosis, from the initial phase to fibrous cap and plaque formation. In the arterial wall, as with macrophages and vascular smooth muscle cells, fibroblasts are exposed to a myriad of LDL lipids, including the lipid species formed during the oxidation of their polyunsaturated fatty acids of cholesteryl esters (PUFA-CEs). Recently, our group identified the final oxidation products of the PUFA-CEs, cholesteryl hemiesters (ChE), in tissues from cardiovascular disease patients. Cholesteryl hemiazelate (ChA), the most prevalent lipid of this family, is sufficient to impact lysosome function in macrophages and vascular smooth muscle cells, with consequences for their homeostasis. Here, we show that the lysosomal compartment of ChA-treated fibroblasts also becomes dysfunctional. Indeed, fibroblasts exposed to ChA exhibited a perinuclear accumulation of enlarged lysosomes full of neutral lipids. However, this outcome did not trigger de novo lysosome biogenesis, and only the lysosomal transcription factor E3 (TFE3) was slightly transcriptionally upregulated. As a consequence, autophagy was inhibited, probably via mTORC1 activation, culminating in fibroblasts' apoptosis. Our findings suggest that the impairment of lysosome function and autophagy and the induction of apoptosis in fibroblasts may represent an additional mechanism by which ChA can contribute to the progression of atherosclerosis.
Keyphrases
- cardiovascular disease
- vascular smooth muscle cells
- extracellular matrix
- oxidative stress
- end stage renal disease
- endoplasmic reticulum stress
- cell death
- transcription factor
- newly diagnosed
- ejection fraction
- angiotensin ii
- fluorescent probe
- type diabetes
- peritoneal dialysis
- fatty acid
- signaling pathway
- nitric oxide
- metabolic syndrome
- cell proliferation