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2. Surfactant alteration and replacement in acute respiratory distress syndrome

Author

Walmrath Dieter, Grimminger Friedrich, Markart Philipp, Schmidt Reinhold, Ruppert Clemens, Günther Andreas, and Seeger Werner

Subjects
acute lung injury, ARDS, pulmonary surfactant, surfactant replacement, Diseases of the respiratory system, RC705-779
Abstract

Abstract The acute respiratory distress syndrome (ARDS) is a frequent, life-threatening disease in which a marked increase in alveolar surface tension has been repeatedly observed. It is caused by factors including a lack of surface-active compounds, changes in the phospholipid, fatty acid, neutral lipid, and surfactant apoprotein composition, imbalance of the extracellular surfactant subtype distribution, inhibition of surfactant function by plasma protein leakage, incorporation of surfactant phospholipids and apoproteins into polymerizing fibrin, and damage/inhibition of surfactant compounds by inflammatory mediators. There is now good evidence that these surfactant abnormalities promote alveolar instability and collapse and, consequently, loss of compliance and the profound gas exchange abnormalities seen in ARDS. An acute improvement of gas exchange properties together with a far-reaching restoration of surfactant properties was encountered in recently performed pilot studies. Here we summarize what is known about the kind and severity of surfactant changes occuring in ARDS, the contribution of these changes to lung failure, and the role of surfactant administration for therapy of ARDS.

Published
2001
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3. Comparison of Contemporary Risk Scores in All Groups of Pulmonary Hypertension: A Pulmonary Vascular Research Institute GoDeep Meta-Registry Analysis

Author

Antoine, Tobiah, Backofen, Achim, Cannon, John, Damonte, Victoria, Echazarreta, Diego, Eichstaedt, Christina, Elwing, Jean, Förster, Kai, Gruenig, Ekkehard, Hilgendorff, Anne, Jose, Arun, Junaeda, Ernesto, Krieb, Philipp, Marquardt, Kurt, Osborn, Karen, Pepke-Zaba, Johanna, Tilea, Ioan, Varga, Andreea, Yogeswaran, Athiththan, Gall, Henning, Fünderich, Meike, Wilkins, Martin R., Howard, Luke, Kiely, David G., Lawrie, Allan, Hassoun, Paul M., Sirenklo, Yuriy, Torbas, Olena, Sweatt, Andrew J., Zamanian, Roham T., Williams, Paul G., Frauendorf, Marlize, Arvanitaki, Alexandra, Giannakoulas, George, Saleh, Khaled, Sabbour, Hani, Cajigas, Hector R., Frantz, Robert, Al Ghouleh, Imad, Chan, Stephen Y., Brittain, Evan, Annis, Jeffrey S., Pepe, Antonella, Ghio, Stefano, Orfanos, Stylianos, Anthi, Anastasia, Majeed, Raphael W., Wilhelm, Jochen, Ghofrani, Hossein Ardeschir, Richter, Manuel J., Grimminger, Friedrich, Sahay, Sandeep, Tello, Khodr, and Seeger, Werner

Published
2024
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5. Phosphodiesterase 5 Inhibitor Treatment Is Associated With Improved Survival in Pulmonary Hypertension Associated With COPD in the Pulmonary Vascular Research Institute GoDeep Meta-Registry

Author

Tello, Khodr, Yogeswaran, Athiththan, Majeed, Raphael W., Kiely, David G., Lawrie, Allan, Brittain, Evan, Annis, Jeffrey S., Olschewski, Horst, Kovacs, Gabor, Hassoun, Paul M., Balasubramanian, Aparna, Konswa, Ziad, Sweatt, Andrew J., Zamanian, Roham T., Wilkins, Martin R., Howard, Luke, Arvanitaki, Alexandra, Giannakoulas, George, Cajigas, Hector R., Frantz, Robert, Williams, Paul G., Frauendorf, Marlize, Marquardt, Kurt, Antoine, Tobiah, Fuenderich, Meike, Richter, Manuel, Grimminger, Friedrich, Ghofrani, Hossein-Ardeschir, Wilhelm, Jochen, and Seeger, Werner

Published
2024
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6. Effects of hypercapnia and NO synthase inhibition in sustained hypoxic pulmonary vasoconstriction

Author

Ketabchi Farzaneh, Ghofrani Hossein A, Schermuly Ralph T, Seeger Werner, Grimminger Friedrich, Egemnazarov Bakytbek, Shid-Moosavi S Mostafa, Dehghani Gholam A, Weissmann Norbert, and Sommer Natascha

Subjects
hypoxia, hypercapnia, acidosis, nitric oxide, hypoxic pulmonary vasoconstriction, Diseases of the respiratory system, RC705-779
Abstract

Abstract Background Acute respiratory disorders may lead to sustained alveolar hypoxia with hypercapnia resulting in impaired pulmonary gas exchange. Hypoxic pulmonary vasoconstriction (HPV) optimizes gas exchange during local acute (0-30 min), as well as sustained (> 30 min) hypoxia by matching blood perfusion to alveolar ventilation. Hypercapnia with acidosis improves pulmonary gas exchange in repetitive conditions of acute hypoxia by potentiating HPV and preventing pulmonary endothelial dysfunction. This study investigated, if the beneficial effects of hypercapnia with acidosis are preserved during sustained hypoxia as it occurs, e.g in permissive hypercapnic ventilation in intensive care units. Furthermore, the effects of NO synthase inhibitors under such conditions were examined. Method We employed isolated perfused and ventilated rabbit lungs to determine the influence of hypercapnia with or without acidosis (pH corrected with sodium bicarbonate), and inhibitors of endothelial as well as inducible NO synthase on acute or sustained HPV (180 min) and endothelial permeability. Results In hypercapnic acidosis, HPV was intensified in sustained hypoxia, in contrast to hypercapnia without acidosis when HPV was amplified during both phases. L-NG-Nitroarginine (L-NNA), a non-selective NO synthase inhibitor, enhanced acute as well as sustained HPV under all conditions, however, the amplification of sustained HPV induced by hypercapnia with or without acidosis compared to normocapnia disappeared. In contrast 1400 W, a selective inhibitor of inducible NO synthase (iNOS), decreased HPV in normocapnia and hypercapnia without acidosis at late time points of sustained HPV and selectively reversed the amplification of sustained HPV during hypercapnia without acidosis. Hypoxic hypercapnia without acidosis increased capillary filtration coefficient (Kfc). This increase disappeared after administration of 1400 W. Conclusion Hypercapnia with and without acidosis increased HPV during conditions of sustained hypoxia. The increase of sustained HPV and endothelial permeability in hypoxic hypercapnia without acidosis was iNOS dependent.

