Your search keyword '"Haeussinger, Dieter"' showing total 33 results

1. Characterization of HIV-1 drug resistance among patients with failure of second-line combined antiretroviral therapy in central Ethiopia

Author

Tufa, Tafese Beyene, Fuchs, Andre, Orth, Hans Martin, Luebke, Nadine, Knops, Elena, Heger, Eva, Jarso, Godana, Hurissa, Zewdu, Eggers, Yannik, Haeussinger, Dieter, Luedde, Tom, Jensen, Bjoern-Erik Ole, Kaiser, Rolf, Feldt, Torsten, Tufa, Tafese Beyene, Fuchs, Andre, Orth, Hans Martin, Luebke, Nadine, Knops, Elena, Heger, Eva, Jarso, Godana, Hurissa, Zewdu, Eggers, Yannik, Haeussinger, Dieter, Luedde, Tom, Jensen, Bjoern-Erik Ole, Kaiser, Rolf, and Feldt, Torsten

Abstract

Background As a consequence of the improved availability of combined antiretroviral therapy (cART) in resource-limited countries, an emergence of HIV drug resistance (HIVDR) has been observed. We assessed the prevalence and spectrum of HIVDR in patients with failure of second-line cART at two HIV clinics in central Ethiopia. Methods HIV drug resistance was analysed in HIV-1-infected patients with virological failure of second-line cART using the geno2pheno application. Results Among 714 patients receiving second-line cART, 44 (6.2%) fulfilled the criteria for treatment failure and 37 were eligible for study inclusion. Median age was 42 years [interquartile range (IQR): 20-45] and 62.2% were male. At initiation of first-line cART, 23 (62.2%) were WHO stage III, mean CD4 cell count was 170.6 (range: 16-496) cells/mu L and median (IQR) HIV-1 viral load was 30 220 (7963-82 598) copies/mL. Most common second-line cART regimens at the time of failure were tenofovir disoproxil fumarate (TDF)-lamivudine (3TC)-ritonavir-boosted atazanavir (ATV/r) (19/37, 51.4%) and zidovudine (ZDV)-3TC-ATV/r (9/37, 24.3%). Genotypic HIV-1 resistance testing was successful in 35 (94.6%) participants. We found at least one resistance mutation in 80% of patients and 40% carried a protease inhibitor (PI)-associated mutation. Most common mutations were M184V (57.1%), Y188C (25.7%), M46I/L (25.7%) and V82A/M (25.7%). High-level resistance against the PI ATV (10/35, 28.6%) and lopinavir (LPV) (5/35, 14.3%) was reported. As expected, no resistance mutations conferring integrase inhibitor resistance were detected. Conclusions We found a high prevalence of resistance mutations, also against PIs (40%), as the national standard second-line cART components. Resistance testing before switching to second- or third-line cART is warranted.

Published

2022

2. Characterization of HIV-1 drug resistance among patients with failure of second-line combined antiretroviral therapy in central Ethiopia

Author

Tufa, Tafese Beyene, Fuchs, Andre, Orth, Hans Martin, Luebke, Nadine, Knops, Elena, Heger, Eva, Jarso, Godana, Hurissa, Zewdu, Eggers, Yannik, Haeussinger, Dieter, Luedde, Tom, Jensen, Bjoern-Erik Ole, Kaiser, Rolf, Feldt, Torsten, Tufa, Tafese Beyene, Fuchs, Andre, Orth, Hans Martin, Luebke, Nadine, Knops, Elena, Heger, Eva, Jarso, Godana, Hurissa, Zewdu, Eggers, Yannik, Haeussinger, Dieter, Luedde, Tom, Jensen, Bjoern-Erik Ole, Kaiser, Rolf, and Feldt, Torsten

Abstract

Background As a consequence of the improved availability of combined antiretroviral therapy (cART) in resource-limited countries, an emergence of HIV drug resistance (HIVDR) has been observed. We assessed the prevalence and spectrum of HIVDR in patients with failure of second-line cART at two HIV clinics in central Ethiopia. Methods HIV drug resistance was analysed in HIV-1-infected patients with virological failure of second-line cART using the geno2pheno application. Results Among 714 patients receiving second-line cART, 44 (6.2%) fulfilled the criteria for treatment failure and 37 were eligible for study inclusion. Median age was 42 years [interquartile range (IQR): 20-45] and 62.2% were male. At initiation of first-line cART, 23 (62.2%) were WHO stage III, mean CD4 cell count was 170.6 (range: 16-496) cells/mu L and median (IQR) HIV-1 viral load was 30 220 (7963-82 598) copies/mL. Most common second-line cART regimens at the time of failure were tenofovir disoproxil fumarate (TDF)-lamivudine (3TC)-ritonavir-boosted atazanavir (ATV/r) (19/37, 51.4%) and zidovudine (ZDV)-3TC-ATV/r (9/37, 24.3%). Genotypic HIV-1 resistance testing was successful in 35 (94.6%) participants. We found at least one resistance mutation in 80% of patients and 40% carried a protease inhibitor (PI)-associated mutation. Most common mutations were M184V (57.1%), Y188C (25.7%), M46I/L (25.7%) and V82A/M (25.7%). High-level resistance against the PI ATV (10/35, 28.6%) and lopinavir (LPV) (5/35, 14.3%) was reported. As expected, no resistance mutations conferring integrase inhibitor resistance were detected. Conclusions We found a high prevalence of resistance mutations, also against PIs (40%), as the national standard second-line cART components. Resistance testing before switching to second- or third-line cART is warranted.

Published

2022

3. Granulocyte-colony stimulating factor (G-CSF) to treat acute-on- chronic liver failure: A multicenter randomized trial (GRAFT study)

Author

Engelmann, Cornelius, Herber, Adam, Franke, Annegret, Bruns, Tony, Reuken, Philipp, Schiefke, Ingolf, Zipprich, Alexander, Zeuzem, Stefan, Goeser, Tobias, Canbay, Ali, Berg, Christoph, Trebicka, Jonel, Uschner, Frank E., Chang, Johannes, Mueller, Tobias, Aehling, Niklas, Schmelzle, Moritz, Splith, Katrin, Lammert, Frank, Lange, Christian M., Sarrazin, Christoph, Trautwein, Christian, Manns, Michael, Haeussinger, Dieter, Pfeiffenberger, Jan, Galle, Peter R., Schmiedeknecht, Anett, Berg, Thomas, Engelmann, Cornelius, Herber, Adam, Franke, Annegret, Bruns, Tony, Reuken, Philipp, Schiefke, Ingolf, Zipprich, Alexander, Zeuzem, Stefan, Goeser, Tobias, Canbay, Ali, Berg, Christoph, Trebicka, Jonel, Uschner, Frank E., Chang, Johannes, Mueller, Tobias, Aehling, Niklas, Schmelzle, Moritz, Splith, Katrin, Lammert, Frank, Lange, Christian M., Sarrazin, Christoph, Trautwein, Christian, Manns, Michael, Haeussinger, Dieter, Pfeiffenberger, Jan, Galle, Peter R., Schmiedeknecht, Anett, and Berg, Thomas

Abstract

Background & Aims: Based on positive results from small single center studies, granulocyte-colony stimulating factor (G-CSF) is being widely used for the treatment of patients with acute-on chronic liver failure (ACLF). Herein, we aimed to evaluate the safety and efficacy of G-CSF in patients with ACLF. Methods: In this multicenter, prospective, controlled, open-label phase II study, 176 patients with ACLF (EASL-CLIF criteria) were randomized to receive G-CSF (5 mu g/kg daily for the first 5 days and every third day thereafter until day 26) plus standard medical therapy (SMT) (n = 88) or SMT alone. The primary effi- cacy endpoint was 90-day transplant-free survival analyzed by Cox regression modeling. The key secondary endpoints were overall and transplant-free survival after 360 days, the development of ACLF-related complications, and the course of liver function scores during the entire observation period. Results: Patients treated with G-CSF had a 90-day transplant free survival rate of 34.1% compared to 37.5% in the SMT group (hazard ratio [HR] 1.05; 95% CI 0.711-1.551; p = 0.805). Transplant-free and overall survival at 360 days did not differ between the 2 arms (HR 0.998; 95% CI 0.697-1.430; p = 0.992 and HR 1.058; 95% CI 0.727-1.548; p = 0.768, respectively). G-CSF did not improve liver function scores, the occurrence of infections, or survival in subgroups of patients without infections, with alcohol-related ACLF, or with ACLF defined by the APASL criteria. Sixty-one serious adverse events were reported in the GCSF+SMT group and 57 were reported in the SMT group. In total, 7 drug-related serious adverse reactions occurred in the G-CSF group. The study was prematurely terminated due to futility after conditional power calculation. Conclusions: In contrast to previous findings, G-CSF had no significant beneficial effect on patients with ACLF in this multicenter controlled trial, which suggests that it should not be used as a standard treatment for ACLF. Clinic

