Single-Cell Genomics Reveals a Novel Cell State During Smooth Muscle Cell Phenotypic Switching and Potential Therapeutic Targets for Atherosclerosis in Mouse and Human.

Pan, Huize; Xue, Chenyi; Auerbach, Benjamin J; Fan, Jiaxin; Bashore, Alexander C; Cui, Jian; Yang, Dina Y; Trignano, Sarah B; Liu, Wen; Shi, Jianting; Ihuegbu, Chinyere O; Bush, Erin C; Worley, Jeremy; Vlahos, Lukas; Laise, Pasquale; Solomon, Robert A; Connolly, Edward S; Califano, Andrea; Sims, Peter A; Zhang, Hanrui; Li, Mingyao; Reilly, Muredach P

Pan, Huize; Xue, Chenyi; Auerbach, Benjamin J; Fan, Jiaxin; Bashore, Alexander C; Cui, Jian; Yang, Dina Y; Trignano, Sarah B; Liu, Wen; Shi, Jianting; Ihuegbu, Chinyere O; Bush, Erin C; Worley, Jeremy; Vlahos, Lukas; Laise, Pasquale; Solomon, Robert A; Connolly, Edward S; Califano, Andrea; Sims, Peter A; Zhang, Hanrui; Li, Mingyao; Reilly, Muredach P.

Afiliação

Pan H; Division of Cardiology, Department of Medicine (H.P., C.X., A.C.B., J.C., D.Y.Y., S.B.T., W.L., J.S., C.O.I., H.Z., M.P.R.), Columbia University Irving Medical Center, New York.
Xue C; Division of Cardiology, Department of Medicine (H.P., C.X., A.C.B., J.C., D.Y.Y., S.B.T., W.L., J.S., C.O.I., H.Z., M.P.R.), Columbia University Irving Medical Center, New York.
Auerbach BJ; Graduate Group in Genomics and Computational Biology (B.J.A.), University of Pennsylvania, Philadelphia.
Fan J; Department of Biostatistics, Epidemiology, and Informatics (J.F., M.L.), University of Pennsylvania, Philadelphia.
Bashore AC; Division of Cardiology, Department of Medicine (H.P., C.X., A.C.B., J.C., D.Y.Y., S.B.T., W.L., J.S., C.O.I., H.Z., M.P.R.), Columbia University Irving Medical Center, New York.
Cui J; Division of Cardiology, Department of Medicine (H.P., C.X., A.C.B., J.C., D.Y.Y., S.B.T., W.L., J.S., C.O.I., H.Z., M.P.R.), Columbia University Irving Medical Center, New York.
Yang DY; Division of Cardiology, Department of Medicine (H.P., C.X., A.C.B., J.C., D.Y.Y., S.B.T., W.L., J.S., C.O.I., H.Z., M.P.R.), Columbia University Irving Medical Center, New York.
Trignano SB; Division of Cardiology, Department of Medicine (H.P., C.X., A.C.B., J.C., D.Y.Y., S.B.T., W.L., J.S., C.O.I., H.Z., M.P.R.), Columbia University Irving Medical Center, New York.
Liu W; Division of Cardiology, Department of Medicine (H.P., C.X., A.C.B., J.C., D.Y.Y., S.B.T., W.L., J.S., C.O.I., H.Z., M.P.R.), Columbia University Irving Medical Center, New York.
Shi J; Division of Cardiology, Department of Medicine (H.P., C.X., A.C.B., J.C., D.Y.Y., S.B.T., W.L., J.S., C.O.I., H.Z., M.P.R.), Columbia University Irving Medical Center, New York.
Ihuegbu CO; Division of Cardiology, Department of Medicine (H.P., C.X., A.C.B., J.C., D.Y.Y., S.B.T., W.L., J.S., C.O.I., H.Z., M.P.R.), Columbia University Irving Medical Center, New York.
Bush EC; Department of Systems Biology (E.C.B., J.W., L.V., P.L. A.C., P.A.S.), Columbia University Irving Medical Center, New York.
Worley J; Department of Systems Biology (E.C.B., J.W., L.V., P.L. A.C., P.A.S.), Columbia University Irving Medical Center, New York.
Vlahos L; Department of Systems Biology (E.C.B., J.W., L.V., P.L. A.C., P.A.S.), Columbia University Irving Medical Center, New York.
Laise P; Department of Systems Biology (E.C.B., J.W., L.V., P.L. A.C., P.A.S.), Columbia University Irving Medical Center, New York.
Solomon RA; Department of Neurologic Surgery, New York-Presbyterian Hospital/Columbia University Irving Medical Center (R.A.S., E.S.C.).
Connolly ES; Department of Neurologic Surgery, New York-Presbyterian Hospital/Columbia University Irving Medical Center (R.A.S., E.S.C.).
Califano A; Department of Systems Biology (E.C.B., J.W., L.V., P.L. A.C., P.A.S.), Columbia University Irving Medical Center, New York.
Sims PA; Herbert Irving Comprehensive Cancer Center (A.C.), Columbia University Irving Medical Center, New York.
Zhang H; JP Sulzberger Columbia Genome Center (A.C.), Columbia University Irving Medical Center, New York.
Li M; Department of Biomedical Informatics (A.C.), Columbia University Irving Medical Center, New York.
Reilly MP; Department of Biochemistry and Molecular Biophysics (A.C., P.A.S.), Columbia University Irving Medical Center, New York.