Published
2012
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7. Therapeutic efficacy of TBC3711 in monocrotaline-induced pulmonary hypertension

Author

Brandes Ralf P, Janssen Wiebke, Cornitescu Teodora, Sydykov Akylbek, Dahal Bhola K, Luitel Himal, Kojonazarov Baktybek, Kosanovic Djuro, Davie Neil, Ghofrani Hossein A, Weissmann Norbert, Grimminger Friedrich, Seeger Werner, and Schermuly Ralph T

Subjects
Diseases of the respiratory system, RC705-779
Abstract

Abstract Background Endothelin-1 signalling plays an important role in pathogenesis of pulmonary hypertension. Although different endothelin-A receptor antagonists are developed, a novel therapeutic option to cure the disease is still needed. This study aims to investigate the therapeutic efficacy of the selective endothelin-A receptor antagonist TBC3711 in monocrotaline-induced pulmonary hypertension in rats. Methods Monocrotaline-injected male Sprague-Dawley rats were randomized and treated orally from day 21 to 35 either with TBC3711 (Dose: 30 mg/kg body weight/day) or placebo. Echocardiographic measurements of different hemodynamic and right-heart hypertrophy parameters were performed. After day 35, rats were sacrificed for invasive hemodynamic and right-heart hypertrophy measurements. Additionally, histologic assessment of pulmonary vascular and right-heart remodelling was performed. Results The novel endothelin-A receptor antagonist TBC3711 significantly attenuated monocrotaline-induced pulmonary hypertension, as evident from improved hemodynamics and right-heart hypertrophy in comparison with placebo group. In addition, muscularization and medial wall thickness of distal pulmonary vessels were ameliorated. The histologic evaluation of the right ventricle showed a significant reduction in fibrosis and cardiomyocyte size, suggesting an improvement in right-heart remodelling. Conclusion The results of this study suggest that the selective endothelin-A receptor antagonist TBC3711 demonstrates therapeutic benefit in rats with established pulmonary hypertension, thus representing a useful therapeutic approach for treatment of pulmonary hypertension.

Published
2011
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8. Involvement of mast cells in monocrotaline-induced pulmonary hypertension in rats

Author

Ghofrani Hossein A, Reiss Irwin, Hoffmann Julia, Savai Rajkumar, Cornitescu Teodora, Kaulen Christina, Kosanovic Djuro, Dahal Bhola K, Weissmann Norbert, Kuebler Wolfgang M, Seeger Werner, Grimminger Friedrich, and Schermuly Ralph T

Subjects
Diseases of the respiratory system, RC705-779
Abstract

Abstract Background Mast cells (MCs) are implicated in inflammation and tissue remodeling. Accumulation of lung MCs is described in pulmonary hypertension (PH); however, whether MC degranulation and c-kit, a tyrosine kinase receptor critically involved in MC biology, contribute to the pathogenesis and progression of PH has not been fully explored. Methods Pulmonary MCs of idiopathic pulmonary arterial hypertension (IPAH) patients and monocrotaline-injected rats (MCT-rats) were examined by histochemistry and morphometry. Effects of the specific c-kit inhibitor PLX and MC stabilizer cromolyn sodium salt (CSS) were investigated in MCT-rats both by the preventive and therapeutic approaches. Hemodynamic and right ventricular hypertrophy measurements, pulmonary vascular morphometry and analysis of pulmonary MC localization/counts/activation were performed in animal model studies. Results There was a prevalence of pulmonary MCs in IPAH patients and MCT-rats as compared to the donors and healthy rats, respectively. Notably, the perivascular MCs were increased and a majority of them were degranulated in lungs of IPAH patients and MCT-rats (p < 0.05 versus donor and control, respectively). In MCT-rats, the pharmacological inhibitions of MC degranulation and c-kit with CSS and PLX, respectively by a preventive approach (treatment from day 1 to 21 of MCT-injection) significantly attenuated right ventricular systolic pressure (RVSP) and right ventricular hypertrophy (RVH). Moreover, vascular remodeling, as evident from the significantly decreased muscularization and medial wall thickness of distal pulmonary vessels, was improved. However, treatments with CSS and PLX by a therapeutic approach (from day 21 to 35 of MCT-injection) neither improved hemodynamics and RVH nor vascular remodeling. Conclusions The accumulation and activation of perivascular MCs in the lungs are the histopathological features present in clinical (IPAH patients) and experimental (MCT-rats) PH. Moreover, the accumulation and activation of MCs in the lungs contribute to the development of PH in MCT-rats. Our findings reveal an important pathophysiological insight into the role of MCs in the pathogenesis of PH in MCT- rats.

Published
2011
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9. Diacylglycerol regulates acute hypoxic pulmonary vasoconstriction via TRPC6

Author

Grimminger Friedrich, Seeger Werner, Schermuly Ralph T, Ghofrani Hossein A, Rupp Markus, Fuchs Beate, Gudermann Thomas, Dietrich Alexander, and Weissmann Norbert

Subjects
Diseases of the respiratory system, RC705-779
Abstract

Abstract Background Hypoxic pulmonary vasoconstriction (HPV) is an essential mechanism of the lung that matches blood perfusion to alveolar ventilation to optimize gas exchange. Recently we have demonstrated that acute but not sustained HPV is critically dependent on the classical transient receptor potential 6 (TRPC6) channel. However, the mechanism of TRPC6 activation during acute HPV remains elusive. We hypothesize that a diacylglycerol (DAG)-dependent activation of TRPC6 regulates acute HPV. Methods We investigated the effect of the DAG analog 1-oleoyl-2-acetyl-sn-glycerol (OAG) on normoxic vascular tone in isolated perfused and ventilated mouse lungs from TRPC6-deficient and wild-type mice. Moreover, the effects of OAG, the DAG kinase inhibitor R59949 and the phospholipase C inhibitor U73122 on the strength of HPV were investigated compared to those on non-hypoxia-induced vasoconstriction elicited by the thromboxane mimeticum U46619. Results OAG increased normoxic vascular tone in lungs from wild-type mice, but not in lungs from TRPC6-deficient mice. Under conditions of repetitive hypoxic ventilation, OAG as well as R59949 dose-dependently attenuated the strength of acute HPV whereas U46619-induced vasoconstrictions were not reduced. Like OAG, R59949 mimicked HPV, since it induced a dose-dependent vasoconstriction during normoxic ventilation. In contrast, U73122, a blocker of DAG synthesis, inhibited acute HPV whereas U73343, the inactive form of U73122, had no effect on HPV. Conclusion These findings support the conclusion that the TRPC6-dependency of acute HPV is induced via DAG.

Published
2011
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10. Phosphodiesterase 6 subunits are expressed and altered in idiopathic pulmonary fibrosis

Author

Klepetko Walter, Eickelberg Oliver, Konigshoff Melanie, Ghofrani Hossein A, Weissmann Norbert, Savai Rajkumar, Guenther Andreas, Nikolova Sevdalina, Voswinckel Robert, Seeger Werner, Grimminger Friedrich, Schermuly Ralph T, and Pullamsetti Soni S

Subjects
Diseases of the respiratory system, RC705-779
Abstract

Abstract Background Idiopathic Pulmonary Fibrosis (IPF) is an unresolved clinical issue. Phosphodiesterases (PDEs) are known therapeutic targets for various proliferative lung diseases. Lung PDE6 expression and function has received little or no attention. The present study aimed to characterize (i) PDE6 subunits expression in human lung, (ii) PDE6 subunits expression and alteration in IPF and (iii) functionality of the specific PDE6D subunit in alveolar epithelial cells (AECs). Methodology/Principal Findings PDE6 subunits expression in transplant donor (n = 6) and IPF (n = 6) lungs was demonstrated by real-time quantitative (q)RT-PCR and immunoblotting analysis. PDE6D mRNA and protein levels and PDE6G/H protein levels were significantly down-regulated in the IPF lungs. Immunohistochemical analysis showed alveolar epithelial localization of the PDE6 subunits. This was confirmed by qRT-PCR from human primary alveolar type (AT)II cells, demonstrating the down-regulation pattern of PDE6D in IPF-derived ATII cells. In vitro, PDE6D protein depletion was provoked by transforming growth factor (TGF)-β1 in A549 AECs. PDE6D siRNA-mediated knockdown and an ectopic expression of PDE6D modified the proliferation rate of A549 AECs. These effects were mediated by increased intracellular cGMP levels and decreased ERK phosphorylation. Conclusions/Significance Collectively, we report previously unrecognized PDE6 expression in human lungs, significant alterations of the PDE6D and PDE6G/H subunits in IPF lungs and characterize the functional role of PDE6D in AEC proliferation.