Published

2021

4. Downregulation of TGR5 (GPBAR1) in biliary epithelial cells contributes to the pathogenesis of sclerosing cholangitis

Author

Reich, Maria, Spomer, Lina, Klindt, Caroline, Fuchs, Katharina, Stindt, Jan, Deutschmann, Kathleen, Hohne, Johanna, Liaskou, Evaggelia, Hov, Johannes R., Karlsen, Tom H., Beuers, Ulrich, Verheij, Joanne, Ferreira-Gonzalez, Sofia, Hirschfield, Gideon, Forbes, Stuart J., Schramm, Christoph, Esposito, Irene, Nierhoff, Dirk, Fickert, Peter, Fuchs, Claudia Daniela, Trauner, Michael, Garcia-Beccaria, Maria, Gabernet, Gisela, Nahnsen, Sven, Mallm, Jan-Philipp, Vogel, Marina, Schoonjans, Kristina, Lautwein, Tobias, Koehrer, Karl, Haeussinger, Dieter, Luedde, Tom, Heikenwalder, Mathias, Keitel, Verena, Reich, Maria, Spomer, Lina, Klindt, Caroline, Fuchs, Katharina, Stindt, Jan, Deutschmann, Kathleen, Hohne, Johanna, Liaskou, Evaggelia, Hov, Johannes R., Karlsen, Tom H., Beuers, Ulrich, Verheij, Joanne, Ferreira-Gonzalez, Sofia, Hirschfield, Gideon, Forbes, Stuart J., Schramm, Christoph, Esposito, Irene, Nierhoff, Dirk, Fickert, Peter, Fuchs, Claudia Daniela, Trauner, Michael, Garcia-Beccaria, Maria, Gabernet, Gisela, Nahnsen, Sven, Mallm, Jan-Philipp, Vogel, Marina, Schoonjans, Kristina, Lautwein, Tobias, Koehrer, Karl, Haeussinger, Dieter, Luedde, Tom, Heikenwalder, Mathias, and Keitel, Verena

Abstract

Background & Aims: Primary sclerosing cholangitis (PSC) is characterized by chronic inflammation and progressive fibrosis of the biliary tree. The bile acid receptor TGR5 (GPBAR1) is found on biliary epithelial cells (BECs), where it promotes secretion, proliferation and tight junction integrity. Thus, we speculated that changes in TGR5-expression in BECs may contribute to PSC pathogenesis. Methods: TGR5-expression and-localization were analyzed in PSC livers and liver tissue, isolated bile ducts and BECs from Abcb4(-/-) , Abcb4(-/-)/Tgr5(Tg) and ursodeoxycholic acid (UDCA)-or 24-norursodeoxycholic acid (norUDCA)-fed Abcb(4-/-) mice. The effects of IL8/IL8 homologues on TGR5 mRNA and protein levels were studied. BEC gene expression was analyzed by single-cell transcriptomics (scRNA-seq) from distinct mouse models. Results: TGR5 mRNA expression and immunofluorescence staining intensity were reduced in BECs of PSC and Abcb4(-/-) livers, in Abcb4(-/-) extrahepatic bile ducts, but not in intrahepatic macrophages. No changes in TGR5 BEC fluorescence intensity were detected in liver tissue of other liver diseases, including primary biliary cholangitis. Incubation of BECs with IL8/IL8 homologues, but not with other cytokines, reduced TGR5 mRNA and protein levels. BECs from Abcb4(-/-) mice had lower levels of phosphorylated Erk and higher expression levels of Icam1, Vcam1 and Tgfb2. Overexpression of Tgr5 abolished the activated inflammatory phenotype characteristic of Abcb4(-/-) BECs. NorUDCA-feeding restored TGR5-expression levels in BECs in Abcb4(-/-) livers. Conclusions: Reduced TGR5 levels in BECs from patients with PSC and Abcb4(-/-) mice promote development of a reactive BEC phenotype, aggravate biliary injury and thus contribute to the pathogenesis of sclerosing cholangitis. Restoration of biliary TGR5-expression levels represents a previously unknown mechanism of action of norUDCA. Lay summary: Primary sclerosing cholangitis (PSC) is a chronic cholestatic liver dis

Published

2021

5. Granulocyte-colony stimulating factor (G-CSF) to treat acute-on- chronic liver failure: A multicenter randomized trial (GRAFT study)

Author

Engelmann, Cornelius, Herber, Adam, Franke, Annegret, Bruns, Tony, Reuken, Philipp, Schiefke, Ingolf, Zipprich, Alexander, Zeuzem, Stefan, Goeser, Tobias, Canbay, Ali, Berg, Christoph, Trebicka, Jonel, Uschner, Frank E., Chang, Johannes, Mueller, Tobias, Aehling, Niklas, Schmelzle, Moritz, Splith, Katrin, Lammert, Frank, Lange, Christian M., Sarrazin, Christoph, Trautwein, Christian, Manns, Michael, Haeussinger, Dieter, Pfeiffenberger, Jan, Galle, Peter R., Schmiedeknecht, Anett, Berg, Thomas, Engelmann, Cornelius, Herber, Adam, Franke, Annegret, Bruns, Tony, Reuken, Philipp, Schiefke, Ingolf, Zipprich, Alexander, Zeuzem, Stefan, Goeser, Tobias, Canbay, Ali, Berg, Christoph, Trebicka, Jonel, Uschner, Frank E., Chang, Johannes, Mueller, Tobias, Aehling, Niklas, Schmelzle, Moritz, Splith, Katrin, Lammert, Frank, Lange, Christian M., Sarrazin, Christoph, Trautwein, Christian, Manns, Michael, Haeussinger, Dieter, Pfeiffenberger, Jan, Galle, Peter R., Schmiedeknecht, Anett, and Berg, Thomas

Abstract

Background & Aims: Based on positive results from small single center studies, granulocyte-colony stimulating factor (G-CSF) is being widely used for the treatment of patients with acute-on chronic liver failure (ACLF). Herein, we aimed to evaluate the safety and efficacy of G-CSF in patients with ACLF. Methods: In this multicenter, prospective, controlled, open-label phase II study, 176 patients with ACLF (EASL-CLIF criteria) were randomized to receive G-CSF (5 mu g/kg daily for the first 5 days and every third day thereafter until day 26) plus standard medical therapy (SMT) (n = 88) or SMT alone. The primary effi- cacy endpoint was 90-day transplant-free survival analyzed by Cox regression modeling. The key secondary endpoints were overall and transplant-free survival after 360 days, the development of ACLF-related complications, and the course of liver function scores during the entire observation period. Results: Patients treated with G-CSF had a 90-day transplant free survival rate of 34.1% compared to 37.5% in the SMT group (hazard ratio [HR] 1.05; 95% CI 0.711-1.551; p = 0.805). Transplant-free and overall survival at 360 days did not differ between the 2 arms (HR 0.998; 95% CI 0.697-1.430; p = 0.992 and HR 1.058; 95% CI 0.727-1.548; p = 0.768, respectively). G-CSF did not improve liver function scores, the occurrence of infections, or survival in subgroups of patients without infections, with alcohol-related ACLF, or with ACLF defined by the APASL criteria. Sixty-one serious adverse events were reported in the GCSF+SMT group and 57 were reported in the SMT group. In total, 7 drug-related serious adverse reactions occurred in the G-CSF group. The study was prematurely terminated due to futility after conditional power calculation. Conclusions: In contrast to previous findings, G-CSF had no significant beneficial effect on patients with ACLF in this multicenter controlled trial, which suggests that it should not be used as a standard treatment for ACLF. Clinic