Circulation ; 142(21): 2060-2075, 2020 11 24.

Article em En | MEDLINE | ID: mdl-32962412

ABSTRACT

ABSTRACT

BACKGROUND:

Smooth muscle cells (SMCs) play significant roles in atherosclerosis via phenotypic switching, a pathological process in which SMC dedifferentiation, migration, and transdifferentiation into other cell types. Yet how SMCs contribute to the pathophysiology of atherosclerosis remains elusive.

METHODS:

To reveal the trajectories of SMC transdifferentiation during atherosclerosis and to identify molecular targets for disease therapy, we combined SMC fate mapping and single-cell RNA sequencing of both mouse and human atherosclerotic plaques. We also performed cell biology experiments on isolated SMC-derived cells, conducted integrative human genomics, and used pharmacological studies targeting SMC-derived cells both in vivo and in vitro.

RESULTS:

We found that SMCs transitioned to an intermediate cell state during atherosclerosis, which was also found in human atherosclerotic plaques of carotid and coronary arteries. SMC-derived intermediate cells, termed "SEM" cells (stem cell, endothelial cell, monocyte), were multipotent and could differentiate into macrophage-like and fibrochondrocyte-like cells, as well as return toward the SMC phenotype. Retinoic acid (RA) signaling was identified as a regulator of SMC to SEM cell transition, and RA signaling was dysregulated in symptomatic human atherosclerosis. Human genomics revealed enrichment of genome-wide association study signals for coronary artery disease in RA signaling target gene loci and correlation between coronary artery disease risk alleles and repressed expression of these genes. Activation of RA signaling by all-trans RA, an anticancer drug for acute promyelocytic leukemia, blocked SMC transition to SEM cells, reduced atherosclerotic burden, and promoted fibrous cap stability.

CONCLUSIONS:

Integration of cell-specific fate mapping, single-cell genomics, and human genetics adds novel insights into the complexity of SMC biology and reveals regulatory pathways for therapeutic targeting of SMC transitions in atherosclerotic cardiovascular disease.

Assuntos

Aterosclerose/genética; Aterosclerose/patologia; Diferenciação Celular/fisiologia; Genômica/métodos; Miócitos de Músculo Liso/patologia; Fenótipo; Animais; Aterosclerose/terapia; Desdiferenciação Celular/fisiologia; Movimento Celular/fisiologia; Transdiferenciação Celular/fisiologia; Células Cultivadas; Feminino; Terapia Genética/tendências; Humanos; Masculino; Camundongos; Camundongos Endogâmicos C57BL; Camundongos Knockout; Camundongos Transgênicos; Miócitos de Músculo Liso/fisiologia; Análise de Sequência de RNA/métodos

Palavras-chave

atherosclerosis; cardiovascular disease; retinoic acid signaling; single-cell RNA sequencing; smooth muscle cell

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Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Assunto principal: Fenótipo / Diferenciação Celular / Genômica / Miócitos de Músculo Liso / Aterosclerose Limite: Animals / Female / Humans / Male Idioma: En Revista: Circulation Ano de publicação: 2020 Tipo de documento: Article

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