PPARÎ³-p53-Mediated Vasculoregenerative Program to Reverse Pulmonary Hypertension.

Hennigs, Jan K; Cao, Aiqin; Li, Caiyun G; Shi, Minyi; Mienert, Julia; Miyagawa, Kazuya; Körbelin, Jakob; Marciano, David P; Chen, Pin-I; Roughley, Matthew; Elliott, Matthew V; Harper, Rebecca L; Bill, Matthew A; Chappell, James; Moonen, Jan-Renier; Diebold, Isabel; Wang, Lingli; Snyder, Michael P; Rabinovitch, Marlene

Hennigs, Jan K; Cao, Aiqin; Li, Caiyun G; Shi, Minyi; Mienert, Julia; Miyagawa, Kazuya; Körbelin, Jakob; Marciano, David P; Chen, Pin-I; Roughley, Matthew; Elliott, Matthew V; Harper, Rebecca L; Bill, Matthew A; Chappell, James; Moonen, Jan-Renier; Diebold, Isabel; Wang, Lingli; Snyder, Michael P; Rabinovitch, Marlene.

Affiliation

Hennigs JK; Vera Moulton Wall Center for Pulmonary Vascular Disease (J.K.H., A.C., C.G.L., K.M., P.-I.C., M.R., M.V.E., R.L.H., M.A.B., J.C., J.-R.M., I.D., L.W.), Stanford University School of Medicine.
Cao A; Cardiovascular Institute (J.K.H., A.C., C.G.L., M.S., K.M., D.P.M., P.-I.C., M.R., M.V.E., R.L.H., M.A.B., J.C., J.-R.M., I.D., L.W., M.P.S., M.R.), Stanford University School of Medicine.
Li CG; Department of Pediatrics (J.K.H., A.C., C.G.L., K.M., D.P.M., P.-I.C., M.R., M.V.E., R.L.H., M.A.B., J.C., J.-R.M., I.D., L.W., M.R.), Stanford University School of Medicine.
Shi M; Department of Pneumology and Center for Pulmonary Arterial Hypertension Hamburg (J.K.H., J.M., J.K.), University Medical Center Hamburg-Eppendorf, Germany.
Mienert J; II. Department of Medicine (J.K.H., J.M., J.K.), University Medical Center Hamburg-Eppendorf, Germany.
Miyagawa K; Vera Moulton Wall Center for Pulmonary Vascular Disease (J.K.H., A.C., C.G.L., K.M., P.-I.C., M.R., M.V.E., R.L.H., M.A.B., J.C., J.-R.M., I.D., L.W.), Stanford University School of Medicine.
Körbelin J; Cardiovascular Institute (J.K.H., A.C., C.G.L., M.S., K.M., D.P.M., P.-I.C., M.R., M.V.E., R.L.H., M.A.B., J.C., J.-R.M., I.D., L.W., M.P.S., M.R.), Stanford University School of Medicine.
Marciano DP; Department of Pediatrics (J.K.H., A.C., C.G.L., K.M., D.P.M., P.-I.C., M.R., M.V.E., R.L.H., M.A.B., J.C., J.-R.M., I.D., L.W., M.R.), Stanford University School of Medicine.
Chen PI; Vera Moulton Wall Center for Pulmonary Vascular Disease (J.K.H., A.C., C.G.L., K.M., P.-I.C., M.R., M.V.E., R.L.H., M.A.B., J.C., J.-R.M., I.D., L.W.), Stanford University School of Medicine.
Roughley M; Cardiovascular Institute (J.K.H., A.C., C.G.L., M.S., K.M., D.P.M., P.-I.C., M.R., M.V.E., R.L.H., M.A.B., J.C., J.-R.M., I.D., L.W., M.P.S., M.R.), Stanford University School of Medicine.
Elliott MV; Department of Pediatrics (J.K.H., A.C., C.G.L., K.M., D.P.M., P.-I.C., M.R., M.V.E., R.L.H., M.A.B., J.C., J.-R.M., I.D., L.W., M.R.), Stanford University School of Medicine.
Harper RL; Department of Radiation Oncology (C.G.L.), Stanford University School of Medicine.
Bill MA; Cardiovascular Institute (J.K.H., A.C., C.G.L., M.S., K.M., D.P.M., P.-I.C., M.R., M.V.E., R.L.H., M.A.B., J.C., J.-R.M., I.D., L.W., M.P.S., M.R.), Stanford University School of Medicine.
Chappell J; Department of Genetics (M.S., D.P.M., J.C., M.P.S.), Stanford University School of Medicine.
Moonen JR; Department of Pneumology and Center for Pulmonary Arterial Hypertension Hamburg (J.K.H., J.M., J.K.), University Medical Center Hamburg-Eppendorf, Germany.
Diebold I; II. Department of Medicine (J.K.H., J.M., J.K.), University Medical Center Hamburg-Eppendorf, Germany.
Wang L; Vera Moulton Wall Center for Pulmonary Vascular Disease (J.K.H., A.C., C.G.L., K.M., P.-I.C., M.R., M.V.E., R.L.H., M.A.B., J.C., J.-R.M., I.D., L.W.), Stanford University School of Medicine.
Snyder MP; Cardiovascular Institute (J.K.H., A.C., C.G.L., M.S., K.M., D.P.M., P.-I.C., M.R., M.V.E., R.L.H., M.A.B., J.C., J.-R.M., I.D., L.W., M.P.S., M.R.), Stanford University School of Medicine.
Rabinovitch M; Department of Pediatrics (J.K.H., A.C., C.G.L., K.M., D.P.M., P.-I.C., M.R., M.V.E., R.L.H., M.A.B., J.C., J.-R.M., I.D., L.W., M.R.), Stanford University School of Medicine.