Published

2021

6. Downregulation of TGR5 (GPBAR1) in biliary epithelial cells contributes to the pathogenesis of sclerosing cholangitis

Author

Reich, Maria, Spomer, Lina, Klindt, Caroline, Fuchs, Katharina, Stindt, Jan, Deutschmann, Kathleen, Hohne, Johanna, Liaskou, Evaggelia, Hov, Johannes R., Karlsen, Tom H., Beuers, Ulrich, Verheij, Joanne, Ferreira-Gonzalez, Sofia, Hirschfield, Gideon, Forbes, Stuart J., Schramm, Christoph, Esposito, Irene, Nierhoff, Dirk, Fickert, Peter, Fuchs, Claudia Daniela, Trauner, Michael, Garcia-Beccaria, Maria, Gabernet, Gisela, Nahnsen, Sven, Mallm, Jan-Philipp, Vogel, Marina, Schoonjans, Kristina, Lautwein, Tobias, Koehrer, Karl, Haeussinger, Dieter, Luedde, Tom, Heikenwalder, Mathias, Keitel, Verena, Reich, Maria, Spomer, Lina, Klindt, Caroline, Fuchs, Katharina, Stindt, Jan, Deutschmann, Kathleen, Hohne, Johanna, Liaskou, Evaggelia, Hov, Johannes R., Karlsen, Tom H., Beuers, Ulrich, Verheij, Joanne, Ferreira-Gonzalez, Sofia, Hirschfield, Gideon, Forbes, Stuart J., Schramm, Christoph, Esposito, Irene, Nierhoff, Dirk, Fickert, Peter, Fuchs, Claudia Daniela, Trauner, Michael, Garcia-Beccaria, Maria, Gabernet, Gisela, Nahnsen, Sven, Mallm, Jan-Philipp, Vogel, Marina, Schoonjans, Kristina, Lautwein, Tobias, Koehrer, Karl, Haeussinger, Dieter, Luedde, Tom, Heikenwalder, Mathias, and Keitel, Verena

Abstract

Background & Aims: Primary sclerosing cholangitis (PSC) is characterized by chronic inflammation and progressive fibrosis of the biliary tree. The bile acid receptor TGR5 (GPBAR1) is found on biliary epithelial cells (BECs), where it promotes secretion, proliferation and tight junction integrity. Thus, we speculated that changes in TGR5-expression in BECs may contribute to PSC pathogenesis. Methods: TGR5-expression and-localization were analyzed in PSC livers and liver tissue, isolated bile ducts and BECs from Abcb4(-/-) , Abcb4(-/-)/Tgr5(Tg) and ursodeoxycholic acid (UDCA)-or 24-norursodeoxycholic acid (norUDCA)-fed Abcb(4-/-) mice. The effects of IL8/IL8 homologues on TGR5 mRNA and protein levels were studied. BEC gene expression was analyzed by single-cell transcriptomics (scRNA-seq) from distinct mouse models. Results: TGR5 mRNA expression and immunofluorescence staining intensity were reduced in BECs of PSC and Abcb4(-/-) livers, in Abcb4(-/-) extrahepatic bile ducts, but not in intrahepatic macrophages. No changes in TGR5 BEC fluorescence intensity were detected in liver tissue of other liver diseases, including primary biliary cholangitis. Incubation of BECs with IL8/IL8 homologues, but not with other cytokines, reduced TGR5 mRNA and protein levels. BECs from Abcb4(-/-) mice had lower levels of phosphorylated Erk and higher expression levels of Icam1, Vcam1 and Tgfb2. Overexpression of Tgr5 abolished the activated inflammatory phenotype characteristic of Abcb4(-/-) BECs. NorUDCA-feeding restored TGR5-expression levels in BECs in Abcb4(-/-) livers. Conclusions: Reduced TGR5 levels in BECs from patients with PSC and Abcb4(-/-) mice promote development of a reactive BEC phenotype, aggravate biliary injury and thus contribute to the pathogenesis of sclerosing cholangitis. Restoration of biliary TGR5-expression levels represents a previously unknown mechanism of action of norUDCA. Lay summary: Primary sclerosing cholangitis (PSC) is a chronic cholestatic liver dis

Published

2021

7. Ten-year follow-up of a randomized controlled clinical trial in chronic hepatitis delta

Author

Yurdaydın, Cihan, Wranke, Anika; Hardtke, Svenja; Heidrich, Benjamin; Dalekos, George; Yalçın, Kendal; Tabak, Fehmi; Gürel, Selim; Çakaloğlu, Yılmaz; Akarca, Ulus S.; Lammert, Frank; Haeussinger, Dieter; Mueller, Tobias; Woebse, Michael; Manns, Michael P.; İdilman, Ramazan; Cornberg, Markus; Wedemeyer, Heiner, School of Medicine, Yurdaydın, Cihan, Wranke, Anika; Hardtke, Svenja; Heidrich, Benjamin; Dalekos, George; Yalçın, Kendal; Tabak, Fehmi; Gürel, Selim; Çakaloğlu, Yılmaz; Akarca, Ulus S.; Lammert, Frank; Haeussinger, Dieter; Mueller, Tobias; Woebse, Michael; Manns, Michael P.; İdilman, Ramazan; Cornberg, Markus; Wedemeyer, Heiner, and School of Medicine

Abstract

Hepatitis delta virus (HDV) infection causes the most severe form of viral hepatitis. PEG-interferon alpha-2a (PEG-IFN alpha-2a) is the only effective treatment but its long-term clinical impact is unclear. The aim of this study was to investigate the long-term outcome after 48 weeks of pegylated interferon alpha-2a therapy. We performed a retrospective follow-up study of the Hep-Net-International-Delta-Hepatitis-Intervention-Study 1 (HIDIT-I trial). Patients had received 48 weeks of treatment with either PEG-IFN alpha-2a plus adefovir dipivoxil (ADV) (Group I), PEG-IFN alpha-2a alone (Group II) or adefovir dipivoxil alone (Group III). Liver-related complications were defined as liver-related death, liver transplantation, liver cancer and hepatic decompensation defined as development of Child-Pugh scores B or C or an increase in Model for End-stage Liver Disease (MELD) scores of five or more points in relation to baseline values. Patients were considered for further analysis when they were retreated with PEG-IFN alpha-2a. Follow-up data (at least 1 visit beyond post-treatment week 24) were available for 60 patients [Group I, (n = 19), Group II (n = 20), Group III (n = 21)]. Mean time of follow-up was 8.9 (1.6 - 13.4) years. 19 patients were retreated with IFN-based therapy: 42% (n = 8) in PEG-IFN alpha-2a arms and 58% (n = 11) in the adefovir only arm. Clinical complications on long-term follow-up occurred in 17 patients and were associated with nonresponse to therapy and baseline cirrhosis. The annual event-free survival rate in patients with cirrhosis vs noncirrhotic patients at year 5 and 10 was 70% vs 91% and 35% vs 76%. Long-term follow-up of a large randomized clinical trial suggests that off-treatment HDV RNA response to PEG-IFN alpha-2a treatment leads to improved clinical long-term outcome., German Centre for Infection Research (DZIF), Hannover-Braunschweig; HepNet Study-House; German Liver Foundation; EASL Registry Grant

Published

2020

8. Biallelic mutation of human SLC6A6 encoding the taurine transporter TAUT is linked to early retinal degeneration

Author

Preising, Markus N., Goerg, Boris, Friedburg, Christoph, Qvartskhava, Natalia, Budde, Birgit S., Bonus, Michele, Toliat, Mohammad R., Pfleger, Christopher, Altmueller, Janine, Herebian, Diran, Beyer, Mila, Zoellner, Helge J., Wittsack, Hans-Joerg, Schaper, Joerg, Klee, Dirk, Zechner, Ulrich, Nuernberg, Peter, Schipper, Joerg, Schnitzler, Alfons, Gohlke, Holger, Lorenz, Birgit, Haeussinger, Dieter, Bolz, Hanno J., Preising, Markus N., Goerg, Boris, Friedburg, Christoph, Qvartskhava, Natalia, Budde, Birgit S., Bonus, Michele, Toliat, Mohammad R., Pfleger, Christopher, Altmueller, Janine, Herebian, Diran, Beyer, Mila, Zoellner, Helge J., Wittsack, Hans-Joerg, Schaper, Joerg, Klee, Dirk, Zechner, Ulrich, Nuernberg, Peter, Schipper, Joerg, Schnitzler, Alfons, Gohlke, Holger, Lorenz, Birgit, Haeussinger, Dieter, and Bolz, Hanno J.

