Your search keyword '"Distler, J. H. W."' showing total 12 results

1. Stiff skin syndrome: evidence for an inflammation-independent fibrosis?

Author

Guiducci, S, Distler, J H W, Milia, A F, Miniati, I, Rogai, V, Manetti, M, Falcini, F, Ibba-Manneschi, L, Gay, S, Distler, O, Matucci-Cerinic, M, Guiducci, S, Distler, J H W, Milia, A F, Miniati, I, Rogai, V, Manetti, M, Falcini, F, Ibba-Manneschi, L, Gay, S, Distler, O, and Matucci-Cerinic, M

Abstract

Objectives. Stiff skin syndrome (SSS) is a rare scleroderma-like syndrome of unknown aetiology. A 16-year-old boy presented with thoracic and abdominal asymmetry, and 'orange peel' cutaneous lesions, with fibrotic stone-hard indurations at the buttocks, thighs and arms leading to secondary joint contractures of the extremities. Our aim was to analyse the expression of extracellular matrix (ECM) molecules and pro-fibrotic cytokines in the dermis and epidermis of SSS. Methods. The diagnosis of SSS was confirmed by clinical and histopathological examination. Collagen type 1 alpha-2 chain (Col1A2), fibronectin-1, thrombospondin-1, TGF-beta, connective tissue growth factor (CTGF), IL-6, -1beta, ET-1, Fibroblast growth factor receptor 3 (FGFR-3) and MCP-1 expression was analysed in SSS and age- and sex-matched healthy control skin by real-time PCR. VEGF expression was also studied. Results. Histopathological examination showed flattened dermal papillae, a scarce presence of sub-epidermal microvessels and mild dermal fibrosis, but no inflammatory infiltrates. In the SSS dermis, the expression of IL-1beta, -6 and MCP-1 was low, whereas VEGF was intensively expressed. No differences were observed for TGF-beta, CTGF and ET-1. In contrast, col1A2, fibronectin-1 and thrombospondin-1 were overexpressed in the SSS dermis. Conclusion. In our SSS patient, an overexpression of ECM proteins was detected, whereas no inflammatory infiltrates or up-regulation of pro-fibrotic cytokines were found. The data suggest that fibrosis in SSS might be independent from inflammation.

Published

2009

2. Monocyte chemoattractant proteins in the pathogenesis of systemic sclerosis

Author

Distler, J H W, Akhmetshina, A, Schett, G, Distler, O, Distler, J H W, Akhmetshina, A, Schett, G, and Distler, O

Abstract

Activation of the immune system and increased synthesis of extracellular matrix proteins by fibroblasts are hallmarks in the pathogenesis of SSc. The molecular mechanisms underlying the infiltration of inflammatory cells into the skin and the subsequent activation of fibroblasts are still largely unknown. Chemokines are a family of small molecules that are classified according to the position of the NH(2)-terminal cysteine motif. Recent data indicate that chemokines and in particular two members of the subfamily of monocyte chemoattractant proteins, MCP-1 (CCL-2) and MCP-3 (CCL-7), might be involved in the pathogenesis of SSc. MCP-1 and -3 are overexpressed by SSc fibroblasts and in skin lesions from SSc patients compared to healthy controls. MCP-1 and -3 are chemotactic for inflammatory cells and stimulate their migration into the skin. In addition to their pro-inflammatory effects, MCP-1 and -3 contribute to tissue fibrosis by activating the synthesis of extracellular matrix proteins in SSc fibroblasts. Therapeutic strategies targeting MCP-1 have revealed promising results in several animal models of SSc. Antagonists against the receptor CCR2 are currently tested in clinical trials of a variety of diseases and also represent interesting candidates for target-directed therapy in SSc.

