Myeloperoxidase aggravates pulmonary arterial hypertension by activation of vascular Rho-kinase
Anna Klinke, Eva Berghausen, Kai Friedrichs, Simon Molz, Denise Lau, Lisa Remane, Matthias Berlin, Charlotte Kaltwasser, Matti Adam, Dennis Mehrkens, Martin Mollenhauer, Kashish Manchanda, Thorben Ravekes, Gustavo A. Heresi, Metin Aytekin, Raed A. Dweik, Jan K. Hennigs, Lukas Kubala, Erik Michaëlsson, Stephan Rosenkranz, Tanja K. Rudolph, Stanley L. Hazen, Hans Klose, Ralph T. Schermuly, Volker Rudolph, Stephan Baldus
Anna Klinke, Eva Berghausen, Kai Friedrichs, Simon Molz, Denise Lau, Lisa Remane, Matthias Berlin, Charlotte Kaltwasser, Matti Adam, Dennis Mehrkens, Martin Mollenhauer, Kashish Manchanda, Thorben Ravekes, Gustavo A. Heresi, Metin Aytekin, Raed A. Dweik, Jan K. Hennigs, Lukas Kubala, Erik Michaëlsson, Stephan Rosenkranz, Tanja K. Rudolph, Stanley L. Hazen, Hans Klose, Ralph T. Schermuly, Volker Rudolph, Stephan Baldus
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Research Article Cardiology Inflammation

Myeloperoxidase aggravates pulmonary arterial hypertension by activation of vascular Rho-kinase

Abstract

Pulmonary arterial hypertension (PAH) remains a disease with limited therapeutic options and dismal prognosis. Despite its etiologic heterogeneity, the underlying unifying pathophysiology is characterized by increased vascular tone and adverse remodeling of the pulmonary circulation. Myeloperoxidase (MPO), an enzyme abundantly expressed in neutrophils, has potent vasoconstrictive and profibrotic properties, thus qualifying as a potential contributor to this disease. Here, we sought to investigate whether MPO is causally linked to the pathophysiology of PAH. Investigation of 2 independent clinical cohorts revealed that MPO plasma levels were elevated in subjects with PAH and predicted adverse outcome. Experimental analyses showed that, upon hypoxia, right ventricular pressure was less increased in Mpo–/– than in WT mice. The hypoxia-induced activation of the Rho-kinase pathway, a critical subcellular signaling pathway yielding vasoconstriction and structural vascular remodeling, was blunted in Mpo–/– mice. Mice subjected to i.v. infusion of MPO revealed activation of Rho-kinase and increased right ventricular pressure, which was prevented by coinfusion of the Rho-kinase inhibitor Y-27632. In the Sugen5416/hypoxia rat model, PAH was attenuated by the MPO inhibitor AZM198. The current data demonstrate a tight mechanistic link between MPO, the activation of Rho-kinase, and adverse pulmonary vascular function, thus pointing toward a potentially novel avenue of treatment.

Authors

Anna Klinke, Eva Berghausen, Kai Friedrichs, Simon Molz, Denise Lau, Lisa Remane, Matthias Berlin, Charlotte Kaltwasser, Matti Adam, Dennis Mehrkens, Martin Mollenhauer, Kashish Manchanda, Thorben Ravekes, Gustavo A. Heresi, Metin Aytekin, Raed A. Dweik, Jan K. Hennigs, Lukas Kubala, Erik Michaëlsson, Stephan Rosenkranz, Tanja K. Rudolph, Stanley L. Hazen, Hans Klose, Ralph T. Schermuly, Volker Rudolph, Stephan Baldus

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Figure 3

Pulmonary nitric oxide bioavailability.

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Pulmonary nitric oxide bioavailability. Pulmonary artery nitric oxide (N...
Pulmonary artery nitric oxide (NO) bioavailability is not affected in Mpo–/– mice upon hypoxia (HOX). (A) Mice were maintained for 28 days under normoxia (NOX) or HOX (10% O2), and the Rho-kinase inhibitor Y-27632 was administered 1 hour prior to sacrifice. Relaxation of explanted pulmonary arteries in response to acetylcholine (ACh) was assessed by isometric force measurements and expressed as % of maximal prostaglandin F2α-mediated constriction with mean ± SEM. n = 5 (WT NOX), 6 (Mpo–/– NOX), 4 (WT HOX), 5 (Mpo–/– HOX), 7 (WT Y27632), 6 (Mpo–/– Y27632). Statistical analysis was performed by 1-way ANOVA for repeated measures. Differences are not statistically significant. (B) Lung homogenates of mice after 28 days of NOX or HOX were analyzed by Western blot, and protein amount of phosphorylated vasodilator stimulated phosphoprotein (p-VASP, Ser-157) in relation to dephosphorylated VASP was assessed. n = 5 (WT NOX), 4 (Mpo–/– NOX), 5 (WT HOX), 4 (Mpo–/– HOX); **P < 0.01. (C) Protein amount of inducible NO-synthase (iNOS) related to GAPDH was assessed in lung homogenates of mice after 28 days of NOX or HOX. n = 5 (WT NOX), 5 (Mpo–/– NOX), 6 (WT HOX), 5 (Mpo–/– HOX); *P < 0.05, **P < 0.01. Data in B and C represent median with interquartile range; whiskers indicate minimum to maximum. Statistical analysis was performed with 1-way ANOVA with LSD post hoc test.