Abstract

We previously reported that inactivation of the transmembrane taurine transporter (TauT or solute carrier 6a6) causes early retinal degeneration in mice. Compatible with taurine's indispensability for cell volume homeostasis, protein stabilization, cytoprotection, antioxidation, and immuno- and neuromodulation, mice develop multisystemic dysfunctions (hearing loss; liver fibrosis; and behavioral, heart, and skeletal muscle abnormalities) later on. Here, by genetic, cell biologic, in vivo H-1-magnetic resonance spectroscopy and molecular dynamics simulation studies, we conducted in-depth characterization of a novel disorder: human TAUT deficiency. Loss of TAUT function due to a homozygous missense mutation caused panretinal degeneration in 2 brothers. TAUT(p.A78E) still localized in the plasma membrane but is predicted to impact structural stabilization. H-3-taurine uptake by peripheral blood mononuclear cells was reduced by 95%, and taurine levels were severely reduced in plasma, skeletal muscle, and brain. Extraocular dysfunctions were not yet detected, but significantly increased urinary excretion of 8-oxo-7,8-dihydroguanosine indicated generally enhanced (yet clinically unapparent) oxidative stress and RNA oxidation, warranting continuous broad surveillance.-Preising, M. N., Gorg, B., Friedburg, C., Qvartskhava, N., Budde, B. S., Bonus, M., Toliat, M. R., Pfleger, C., Altmuller, J., Herebian, D., Beyer, M., Zollner, H. J., Wittsack, H.-J., Schaper, J., Klee, D., Zechner, U., Nurnberg, P., Schipper, J., Schnitzler, A., Gohlke, H., Lorenz, B., Haussinger, D., Bolz, H. J. Biallelic mutation of human SLC6A6 encoding the taurine transporter TAUT is linked to early retinal degeneration.

Published

2019

9. Biallelic mutation of human SLC6A6 encoding the taurine transporter TAUT is linked to early retinal degeneration

Author

Preising, Markus N., Goerg, Boris, Friedburg, Christoph, Qvartskhava, Natalia, Budde, Birgit S., Bonus, Michele, Toliat, Mohammad R., Pfleger, Christopher, Altmueller, Janine, Herebian, Diran, Beyer, Mila, Zoellner, Helge J., Wittsack, Hans-Joerg, Schaper, Joerg, Klee, Dirk, Zechner, Ulrich, Nuernberg, Peter, Schipper, Joerg, Schnitzler, Alfons, Gohlke, Holger, Lorenz, Birgit, Haeussinger, Dieter, Bolz, Hanno J., Preising, Markus N., Goerg, Boris, Friedburg, Christoph, Qvartskhava, Natalia, Budde, Birgit S., Bonus, Michele, Toliat, Mohammad R., Pfleger, Christopher, Altmueller, Janine, Herebian, Diran, Beyer, Mila, Zoellner, Helge J., Wittsack, Hans-Joerg, Schaper, Joerg, Klee, Dirk, Zechner, Ulrich, Nuernberg, Peter, Schipper, Joerg, Schnitzler, Alfons, Gohlke, Holger, Lorenz, Birgit, Haeussinger, Dieter, and Bolz, Hanno J.

Abstract

We previously reported that inactivation of the transmembrane taurine transporter (TauT or solute carrier 6a6) causes early retinal degeneration in mice. Compatible with taurine's indispensability for cell volume homeostasis, protein stabilization, cytoprotection, antioxidation, and immuno- and neuromodulation, mice develop multisystemic dysfunctions (hearing loss; liver fibrosis; and behavioral, heart, and skeletal muscle abnormalities) later on. Here, by genetic, cell biologic, in vivo H-1-magnetic resonance spectroscopy and molecular dynamics simulation studies, we conducted in-depth characterization of a novel disorder: human TAUT deficiency. Loss of TAUT function due to a homozygous missense mutation caused panretinal degeneration in 2 brothers. TAUT(p.A78E) still localized in the plasma membrane but is predicted to impact structural stabilization. H-3-taurine uptake by peripheral blood mononuclear cells was reduced by 95%, and taurine levels were severely reduced in plasma, skeletal muscle, and brain. Extraocular dysfunctions were not yet detected, but significantly increased urinary excretion of 8-oxo-7,8-dihydroguanosine indicated generally enhanced (yet clinically unapparent) oxidative stress and RNA oxidation, warranting continuous broad surveillance.-Preising, M. N., Gorg, B., Friedburg, C., Qvartskhava, N., Budde, B. S., Bonus, M., Toliat, M. R., Pfleger, C., Altmuller, J., Herebian, D., Beyer, M., Zollner, H. J., Wittsack, H.-J., Schaper, J., Klee, D., Zechner, U., Nurnberg, P., Schipper, J., Schnitzler, A., Gohlke, H., Lorenz, B., Haussinger, D., Bolz, H. J. Biallelic mutation of human SLC6A6 encoding the taurine transporter TAUT is linked to early retinal degeneration.

Published

2019

10. Anal chromoendoscopy using gastroenterological videoendoscopes: A new method to perform high resolution anoscopy for diagnosing intraepithelial neoplasia and anal carcinoma in HIV-infected patients

Author

Oette, Mark, Wieland, Ulrike, Schuenemann, Marko, Haes, Johannes, Reuter, Stefan, Jensen, Bjorn Erik Ole, Sagir, Abdurrahman, Pfister, Herbert, Haeussinger, Dieter, Oette, Mark, Wieland, Ulrike, Schuenemann, Marko, Haes, Johannes, Reuter, Stefan, Jensen, Bjorn Erik Ole, Sagir, Abdurrahman, Pfister, Herbert, and Haeussinger, Dieter

Abstract

Introduction Anal carcinoma represents an increasing problem in HIV-infected patients. Anal intraepithelial neoplasia (AIN), the precursor lesion, is currently diagnosed by high-resolution anoscopy (HRA) using optical magnification derived from gynecological colposcopy. This prospective study evaluates anal chromoendoscopy (ACE) using standard gastroenterological video-endoscopes in diagnosing AIN. Methods After clinical examination, proctoscopy and surface staining with acetic acid followed by Lugol's solution, ACE was performed with a mucosectomy cap on the tip of the endoscope. Biopsy specimens were collected from areas with a pathological staining pattern and from areas with normal appearance; combined results were considered as reference. Results Two hundred eleven HIV-positive patients seen between 2007 and 2013 were evaluated. Of these, 95.7 % were males, and the median age was 45 years. In 86.7 %, the mode of HIV transmission was sex among males. Combination antiretroviral treatment was applied in 75.8 %. The sensitivity of ACE in diagnosing AIN was 0.85, the specificity was 0.55, the positive predictive value was 0.50, and the negative predictive value (NPV) was 0.87. Diagnostic performance increased in individuals with high-grade lesions (NPV: 0.99) and in the second study period from 2011 to 2013. Side effects were rare and of minor clinical relevance. Conclusions Anal chromoendoscopy is safe and effective in diagnosing AIN in a population of HIV-infected patients. It is particularly useful for the exclusion of high-grade lesions that have the strongest risk of progression to anal carcinoma. Therefore, ACE may become a valuable new tool to manage AIN and to prevent anal malignancy in HIV-positive patients.

Published

2017

11. Spatiotemporally restricted arenavirus replication induces immune surveillance and type I interferon-dependent tumour regression

Author

Kalkavan, Halime, Sharma, Piyush, Kasper, Stefan, Helfrich, Iris, Pandyra, Aleksandra A., Gassa, Asmae, Virchow, Isabel, Flatz, Lukas, Brandenburg, Tim, Namineni, Sukumar, Heikenwalder, Mathias, Hoechst, Bastian, Knolle, Percy A., Wollmann, Guido, von Laer, Dorothee, Drexler, Ingo, Rathbun, Jessica, Cannon, Paula M., Scheu, Stefanie, Bauer, Jens, Chauhan, Jagat, Haeussinger, Dieter, Willimsky, Gerald, Lohning, Max, Schadendorf, Dirk, Brandau, Sven, Schuler, Martin, Lang, Philipp A., Lang, Karl S., Kalkavan, Halime, Sharma, Piyush, Kasper, Stefan, Helfrich, Iris, Pandyra, Aleksandra A., Gassa, Asmae, Virchow, Isabel, Flatz, Lukas, Brandenburg, Tim, Namineni, Sukumar, Heikenwalder, Mathias, Hoechst, Bastian, Knolle, Percy A., Wollmann, Guido, von Laer, Dorothee, Drexler, Ingo, Rathbun, Jessica, Cannon, Paula M., Scheu, Stefanie, Bauer, Jens, Chauhan, Jagat, Haeussinger, Dieter, Willimsky, Gerald, Lohning, Max, Schadendorf, Dirk, Brandau, Sven, Schuler, Martin, Lang, Philipp A., and Lang, Karl S.

