HDL regulates TGFß-receptor lipid raft partitioning, restoring contractile features of cholesterol-loaded vascular smooth muscle cells

BACKGROUND: Cholesterol-loading of mouse aortic vascular smooth muscle cells (mVSMCs) downregulates miR-143/145, a master regulator of the contractile state downstream of TGFβ signaling. In vitro, this results in transitioning from a contractile mVSMC to a macrophage-like state. This process likely...

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Autores principales: Nagesh, Prashanth Thevkar, Nishi, Hitoo, Rawal, Shruti, Zahr, Tarik, Miano, Joseph M., Sorci-Thomas, Mary, Xu, Hao, Akbar, Naveed, Choudhury, Robin P, Misra, Ashish, Fisher, Edward A
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cold Spring Harbor Laboratory 2023
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10614922/
https://www.ncbi.nlm.nih.gov/pubmed/37905061
http://dx.doi.org/10.1101/2023.10.19.562786
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author Nagesh, Prashanth Thevkar
Nishi, Hitoo
Rawal, Shruti
Zahr, Tarik
Miano, Joseph M.
Sorci-Thomas, Mary
Xu, Hao
Akbar, Naveed
Choudhury, Robin P
Misra, Ashish
Fisher, Edward A
author_facet Nagesh, Prashanth Thevkar
Nishi, Hitoo
Rawal, Shruti
Zahr, Tarik
Miano, Joseph M.
Sorci-Thomas, Mary
Xu, Hao
Akbar, Naveed
Choudhury, Robin P
Misra, Ashish
Fisher, Edward A
author_sort Nagesh, Prashanth Thevkar
collection PubMed
description BACKGROUND: Cholesterol-loading of mouse aortic vascular smooth muscle cells (mVSMCs) downregulates miR-143/145, a master regulator of the contractile state downstream of TGFβ signaling. In vitro, this results in transitioning from a contractile mVSMC to a macrophage-like state. This process likely occurs in vivo based on studies in mouse and human atherosclerotic plaques. OBJECTIVES: To test whether cholesterol-loading reduces VSMC TGFβ signaling and if cholesterol efflux will restore signaling and the contractile state in vitro and in vivo. METHODS: Human coronary artery (h)VSMCs were cholesterol-loaded, then treated with HDL (to promote cholesterol efflux). For in vivo studies, partial conditional deletion of Tgfβr2 in lineage-traced VSMC mice was induced. Mice wild-type for VSMC Tgfβr2 or partially deficient (Tgfβr2+/−) were made hypercholesterolemic to establish atherosclerosis. Mice were then treated with apoA1 (which forms HDL). RESULTS: Cholesterol-loading of hVSMCs downregulated TGFβ signaling and contractile gene expression; macrophage markers were induced. TGFβ signaling positively regulated miR-143/145 expression, increasing Acta2 expression and suppressing KLF4. Cholesterol-loading localized TGFβ receptors into lipid rafts, with consequent TGFβ signaling downregulation. Notably, in cholesterol-loaded hVSMCs HDL particles displaced receptors from lipid rafts and increased TGFβ signaling, resulting in enhanced miR-145 expression and decreased KLF4-dependent macrophage features. ApoA1 infusion into Tgfβr2+/− mice restored Acta2 expression and decreased macrophage-marker expression in plaque VSMCs, with evidence of increased TGFβ signaling. CONCLUSIONS: Cholesterol suppresses TGFβ signaling and the contractile state in hVSMC through partitioning of TGFβ receptors into lipid rafts. These changes can be reversed by promotion of cholesterol efflux, consistent with evidence in vivo.
