Endothelial Heterogeneity in the Response to Autophagy Drives Small Vessel Muscularization in Pulmonary Hypertension.

Zhang, Qi; Yaoita, Nobuhiro; Tabuchi, Arata; Liu, Shaofei; Chen, Shiau-Haln; Li, Qiuhua; Hegemann, Niklas; Li, Caihong; Rodor, Julie; Timm, Sara; Laban, Hebatullah; Finkel, Toren; Stevens, Troy; Alvarez, Diego F; Erfinanda, Lasti; de Perrot, Marc; Kucherenko, Mariya M; Knosalla, Christoph; Ochs, Matthias; Dimmeler, Stefanie; Korff, Thomas; Verma, Subodh; Baker, Andrew H; Kuebler, Wolfgang M

Zhang, Qi; Yaoita, Nobuhiro; Tabuchi, Arata; Liu, Shaofei; Chen, Shiau-Haln; Li, Qiuhua; Hegemann, Niklas; Li, Caihong; Rodor, Julie; Timm, Sara; Laban, Hebatullah; Finkel, Toren; Stevens, Troy; Alvarez, Diego F; Erfinanda, Lasti; de Perrot, Marc; Kucherenko, Mariya M; Knosalla, Christoph; Ochs, Matthias; Dimmeler, Stefanie; Korff, Thomas; Verma, Subodh; Baker, Andrew H; Kuebler, Wolfgang M.

Affiliation

Zhang Q; Institute of Physiology (Q.Z., N.Y., A.T., S.L., Q.L., N.H., C.L., L.E., M.M.K., W.M.K.), Charité-Universitätsmedizin, Berlin, Germany.
Yaoita N; Department of Cardiology, First Affiliated Hospital, Zhejiang University School of Medicine, Hangzhou, China (Q.Z.).
Tabuchi A; Institute of Physiology (Q.Z., N.Y., A.T., S.L., Q.L., N.H., C.L., L.E., M.M.K., W.M.K.), Charité-Universitätsmedizin, Berlin, Germany.
Liu S; Institute of Physiology (Q.Z., N.Y., A.T., S.L., Q.L., N.H., C.L., L.E., M.M.K., W.M.K.), Charité-Universitätsmedizin, Berlin, Germany.
Chen SH; Institute of Physiology (Q.Z., N.Y., A.T., S.L., Q.L., N.H., C.L., L.E., M.M.K., W.M.K.), Charité-Universitätsmedizin, Berlin, Germany.
Li Q; German Center for Cardiovascular Research, Partner Site Berlin (S.L., N.H., M.M.K., C.K., W.M.K.).
Hegemann N; Centre for Cardiovascular Science, University of Edinburgh, United Kingdom (S.-H.C., J.R., A.H.B.).
Li C; Institute of Physiology (Q.Z., N.Y., A.T., S.L., Q.L., N.H., C.L., L.E., M.M.K., W.M.K.), Charité-Universitätsmedizin, Berlin, Germany.
Rodor J; Institute of Physiology (Q.Z., N.Y., A.T., S.L., Q.L., N.H., C.L., L.E., M.M.K., W.M.K.), Charité-Universitätsmedizin, Berlin, Germany.
Timm S; German Center for Cardiovascular Research, Partner Site Berlin (S.L., N.H., M.M.K., C.K., W.M.K.).
Laban H; Department of Cardiothoracic and Vascular Surgery, Deutsches Herzzentrum der Charité, Berlin, Germany (N.H., M.M.K., C.K.).
Finkel T; Charité-Universitätsmedizin Berlin, Corporate Member of Freie Universität Berlin and Humboldt Universität zu Berlin, Germany (N.H., M.M.K., C.K.).
Stevens T; Institute of Physiology (Q.Z., N.Y., A.T., S.L., Q.L., N.H., C.L., L.E., M.M.K., W.M.K.), Charité-Universitätsmedizin, Berlin, Germany.
Alvarez DF; Centre for Cardiovascular Science, University of Edinburgh, United Kingdom (S.-H.C., J.R., A.H.B.).
Erfinanda L; Core Facility Electron Microscopy (S.T., M.O.), Charité-Universitätsmedizin, Berlin, Germany.
de Perrot M; Institute of Physiology and Pathophysiology, Department of Cardiovascular Physiology (H.L.), Heidelberg University, Germany.
Kucherenko MM; German Center for Cardiovascular Research, Partner Site Heidelberg/Mannheim, Heidelberg (H.L.).
Knosalla C; Department of Medicine, Division of Cardiology, University of Pittsburgh, PA (T.F.).
Ochs M; Department of Physiology and Cell Biology, College of Medicine, University of South Alabama, Mobile (T.S.).
Dimmeler S; Department of Physiology and Pharmacology, College of Osteopathic Medicine, Sam Houston State University, Conroe, TX (D.F.A.).
Korff T; Institute of Physiology (Q.Z., N.Y., A.T., S.L., Q.L., N.H., C.L., L.E., M.M.K., W.M.K.), Charité-Universitätsmedizin, Berlin, Germany.
Verma S; Division of Thoracic Surgery, Toronto General Hospital, Canada (M.d.P.).
Baker AH; Department of Surgery (M.d.P., W.M.K.), University of Toronto, Canada.
Kuebler WM; Institute of Physiology (Q.Z., N.Y., A.T., S.L., Q.L., N.H., C.L., L.E., M.M.K., W.M.K.), Charité-Universitätsmedizin, Berlin, Germany.