Abstract

Immune-mediated effector molecules can limit cancer growth, but lack of sustained immune activation in the tumour microenvironment restricts antitumour immunity. New therapeutic approaches that induce a strong and prolonged immune activation would represent a major immunotherapeutic advance. Here we show that the arenaviruses lymphocytic choriomeningitis virus (LCMV) and the clinically used Junin virus vaccine (Candid# 1) preferentially replicate in tumour cells in a variety of murine and human cancer models. Viral replication leads to prolonged local immune activation, rapid regression of localized and metastatic cancers, and long-term disease control. Mechanistically, LCMV induces antitumour immunity, which depends on the recruitment of interferon-producing Ly6C(+) monocytes and additionally enhances tumour-specific CD8(+) T cells. In comparison with other clinically evaluated oncolytic viruses and to PD-1 blockade, LCMV treatment shows promising antitumoural benefits. In conclusion, therapeutically administered arenavirus replicates in cancer cells and induces tumour regression by enhancing local immune responses.

Published

2017

12. Detection of a genetic footprint of the sofosbuvir resistance-associated substitution S282T after HCV treatment failure

Author

Walker, Andreas, Filke, Sandra, Luebke, Nadine, Obermeier, Martin, Kaiser, Rolf, Haeussinger, Dieter, Timm, Joerg, Bock, Hans H., Walker, Andreas, Filke, Sandra, Luebke, Nadine, Obermeier, Martin, Kaiser, Rolf, Haeussinger, Dieter, Timm, Joerg, and Bock, Hans H.

Abstract

Background: The major resistance-associated substitution for sofosbuvir (S282T) in HCV NS5B causes severe viral fitness costs and rapidly reverts back to prototype in the absence of selection pressure. Accordingly, resistance against sofosbuvir is rarely detected even in patients after treatment failure. Case presentation: We report a case of a GT3a infected patient with viral breakthrough under SOF/DCV therapy. At the time of breakthrough the RAS S282T was predominant in NS5B and then rapidly disappeared during follow-up by week 12 after treatment. Interestingly, despite only serine was encoded in position 282 during follow-up, two distinct genetic pathways for reversion were detectable. In 31% of the quasispecies the original codon for serine was present whereas in the majority of the quasispecies an alternative codon was selected. This alternative codon usage was unique for all GT3a isolates from the HCV database and remained detectable as a genetic footprint for prior resistance selection at the RNA level for at least 6 months. Conclusions: Comparative analyses of viral sequences at the codon level before and after DAA treatment may help to elucidate the patient's history of resistance selection, which is particularly valuable for highly unfit substitutions that are detectable only for a short period of time. If such codon changes increase the risk of re-selection of resistance upon a second exposure to SOF remains to be addressed.

Published

2017

13. Control measures following a case of imported Lassa fever from Togo, North Rhine Westphalia, Germany, 2016

Author

Lehmann, Clara, Kochanek, Matthias, Abdulla, Diana, Becker, Stephan, Boell, Boris, Bunte, Anne, Cadar, Daniel, Dormann, Arno, Eickmann, Markus, Emmerich, Petra, Feldt, Torsten, Frank, Christina, Fries, Jochen, Gabriel, Martin, Goetsch, Udo, Gottschalk, Rene, Guenther, Stephan, Hallek, Michael, Haeussinger, Dieter, Herzog, Christian, Jensen, Bjoern, Kolibay, Felix, Krakau, Michael, Langebartels, Georg, Rieger, Toni, Schaade, Lars, Schmidt-Chanasit, Jonas, Schoemig, Edgar, Schuettfort, Gundolf, Shimabukuro-Vornhagen, Alexander, von Bergwelt-Baildon, Michael, Wieland, Ulrike, Wiesmueller, Gerhard, Wolf, Timo, Faetkenheuer, Gerd, Lehmann, Clara, Kochanek, Matthias, Abdulla, Diana, Becker, Stephan, Boell, Boris, Bunte, Anne, Cadar, Daniel, Dormann, Arno, Eickmann, Markus, Emmerich, Petra, Feldt, Torsten, Frank, Christina, Fries, Jochen, Gabriel, Martin, Goetsch, Udo, Gottschalk, Rene, Guenther, Stephan, Hallek, Michael, Haeussinger, Dieter, Herzog, Christian, Jensen, Bjoern, Kolibay, Felix, Krakau, Michael, Langebartels, Georg, Rieger, Toni, Schaade, Lars, Schmidt-Chanasit, Jonas, Schoemig, Edgar, Schuettfort, Gundolf, Shimabukuro-Vornhagen, Alexander, von Bergwelt-Baildon, Michael, Wieland, Ulrike, Wiesmueller, Gerhard, Wolf, Timo, and Faetkenheuer, Gerd

Abstract

In a patient transferred from Togo to Cologne, Germany, Lassa fever was diagnosed 12 days post mortem. Sixty-two contacts in Cologne were categorised according to the level of exposure, and gradual infection control measures were applied. No clinical signs of Lassa virus infection or Lassa specific antibodies were observed in the 62 contacts. Thirty-three individuals had direct contact to blood, other body fluids or tissue of the patients. Notably, with standard precautions, no transmission occurred between the index patient and healthcare workers. However, one secondary infection occurred in an undertaker exposed to the corpse in Rhineland-Palatinate, who was treated on the isolation unit at the University Hospital of Frankfurt. After German authorities raised an alert regarding the imported Lassa fever case, an American healthcare worker who had cared for the index patient in Togo, and who presented with diarrhoea, vomiting and fever, was placed in isolation and medevacked to the United States. The event and the transmission of Lassa virus infection outside of Africa underlines the need for early diagnosis and use of adequate personal protection equipment (PPE), when highly contagious infections cannot be excluded. It also demonstrates that larger outbreaks can be prevented by infection control measures, including standard PPE.

Published

2017

14. Anal chromoendoscopy using gastroenterological videoendoscopes: A new method to perform high resolution anoscopy for diagnosing intraepithelial neoplasia and anal carcinoma in HIV-infected patients

Author

Oette, Mark, Wieland, Ulrike, Schuenemann, Marko, Haes, Johannes, Reuter, Stefan, Jensen, Bjorn Erik Ole, Sagir, Abdurrahman, Pfister, Herbert, Haeussinger, Dieter, Oette, Mark, Wieland, Ulrike, Schuenemann, Marko, Haes, Johannes, Reuter, Stefan, Jensen, Bjorn Erik Ole, Sagir, Abdurrahman, Pfister, Herbert, and Haeussinger, Dieter

Abstract

Introduction Anal carcinoma represents an increasing problem in HIV-infected patients. Anal intraepithelial neoplasia (AIN), the precursor lesion, is currently diagnosed by high-resolution anoscopy (HRA) using optical magnification derived from gynecological colposcopy. This prospective study evaluates anal chromoendoscopy (ACE) using standard gastroenterological video-endoscopes in diagnosing AIN. Methods After clinical examination, proctoscopy and surface staining with acetic acid followed by Lugol's solution, ACE was performed with a mucosectomy cap on the tip of the endoscope. Biopsy specimens were collected from areas with a pathological staining pattern and from areas with normal appearance; combined results were considered as reference. Results Two hundred eleven HIV-positive patients seen between 2007 and 2013 were evaluated. Of these, 95.7 % were males, and the median age was 45 years. In 86.7 %, the mode of HIV transmission was sex among males. Combination antiretroviral treatment was applied in 75.8 %. The sensitivity of ACE in diagnosing AIN was 0.85, the specificity was 0.55, the positive predictive value was 0.50, and the negative predictive value (NPV) was 0.87. Diagnostic performance increased in individuals with high-grade lesions (NPV: 0.99) and in the second study period from 2011 to 2013. Side effects were rare and of minor clinical relevance. Conclusions Anal chromoendoscopy is safe and effective in diagnosing AIN in a population of HIV-infected patients. It is particularly useful for the exclusion of high-grade lesions that have the strongest risk of progression to anal carcinoma. Therefore, ACE may become a valuable new tool to manage AIN and to prevent anal malignancy in HIV-positive patients.