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spelling pubmed-106149222023-10-31 HDL regulates TGFß-receptor lipid raft partitioning, restoring contractile features of cholesterol-loaded vascular smooth muscle cells Nagesh, Prashanth Thevkar Nishi, Hitoo Rawal, Shruti Zahr, Tarik Miano, Joseph M. Sorci-Thomas, Mary Xu, Hao Akbar, Naveed Choudhury, Robin P Misra, Ashish Fisher, Edward A bioRxiv Article BACKGROUND: Cholesterol-loading of mouse aortic vascular smooth muscle cells (mVSMCs) downregulates miR-143/145, a master regulator of the contractile state downstream of TGFβ signaling. In vitro, this results in transitioning from a contractile mVSMC to a macrophage-like state. This process likely occurs in vivo based on studies in mouse and human atherosclerotic plaques. OBJECTIVES: To test whether cholesterol-loading reduces VSMC TGFβ signaling and if cholesterol efflux will restore signaling and the contractile state in vitro and in vivo. METHODS: Human coronary artery (h)VSMCs were cholesterol-loaded, then treated with HDL (to promote cholesterol efflux). For in vivo studies, partial conditional deletion of Tgfβr2 in lineage-traced VSMC mice was induced. Mice wild-type for VSMC Tgfβr2 or partially deficient (Tgfβr2+/−) were made hypercholesterolemic to establish atherosclerosis. Mice were then treated with apoA1 (which forms HDL). RESULTS: Cholesterol-loading of hVSMCs downregulated TGFβ signaling and contractile gene expression; macrophage markers were induced. TGFβ signaling positively regulated miR-143/145 expression, increasing Acta2 expression and suppressing KLF4. Cholesterol-loading localized TGFβ receptors into lipid rafts, with consequent TGFβ signaling downregulation. Notably, in cholesterol-loaded hVSMCs HDL particles displaced receptors from lipid rafts and increased TGFβ signaling, resulting in enhanced miR-145 expression and decreased KLF4-dependent macrophage features. ApoA1 infusion into Tgfβr2+/− mice restored Acta2 expression and decreased macrophage-marker expression in plaque VSMCs, with evidence of increased TGFβ signaling. CONCLUSIONS: Cholesterol suppresses TGFβ signaling and the contractile state in hVSMC through partitioning of TGFβ receptors into lipid rafts. These changes can be reversed by promotion of cholesterol efflux, consistent with evidence in vivo. Cold Spring Harbor Laboratory 2023-10-19 /pmc/articles/PMC10614922/ /pubmed/37905061 http://dx.doi.org/10.1101/2023.10.19.562786 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License (https://creativecommons.org/licenses/by-nc-nd/4.0/) , which allows reusers to copy and distribute the material in any medium or format in unadapted form only, for noncommercial purposes only, and only so long as attribution is given to the creator.
spellingShingle Article
Nagesh, Prashanth Thevkar
Nishi, Hitoo
Rawal, Shruti
Zahr, Tarik
Miano, Joseph M.
Sorci-Thomas, Mary
Xu, Hao
Akbar, Naveed
Choudhury, Robin P
Misra, Ashish
Fisher, Edward A
HDL regulates TGFß-receptor lipid raft partitioning, restoring contractile features of cholesterol-loaded vascular smooth muscle cells
title HDL regulates TGFß-receptor lipid raft partitioning, restoring contractile features of cholesterol-loaded vascular smooth muscle cells
title_full HDL regulates TGFß-receptor lipid raft partitioning, restoring contractile features of cholesterol-loaded vascular smooth muscle cells
title_fullStr HDL regulates TGFß-receptor lipid raft partitioning, restoring contractile features of cholesterol-loaded vascular smooth muscle cells
title_full_unstemmed HDL regulates TGFß-receptor lipid raft partitioning, restoring contractile features of cholesterol-loaded vascular smooth muscle cells
title_short HDL regulates TGFß-receptor lipid raft partitioning, restoring contractile features of cholesterol-loaded vascular smooth muscle cells
title_sort hdl regulates tgfß-receptor lipid raft partitioning, restoring contractile features of cholesterol-loaded vascular smooth muscle cells
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10614922/
https://www.ncbi.nlm.nih.gov/pubmed/37905061
http://dx.doi.org/10.1101/2023.10.19.562786
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