Published

2009

3. Mechanisms of vascular damage in SSc--implications for vascular treatment strategies

Author

Guiducci, S, Distler, O, Distler, J H W, Matucci-Cerinic, M, Guiducci, S, Distler, O, Distler, J H W, and Matucci-Cerinic, M

Abstract

Vascular abnormalities are a major component of SSc, but little is known about the events or mechanisms that initiate vascular injury and prevent its repair. In SSc, angiogenesis is incomplete or lacking despite the increased expression of a large array of pro-angiogenic factors such as VEGF. Conflicting results have recently been published concerning the presence and role of vasculogenesis and circulating endothelial progenitor cells in SSc. It remains to be established if these endothelial progenitor cells are a marker of endothelial disease or a cause of insufficient vascular repair. Human mesenchymal stem cells (MSCs) may be an alternative source for endothelial progenitor cells, and it has been observed that the angiogenic potential of endothelial-like MSCs is reduced. Other mechanisms of vascular damage include oxidative stress and factors released from activated platelets. In addition, growth factors such as ET-1 and PDGF induce proliferation of vascular smooth muscle cells resulting in intimal thickening. For the development of new therapeutic strategies, it is important to realize that the different vascular pathologies—uncompensated loss of capillaries on one hand and vascular remodelling with a proliferative vasculopathy on the other—might require different treatment approaches

Published

2008

4. Imatinib as a novel therapeutic approach for fibrotic disorders

Author

Distler, J H W, Distler, O, Distler, J H W, and Distler, O

Published

2008

5. Criteria to select molecular targets for anti-fibrotic therapy

Author

Distler, J H W, Distler, O, Distler, J H W, and Distler, O

Abstract

Tissue fibrosis is a major cause of morbidity and mortality in SSc. An increasing number of promising molecular targets for anti-fibrotic therapies have been described recently. However, the number of patients eligible for clinical trials is limited in SSc. The present article discusses criteria to select the most promising molecular targets for clinical trials in SSc. Based on consensus among experts, important criteria for the selection of molecular-based therapies were as follows: First, there should be strong experimental evidence that targeting the molecule of interest inhibits fibrosis. Optimally, the anti-fibrotic effects should be confirmed in at least two complementary animal models of SSc. Second, inhibitors of the molecule of interest should be clinically available. Third, clinical experience with the drug of interest in other diseases hastens the initiation of clinical trials and reduces the risk of unexpected side-effects. Finally, funding for clinical trials with the drug of interest in SSc should be available. We propose that the priority of novel targets for evaluation in clinical trials in SSc might be selected based on these consensus criteria

Published

2008

6. Intracellular tyrosine kinases as novel targets for anti-fibrotic therapy in systemic sclerosis

Author

Distler, J H W, Distler, O, Distler, J H W, and Distler, O

Abstract

Tissue fibrosis is a major cause of death in SSc, but therapies that target selectively fibrosis are not yet available for routine clinical use. Recent pre-clinical studies suggest that selective tyrosine kinase inhibitors that target c-Abl, PDGF receptor or Src kinases might be promising targets for anti-fibrotic approaches. Dual inhibition of c-Abl and PDGF receptor by imatinib and nilotinib, and inhibition of Src kinases either selectively by SU6656 or in combination with c-Abl and PDGF by dasatinib exerted potent anti-fibrotic effects. Imatinib, nilotinib, dasatinib and SU6656 reduced dose-dependently the synthesis of extracellular matrix protein in human dermal fibroblasts in vitro and prevented fibrosis in the mouse model of bleomycin-induced skin fibrosis. Clinical data from patients with chronic myelogenous leukaemia suggest that imatinib, nilotinib and dasatinib are well tolerated. Based on the promising pre-clinical data, imatinib is currently evaluated in clinical trials for the treatment of fibrosis in SSc and trials with other tyrosine kinase inhibitors are in preparation

Published

2008

7. Monocyte chemoattractant proteins in the pathogenesis of systemic sclerosis.

Author

Distler JH, Akhmetshina A, Schett G, and Distler O

Subjects

Animals, Chemokines immunology, Chemotaxis, Leukocyte, Extracellular Matrix Proteins biosynthesis, Fibroblasts metabolism, Humans, Models, Animal, Receptors, Chemokine metabolism, Scleroderma, Systemic immunology, Scleroderma, Systemic metabolism, Skin immunology, Skin metabolism, Skin pathology, Monocyte Chemoattractant Proteins physiology, Scleroderma, Systemic etiology

Abstract

Activation of the immune system and increased synthesis of extracellular matrix proteins by fibroblasts are hallmarks in the pathogenesis of SSc. The molecular mechanisms underlying the infiltration of inflammatory cells into the skin and the subsequent activation of fibroblasts are still largely unknown. Chemokines are a family of small molecules that are classified according to the position of the NH(2)-terminal cysteine motif. Recent data indicate that chemokines and in particular two members of the subfamily of monocyte chemoattractant proteins, MCP-1 (CCL-2) and MCP-3 (CCL-7), might be involved in the pathogenesis of SSc. MCP-1 and -3 are overexpressed by SSc fibroblasts and in skin lesions from SSc patients compared to healthy controls. MCP-1 and -3 are chemotactic for inflammatory cells and stimulate their migration into the skin. In addition to their pro-inflammatory effects, MCP-1 and -3 contribute to tissue fibrosis by activating the synthesis of extracellular matrix proteins in SSc fibroblasts. Therapeutic strategies targeting MCP-1 have revealed promising results in several animal models of SSc. Antagonists against the receptor CCR2 are currently tested in clinical trials of a variety of diseases and also represent interesting candidates for target-directed therapy in SSc.

Published

2009

8. Imatinib as a novel therapeutic approach for fibrotic disorders.

Author

Distler JH and Distler O

Subjects

Benzamides, Drug Evaluation, Preclinical, Fibrosis, Humans, Imatinib Mesylate, Treatment Outcome, Piperazines therapeutic use, Protein Kinase Inhibitors therapeutic use, Pulmonary Fibrosis drug therapy, Pyrimidines therapeutic use

Published

2009

9. Criteria to select molecular targets for anti-fibrotic therapy.

Author

Distler JH and Distler O

Subjects

Animals, Clinical Trials as Topic, Drug Costs, Fibrosis drug therapy, Humans, Models, Animal, Research Design, Scleroderma, Systemic metabolism, Scleroderma, Systemic pathology, Skin metabolism, Skin pathology, Scleroderma, Systemic drug therapy

Abstract

Tissue fibrosis is a major cause of morbidity and mortality in SSc. An increasing number of promising molecular targets for anti-fibrotic therapies have been described recently. However, the number of patients eligible for clinical trials is limited in SSc. The present article discusses criteria to select the most promising molecular targets for clinical trials in SSc. Based on consensus among experts, important criteria for the selection of molecular-based therapies were as follows: First, there should be strong experimental evidence that targeting the molecule of interest inhibits fibrosis. Optimally, the anti-fibrotic effects should be confirmed in at least two complementary animal models of SSc. Second, inhibitors of the molecule of interest should be clinically available. Third, clinical experience with the drug of interest in other diseases hastens the initiation of clinical trials and reduces the risk of unexpected side-effects. Finally, funding for clinical trials with the drug of interest in SSc should be available. We propose that the priority of novel targets for evaluation in clinical trials in SSc might be selected based on these consensus criteria.