Published

2017

15. Spatiotemporally restricted arenavirus replication induces immune surveillance and type I interferon-dependent tumour regression

Author

Kalkavan, Halime, Sharma, Piyush, Kasper, Stefan, Helfrich, Iris, Pandyra, Aleksandra A., Gassa, Asmae, Virchow, Isabel, Flatz, Lukas, Brandenburg, Tim, Namineni, Sukumar, Heikenwalder, Mathias, Hoechst, Bastian, Knolle, Percy A., Wollmann, Guido, von Laer, Dorothee, Drexler, Ingo, Rathbun, Jessica, Cannon, Paula M., Scheu, Stefanie, Bauer, Jens, Chauhan, Jagat, Haeussinger, Dieter, Willimsky, Gerald, Lohning, Max, Schadendorf, Dirk, Brandau, Sven, Schuler, Martin, Lang, Philipp A., Lang, Karl S., Kalkavan, Halime, Sharma, Piyush, Kasper, Stefan, Helfrich, Iris, Pandyra, Aleksandra A., Gassa, Asmae, Virchow, Isabel, Flatz, Lukas, Brandenburg, Tim, Namineni, Sukumar, Heikenwalder, Mathias, Hoechst, Bastian, Knolle, Percy A., Wollmann, Guido, von Laer, Dorothee, Drexler, Ingo, Rathbun, Jessica, Cannon, Paula M., Scheu, Stefanie, Bauer, Jens, Chauhan, Jagat, Haeussinger, Dieter, Willimsky, Gerald, Lohning, Max, Schadendorf, Dirk, Brandau, Sven, Schuler, Martin, Lang, Philipp A., and Lang, Karl S.

Abstract

Immune-mediated effector molecules can limit cancer growth, but lack of sustained immune activation in the tumour microenvironment restricts antitumour immunity. New therapeutic approaches that induce a strong and prolonged immune activation would represent a major immunotherapeutic advance. Here we show that the arenaviruses lymphocytic choriomeningitis virus (LCMV) and the clinically used Junin virus vaccine (Candid# 1) preferentially replicate in tumour cells in a variety of murine and human cancer models. Viral replication leads to prolonged local immune activation, rapid regression of localized and metastatic cancers, and long-term disease control. Mechanistically, LCMV induces antitumour immunity, which depends on the recruitment of interferon-producing Ly6C(+) monocytes and additionally enhances tumour-specific CD8(+) T cells. In comparison with other clinically evaluated oncolytic viruses and to PD-1 blockade, LCMV treatment shows promising antitumoural benefits. In conclusion, therapeutically administered arenavirus replicates in cancer cells and induces tumour regression by enhancing local immune responses.

Published

2017

16. Detection of a genetic footprint of the sofosbuvir resistance-associated substitution S282T after HCV treatment failure

Author

Walker, Andreas, Filke, Sandra, Luebke, Nadine, Obermeier, Martin, Kaiser, Rolf, Haeussinger, Dieter, Timm, Joerg, Bock, Hans H., Walker, Andreas, Filke, Sandra, Luebke, Nadine, Obermeier, Martin, Kaiser, Rolf, Haeussinger, Dieter, Timm, Joerg, and Bock, Hans H.

Abstract

Background: The major resistance-associated substitution for sofosbuvir (S282T) in HCV NS5B causes severe viral fitness costs and rapidly reverts back to prototype in the absence of selection pressure. Accordingly, resistance against sofosbuvir is rarely detected even in patients after treatment failure. Case presentation: We report a case of a GT3a infected patient with viral breakthrough under SOF/DCV therapy. At the time of breakthrough the RAS S282T was predominant in NS5B and then rapidly disappeared during follow-up by week 12 after treatment. Interestingly, despite only serine was encoded in position 282 during follow-up, two distinct genetic pathways for reversion were detectable. In 31% of the quasispecies the original codon for serine was present whereas in the majority of the quasispecies an alternative codon was selected. This alternative codon usage was unique for all GT3a isolates from the HCV database and remained detectable as a genetic footprint for prior resistance selection at the RNA level for at least 6 months. Conclusions: Comparative analyses of viral sequences at the codon level before and after DAA treatment may help to elucidate the patient's history of resistance selection, which is particularly valuable for highly unfit substitutions that are detectable only for a short period of time. If such codon changes increase the risk of re-selection of resistance upon a second exposure to SOF remains to be addressed.

Published

2017

17. Control measures following a case of imported Lassa fever from Togo, North Rhine Westphalia, Germany, 2016

Author

Lehmann, Clara, Kochanek, Matthias, Abdulla, Diana, Becker, Stephan, Boell, Boris, Bunte, Anne, Cadar, Daniel, Dormann, Arno, Eickmann, Markus, Emmerich, Petra, Feldt, Torsten, Frank, Christina, Fries, Jochen, Gabriel, Martin, Goetsch, Udo, Gottschalk, Rene, Guenther, Stephan, Hallek, Michael, Haeussinger, Dieter, Herzog, Christian, Jensen, Bjoern, Kolibay, Felix, Krakau, Michael, Langebartels, Georg, Rieger, Toni, Schaade, Lars, Schmidt-Chanasit, Jonas, Schoemig, Edgar, Schuettfort, Gundolf, Shimabukuro-Vornhagen, Alexander, von Bergwelt-Baildon, Michael, Wieland, Ulrike, Wiesmueller, Gerhard, Wolf, Timo, Faetkenheuer, Gerd, Lehmann, Clara, Kochanek, Matthias, Abdulla, Diana, Becker, Stephan, Boell, Boris, Bunte, Anne, Cadar, Daniel, Dormann, Arno, Eickmann, Markus, Emmerich, Petra, Feldt, Torsten, Frank, Christina, Fries, Jochen, Gabriel, Martin, Goetsch, Udo, Gottschalk, Rene, Guenther, Stephan, Hallek, Michael, Haeussinger, Dieter, Herzog, Christian, Jensen, Bjoern, Kolibay, Felix, Krakau, Michael, Langebartels, Georg, Rieger, Toni, Schaade, Lars, Schmidt-Chanasit, Jonas, Schoemig, Edgar, Schuettfort, Gundolf, Shimabukuro-Vornhagen, Alexander, von Bergwelt-Baildon, Michael, Wieland, Ulrike, Wiesmueller, Gerhard, Wolf, Timo, and Faetkenheuer, Gerd

Abstract

In a patient transferred from Togo to Cologne, Germany, Lassa fever was diagnosed 12 days post mortem. Sixty-two contacts in Cologne were categorised according to the level of exposure, and gradual infection control measures were applied. No clinical signs of Lassa virus infection or Lassa specific antibodies were observed in the 62 contacts. Thirty-three individuals had direct contact to blood, other body fluids or tissue of the patients. Notably, with standard precautions, no transmission occurred between the index patient and healthcare workers. However, one secondary infection occurred in an undertaker exposed to the corpse in Rhineland-Palatinate, who was treated on the isolation unit at the University Hospital of Frankfurt. After German authorities raised an alert regarding the imported Lassa fever case, an American healthcare worker who had cared for the index patient in Togo, and who presented with diarrhoea, vomiting and fever, was placed in isolation and medevacked to the United States. The event and the transmission of Lassa virus infection outside of Africa underlines the need for early diagnosis and use of adequate personal protection equipment (PPE), when highly contagious infections cannot be excluded. It also demonstrates that larger outbreaks can be prevented by infection control measures, including standard PPE.

Published

2017

18. Virus-specific antibodies allow viral replication in the marginal zone, thereby promoting CD8(+)T-cell priming and viral control

Author

Duhan, Vikas, Khairnar, Vishal, Friedrich, Sarah-Kim, Zhou, Fan, Gassa, Asmae, Honke, Nadine, Shaabani, Namir, Gailus, Nicole, Botezatu, Lacramioara, Khandanpour, Cyrus, Dittmer, Ulf, Haeussinger, Dieter, Recher, Mike, Hardt, Cornelia, Lang, Philipp A., Lang, Karl S., Duhan, Vikas, Khairnar, Vishal, Friedrich, Sarah-Kim, Zhou, Fan, Gassa, Asmae, Honke, Nadine, Shaabani, Namir, Gailus, Nicole, Botezatu, Lacramioara, Khandanpour, Cyrus, Dittmer, Ulf, Haeussinger, Dieter, Recher, Mike, Hardt, Cornelia, Lang, Philipp A., and Lang, Karl S.

Abstract

Clinically used human vaccination aims to induce specific antibodies that can guarantee long-term protection against a pathogen. The reasons that other immune components often fail to induce protective immunity are still debated. Recently we found that enforced viral replication in secondary lymphoid organs is essential for immune activation. In this study we used the lymphocytic choriomeningitis virus (LCMV) to determine whether enforced virus replication occurs in the presence of virus-specific antibodies or virus-specific CD8(+)T cells. We found that after systemic recall infection with LCMV-WE the presence of virus-specific antibodies allowed intracellular replication of virus in the marginal zone of spleen. In contrast, specific antibodies limited viral replication in liver, lung, and kidney. Upon recall infection with the persistent virus strain LCMV-Docile, viral replication in spleen was essential for the priming of CD8(+)T cells and for viral control. In contrast to specific antibodies, memory CD8(+)T cells inhibited viral replication in marginal zone but failed to protect mice from persistent viral infection. We conclude that virus-specific antibodies limit viral infection in peripheral organs but still allow replication of LCMV in the marginal zone, a mechanism that allows immune boosting during recall infection and thereby guarantees control of persistent virus.

