Loss of lung microvascular endothelial Piezo2 expression impairs NO synthesis, induces EndMT, and is associated with pulmonary hypertension

Siyu Tian; Zongye Cai; Payel Sen; Denise van Uden; Esther van de Kamp; Raphael Thuillet; Ly Tu; Christophe Guignabert; Karin Boomars; Kim Van der Heiden; Maarten M Brandt; Daphne Merkus

doi:10.1152/ajpheart.00220.2022

Loss of lung microvascular endothelial Piezo2 expression impairs NO synthesis, induces EndMT, and is associated with pulmonary hypertension

Am J Physiol Heart Circ Physiol. 2022 Nov 1;323(5):H958-H974. doi: 10.1152/ajpheart.00220.2022. Epub 2022 Sep 23.

Authors

Siyu Tian¹, Zongye Cai¹, Payel Sen^{2

3}, Denise van Uden⁴, Esther van de Kamp¹, Raphael Thuillet^{5

6}, Ly Tu^{5

6}, Christophe Guignabert^{5

6}, Karin Boomars⁴, Kim Van der Heiden⁷, Maarten M Brandt¹, Daphne Merkus^{1

2

3}

Affiliations

¹ Experimental Cardiology, Department of Cardiology, Thoraxcenter, Erasmus University Medical Center, Rotterdam, The Netherlands.
² Walter Brendel Center of Experimental Medicine, University Clinic Munich, Munich, Germany.
³ German Center for Cardiovascular Research, Partner Site Munich, Munich Heart Alliance, Munich, Germany.
⁴ Department of Pulmonary Medicine, Erasmus MC, University Medical Center, Rotterdam, The Netherlands.
⁵ INSERM UMR_S 999, Hôpital Marie Lannelongue, Le Plessis-Robinson, France.
⁶ School of Medicine, Université Paris-Saclay, Le Kremlin-Bicêtre, France.
⁷ Biomedical Engineering, Department of Cardiology, Thoraxcenter, Erasmus University Medical Center, Rotterdam, The Netherlands.

PMID: 36149769
DOI: 10.1152/ajpheart.00220.2022

Abstract

Mechanical forces are translated into biochemical stimuli by mechanotransduction channels, such as the mechanically activated cation channel Piezo2. Lung Piezo2 expression has recently been shown to be restricted to endothelial cells. Hence, we aimed to investigate the role of Piezo2 in regulation of pulmonary vascular function and structure, as well as its contribution to development of pulmonary arterial hypertension (PAH). The expression of Piezo2 was significantly reduced in pulmonary microvascular endothelial cells (MVECs) from patients with PAH, in lung tissue from mice with a Bmpr2^+/R899X knock-in mutation commonly found in patients with pulmonary hypertension, and in lung tissue of monocrotaline (MCT) and sugen-hypoxia-induced PH (SuHx) PAH rat models, as well as from a swine model with pulmonary vein banding. In MVECs, Piezo2 expression was reduced in response to abnormal shear stress, hypoxia, and TGFβ stimulation. Functional studies in MVECs exposed to shear stress illustrated that siRNA-mediated Piezo2 knockdown impaired endothelial alignment, calcium influx, phosphorylation of AKT, and nitric oxide production. In addition, siPiezo2 reduced the expression of the endothelial marker PECAM-1 and increased the expression of vascular smooth muscle markers ACTA2, SM22a, and calponin. Thus, Piezo2 acts as a mechanotransduction channel in pulmonary MVECs, stimulating shear-induced production of nitric oxide and is essentially involved in preventing endothelial to mesenchymal transition. Its blunted expression in pulmonary hypertension could impair the vasodilator capacity and stimulate vascular remodeling, indicating that Piezo2 might be an interesting therapeutic target to attenuate progression of the disease.NEW & NOTEWORTHY The mechanosensory ion channel Piezo2 is exclusively expressed in lung microvascular endothelial cells (MVECs). Patient MVECs as well as animal models of pulmonary (arterial) hypertension showed lower expression of Piezo2 in the lung. Mechanistically, Piezo2 is required for calcium influx and NO production in response to shear stress, whereas stimuli known to induce endothelial to mesenchymal transition (EndMT) reduce Piezo2 expression in MVECs, and Piezo2 knockdown induces a gene and protein expression pattern consistent with EndMT.

Keywords: Piezo2 channel; endothelial-to-mesenchymal transition; lung microvascular endothelial cell; pulmonary hypertension; shear stress.

Publication types

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

MeSH terms

Animals
Calcium / metabolism
Cells, Cultured
Disease Models, Animal
Endothelial Cells / metabolism
Hypertension, Pulmonary* / chemically induced
Hypertension, Pulmonary* / genetics
Hypertension, Pulmonary* / metabolism
Hypoxia
Ion Channels / genetics
Ion Channels / metabolism
Lung / metabolism
Mechanotransduction, Cellular
Mice
Nitric Oxide / metabolism
Pulmonary Arterial Hypertension* / genetics
Pulmonary Artery
Rats
Swine

Substances

Calcium
Nitric Oxide
Piezo2 protein, mouse
Ion Channels
piezo2 protein, rat