Human Plaque Myofibroblasts to Study Mechanisms of Atherosclerosis

Publication date

2023-11-07

Authors

Buono, Michele F.
Diez Benavente, ErnestORCID 0000-0002-4313-4290
Slenders, LotteORCID 0000-0003-3794-7604
Methorst, Daisey
Tessels, Daniëlle
Mili, Eloi
Finger, Roxy
Kapteijn, Daniek
Daniels, Mark A.
van den Dungen, Noortje A. M.

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Document Type

Article

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Abstract

Background Plaque myofibroblasts are critical players in the initiation and advancement of atherosclerotic disease. They are involved in the production of extracellular matrix, the formation of the fibrous cap, and the underlying lipidic core via modulation processes in response to different environmental cues. Despite clear phenotypic differences between myofibroblast cells and healthy vascular smooth muscle cells, smooth muscle cells are still widely used as a cellular model in atherosclerotic research. Methods and Results Here, we present a conditioned outgrowth method to isolate and culture myofibroblast cells from plaques. We obtained these cells from 27 donors (24 carotid and 3 femoral endarterectomies). We show that they keep their proliferative capacity for 8 passages, are transcriptionally stable, retain donor-specific gene expression programs, and express extracellular matrix proteins (FN1, COL1A1, and DCN) and smooth muscle cell markers (ACTA2, MYH11, and CNN1). Single-cell transcriptomics reveals that the cells in culture closely resemble the plaque myofibroblasts. Chromatin immunoprecipitation sequencing shows the presence of histone H3 lysine 4 dimethylation at the MYH11 promoter, pointing to their smooth muscle cell origin. Finally, we demonstrated that plaque myofibroblasts can be efficiently transduced (>97%) and are capable of taking up oxidized low-density lipoprotein and undergoing calcification. Conclusions In conclusion, we present a method to isolate and culture cells that retain plaque myofibroblast phenotypical and functional capabilities, making them a suitable in vitro model for studying selected mechanisms of atherosclerosis.

Keywords

disease modeling, myofibroblast, phenotypic modulation, plaque cells, smooth muscle cell, Cardiology and Cardiovascular Medicine

Citation

Buono, M F, Benavente, E D, Slenders, L, Methorst, D, Tessels, D, Mili, E, Finger, R, Kapteijn, D, Daniels, M, van den Dungen, N A M, Calis, J J A, Mol, B M, de Borst, G J, de Kleijn, D P V, Pasterkamp, G, den Ruijter, H M & Mokry, M 2023, 'Human Plaque Myofibroblasts to Study Mechanisms of Atherosclerosis', Journal of the American Heart Association, vol. 12, no. 21, e030243. https://doi.org/10.1161/JAHA.123.030243