Published

2016

19. Model-guided identification of a therapeutic strategy to reduce hyperammonemia in liver diseases

Author

Ghallab, Ahmed, Celliere, Geraldine, Henkel, Sebastian G., Driesch, Dominik, Hoehme, Stefan, Hofmann, Ute, Zellmer, Sebastian, Godoy, Patricio, Sachinidis, Agapios, Blaszkewicz, Meinolf, Reif, Raymond, Marchan, Rosemarie, Kuepfer, Lars, Haeussinger, Dieter, Drasdo, Dirk, Gebhardt, Rolf, Hengstler, Jan G., Ghallab, Ahmed, Celliere, Geraldine, Henkel, Sebastian G., Driesch, Dominik, Hoehme, Stefan, Hofmann, Ute, Zellmer, Sebastian, Godoy, Patricio, Sachinidis, Agapios, Blaszkewicz, Meinolf, Reif, Raymond, Marchan, Rosemarie, Kuepfer, Lars, Haeussinger, Dieter, Drasdo, Dirk, Gebhardt, Rolf, and Hengstler, Jan G.

Abstract

Background & Aims: Recently, spatial-temporal/metabolic mathematical models have been established that allow the simulation of metabolic processes in tissues. We applied these models to decipher ammonia detoxification mechanisms in the liver. Methods: An integrated metabolic-spatial-temporal model was used to generate hypotheses of ammonia metabolism. Predicted mechanisms were validated using time-resolved analyses of nitrogen metabolism, activity analyses, immunostaining and gene expression after induction of liver damage in mice. Moreover, blood from the portal vein, liver vein and mixed venous blood was analyzed in a time dependent manner. Results: Modeling revealed an underestimation of ammonia consumption after liver damage when only the currently established mechanisms of ammonia detoxification were simulated. By iterative cycles of modeling and experiments, the reductive amidation of alpha-ketoglutarate (alpha-KG) via glutamate dehydrogenase (GDH) was identified as the lacking component. GDH is released from damaged hepatocytes into the blood where it consumes ammonia to generate glutamate, thereby providing systemic protection against hyperammonemia. This mechanism was exploited therapeutically in a mouse model of hyperammonemia by injecting GDH together with optimized doses of cofactors. Intravenous injection of GDH (720 U/kg), alpha-KG (280 mg/kg) and NADPH (180 mg/kg) reduced the elevated blood ammonia concentrations (>200 mu M) to levels close to normal within only 15 min. Conclusion: If successfully translated to patients the GDH-based therapy might provide a less aggressive therapeutic alternative for patients with severe hyperammonemia. (C) 2015 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.

Published

2016

20. The RESINA data support the individualized therapy based on primary resistance testing

Author

Knops, Elena, Schuelter, Eugen, Luebke, Nadine, Neumann-Fraune, Maria, Heger, Eva, Sierra-Aragon, Saleta, Mueller, Claudia, Oette, Mark, Faetkenheuer, Gerd, Hower, Martin, Knechten, Heribert, Schuebel, Niels, Esser, Stefan, Scholten, Stefan, Haeussinger, Dieter, Kaiser, Rolf, Jensen, Bjoern, Knops, Elena, Schuelter, Eugen, Luebke, Nadine, Neumann-Fraune, Maria, Heger, Eva, Sierra-Aragon, Saleta, Mueller, Claudia, Oette, Mark, Faetkenheuer, Gerd, Hower, Martin, Knechten, Heribert, Schuebel, Niels, Esser, Stefan, Scholten, Stefan, Haeussinger, Dieter, Kaiser, Rolf, and Jensen, Bjoern

Published

2016

21. Treatment of HIV and acute myeloid leukaemia by allogeneic CCR5-d32 blood stem cell transplantation

Author

Knops, Elena, Kobbe, Guido, Kaiser, Rolf, Luebke, Nadine, Dunay, Gabor, Wensing, Annemarie, Martinez-Picado, Javier, Nijhuis, Monique, Fischer, Johannes, Huettig, Falk, Haas, Rainer, Haeussinger, Dieter, Jensen, Bjoern, Knops, Elena, Kobbe, Guido, Kaiser, Rolf, Luebke, Nadine, Dunay, Gabor, Wensing, Annemarie, Martinez-Picado, Javier, Nijhuis, Monique, Fischer, Johannes, Huettig, Falk, Haas, Rainer, Haeussinger, Dieter, and Jensen, Bjoern

Published

2016

22. Virus-specific antibodies allow viral replication in the marginal zone, thereby promoting CD8(+)T-cell priming and viral control

Author

Duhan, Vikas, Khairnar, Vishal, Friedrich, Sarah-Kim, Zhou, Fan, Gassa, Asmae, Honke, Nadine, Shaabani, Namir, Gailus, Nicole, Botezatu, Lacramioara, Khandanpour, Cyrus, Dittmer, Ulf, Haeussinger, Dieter, Recher, Mike, Hardt, Cornelia, Lang, Philipp A., Lang, Karl S., Duhan, Vikas, Khairnar, Vishal, Friedrich, Sarah-Kim, Zhou, Fan, Gassa, Asmae, Honke, Nadine, Shaabani, Namir, Gailus, Nicole, Botezatu, Lacramioara, Khandanpour, Cyrus, Dittmer, Ulf, Haeussinger, Dieter, Recher, Mike, Hardt, Cornelia, Lang, Philipp A., and Lang, Karl S.

Abstract

Clinically used human vaccination aims to induce specific antibodies that can guarantee long-term protection against a pathogen. The reasons that other immune components often fail to induce protective immunity are still debated. Recently we found that enforced viral replication in secondary lymphoid organs is essential for immune activation. In this study we used the lymphocytic choriomeningitis virus (LCMV) to determine whether enforced virus replication occurs in the presence of virus-specific antibodies or virus-specific CD8(+)T cells. We found that after systemic recall infection with LCMV-WE the presence of virus-specific antibodies allowed intracellular replication of virus in the marginal zone of spleen. In contrast, specific antibodies limited viral replication in liver, lung, and kidney. Upon recall infection with the persistent virus strain LCMV-Docile, viral replication in spleen was essential for the priming of CD8(+)T cells and for viral control. In contrast to specific antibodies, memory CD8(+)T cells inhibited viral replication in marginal zone but failed to protect mice from persistent viral infection. We conclude that virus-specific antibodies limit viral infection in peripheral organs but still allow replication of LCMV in the marginal zone, a mechanism that allows immune boosting during recall infection and thereby guarantees control of persistent virus.

Published

2016

23. Model-guided identification of a therapeutic strategy to reduce hyperammonemia in liver diseases

Author

Ghallab, Ahmed, Celliere, Geraldine, Henkel, Sebastian G., Driesch, Dominik, Hoehme, Stefan, Hofmann, Ute, Zellmer, Sebastian, Godoy, Patricio, Sachinidis, Agapios, Blaszkewicz, Meinolf, Reif, Raymond, Marchan, Rosemarie, Kuepfer, Lars, Haeussinger, Dieter, Drasdo, Dirk, Gebhardt, Rolf, Hengstler, Jan G., Ghallab, Ahmed, Celliere, Geraldine, Henkel, Sebastian G., Driesch, Dominik, Hoehme, Stefan, Hofmann, Ute, Zellmer, Sebastian, Godoy, Patricio, Sachinidis, Agapios, Blaszkewicz, Meinolf, Reif, Raymond, Marchan, Rosemarie, Kuepfer, Lars, Haeussinger, Dieter, Drasdo, Dirk, Gebhardt, Rolf, and Hengstler, Jan G.