Published

2008

10. Intracellular tyrosine kinases as novel targets for anti-fibrotic therapy in systemic sclerosis.

Author

Distler JH and Distler O

Subjects

Animals, Benzamides, Clinical Trials as Topic, Dasatinib, Fibrosis, Humans, Imatinib Mesylate, Indoles therapeutic use, Scleroderma, Systemic enzymology, Skin enzymology, Sulfonamides therapeutic use, Thiazoles therapeutic use, Piperazines therapeutic use, Protein Kinase Inhibitors therapeutic use, Proto-Oncogene Proteins c-abl antagonists & inhibitors, Pyrimidines therapeutic use, Scleroderma, Systemic drug therapy

Abstract

Tissue fibrosis is a major cause of death in SSc, but therapies that target selectively fibrosis are not yet available for routine clinical use. Recent pre-clinical studies suggest that selective tyrosine kinase inhibitors that target c-Abl, PDGF receptor or Src kinases might be promising targets for anti-fibrotic approaches. Dual inhibition of c-Abl and PDGF receptor by imatinib and nilotinib, and inhibition of Src kinases either selectively by SU6656 or in combination with c-Abl and PDGF by dasatinib exerted potent anti-fibrotic effects. Imatinib, nilotinib, dasatinib and SU6656 reduced dose-dependently the synthesis of extracellular matrix protein in human dermal fibroblasts in vitro and prevented fibrosis in the mouse model of bleomycin-induced skin fibrosis. Clinical data from patients with chronic myelogenous leukaemia suggest that imatinib, nilotinib and dasatinib are well tolerated. Based on the promising pre-clinical data, imatinib is currently evaluated in clinical trials for the treatment of fibrosis in SSc and trials with other tyrosine kinase inhibitors are in preparation.

Published

2008

11. Mechanisms of vascular damage in SSc--implications for vascular treatment strategies.

Author

Guiducci S, Distler O, Distler JH, and Matucci-Cerinic M

Subjects

Fibrosis, Humans, Inflammation, Microcirculation, Neovascularization, Physiologic, Scleroderma, Systemic complications, Scleroderma, Systemic immunology, Vascular Diseases complications, Endothelial Cells pathology, Scleroderma, Systemic pathology

Abstract

Vascular abnormalities are a major component of SSc, but little is known about the events or mechanisms that initiate vascular injury and prevent its repair. In SSc, angiogenesis is incomplete or lacking despite the increased expression of a large array of pro-angiogenic factors such as VEGF. Conflicting results have recently been published concerning the presence and role of vasculogenesis and circulating endothelial progenitor cells in SSc. It remains to be established if these endothelial progenitor cells are a marker of endothelial disease or a cause of insufficient vascular repair. Human mesenchymal stem cells (MSCs) may be an alternative source for endothelial progenitor cells, and it has been observed that the angiogenic potential of endothelial-like MSCs is reduced. Other mechanisms of vascular damage include oxidative stress and factors released from activated platelets. In addition, growth factors such as ET-1 and PDGF induce proliferation of vascular smooth muscle cells resulting in intimal thickening. For the development of new therapeutic strategies, it is important to realize that the different vascular pathologies--uncompensated loss of capillaries on one hand and vascular remodelling with a proliferative vasculopathy on the other--might require different treatment approaches.

Published

2008

12. Angiogenesis and vasculogenesis in systemic sclerosis.

Author

Distler JH, Gay S, and Distler O

Subjects

Apoptosis, Endothelial Cells pathology, Humans, Scleroderma, Systemic metabolism, Up-Regulation, Neovascularization, Pathologic, Scleroderma, Systemic physiopathology, Vascular Endothelial Growth Factor A metabolism

Abstract

In addition to inflammatory infiltrates and an accumulation of extracellular matrix proteins, vascular changes are a hallmark in the pathogenesis of systemic sclerosis (SSc). Consistent with the ongoing endothelial cell apoptosis, several markers of EC damage are up-regulated in the serum of SSc patients. Surprizingly, vascular endothelial growth factor (VEGF), a very potent angiogenic molecule, is overexpressed in SSc patients despite the insufficient angiogenesis. VEGF can protect patients from fingertip ulcers, but a prolonged overexpression of VEGF might have paradoxical effects leading to the formation of irregular vessels similar to that observed in SSc. Besides defective angiogenesis, recent studies suggest that vasculogenesis is also impaired in SSc patients with reduced numbers and functional defects of endothelial progenitor cells.

Published

2006