Circulation ; 150(6): 466-487, 2024 Aug 06.

Article in En | MEDLINE | ID: mdl-38873770

ABSTRACT

ABSTRACT

BACKGROUND:

Endothelial cell (EC) apoptosis and proliferation of apoptosis-resistant cells is a hallmark of pulmonary hypertension (PH). Yet, why some ECs die and others proliferate and how this contributes to vascular remodeling is unclear. We hypothesized that this differential response may (1) relate to different EC subsets, namely pulmonary artery (PAECs) versus microvascular ECs (MVECs); (2) be attributable to autophagic activation in both EC subtypes; and (3) cause replacement of MVECs by PAECs with subsequent distal vessel muscularization.

METHODS:

EC subset responses to chronic hypoxia were assessed by single-cell RNA sequencing of murine lungs. Proliferative versus apoptotic responses, activation, and role of autophagy were assessed in human and rat PAECs and MVECs, and in precision-cut lung slices of wild-type mice or mice with endothelial deficiency in the autophagy-related gene 7 (Atg7EN-KO). Abundance of PAECs versus MVECs in precapillary microvessels was assessed in lung tissue from patients with PH and animal models on the basis of structural or surface markers.

RESULTS:

In vitro and in vivo, PAECs proliferated in response to hypoxia, whereas MVECs underwent apoptosis. Single-cell RNA sequencing analyses support these findings in that hypoxia induced an antiapoptotic, proliferative phenotype in arterial ECs, whereas capillary ECs showed a propensity for cell death. These distinct responses were prevented in hypoxic Atg7EN-KO mice or after ATG7 silencing, yet replicated by autophagy stimulation. In lung tissue from mice, rats, or patients with PH, the abundance of PAECs in precapillary arterioles was increased, and that of MVECs reduced relative to controls, indicating replacement of microvascular by macrovascular ECs. EC replacement was prevented by genetic or pharmacological inhibition of autophagy in vivo. Conditioned medium from hypoxic PAECs yet not MVECs promoted pulmonary artery smooth muscle cell proliferation and migration in a platelet-derived growth factor-dependent manner. Autophagy inhibition attenuated PH development and distal vessel muscularization in preclinical models.

CONCLUSIONS:

Autophagic activation by hypoxia induces in parallel PAEC proliferation and MVEC apoptosis. These differential responses cause a progressive replacement of MVECs by PAECs in precapillary pulmonary arterioles, thus providing a macrovascular context that in turn promotes pulmonary artery smooth muscle cell proliferation and migration, ultimately driving distal vessel muscularization and the development of PH.

Subject(s)

Apoptosis; Autophagy; Endothelial Cells; Hypertension, Pulmonary; Pulmonary Artery; Animals; Humans; Hypertension, Pulmonary/pathology; Hypertension, Pulmonary/physiopathology; Hypertension, Pulmonary/metabolism; Hypertension, Pulmonary/genetics; Endothelial Cells/metabolism; Endothelial Cells/pathology; Mice; Pulmonary Artery/pathology; Pulmonary Artery/metabolism; Pulmonary Artery/physiopathology; Rats; Cell Proliferation; Male; Vascular Remodeling; Mice, Knockout; Autophagy-Related Protein 7/genetics; Autophagy-Related Protein 7/metabolism; Disease Models, Animal; Hypoxia/metabolism; Hypoxia/pathology; Cells, Cultured; Mice, Inbred C57BL

Key words

autophagy; endothelial cells; hypertension, pulmonary; vascular remodeling

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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Pulmonary Artery / Autophagy / Apoptosis / Endothelial Cells / Hypertension, Pulmonary Limits: Animals / Humans / Male Language: En Journal: Circulation Year: 2024 Type: Article Affiliation country: Germany

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