Abstract

Background & Aims: Recently, spatial-temporal/metabolic mathematical models have been established that allow the simulation of metabolic processes in tissues. We applied these models to decipher ammonia detoxification mechanisms in the liver. Methods: An integrated metabolic-spatial-temporal model was used to generate hypotheses of ammonia metabolism. Predicted mechanisms were validated using time-resolved analyses of nitrogen metabolism, activity analyses, immunostaining and gene expression after induction of liver damage in mice. Moreover, blood from the portal vein, liver vein and mixed venous blood was analyzed in a time dependent manner. Results: Modeling revealed an underestimation of ammonia consumption after liver damage when only the currently established mechanisms of ammonia detoxification were simulated. By iterative cycles of modeling and experiments, the reductive amidation of alpha-ketoglutarate (alpha-KG) via glutamate dehydrogenase (GDH) was identified as the lacking component. GDH is released from damaged hepatocytes into the blood where it consumes ammonia to generate glutamate, thereby providing systemic protection against hyperammonemia. This mechanism was exploited therapeutically in a mouse model of hyperammonemia by injecting GDH together with optimized doses of cofactors. Intravenous injection of GDH (720 U/kg), alpha-KG (280 mg/kg) and NADPH (180 mg/kg) reduced the elevated blood ammonia concentrations (>200 mu M) to levels close to normal within only 15 min. Conclusion: If successfully translated to patients the GDH-based therapy might provide a less aggressive therapeutic alternative for patients with severe hyperammonemia. (C) 2015 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.

Published

2016

24. Treatment of HIV and acute myeloid leukaemia by allogeneic CCR5-d32 blood stem cell transplantation

Author

Knops, Elena, Kobbe, Guido, Kaiser, Rolf, Luebke, Nadine, Dunay, Gabor, Wensing, Annemarie, Martinez-Picado, Javier, Nijhuis, Monique, Fischer, Johannes, Huettig, Falk, Haas, Rainer, Haeussinger, Dieter, Jensen, Bjoern, Knops, Elena, Kobbe, Guido, Kaiser, Rolf, Luebke, Nadine, Dunay, Gabor, Wensing, Annemarie, Martinez-Picado, Javier, Nijhuis, Monique, Fischer, Johannes, Huettig, Falk, Haas, Rainer, Haeussinger, Dieter, and Jensen, Bjoern

Published

2016

25. The RESINA data support the individualized therapy based on primary resistance testing

Author

Knops, Elena, Schuelter, Eugen, Luebke, Nadine, Neumann-Fraune, Maria, Heger, Eva, Sierra-Aragon, Saleta, Mueller, Claudia, Oette, Mark, Faetkenheuer, Gerd, Hower, Martin, Knechten, Heribert, Schuebel, Niels, Esser, Stefan, Scholten, Stefan, Haeussinger, Dieter, Kaiser, Rolf, Jensen, Bjoern, Knops, Elena, Schuelter, Eugen, Luebke, Nadine, Neumann-Fraune, Maria, Heger, Eva, Sierra-Aragon, Saleta, Mueller, Claudia, Oette, Mark, Faetkenheuer, Gerd, Hower, Martin, Knechten, Heribert, Schuebel, Niels, Esser, Stefan, Scholten, Stefan, Haeussinger, Dieter, Kaiser, Rolf, and Jensen, Bjoern

Published

2016

26. IFN-gamma licenses CD11b(+) cells to induce progression of systemic lupus erythematosus

Author

Shaabani, Namir, Honke, Nadine, Dolff, Sebastian, Goerg, Boris, Khairnar, Vishal, Merches, Katja, Duhan, Vikas, Metzger, Sabine, Recher, Mike, Barthuber, Carmen, Hardt, Cornelia, Proksch, Peter, Haeussinger, Dieter, Witzke, Oliver, Lang, Philipp A., Lang, Karl S., Shaabani, Namir, Honke, Nadine, Dolff, Sebastian, Goerg, Boris, Khairnar, Vishal, Merches, Katja, Duhan, Vikas, Metzger, Sabine, Recher, Mike, Barthuber, Carmen, Hardt, Cornelia, Proksch, Peter, Haeussinger, Dieter, Witzke, Oliver, Lang, Philipp A., and Lang, Karl S.

Abstract

Autoantibodies are a hallmark of autoimmune diseases, such as rheumatoid arthritis, autoimmune hepatitis, and systemic lupus erythematosus (SLE). High titers of anti-nuclear antibodies are used as surrogate marker for SLE, however their contribution to pathogenesis remains unclear. Using murine model of SLE and human samples, we studied the effect of immune stimulation on relapsing of SLE. Although autoantibodies bound to target cells in vivo, only additional activation of CD8(+) T cells converted this silent autoimmunity into overt disease. In mice as well as in humans CU8(+) T cells derived IFN-gamma enhanced expression of Fc-receptors on CD11b(+) cells. High expression of Fc-receptors allowed CD11b(+) cells to bind to antibody covered target cells and to destroy them in vivo. We found that autoantibodies induce clinically relevant disease when adaptive immunity, specific for disease non-related antigen, is activated. (C) 2015 Elsevier Ltd. All rights reserved.

Published

2015

27. IFN-gamma licenses CD11b(+) cells to induce progression of systemic lupus erythematosus

Author

Shaabani, Namir, Honke, Nadine, Dolff, Sebastian, Goerg, Boris, Khairnar, Vishal, Merches, Katja, Duhan, Vikas, Metzger, Sabine, Recher, Mike, Barthuber, Carmen, Hardt, Cornelia, Proksch, Peter, Haeussinger, Dieter, Witzke, Oliver, Lang, Philipp A., Lang, Karl S., Shaabani, Namir, Honke, Nadine, Dolff, Sebastian, Goerg, Boris, Khairnar, Vishal, Merches, Katja, Duhan, Vikas, Metzger, Sabine, Recher, Mike, Barthuber, Carmen, Hardt, Cornelia, Proksch, Peter, Haeussinger, Dieter, Witzke, Oliver, Lang, Philipp A., and Lang, Karl S.

Abstract

Autoantibodies are a hallmark of autoimmune diseases, such as rheumatoid arthritis, autoimmune hepatitis, and systemic lupus erythematosus (SLE). High titers of anti-nuclear antibodies are used as surrogate marker for SLE, however their contribution to pathogenesis remains unclear. Using murine model of SLE and human samples, we studied the effect of immune stimulation on relapsing of SLE. Although autoantibodies bound to target cells in vivo, only additional activation of CD8(+) T cells converted this silent autoimmunity into overt disease. In mice as well as in humans CU8(+) T cells derived IFN-gamma enhanced expression of Fc-receptors on CD11b(+) cells. High expression of Fc-receptors allowed CD11b(+) cells to bind to antibody covered target cells and to destroy them in vivo. We found that autoantibodies induce clinically relevant disease when adaptive immunity, specific for disease non-related antigen, is activated. (C) 2015 Elsevier Ltd. All rights reserved.

Published

2015

28. Type I Interferon Protects Antiviral CD8(+) T Cells from NK Cell Cytotoxicity

Author

Xu, Haifeng C., Grusdat, Melanie, Pandyra, Aleksandra A., Polz, Robin, Huang, Jun, Sharma, Piyush, Deenen, Rene, Koehrer, Karl, Rahbar, Ramtin, Diefenbach, Andreas, Gibbert, Kathrin, Loehning, Max, Hoecker, Lena, Waibler, Zoe, Haeussinger, Dieter, Mak, Tak W., Ohashi, Pamela S., Lang, Karl S., Lang, Philipp A., Xu, Haifeng C., Grusdat, Melanie, Pandyra, Aleksandra A., Polz, Robin, Huang, Jun, Sharma, Piyush, Deenen, Rene, Koehrer, Karl, Rahbar, Ramtin, Diefenbach, Andreas, Gibbert, Kathrin, Loehning, Max, Hoecker, Lena, Waibler, Zoe, Haeussinger, Dieter, Mak, Tak W., Ohashi, Pamela S., Lang, Karl S., and Lang, Philipp A.

Abstract

Despite development of new antiviral drugs, viral infections are still a major health problem. The most potent antiviral defense mechanism is the innate production of type I interferon (IFN-I), which not only limits virus replication but also promotes antiviral T cell immunity through mechanisms, which remain insufficiently studied. Using the murine lymphocytic choriomeningitis virus model system, we show here that IFN-I signaling on T cells prevented their rapid elimination in vivo. Microarray analyses uncovered that IFN-I triggered the expression of selected inhibitory NK-cell-receptor ligands. Consequently, T cell immunity of IFN-I receptor (IFNAR)-deficient T cells could be restored by NK cell depletion or in NK-cell-deficient hosts (Nfil3(-/-)).The elimination of Ifnar1(-/-) T cells was dependent on NK-cell-mediated perforin expression. In summary, we identified IFN-I as a key player regulating the protection of T cells against regulatory NK cell function.

Published

2014

29. Type I Interferon Protects Antiviral CD8(+) T Cells from NK Cell Cytotoxicity

Author

Xu, Haifeng C., Grusdat, Melanie, Pandyra, Aleksandra A., Polz, Robin, Huang, Jun, