Phenotypic Modulation of Smooth Muscle Cells in Atherosclerosis Is Associated With Downregulation of LMOD1, SYNPO2, PDLIM7, PLN, and SYNM

Ljubica Perisic Matic; Urszula Rykaczewska; Anton Razuvaev; Maria Sabater-Lleal; Mariette Lengquist; Clint L Miller; Ida Ericsson; Samuel Röhl; Malin Kronqvist; Silvia Aldi; Joelle Magné; Valentina Paloschi; Mattias Vesterlund; Yuhuang Li; Hong Jin; Maria Gonzalez Diez; Joy Roy; Damiano Baldassarre; Fabrizio Veglia; Steve E Humphries; Ulf de Faire; Elena Tremoli; Jacob Odeberg; Vladana Vukojević; Janne Lehtiö; Lars Maegdefessel; Ewa Ehrenborg; Gabrielle Paulsson-Berne; Göran K Hansson; Jan H N Lindeman; Per Eriksson; Thomas Quertermous; Anders Hamsten; Ulf Hedin

doi:10.1161/ATVBAHA.116.307893

Phenotypic Modulation of Smooth Muscle Cells in Atherosclerosis Is Associated With Downregulation of LMOD1, SYNPO2, PDLIM7, PLN, and SYNM

Arterioscler Thromb Vasc Biol. 2016 Sep;36(9):1947-61. doi: 10.1161/ATVBAHA.116.307893. Epub 2016 Jul 28.

Authors

Ljubica Perisic Matic¹, Urszula Rykaczewska², Anton Razuvaev², Maria Sabater-Lleal², Mariette Lengquist², Clint L Miller², Ida Ericsson², Samuel Röhl², Malin Kronqvist², Silvia Aldi², Joelle Magné², Valentina Paloschi², Mattias Vesterlund², Yuhuang Li², Hong Jin², Maria Gonzalez Diez², Joy Roy², Damiano Baldassarre², Fabrizio Veglia², Steve E Humphries², Ulf de Faire², Elena Tremoli², Jacob Odeberg², Vladana Vukojević², Janne Lehtiö², Lars Maegdefessel², Ewa Ehrenborg², Gabrielle Paulsson-Berne², Göran K Hansson², Jan H N Lindeman², Per Eriksson², Thomas Quertermous², Anders Hamsten², Ulf Hedin²

Affiliations

¹ From the Departments of Molecular Medicine and Surgery (L.P.M., U.R., A.R., M.L., I.E., S.R., M.K., S.A., J.R., U.H.), Medicine (M.S.-L., J.M., V.P., Y.L., H.J., M.G.D., L.M., E.E., G.P.-B., G.K.H., P.E., A.H.), Division of Cardiovascular Epidemiology, Institute of Environmental Medicine (U.d.F.), and Department of Clinical Neuroscience, Center for Molecular Medicine (V.V.), Karolinska Institutet, Solna, Sweden; Division of Vascular Surgery, Stanford University, CA (C.L.M., T.Q.); Science for Life Laboratory, Solna, Sweden (M.V., J.L.); Dipartimento di Scienze Farmacologiche e Biomolecolari, Università di Milano, Italy (D.B., E.T.); Dipartimento di Scienze Cliniche e di Comunità, Centro Cardiologico Monzino, IRCCS, Milan, Italy (D.B., F.V., E.T.); British Heart Foundation Laboratories, Department of Medicine, University College of London, United Kingdom (S.E.H.); Department of Cardiology, Karolinska University Hospital Solna, Karolinska Institutet, Stockholm, Sweden (U.d.F.); Science for Life Laboratory, Department of Proteomics, Stockholm, Sweden (J.O.); and Department of Vascular Surgery, Leiden University Medical Center, The Netherlands (J.H.N.L.). Ljubica.Perisic@ki.se.
² From the Departments of Molecular Medicine and Surgery (L.P.M., U.R., A.R., M.L., I.E., S.R., M.K., S.A., J.R., U.H.), Medicine (M.S.-L., J.M., V.P., Y.L., H.J., M.G.D., L.M., E.E., G.P.-B., G.K.H., P.E., A.H.), Division of Cardiovascular Epidemiology, Institute of Environmental Medicine (U.d.F.), and Department of Clinical Neuroscience, Center for Molecular Medicine (V.V.), Karolinska Institutet, Solna, Sweden; Division of Vascular Surgery, Stanford University, CA (C.L.M., T.Q.); Science for Life Laboratory, Solna, Sweden (M.V., J.L.); Dipartimento di Scienze Farmacologiche e Biomolecolari, Università di Milano, Italy (D.B., E.T.); Dipartimento di Scienze Cliniche e di Comunità, Centro Cardiologico Monzino, IRCCS, Milan, Italy (D.B., F.V., E.T.); British Heart Foundation Laboratories, Department of Medicine, University College of London, United Kingdom (S.E.H.); Department of Cardiology, Karolinska University Hospital Solna, Karolinska Institutet, Stockholm, Sweden (U.d.F.); Science for Life Laboratory, Department of Proteomics, Stockholm, Sweden (J.O.); and Department of Vascular Surgery, Leiden University Medical Center, The Netherlands (J.H.N.L.).

