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Dive into the research topics where Hans Saegesser is active.

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Featured researches published by Hans Saegesser.


Journal of Hepatology | 2010

Potent antifibrotic activity of mTOR inhibitors sirolimus and everolimus but not of cyclosporine A and tacrolimus in experimental liver fibrosis

E. Patsenker; V. Schneider; Monika Ledermann; Hans Saegesser; C Dorn; Claus Hellerbrand; Felix Stickel

BACKGROUND & AIMS Recurrence of chronic hepatitis C and progressive fibrosis in liver transplants is frequent and impairs both graft and patient survival. Whether or not the choice of immunosuppression affects progression of fibrosis remains unclear. The aim of the present study was to compare the potential of the commonly used immunosuppressants to halt experimental liver fibrosis progression. METHODS To induce liver fibrosis, rats underwent bile duct ligation and treatment with sirolimus (2mg/kg), everolimus (3mg/kg), tacrolimus (1mg/kg), and cyclosporin A (10mg/kg) daily for 5 weeks. Fibrosis, inflammation, and portal pressure were evaluated by histology, hydroxyproline levels, morphometry, hemodynamics, and hepatic gene expression. RESULTS Sirolimus and everolimus decreased fibrosis up to 70%, improved portal pressure, reduced ascites, and showed potent down-regulation of pro-fibrogenic genes, paralleled by a strong increase in matrix degradation (collagenase) activity; in contrast, tacrolimus and cyclosporine A had no or even aggravating effects on liver fibrosis in rats. CONCLUSIONS mTOR inhibition by sirolimus and everolimus in experimental liver fibrosis associates with significantly less fibrosis progression and portal hypertension than treatment with calcineurin inhibitors tacrolimus and cyclosporine A. These data suggest that the selection of the immunosuppressant could impact the recurrence of fibrosis in liver allografts.


Liver International | 2005

Endothelial nitric oxide synthase is not essential for the development of fibrosis and portal hypertension in bile duct ligated mice

Abraham Koshy; Andrea De Gottardi; Monika Ledermann; Hans Saegesser; Sidney Shaw; A. Zimmermann; Jürg Reichen

Abstract: Background/Aims: It is postulated that nitric oxide (NO) is responsible for the hyperdynamic circulation of portal hypertension. Therefore, we investigated induction of fibrosis and hyperdynamic circulation in endothelial NO synthase knock‐out (KO) mice.


Journal of Hepatology | 2006

Low-dose oral rapamycin treatment reduces fibrogenesis, improves liver function, and prolongs survival in rats with established liver cirrhosis

Markus Neef; Monika Ledermann; Hans Saegesser; V. Schneider; Juerg Reichen


Journal of Hepatology | 2006

Oral imatinib treatment reduces early fibrogenesis but does not prevent progression in the long term

Markus Neef; Monika Ledermann; Hans Saegesser; V. Schneider; Nicolas Widmer; Laurent A. Decosterd; Bertrand Rochat; Juerg Reichen


Journal of Hepatology | 2007

Corrigendum to “Low-dose oral rapamycin treatment reduces fibrogenesis, improves liver function, and prolongs survival in rats with established liver cirrhosis” [J Hepatol 45 (2006) 786–796]

Markus Neef; Monika Ledermann; Hans Saegesser; V. Schneider; Juerg Reichen


Journal of Hepatology | 2002

Sirolimus, but not losartan, significantly reduces liver fibrosis and mortality in bile duct ligated rats

Andrea De Gottardi; Matthias Unternaehrer; Hans Saegesser; Monika Ledermann; Juerg Reichen


Journal of Hepatology | 2014

P61 avb6 INTEGRIN ANTAGONISM IMPEDES SPHEROID FORMATION OF TUMOR CELLS IN VITRO AND CHOLANGIOCARCINOMA PROGRESSION IN VIVO

E. Patsenker; V. Schneider; Monika Ledermann; Hans Saegesser; A. Keogh; F. Stickel


Journal of Hepatology | 2012

298 EMT IN RAT AND HUMAN CHOLANGIOCARCINOMA BY BROAD SPECTRUM GENE ANALYSIS

E. Patsenker; V. Schneider; Monika Ledermann; Hans Saegesser; A. Keogh; F. Stickel


Journal of Hepatology | 2008

960 LEPTIN-RECEPTOR DEFICIENCY PROTECTS FROM ALCOHOLIC AND NON-ALCOHOLIC LIVER FIBROSIS VIA LACK OF CYTOCHROME P450 2E1 INDUCTION

E. Patsenker; V. Schneider; Monika Ledermann; Hans Saegesser; F. Stickel


Journal of Hepatology | 2007

[327] RAS/MEK/ERK AND TGF-BETA/CTGF PATHWAYS AS POSSIBLE DETERMINANTS OF RESISTANCE TO RAPAMYCIN TREATMENT IN BDL-INDUCED LIVER FIBROSIS. RESULTS OF A GENE ARRAY ANALYSIS

L. Idrissova; Monika Ledermann; Hans Saegesser; V. Schneider; A. Kuhn; Sidney Shaw; Jürg Reichen; Markus Neef

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F. Stickel

University of Erlangen-Nuremberg

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