Circ Res ; 128(3): 401-418, 2021 02 05.

Article in En | MEDLINE | ID: mdl-33322916

ABSTRACT

ABSTRACT

RATIONALE In pulmonary arterial hypertension (PAH), endothelial dysfunction and obliterative vascular disease are associated with DNA damage and impaired signaling of BMPR2 (bone morphogenetic protein type 2 receptor) via two downstream transcription factors, PPARÎ³ (peroxisome proliferator-activated receptor gamma), and p53.

OBJECTIVE:

We investigated the vasculoprotective and regenerative potential of a newly identified PPARÎ³-p53 transcription factor complex in the pulmonary endothelium. METHODS AND

RESULTS:

In this study, we identified a pharmacologically inducible vasculoprotective mechanism in pulmonary arterial and lung MV (microvascular) endothelial cells in response to DNA damage and oxidant stress regulated in part by a BMPR2 dependent transcription factor complex between PPARÎ³ and p53. Chromatin immunoprecipitation sequencing and RNA-sequencing established an inducible PPARÎ³-p53 mediated regenerative program regulating 19 genes involved in lung endothelial cell survival, angiogenesis and DNA repair including, EPHA2 (ephrin type-A receptor 2), FHL2 (four and a half LIM domains protein 2), JAG1 (jagged 1), SULF2 (extracellular sulfatase Sulf-2), and TIGAR (TP53-inducible glycolysis and apoptosis regulator). Expression of these genes was partially impaired when the PPARÎ³-p53 complex was pharmacologically disrupted or when BMPR2 was reduced in pulmonary artery endothelial cells (PAECs) subjected to oxidative stress. In endothelial cell-specific Bmpr2-knockout mice unable to stabilize p53 in endothelial cells under oxidative stress, Nutlin-3 rescued endothelial p53 and PPARÎ³-p53 complex formation and induced target genes, such as APLN (apelin) and JAG1, to regenerate pulmonary microvessels and reverse pulmonary hypertension. In PAECs from BMPR2 mutant PAH patients, pharmacological induction of p53 and PPARÎ³-p53 genes repaired damaged DNA utilizing genes from the nucleotide excision repair pathway without provoking PAEC apoptosis.

CONCLUSIONS:

We identified a novel therapeutic strategy that activates a vasculoprotective gene regulation program in PAECs downstream of dysfunctional BMPR2 to rehabilitate PAH PAECs, regenerate pulmonary microvessels, and reverse disease. Our studies pave the way for p53-based vasculoregenerative therapies for PAH by extending the therapeutic focus to PAEC dysfunction and to DNA damage associated with PAH progression.

Subject(s)

Angiogenesis Inducing Agents/pharmacology; Endothelial Cells/drug effects; Imidazoles/pharmacology; Neovascularization, Physiologic/drug effects; PPAR gamma/metabolism; Piperazines/pharmacology; Pulmonary Arterial Hypertension/drug therapy; Pulmonary Artery/drug effects; Regeneration/drug effects; Tumor Suppressor Protein p53/metabolism; Animals; Bone Morphogenetic Protein Receptors, Type II/genetics; Bone Morphogenetic Protein Receptors, Type II/metabolism; Cells, Cultured; Endothelial Cells/metabolism; Endothelial Cells/pathology; Female; Gene Expression Regulation; Humans; Male; Mice; Mice, Knockout; Oxidative Stress; PPAR gamma/genetics; Pulmonary Arterial Hypertension/genetics; Pulmonary Arterial Hypertension/metabolism; Pulmonary Arterial Hypertension/physiopathology; Pulmonary Artery/metabolism; Pulmonary Artery/pathology; Pulmonary Artery/physiopathology; Signal Transduction; Tumor Suppressor Protein p53/genetics

Key words

chromatin immunoprecipitation sequencing; endothelium; epigenomics; genes, p53; hypertension, pulmonary; mice

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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Piperazines / Pulmonary Artery / Regeneration / Tumor Suppressor Protein p53 / Neovascularization, Physiologic / Endothelial Cells / Angiogenesis Inducing Agents / PPAR gamma / Pulmonary Arterial Hypertension / Imidazoles Type of study: Prognostic_studies Limits: Animals / Female / Humans / Male Language: En Journal: Circ Res Year: 2021 Document type: Article

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