Abstract

Objective: Key augmented processes in atherosclerosis have been identified, whereas less is known about downregulated pathways. Here, we applied a systems biology approach to examine suppressed molecular signatures, with the hypothesis that they may provide insight into mechanisms contributing to plaque stability.

Approach and results: Muscle contraction, muscle development, and actin cytoskeleton were the most downregulated pathways (false discovery rate=6.99e-21, 1.66e-6, 2.54e-10, respectively) in microarrays from human carotid plaques (n=177) versus healthy arteries (n=15). In addition to typical smooth muscle cell (SMC) markers, these pathways also encompassed cytoskeleton-related genes previously not associated with atherosclerosis. SYNPO2, SYNM, LMOD1, PDLIM7, and PLN expression positively correlated to typical SMC markers in plaques (Pearson r>0.6, P<0.0001) and in rat intimal hyperplasia (r>0.8, P<0.0001). By immunohistochemistry, the proteins were expressed in SMCs in normal vessels, but largely absent in human plaques and intimal hyperplasia. Subcellularly, most proteins localized to the cytoskeleton in cultured SMCs and were regulated by active enhancer histone modification H3K27ac by chromatin immunoprecipitation-sequencing. Functionally, the genes were downregulated by PDGFB (platelet-derived growth factor beta) and IFNg (interferron gamma), exposure to shear flow stress, and oxLDL (oxidized low-density lipoprotein) loading. Genetic variants in PDLIM7, PLN, and SYNPO2 loci associated with progression of carotid intima-media thickness in high-risk subjects without symptoms of cardiovascular disease (n=3378). By eQTL (expression quantitative trait locus), rs11746443 also associated with PDLIM7 expression in plaques. Mechanistically, silencing of PDLIM7 in vitro led to downregulation of SMC markers and disruption of the actin cytoskeleton, decreased cell spreading, and increased proliferation.

Conclusions: We identified a panel of genes that reflect the altered phenotype of SMCs in vascular disease and could be early sensitive markers of SMC dedifferentiation.

Keywords: actin cytoskeleton; atherosclerosis; downregulation; hyperplasia; smooth muscle cells.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Actin Cytoskeleton / metabolism
Adaptor Proteins, Signal Transducing / genetics
Adaptor Proteins, Signal Transducing / metabolism*
Animals
Apolipoproteins E / deficiency
Apolipoproteins E / genetics
Atherosclerosis / genetics
Atherosclerosis / metabolism
Atherosclerosis / pathology
Autoantigens / genetics
Autoantigens / metabolism*
Calcium-Binding Proteins / genetics
Calcium-Binding Proteins / metabolism*
Carotid Arteries / metabolism
Carotid Arteries / pathology
Carotid Arteries / physiopathology
Carotid Artery Diseases / genetics
Carotid Artery Diseases / metabolism*
Carotid Artery Diseases / pathology
Carotid Artery Diseases / physiopathology
Carotid Artery Injuries / genetics
Carotid Artery Injuries / metabolism
Case-Control Studies
Cell Dedifferentiation
Cells, Cultured
Cytoskeletal Proteins / genetics
Cytoskeletal Proteins / metabolism*
Disease Models, Animal
Down-Regulation
Genetic Association Studies
Humans
Intermediate Filament Proteins / genetics
Intermediate Filament Proteins / metabolism*
LIM Domain Proteins / genetics
LIM Domain Proteins / metabolism*
Male
Mice, Knockout
Microfilament Proteins / genetics
Microfilament Proteins / metabolism*
Middle Aged
Muscle, Smooth, Vascular / metabolism*
Muscle, Smooth, Vascular / pathology
Muscle, Smooth, Vascular / physiopathology
Myocytes, Smooth Muscle / metabolism*
Myocytes, Smooth Muscle / pathology
Neointima
Phenotype
Plaque, Atherosclerotic*
RNA Interference
Rats, Sprague-Dawley
Signal Transduction
Time Factors
Transfection
Vasoconstriction

Substances

Adaptor Proteins, Signal Transducing
Apolipoproteins E
Autoantigens
Calcium-Binding Proteins
Cytoskeletal Proteins
Intermediate Filament Proteins
LIM Domain Proteins
LMOD1 protein, human
Microfilament Proteins
PDLIM7 protein, human
SYNPO2 protein, human
desmuslin
phospholamban

Abstract

Publication types

MeSH terms

Substances

Grants and funding