Published
2010
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11. Nebulization of the acidified sodium nitrite formulation attenuates acute hypoxic pulmonary vasoconstriction

Author

Surber Mark W, Hoglen Niel C, Elliott Garry T, Dahal Bhola K, Schermuly Ralph T, Egemnazarov Bakytbek, Weissmann Norbert, Grimminger Friedrich, Seeger Werner, and Ghofrani Hossein A

Subjects
Diseases of the respiratory system, RC705-779
Abstract

Abstract Background Generalized hypoxic pulmonary vasoconstriction (HPV) occurring during exposure to hypoxia is a detrimental process resulting in an increase in lung vascular resistance. Nebulization of sodium nitrite has been shown to inhibit HPV. The aim of this project was to investigate and compare the effects of nebulization of nitrite and different formulations of acidified sodium nitrite on acute HPV. Methods Ex vivo isolated rabbit lungs perfused with erythrocytes in Krebs-Henseleit buffer (adjusted to 10% hematocrit) and in vivo anesthetized catheterized rabbits were challenged with periods of hypoxic ventilation alternating with periods of normoxic ventilation. After baseline hypoxic challenges, vehicle, sodium nitrite or acidified sodium nitrite was delivered via nebulization. In the ex vivo model, pulmonary arterial pressure and nitric oxide concentrations in exhaled gas were monitored. Nitrite and nitrite/nitrate were measured in samples of perfusion buffer. Pulmonary arterial pressure, systemic arterial pressure, cardiac output and blood gases were monitored in the in vivo model. Results In the ex vivo model, nitrite nebulization attenuated HPV and increased nitric oxide concentrations in exhaled gas and nitrite concentrations in the perfusate. The acidified forms of sodium nitrite induced higher levels of nitric oxide in exhaled gas and had longer vasodilating effects compared to nitrite alone. All nitrite formulations increased concentrations of circulating nitrite to the same degree. In the in vivo model, inhaled nitrite inhibited HPV, while pulmonary arterial pressure, cardiac output and blood gases were not affected. All nitrite formulations had similar potency to inhibit HPV. The tested concentration of appeared tolerable. Conclusion Nitrite alone and in acidified forms effectively and similarly attenuates HPV. However, acidified nitrite formulations induce a more pronounced increase in nitric oxide exhalation.

Published
2010
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12. Effects of phosphodiesterase 4 inhibition on bleomycin-induced pulmonary fibrosis in mice

Author

Ghofrani Hossein A, Weissmann Norbert, Al-tamari Hamza M, Pullamsetti Soni S, Dumitrascu Rio, Udalov Sergey, Guenther Andreas, Voswinckel Robert, Seeger Werner, Grimminger Friedrich, and Schermuly Ralph T

Subjects
Diseases of the respiratory system, RC705-779
Abstract

Abstract Background Pulmonary fibrosis (PF) is a group of devastating and largely irreversible diseases. Phosphodiesterase (PDE) 4 is involved in the processes of remodeling and inflammation, which play key role in tissue fibrosis. The aim of the study was, therefore, to investigate the effect of PDE4 inhibition in experimental model of PF. Methods PF was induced in C57BL/6N mice by instillation of bleomycin. Pharmacological inhibition of PDE4 was achieved by using cilomilast, a selective PDE4 inhibitor. Changes in either lung inflammation or remodeling were evaluated at different stages of experimental PF. Lung inflammation was assessed by bronchoalveolar lavage fluid (BALF) differential cell count and reverse transcription quantitative polymerase chain reaction (RT-qPCR) for inflammatory cytokines. Changes in tissue remodeling were evaluated by pulmonary compliance measurement, quantified pathological examination, measurement of collagen deposition and RT-qPCR for late remodeling markers. Survival in all groups was analyzed as well. Results PDE4 inhibition significantly reduced the total number of alveolar inflammatory cells in BALF of mice with bleomycin-induced PF at early fibrosis stage (days 4 and 7). Number of macrophages and lymphocytes, but not neutrophils, was significantly reduced as well. Treatment decreased lung tumor necrosis factor (TNF)-α mRNA level and increased mRNA level of interleukin (IL)-6 but did not influence IL-1β. At later stage (days 14 and 24) cilomilast improved lung function, which was shown by increase in lung compliance. It also lowered fibrosis degree, as was shown by quantified pathological examination of Hematoxilin-Eosin stained lung sections. Cilomilast had no significant effect on the expression of late remodeling markers such as transforming growth factor (TGF)-β1 and collagen type Ia1 (COL(I)α1). However, it tended to restore the level of lung collagen, assessed by SIRCOL assay and Masson's trichrome staining, and to improve the overall survival. Conclusions Selective PDE4 inhibition suppresses early inflammatory stage and attenuates the late stage of experimental pulmonary fibrosis.

Published
2010
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13. Characterization of a murine model of monocrotaline pyrrole-induced acute lung injury

Author

Pullamsetti Soni S, Savai Rajkumar, Weissmann Norbert, Dony Eva, Koebrich Silke, Dumitrascu Rio, Ghofrani Hossein A, Samidurai Arun, Traupe Horst, Seeger Werner, Grimminger Friedrich, and Schermuly Ralph T

Subjects
Diseases of the respiratory system, RC705-779
Abstract

Abstract Background New animal models of chronic pulmonary hypertension in mice are needed. The injection of monocrotaline is an established model of pulmonary hypertension in rats. The aim of this study was to establish a murine model of pulmonary hypertension by injection of the active metabolite, monocrotaline pyrrole. Methods Survival studies, computed tomographic scanning, histology, bronchoalveolar lavage were performed, and arterial blood gases and hemodynamics were measured in animals which received an intravenous injection of different doses of monocrotaline pyrrole. Results Monocrotaline pyrrole induced pulmonary hypertension in Sprague Dawley rats. When injected into mice, monocrotaline pyrrole induced dose-dependant mortality in C57Bl6/N and BALB/c mice (dose range 6–15 mg/kg bodyweight). At a dose of 10 mg/kg bodyweight, mice developed a typical early-phase acute lung injury, characterized by lung edema, neutrophil influx, hypoxemia and reduced lung compliance. In the late phase, monocrotaline pyrrole injection resulted in limited lung fibrosis and no obvious pulmonary hypertension. Conclusion Monocrotaline and monocrotaline pyrrole pneumotoxicity substantially differs between the animal species.

Published
2008
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14. Iloprost-induced desensitization of the prostacyclin receptor in isolated rabbit lungs

Author

Schrör Karsten, Nilius Sigrid M, Grimminger Friedrich, Ghofrani Hossein A, Weissmann Norbert, Breitenbach Susanne C, Pullamsetti Soni S, Schermuly Ralph T, Meger-Kirchrath Jutta, Seeger Werner, and Rose Frank

Subjects
Diseases of the respiratory system, RC705-779
Abstract

Abstract Background The rapid desensitization of the human prostacyclin (IP) in response to agonist binding has been shown in cell culture. Phosphorylation of the IP receptor by protein kinase C (PKC) has been suggested to be involved in this process. Methods and results In this study we investigated the vasodilatory effects of iloprost, a stable prostacyclin analogue, in perfused rabbit lungs. Continuous infusion of the thromboxane mimetic U46619 was employed to establish stable pulmonary hypertension. A complete loss of the vasodilatory response to iloprost was observed in experiments with continuous iloprost perfusion, maintaining the intravascular concentration of this prostanoid over a 180 min period. When lungs under chronic iloprost infusion were acutely challenged with inhaled iloprost, a corresponding complete loss of vasoreactivity was observed. This desensitization was not dependent on upregulation of cAMP-specific phosphodiesterases or changes in adenylate cyclase activity, as suggested by unaltered dose-response curves to agents directly affecting these enzymes. Application of a prostaglandin E1 receptor antagonist 6-isopropoxy-9-oxoxanthene-2-carboxylic acid (AH 6809) or the PKC inhibitor bisindolylmaleimide I (BIM) enhanced the vasodilatory response to infused iloprost and partially prevented tachyphylaxis. Conclusion A three-hour infusion of iloprost in pulmonary hypertensive rabbit lungs results in complete loss of the lung vasodilatory response to this prostanoid. This rapid desensitization is apparently not linked to changes in adenylate cyclase and phosphodiesterase activation, but may involve PKC function and co-stimulation of the EP1 receptor in addition to the IP receptor by this prostacyclin analogue.

Published
2007
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15. Inhaled tolafentrine reverses pulmonary vascular remodeling via inhibition of smooth muscle cell migration

Author

Weissmann Norbert, Schudt Christian, Ghofrani Hossein, Yilmaz Hüseyin, Krick Stefanie, Pullamsetti Soni, Fuchs Beate, Seeger Werner, Grimminger Friedrich, and Schermuly Ralph

Subjects
Diseases of the respiratory system, RC705-779
Abstract

Abstract Background The aim of the study was to assess the chronic effects of combined phosphodiesterase 3/4 inhibitor tolafentrine, administered by inhalation, during monocrotaline-induced pulmonary arterial hypertension (PAH) in rats. Methods CD rats were given a single subcutaneous injection of monocrotaline to induce PAH. Four weeks after, rats were subjected to inhalation of tolafentrine or sham nebulization in an unrestrained, whole body aerosol exposure system. In these animals (i) the acute pulmonary vasodilatory efficacy of inhaled tolafentrine (ii) the anti-remodeling effect of long-term inhalation of tolafentrine (iii) the effects of tolafentrine on the expression profile of 96 genes encoding cell adhesion and extracellular matrix regulation were examined. In addition, the inhibitory effect of tolafentrine on ex vivo isolated pulmonary artery SMC cell migration was also investigated. Results Monocrotaline injection provoked severe PAH (right ventricular systolic pressure increased from 25.9 ± 4.0 to 68.9 ± 3.2 after 4 weeks and 74.9 ± 5.1 mmHg after 6 weeks), cardiac output depression and right heart hypertrophy. The media thickness of the pulmonary arteries and the proportion of muscularization of small precapillary resistance vessels increased dramatically, and the migratory response of ex-vivo isolated pulmonary artery smooth muscle cells (PASMC) was increased. Micro-arrays and subsequent confirmation with real time PCR demonstrated upregulation of several extracellular matrix regulation and adhesion genes, such as matrixmetalloproteases (MMP) 2, 8, 9, 10, 11, 12, 20, Icam, Itgax, Plat and serpinb2. When chronically nebulized from day 28 to 42 (12 daily aerosol maneuvers), after full establishment of severe pulmonary hypertension, tolafentrine reversed about 60% of all hemodynamic abnormalities, right heart hypertrophy and monocrotaline-induced structural lung vascular changes, including the proportion of pulmonary artery muscularization. The upregulation of extracellular matrix regulation and adhesion genes was reduced by nearly 80% by inhalation of the tolafentrine. When assessed in vitro, tolafentrine blocked the enhanced PASMC migratory response. Conclusion In conclusion, we demonstrate for the first time that inhalation of combined PDE3/4 inhibitor reverses pulmonary hypertension fully developed in response to monocrotaline in rats. This "reverse-remodeling" effect includes structural changes in the lung vascular wall and key molecular pathways of matrix regulation, concomitant with 60% normalization of hemodynamics.

Published
2005
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16. Lung vasodilatory response to inhaled iloprost in experimental pulmonary hypertension: amplification by different type phosphodiesterase inhibitors

Author

Weissmann Norbert, Gall Henning, Ghofrani Hossein, Inholte Christiane, Schermuly Ralph, Weidenbach Andreas, Seeger Werner, and Grimminger Friedrich

Subjects
Diseases of the respiratory system, RC705-779
Abstract

Abstract Inhaled prostanoids and phosphodiesterase (PDE) inhibitors have been suggested for treatment of severe pulmonary hypertension. In catheterized rabbits with acute pulmonary hypertension induced by continuous infusion of the stable thromboxane analogue U46619, we asked whether sildenafil (PDE1/5/6 inhibitor), motapizone (PDE3 inhibitor) or 8-Methoxymethyl-IBMX (PDE1 inhibitor) synergize with inhaled iloprost. Inhalation of iloprost caused a transient pulmonary artery pressure decline, levelling off within per se ineffective dose of each PDE inhibitor (200 μg/kg × min 8-Methoxymethyl-IBMX, 1 μg/kg × min sildenafil, 5 μg/kg × min motapizone) with subsequent iloprost nebulization, marked amplification of the prostanoid induced pulmonary vasodilatory response was noted and the area under the curve of PPA reduction was nearly threefold increased with all approaches, as compared to sole iloprost administration. Further amplification was achieved with the combination of inhaled iloprost with sildenafil plus motapizone, but not with sildenafil plus 8MM-IBMX. Systemic hemodynamics and gas exchange were not altered for all combinations. We conclude that co-administration of minute systemic doses of selective PDE inhibitors with inhaled iloprost markedly enhances and prolongs the pulmonary vasodilatory response to inhaled iloprost, with maintenance of pulmonary selectivity and ventilation perfusion matching. The prominent effect of sildenafil may be operative via both PDE1 and PDE5, and is further enhanced by co-application of a PDE3 inhibitor.

Published
2005
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17. Detection of reactive oxygen species in isolated, perfused lungs by electron spin resonance spectroscopy

Author

Schudt Christian, Schermuly Ralph T, Ghofrani Hossein A, Schütte Hartwig, Schäfer Rolf U, Tiyerili Vedat, Fuchs Beate, Kuzkaya Nermin, Weissmann Norbert, Sydykov Akylbek, Egemnazarow Bakytbek, Seeger Werner, and Grimminger Friedrich

Subjects
Diseases of the respiratory system, RC705-779
Abstract

Abstract Background The sources and measurement of reactive oxygen species (ROS) in intact organs are largely unresolved. This may be related to methodological problems associated with the techniques currently employed for ROS detection. Electron spin resonance (ESR) with spin trapping is a specific method for ROS detection, and may address some these technical problems. Methods We have established a protocol for the measurement of intravascular ROS release from isolated buffer-perfused and ventilated rabbit and mouse lungs, combining lung perfusion with the spin probe l-hydroxy-3-carboxy-2,2,5,5-tetramethylpyrrolidine (CPH) and ESR spectroscopy. We then employed this technique to characterize hypoxia-dependent ROS release, with specific attention paid to NADPH oxidase-dependent superoxide formation as a possible vasoconstrictor pathway. Results While perfusing lungs with CPH over a range of inspired oxygen concentrations (1–21 %), the rate of CP• formation exhibited an oxygen-dependence, with a minimum at 2.5 % O2. Addition of superoxide dismutase (SOD) to the buffer fluid illustrated that a minor proportion of this intravascular ROS leak was attributable to superoxide. Stimulation of the lungs by injection of phorbol-12-myristate-13-acetate (PMA) into the pulmonary artery caused a rapid increase in CP• formation, concomitant with pulmonary vasoconstriction. Both the PMA-induced CPH oxidation and the vasoconstrictor response were largely suppressed by SOD. When the PMA challenge was performed at different oxygen concentrations, maximum superoxide liberation and pulmonary vasoconstriction occurred at 5 % O2. Using a NADPH oxidase inhibitor and NADPH-oxidase deficient mice, we illustrated that the PMA-induced superoxide release was attributable to the stimulation of NADPH oxidases. Conclusion The perfusion of isolated lungs with CPH is suitable for detection of intravascular ROS release by ESR spectroscopy. We employed this technique to demonstrate that 1) PMA-induced vasoconstriction is caused "directly" by superoxide generated from NADPH oxidases and 2) this pathway is pronounced in hypoxia. NADPH oxidases thus may contribute to the hypoxia-dependent regulation of pulmonary vascular tone.

Published
2005
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18. Fibrocytes boost tumor-supportive phenotypic switches in the lung cancer niche via the endothelin system

Author

Weigert, Andreas, Zheng, Xiang, Nenzel, Alina, Turkowski, Kati, Günther, Stefan, Strack, Elisabeth, Sirait-Fischer, Evelyn, Elwakeel, Eiman, Kur, Ivan M., Nikam, Vandana S., Valasarajan, Chanil, Winter, Hauke, Wissgott, Alexander, Voswinkel, Robert, Grimminger, Friedrich, Brüne, Bernhard, Seeger, Werner, Pullamsetti, Soni Savai, and Savai, Rajkumar

Published
2022
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22. Author Correction: Deficiency of Axl aggravates pulmonary arterial hypertension via BMPR2

Author

Novoyatleva, Tatyana, Rai, Nabham, Kojonazarov, Baktybek, Veeroju, Swathi, Ben-Batalla, Isabel, Caruso, Paola, Shihan, Mazen, Presser, Nadine, Götz, Elsa, Lepper, Carina, Herpel, Sebastian, Manaud, Grégoire, Perros, Frédéric, Gall, Henning, Ghofrani, Hossein Ardeschir, Weissmann, Norbert, Grimminger, Friedrich, Wharton, John, Wilkins, Martin, Upton, Paul D., Loges, Sonja, Morrell, Nicholas W., Seeger, Werner, and Schermuly, Ralph T.

Published
2022
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24. Effects of Omega-3 Polyunsaturated Fatty Acids on the Formation of Adipokines, Cytokines, and Oxylipins in Retroperitoneal Adi-Pose Tissue of Mice.

Author

Wenderoth, Tatjana, Feldotto, Martin, Hernandez, Jessica, Schäffer, Julia, Leisengang, Stephan, Pflieger, Fabian Johannes, Bredehöft, Janne, Mayer, Konstantin, Kang, Jing X., Bier, Jens, Grimminger, Friedrich, Paßlack, Nadine, and Rummel, Christoph

Subjects
UNSATURATED fatty acids, WHITE adipose tissue, OMEGA-3 fatty acids, ARACHIDONIC acid, EICOSAPENTAENOIC acid, LIPOXINS, ADIPOKINES
Abstract

Oxylipins and specialized pro-resolving lipid mediators (SPMs) derived from polyunsaturated fatty acids (PUFAs) are mediators that coordinate an active process of inflammation resolution. While these mediators have potential as circulating biomarkers for several disease states with inflammatory components, the source of plasma oxylipins/SPMs remains a matter of debate but may involve white adipose tissue (WAT). Here, we aimed to investigate to what extent high or low omega (n)-3 PUFA enrichment affects the production of cytokines and adipokines (RT-PCR), as well as oxylipins/SPMs (liquid chromatography–tandem mass spectrometry) in the WAT of mice during lipopolysaccharide (LPS)-induced systemic inflammation (intraperitoneal injection, 2.5 mg/kg, 24 h). For this purpose, n-3 PUFA genetically enriched mice (FAT-1), which endogenously synthesize n-3 PUFAs, were compared to wild-type mice (WT) and combined with n-3 PUFA-sufficient or deficient diets. LPS-induced systemic inflammation resulted in the decreased expression of most adipokines and interleukin-6 in WAT, whereas the n-3-sufficient diet increased them compared to the deficient diet. The n-6 PUFA arachidonic acid was decreased in WAT of FAT-1 mice, while n-3 derived PUFAs (eicosapentaenoic acid, docosahexaenoic acid) and their metabolites (oxylipins/SPMs) were increased in WAT by genetic and nutritional n-3 enrichment. Several oxylipins/SPMs were increased by LPS treatment in WAT compared to PBS-treated controls in genetically n-3 enriched FAT-1 mice. Overall, we show that WAT may significantly contribute to circulating oxylipin production. Moreover, n-3-sufficient or n-3-deficient diets alter adipokine production. The precise interplay between cytokines, adipokines, and oxylipins remains to be further investigated. [ABSTRACT FROM AUTHOR]

Published
2024
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26. Comparison of contemporary risk scores in all groups of pulmonary hypertension - a PVRI GoDeep meta-registry analysis

Author

Yogeswaran, Athiththan, primary, Gall, Henning, additional, Fünderich, Meike, additional, Wilkins, Martin R., additional, Howard, Luke, additional, Kiely, David G., additional, Lawrie, Allan, additional, Hassoun, Paul M., additional, Sirenklo, Yuriy, additional, Torbas, Olena, additional, Sweatt, Andrew J., additional, Zamanian, Roham T., additional, Williams, Paul G., additional, Frauendorf, Marlize, additional, Arvanitaki, Alexandra, additional, Giannakoulas, George, additional, Saleh, Khaled, additional, Sabbour, Hani, additional, Cajigas, Hector R., additional, Frantz, Robert, additional, Al Ghouleh, Imad, additional, Chan, Stephen Y., additional, Brittain, Evan, additional, Annis, Jeffrey S., additional, Pepe, Antonella, additional, Ghio, Stefano, additional, Orfanos, Stylianos, additional, Anthi, Anastasia, additional, Majeed, Raphael W., additional, Wilhelm, Jochen, additional, Ghofrani, Hossein Ardeschir, additional, Richter, Manuel J., additional, Grimminger, Friedrich, additional, Sahay, Sandeep, additional, Tello, Khodr, additional, Seeger, Werner, additional, Antoine, Tobiah, additional, Backofen, Achim, additional, Cannon, John, additional, Damonte, Victoria, additional, Echazarreta, Diego, additional, Eichstaedt, Christina, additional, Elwing, Jean, additional, Förster, Kai, additional, Gruenig, Ekkehard, additional, Hilgendorff, Anne, additional, Jose, Arun, additional, Junaeda, Ernesto, additional, Krieb, Philipp, additional, Marquardt, Kurt, additional, Osborn, Karen, additional, Pepke-Zaba, Johanna, additional, Tilea, Ioan, additional, and Varga, Andreea, additional

Published
2024
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28. Air travel in patients suffering from pulmonary hypertension—A prospective, multicentre study.

Author

Yogeswaran, Athiththan, Grimminger, Jan, Tello, Khodr, Becker, Lukas, Seeger, Werner, Grimminger, Friedrich, Sommer, Natascha, Ghofrani, Hossein A., Lange, Tobias J., Stadler, Stefan, Olsson, Karen, Kamp, Jan C., Rosenkranz, Stephan, Gerhardt, Felix, Milger, Katrin, Barnikel, Michaela, Ulrich, Silvia, Saxer, Stéphanie, Grünig, Ekkehard, and Harutynova, Satenik

Subjects
PULMONARY arterial hypertension, AIR travel safety, ADVERSE health care events, PULMONARY hypertension, MEDICAL consultation
Abstract

The PEGASUS study is the first multicentric and prospective assessment of the safety of air travel flying in pulmonary hypertension (PH) (NCT03051763). Data of air travel from 60 patients with PH was available. No severe adverse events occurred. Nine patients self‐reported mild adverse events during flight (13%), while after landing, 12 patients reported events (20%). Solely one patient (2%) had an adverse event leading to medical consultation. In patients with PH and World Health Organization functional classes II and III, air travel was safe. [ABSTRACT FROM AUTHOR]

Published
2024
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29. Microscopic computed tomography with AI-CNN-powered image analysis: the path to phenotype bleomycin-induced lung injury.

Author

Henneke, Ingrid, Pilz, Christina, Wilhelm, Jochen, Alexopoulos, Ioannis, Ezaddoustdar, Aysan, Mukhametshina, Regina, Weissmann, Norbert, Ghofrani, Hossein Ardeschir, Grimminger, Friedrich, Seeger, Werner, Schermuly, Ralph T., Wygrecka, Malgorzata, and Kojonazarov, Baktybek

Subjects
LUNGS, COMPUTED tomography, PATH analysis (Statistics), IMAGE analysis, LUNG injuries, PHENOTYPES
Abstract

Bleomycin (BLM)-induced lung injury in mice is a valuable model for investigating the molecular mechanisms that drive inflammation and fibrosis and for evaluating potential therapeutic approaches to treat the disease. Given high variability in the BLM model, it is critical to accurately phenotype the animals in the course of an experiment. In the present study, we aimed to demonstrate the utility of microscopic computed tomography (µCT) imaging combined with an artificial intelligence (AI)-convolutional neural network (CNN)-powered lung segmentation for rapid phenotyping of BLM mice. µCT was performed in freely breathing C57BL/6J mice under isoflurane anesthesia on days 7 and 21 after BLM administration. Terminal invasive lung function measurement and histological assessment of the left lung collagen content were conducted as well. µCT image analysis demonstrated gradual and time-dependent development of lung injury as evident by alterations in the lung density, air-to-tissue volume ratio, and lung aeration in mice treated with BLM. The right and left lung were unequally affected. µCT-derived parameters such as lung density, air-to-tissue volume ratio, and nonaerated lung volume correlated well with the invasive lung function measurement and left lung collagen content. Our study demonstrates the utility of AI-CNN-powered µCT image analysis for rapid and accurate phenotyping of BLM mice in the course of disease development and progression. NEW & NOTEWORTHY: Microscopic computed tomography (µCT) imaging combined with an artificial intelligence (AI)-convolutional neural network (CNN)-powered lung segmentation is a rapid and powerful tool for noninvasive phenotyping of bleomycin mice over the course of the disease. This, in turn, allows earlier and more reliable identification of therapeutic effects of new drug candidates, ultimately leading to the reduction of unnecessary procedures in animals in pharmacological research. [ABSTRACT FROM AUTHOR]

Published
2024
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31. Data from Metastasis-Associated Protein 2 Represses NF-κB to Reduce Lung Tumor Growth and Inflammation

Author

El-Nikhely, Nefertiti, primary, Karger, Annika, primary, Sarode, Poonam, primary, Singh, Indrabahadur, primary, Weigert, Andreas, primary, Wietelmann, Astrid, primary, Stiewe, Thorsten, primary, Dammann, Reinhard, primary, Fink, Ludger, primary, Grimminger, Friedrich, primary, Barreto, Guillermo, primary, Seeger, Werner, primary, Pullamsetti, Soni S., primary, Rapp, Ulf R., primary, and Savai, Rajkumar, primary

Published
2023
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32. Supplementary Data from Metastasis-Associated Protein 2 Represses NF-κB to Reduce Lung Tumor Growth and Inflammation

Author

El-Nikhely, Nefertiti, primary, Karger, Annika, primary, Sarode, Poonam, primary, Singh, Indrabahadur, primary, Weigert, Andreas, primary, Wietelmann, Astrid, primary, Stiewe, Thorsten, primary, Dammann, Reinhard, primary, Fink, Ludger, primary, Grimminger, Friedrich, primary, Barreto, Guillermo, primary, Seeger, Werner, primary, Pullamsetti, Soni S., primary, Rapp, Ulf R., primary, and Savai, Rajkumar, primary

Published
2023
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34. Deficiency of Axl aggravates pulmonary arterial hypertension via BMPR2

Author

Novoyatleva, Tatyana, Rai, Nabham, Kojonazarov, Baktybek, Veeroju, Swathi, Ben-Batalla, Isabel, Caruso, Paola, Shihan, Mazen, Presser, Nadine, Götz, Elsa, Lepper, Carina, Herpel, Sebastian, Manaud, Grégoire, Perros, Frédéric, Gall, Henning, Ghofrani, Hossein Ardeschir, Weissmann, Norbert, Grimminger, Friedrich, Wharton, John, Wilkins, Martin, Upton, Paul D., Loges, Sonja, Morrell, Nicholas W., Seeger, Werner, and Schermuly, Ralph T.

Published
2021
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35. Microenvironmental Th9 and Th17 lymphocytes induce metastatic spreading in lung cancer

Author

Salazar, Ylia, Zheng, Xiang, Brunn, David, Raifer, Hartmann, Picard, Felix, Zhang, Yajuan, Winter, Hauke, Guenther, Stefan, Weigert, Andreas, Weigmann, Benno, Dumoutier, Laure, Renauld, Jean-Christophe, Waisman, Ari, Schmall, Anja, Tufman, Amanda, Fink, Ludger, Brune, Bernhard, Bopp, Tobias, Grimminger, Friedrich, Seeger, Werner, Pullamsetti, Soni Savai, Huber, Magdalena, and Savai, Rajkumar

Subjects
Lung cancer -- Development and progression, B cells, Cancer research, Stem cells, Cancer metastasis -- Development and progression, Health care industry
Abstract

Immune microenvironment plays a critical role in lung cancer control versus progression and metastasis. In this investigation, we explored the effect of tumor-infiltrating lymphocyte subpopulations on lung cancer biology by studying in vitro cocultures, in vivo mouse models, and human lung cancer tissue. Lymphocyte conditioned media (CM) induced epithelial-mesenchymal transition (EMT) and migration in both primary human lung cancer cells and cell lines. Correspondingly, major accumulation of Th9 and Th17 cells was detected in human lung cancer tissue and correlated with poor survival. Coculturing lung cancer cells with Th9/Th17 cells or exposing them to the respective CM induced EMT in cancer cells and modulated the expression profile of genes implicated in EMT and metastasis. These features were reproduced by the signatory cytokines IL-9 and IL-17, with gene regulatory profiles evoked by these cytokines partly overlapping and partly complementary. Coinjection of Th9/Th17 cells with tumor cells in WT, [Rag1.sup.-/-], [Il9r.sup.-/-], and [Ilra.sup.-/-] mice altered tumor growth and metastasis. Accordingly, inhibition of IL-9 or IL-17 cytokines by neutralizing antibodies decreased EMT and slowed lung cancer progression and metastasis. In conclusion, Th9 and Th17 lymphocytes induce lung cancer cell EMT, thereby promoting migration and metastatic spreading and offering potentially novel therapeutic strategies., Introduction Lung cancer is the leading cause of cancer mortality worldwide, accounting for up to 19% of all cancer-related deaths. Numbers of deaths due to lung cancer are even greater [...]

Published
2020
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36. NADPH oxidase subunit NOXO1 is a target for emphysema treatment in COPD

Author

Seimetz, Michael, Sommer, Natascha, Bednorz, Mariola, Pak, Oleg, Veith, Christine, Hadzic, Stefan, Gredic, Marija, Parajuli, Nirmal, Kojonazarov, Baktybek, Kraut, Simone, Wilhelm, Jochen, Knoepp, Fenja, Henneke, Ingrid, Pichl, Alexandra, Kanbagli, Zeki I., Scheibe, Susan, Fysikopoulos, Athanasios, Wu, Cheng-Yu, Klepetko, Walter, Jaksch, Peter, Eichstaedt, Christina, Grünig, Ekkehard, Hinderhofer, Katrin, Geiszt, Miklós, Müller, Niklas, Rezende, Flavia, Buchmann, Giulia, Wittig, Ilka, Hecker, Matthias, Hecker, Andreas, Padberg, Winfried, Dorfmüller, Peter, Gattenlöhner, Stefan, Vogelmeier, Claus F., Günther, Andreas, Karnati, Srikanth, Baumgart-Vogt, Eveline, Schermuly, Ralph T., Ghofrani, Hossein A., Seeger, Werner, Schröder, Katrin, Grimminger, Friedrich, Brandes, Ralf P., and Weissmann, Norbert

Published
2020
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37. Fibroblast growth factor 10 reverses cigarette smoke- and elastase-induced emphysema and pulmonary hypertension in mice

Author

Hadzic, Stefan, primary, Wu, Cheng-Yu, additional, Gredic, Marija, additional, Pak, Oleg, additional, Loku, Edma, additional, Kraut, Simone, additional, Kojonazarov, Baktybek, additional, Wilhelm, Jochen, additional, Brosien, Monika, additional, Bednorz, Mariola, additional, Seimetz, Michael, additional, Günther, Andreas, additional, Kosanovic, Djuro, additional, Sommer, Natascha, additional, Warburton, David, additional, Li, Xiaokun, additional, Grimminger, Friedrich, additional, Ghofrani, Hossein A., additional, Schermuly, Ralph T., additional, Seeger, Werner, additional, El Agha, Elie, additional, Bellusci, Saverio, additional, and Weissmann, Norbert, additional

Published
2023
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38. Long-term safety and outcome of intravenous treprostinil via an implanted pump in pulmonary hypertension

Author

Richter, Manuel J., Harutyunova, Satenik, Bollmann, Tom, Classen, Simon, Gall, Henning, Gerhardt, MD, Felix, Grimminger, Friedrich, Grimminger, Jan, Grünig, Ekkehard, Guth, Stefan, Halank, Michael, Heine, Alexander, Hoeper, Marius M., Klose, Hans, Lange, Tobias J., Meyer, Katrin, Neurohr, Claus, Nickolaus, Kai, Olsson, Karen M., Opitz, Christian F., Rosenkranz, Stephan, Seyfarth, Hans-Jürgen, Warnke, Christian, Wiedenroth, Christoph, Ghofrani, Hossein A., and Ewert, Ralf

Published
2018
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39. Schistosomiasis causes remodeling of pulmonary vessels in the lung in a heterogeneous localized manner: Detailed study.

Author

Kolosionek, Ewa, King, Jayne, Rollinson, David, Schermuly, Ralph Theo, Grimminger, Friedrich, Graham, Brian B, Morrell, Nicholas, and Butrous, Ghazwan

Subjects
experimental models, inflammation, pulmonary hypertension, schistosomiasis, Cardiorespiratory Medicine and Haematology
Abstract

Schistosomiasis is a global parasitic disease with high impact on public health in tropical areas. Schistosomiasis is a well-described cause of pulmonary arterial hypertension (PAH). The exact pathogenesis is still unclear, though inflammatory mechanisms are suspected. Another unknown is whether the changes in the pulmonary vasculature are generalized or localized. We studied 13 mice infected with cercariae for 12 weeks compared with 10 control mice. In our model, we observed that the liver was a target during infection and was enlarged more than two-fold after infection. However, right heart hypertrophy as measured by RV/(LV + S) ratio was not observed at this time point. Moreover, we noticed that 72% of the sampled lobes (92% of the lungs) harvested from these animals costained evidence of granulomatous changes, secondary to egg deposition. We systemically mapped the distribution of granulomatous lesions in right lung lobes (n = 43) of infected mice. We observed that the distribution of the granulomatous lesions was heterogeneous. Remodeled pulmonary vessels were seen in 26% of the lobes (46% of the lungs) and were observed only in close proximity to the granuloma. No remodeling was observed in the absence of granulomas. These findings support the view that pulmonary vascular remodeling is caused by the local presence of granulomas in PAH associated with schistosomiasis. The heterogeneous nature of the remodeling partly explains why many patients with schistosomiasis do not develop pulmonary hypertension.

Published
2013

40. Case Report: Durable therapy response to Osimertinib in rare EGFR Exon 18 mutated NSCLC

Author

Cekay, Michael, primary, Arndt, Philipp F., additional, Dumitrascu, Rio, additional, Savai, Rajkumar, additional, Braeuninger, Andreas, additional, Gattenloehner, Stefan, additional, Steiner, Dagmar, additional, Roller, Fritz, additional, Tello, Khodr, additional, Hattar, Katja, additional, Seeger, Werner, additional, Sibelius, Ulf, additional, Grimminger, Friedrich, additional, and Eul, Bastian, additional

Published
2023
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41. ADPGK‐AS1 long noncoding RNA switches macrophage metabolic and phenotypic state to promote lung cancer growth

Author

Karger, Annika, primary, Mansouri, Siavash, additional, Leisegang, Matthias S, additional, Weigert, Andreas, additional, Günther, Stefan, additional, Kuenne, Carsten, additional, Wittig, Ilka, additional, Zukunft, Sven, additional, Klatt, Stephan, additional, Aliraj, Blerina, additional, Klotz, Laura V, additional, Winter, Hauke, additional, Mahavadi, Poornima, additional, Fleming, Ingrid, additional, Ruppert, Clemens, additional, Witte, Biruta, additional, Alkoudmani, Ibrahim, additional, Gattenlöhner, Stefan, additional, Grimminger, Friedrich, additional, Seeger, Werner, additional, Pullamsetti, Soni Savai, additional, and Savai, Rajkumar, additional

Published
2023
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43. Macitentan for the treatment of inoperable chronic thromboembolic pulmonary hypertension (MERIT-1): results from the multicentre, phase 2, randomised, double-blind, placebo-controlled study

Author

Ghofrani, Hossein-Ardeschir, Simonneau, Gérald, D'Armini, Andrea M, Fedullo, Peter, Howard, Luke S, Jaïs, Xavier, Jenkins, David P, Jing, Zhi-Cheng, Madani, Michael M, Martin, Nicolas, Mayer, Eckhard, Papadakis, Kelly, Richard, Dominik, Kim, Nick H, Lang, Irene, Kähler, Christian, Delcroix, Marion, Bshouty, Zoheir, Sepulveda Varela, Pablo, Jing, Zhi-Cheng, Yang, Yuanhua, Liu, Jinming, Zhang, Gangcheng, Zhang, Nuofu, Mi, Yuhong, Zhu, Xianyang, Jansa, Pavel, Jaïs, Xavier, Prévot, Grégoire, Bouvaist, Hélène, Sanchez, Olivier, Grimminger, Friedrich, Held, Matthias, Wilkens, Heinrike, Rosenkranz, Stephan, Grünig, Ekkehard, Karlócai, Kristóf, Temesvári, András, Edes, Istvan, Aidietienė, Sigita, Miliauskas, Skaidrius, Pulido Zamudio, Tomas Rene, Jerjes Sanchez, Carlos, Vonk Noordegraaf, Anton, Lewczuk, Jerzy, Podolec, Piotr, Kasprzak, Jarosław, Mularek-Kubzdela, Tatiana, Grzywna, Ryszard, Dheda, Keertan, Moiseeva, Olga, Chernyavskiy, Alexander, Shipulin, Vladimir, Barbarash, Olga, Martynyuk, Tamila, Kim, Hyung-Kwan, Park, Jun-Bean, Lee, Jae Seung, Speich, Rudolf, Ulrich, Silvia, Aubert, John-David, Phrommintikul, Arintaya, Jaimchariyatam, Nattapong, Sompradeekul, Suree, Onen, Zeynep Pinar, Okumus, Gulfer, Solovey, Lyubomyr, Gavrysyuk, Volodymyr, Howard, Luke, Pepke-Zaba, Joanna, Condliffe, Robin, McConnell, John, Kerr, Kim, Nguyen, Lan Hieu, and Pham, Nguyen Vinh

Abstract

Macitentan is beneficial for long-term treatment of pulmonary arterial hypertension. The microvasculopathy of chronic thromboembolic pulmonary hypertension (CTEPH) and pulmonary arterial hypertension are similar.

Published
2024
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47. CEACAM6 as a Novel Therapeutic Target to Boost HO-1-mediated Antioxidant Defense in COPD

Author

Wu, Cheng-Yu, primary, Cilic, Anis, additional, Pak, Oleg, additional, Dartsch, Ruth Charlotte, additional, Wilhelm, Jochen, additional, Wujak, Magdalena, additional, Lo, Kevin, additional, Brosien, Monika, additional, Zhang, Ruoyu, additional, Alkoudmani, Ibrahim, additional, Witte, Biruta, additional, Pedersen, Frauke, additional, Watz, Henrik, additional, Voswinckel, Robert, additional, Günther, Andreas, additional, Ghofrani, Hossein A, additional, Brandes, Ralf P, additional, Schermuly, Ralph T, additional, Grimminger, Friedrich, additional, Seeger, Werner, additional, Sommer, Natascha, additional, Weissmann, Norbert, additional, and Hadzic, Stefan, additional

Published
2023
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48. The HDAC2-SP1 axis orchestrates pro-tumor macrophage polarization

Author

Zheng, Xiang, primary, Sarode, Poonam, additional, Weigert, Andreas, additional, Turkowski, Kati, additional, Chelladurai, Prakash, additional, Günther, Stefan, additional, Kuenne, Carsten, additional, Winter, Hauke, additional, Stenzinger, Albrecht, additional, Reu, Simone, additional, Grimminger, Friedrich, additional, Stiewe, Thorsten, additional, Seeger, Werner, additional, Pullamsetti, Soni Savai., additional, and Savai, Rajkumar, additional

Published
2023
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49. Estimated plasma volume status: association with congestion, cardiorenal syndrome and prognosis in precapillary pulmonary hypertension

Author

Yogeswaran, Athiththan, primary, Richter, Manuel J., additional, Husain-Syed, Faeq, additional, Rako, Zvonimir, additional, Sommer, Natascha, additional, Grimminger, Friedrich, additional, Seeger, Werner, additional, Ghofrani, Hossein Ardeschir, additional, Gall, Henning, additional, and Tello, Khodr, additional

Published
2023
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50. Nicotine promotes e-cigarette vapour-induced lung inflammation and structural alterations

Author

Roxlau, Elsa T., primary, Pak, Oleg, additional, Hadzic, Stefan, additional, Garcia-Castro, Claudia F., additional, Gredic, Marija, additional, Wu, Cheng-Yu, additional, Schäffer, Julia, additional, Selvakumar, Balachandar, additional, Pichl, Alexandra, additional, Spiegelberg, David, additional, Deutscher, Janik, additional, Bednorz, Mariola, additional, Schäfer, Katharina, additional, Kraut, Simone, additional, Kosanovic, Djuro, additional, Zeidan, Esraa M, additional, Kojonazarov, Baktybek, additional, Herold, Susanne, additional, Strielkov, Ievgen, additional, Guenther, Andreas, additional, Wilhelm, Jochen, additional, Khalifa, Mohamed M. A., additional, Taye, Ashraf, additional, Brandes, Ralf P., additional, Hecker, Matthias, additional, Grimminger, Friedrich, additional, Ghofrani, Hossein A., additional, Schermuly, Ralph T., additional, Seeger, Werner, additional, Sommer, Natascha, additional, and Weissmann, Norbert, additional

Published
2023
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