Your search keyword '"Daalhuisen J"' showing total 3 results

1. Pharmacological targeting of protease-activated receptor 2 affords protection from bleomycin-induced pulmonary fibrosis

Author

Lin, C. (Cong), Thusen, J.H. (Jan) von der, Daalhuisen, J. (Joost), Ten Brink, M. (Marieke), Crestani, B. (Bruno), Poll, T. (Tom) van der, Borensztajn, K. (Keren), Arnold Spek, C. (C.), Lin, C. (Cong), Thusen, J.H. (Jan) von der, Daalhuisen, J. (Joost), Ten Brink, M. (Marieke), Crestani, B. (Bruno), Poll, T. (Tom) van der, Borensztajn, K. (Keren), and Arnold Spek, C. (C.)

Abstract

Idiopathic pulmonary fibrosis is the most devastating diffuse fibrosing lung disease that remains refractory to therapy. Despite increasing evidence that protease-activated receptor 2 (PAR-2) contributes to fibrosis, its importance in pulmonary fibrosis is under debate. We addressed whether PAR-2 deficiency persistently reduces bleomycin-induced pulmonary fibrosis or merely delays disease progression and whether pharmacological PAR-2 inhibition limits experimental pulmonary fibrosis. Bleomycin was instilled intranasally into wild-type or PAR-2-deficient mice in the presence/absence of a specific PAR-2 antagonist (P2pal-18S). Pulmonary fibrosis was consistently reduced in PAR-2-deficient mice throughout the fibrotic phase, as evident from reduced Ashcroft scores (29%) and hydroxyproline levels (26%) at d 28. Moreover, P2pal-18S inhibited PAR-2-induced profibrotic responses in both murine and primary human pulmonary fibroblasts (p < 0.05). Once daily treatment with P2pal-18S reduced the severity and extent of fibrotic lesions in lungs of bleomycin-treated wild-type mice but did not further reduce fibrosis in PAR-2-deficient mice. Importantly, P2pal-18S treatment starting even 7 d after the onset of fibrosis limits pulmonary fibrosis as effectively as when treatment was started together with bleomycin instillation. Overall, PAR-2 contributes to the progression of pulmonary fibrosis, and targeting PAR-2 may be a promising therapeutic strategy for treating pulmonary fibrosis.

Published

2015

2. Pharmacological Targeting of Protease-Activated Receptor 2 Affords Protection from Bleomycin-Induced Pulmonary Fibrosis

Author

Lin, C, von der Thusen, J, Daalhuisen, J, ten Brink, M (Mirian), Crestani, B, van der Poll, T, Borensztajn, K, Spek, CA, Lin, C, von der Thusen, J, Daalhuisen, J, ten Brink, M (Mirian), Crestani, B, van der Poll, T, Borensztajn, K, and Spek, CA

Abstract

Idiopathic pulmonary fibrosis is the most devastating diffuse fibrosing lung disease that remains refractory to therapy. Despite increasing evidence that protease-activated receptor 2 (PAR-2) contributes to fibrosis, its importance in pulmonary fibrosis is under debate. We addressed whether PAR-2 deficiency persistently reduces bleomycin-induced pulmonary fibrosis or merely delays disease progression and whether pharmacological PAR-2 inhibition limits experimental pulmonary fibrosis. Bleomycin was instilled intranasally into wild-type or PAR-2-deficient mice in the presence/absence of a specific PAR-2 antagonist (P2pal-18S). Pulmonary fibrosis was consistently reduced in PAR-2-deficient mice throughout the fibrotic phase, as evident from reduced Ashcroft scores (29%) and hydroxyproline levels (26%) at d 28. Moreover, P2pal-18S inhibited PAR-2-induced profibrotic responses in both murine and primary human pulmonary fibroblasts (p < 0.05). Once daily treatment with P2pal-18S reduced the severity and extent of fibrotic lesions in lungs of bleomycin-treated wild-type mice but did not further reduce fibrosis in PAR-2-deficient mice. Importantly, P2pal-18S treatment starting even 7 d after the onset of fibrosis limits pulmonary fibrosis as effectively as when treatment was started together with bleomycin instillation. Overall, PAR-2 contributes to the progression of pulmonary fibrosis, and targeting PAR-2 may be a promising therapeutic strategy for treating pulmonary fibrosis.

Published

2015

3. Protease-activated receptor-2 induces myofibroblast differentiation and tissue factor up-regulation during bleomycin-induced lung injury: Potential role in pulmonary fibrosis

Author

Borensztajn, K. (Keren), Bresser, P. (Paul), Loos, C.M. (Chris) van der, Bot, I. (Ilze), Blink, B. (Bernt) van den, Bakker, M.A. (Michael) den, Daalhuisen, J. (Joost), Groot, A.P. (Angelique), Peppelenbosch, M.P. (Maikel), Thusen, J.H. (Jan) von der, Spek, C.A. (Arnold), Borensztajn, K. (Keren), Bresser, P. (Paul), Loos, C.M. (Chris) van der, Bot, I. (Ilze), Blink, B. (Bernt) van den, Bakker, M.A. (Michael) den, Daalhuisen, J. (Joost), Groot, A.P. (Angelique), Peppelenbosch, M.P. (Maikel), Thusen, J.H. (Jan) von der, and Spek, C.A. (Arnold)

Abstract

Idiopathic pulmonary fibrosis constitutes the most devastating form of fibrotic lung disorders and remains refractory to current therapies. The coagulation cascade is frequently activated during pulmonary fibrosis, but this observation has so far resisted a mechanistic explanation. Recent data suggest that protease-activated receptor (PAR)-2, a receptor activated by (among others) coagulation factor (F)Xa, plays a key role in fibrotic disease; consequently, we assessed the role of PAR-2 in the development of pulmonary fibrosis in this study.

Published

2010