Targeting Epsins to Inhibit Fibroblast Growth Factor Signaling While Potentiating Transforming Growth Factor-ß Signaling Constrains Endothelial-to-Mesenchymal Transition in Atherosclerosis.

Dong, Yunzhou; Wang, Beibei; Du, Mulong; Zhu, Bo; Cui, Kui; Li, Kathryn; Yuan, Ke; Cowan, Douglas B; Bhattacharjee, Sudarshan; Wong, Scott; Shi, Jinjun; Wang, Da-Zhi; Chen, Kaifu; Bischoff, Joyce; Linton, MacRae F; Chen, Hong

Dong, Yunzhou; Wang, Beibei; Du, Mulong; Zhu, Bo; Cui, Kui; Li, Kathryn; Yuan, Ke; Cowan, Douglas B; Bhattacharjee, Sudarshan; Wong, Scott; Shi, Jinjun; Wang, Da-Zhi; Chen, Kaifu; Bischoff, Joyce; Linton, MacRae F; Chen, Hong.

Affiliation

Dong Y; Vascular Biology Program (Y.D., B.W., B.Z., K. Cui, K.L., D.B.C., S.B., S.W., J.B., H.C.), Boston Children's Hospital, MA.
Wang B; Departments of Surgery (Y.D., B.W., B.Z., K. Cui, D.B.C., S.B., J.B., H.C.), Harvard Medical School, Boston, MA.
Du M; Vascular Biology Program (Y.D., B.W., B.Z., K. Cui, K.L., D.B.C., S.B., S.W., J.B., H.C.), Boston Children's Hospital, MA.
Zhu B; Departments of Surgery (Y.D., B.W., B.Z., K. Cui, D.B.C., S.B., J.B., H.C.), Harvard Medical School, Boston, MA.
Cui K; Department of Environmental Health, Harvard T.H. Chan School of Public Health, Boston, MA (M.D.).
Li K; Vascular Biology Program (Y.D., B.W., B.Z., K. Cui, K.L., D.B.C., S.B., S.W., J.B., H.C.), Boston Children's Hospital, MA.
Yuan K; Departments of Surgery (Y.D., B.W., B.Z., K. Cui, D.B.C., S.B., J.B., H.C.), Harvard Medical School, Boston, MA.
Cowan DB; Vascular Biology Program (Y.D., B.W., B.Z., K. Cui, K.L., D.B.C., S.B., S.W., J.B., H.C.), Boston Children's Hospital, MA.
Bhattacharjee S; Departments of Surgery (Y.D., B.W., B.Z., K. Cui, D.B.C., S.B., J.B., H.C.), Harvard Medical School, Boston, MA.
Wong S; Vascular Biology Program (Y.D., B.W., B.Z., K. Cui, K.L., D.B.C., S.B., S.W., J.B., H.C.), Boston Children's Hospital, MA.
Shi J; Department of Medicine (K.Y.), Boston Children's Hospital, MA.
Wang DZ; Pediatrics (K.Y., K. Chen), Harvard Medical School, Boston, MA.
Chen K; Vascular Biology Program (Y.D., B.W., B.Z., K. Cui, K.L., D.B.C., S.B., S.W., J.B., H.C.), Boston Children's Hospital, MA.
Bischoff J; Departments of Surgery (Y.D., B.W., B.Z., K. Cui, D.B.C., S.B., J.B., H.C.), Harvard Medical School, Boston, MA.
Linton MF; Vascular Biology Program (Y.D., B.W., B.Z., K. Cui, K.L., D.B.C., S.B., S.W., J.B., H.C.), Boston Children's Hospital, MA.
Chen H; Departments of Surgery (Y.D., B.W., B.Z., K. Cui, D.B.C., S.B., J.B., H.C.), Harvard Medical School, Boston, MA.

Circulation ; 147(8): 669-685, 2023 02 21.

Article in En | MEDLINE | ID: mdl-36591786

ABSTRACT

ABSTRACT

BACKGROUND:

Epsin endocytic adaptor proteins are implicated in the progression of atherosclerosis; however, the underlying molecular mechanisms have not yet been fully defined. In this study, we determined how epsins enhance endothelial-to-mesenchymal transition (EndoMT) in atherosclerosis and assessed the efficacy of a therapeutic peptide in a preclinical model of this disease.

METHODS:

Using single-cell RNA sequencing combined with molecular, cellular, and biochemical analyses, we investigated the role of epsins in stimulating EndoMT using knockout in Apoe-/- and lineage tracing/proprotein convertase subtilisin/kexin type 9 serine protease mutant viral-induced atherosclerotic mouse models. The therapeutic efficacy of a synthetic peptide targeting atherosclerotic plaques was then assessed in Apoe-/- mice.

RESULTS:

Single-cell RNA sequencing and lineage tracing revealed that epsins 1 and 2 promote EndoMT and that the loss of endothelial epsins inhibits EndoMT marker expression and transforming growth factor-ß signaling in vitro and in atherosclerotic mice, which is associated with smaller lesions in the Apoe-/- mouse model. Mechanistically, the loss of endothelial cell epsins results in increased fibroblast growth factor receptor-1 expression, which inhibits transforming growth factor-ß signaling and EndoMT. Epsins directly bind ubiquitinated fibroblast growth factor receptor-1 through their ubiquitin-interacting motif, which results in endocytosis and degradation of this receptor complex. Consequently, administration of a synthetic ubiquitin-interacting motif-containing peptide atheroma ubiquitin-interacting motif peptide inhibitor significantly attenuates EndoMT and progression of atherosclerosis.

CONCLUSIONS:

We conclude that epsins potentiate EndoMT during atherogenesis by increasing transforming growth factor-ß signaling through fibroblast growth factor receptor-1 internalization and degradation. Inhibition of EndoMT by reducing epsin-fibroblast growth factor receptor-1 interaction with a therapeutic peptide may represent a novel treatment strategy for atherosclerosis.

Subject(s)

Atherosclerosis; Transforming Growth Factor beta; Mice; Animals; Fibroblast Growth Factors; Apolipoproteins E; Atherosclerosis/genetics; Receptors, Fibroblast Growth Factor; Transforming Growth Factors; Ubiquitins

Key words

EndoMT; adaptor proteins, signal transducing; atherosclerosis; endocytosis; epsin; peptides; receptor, fibroblast growth factor, type 1; single-cell gene expression analysis; transforming growth factor beta; vascular diseases

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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Transforming Growth Factor beta / Atherosclerosis Type of study: Prognostic_studies Limits: Animals Language: En Journal: Circulation Year: 2023 Document type: Article

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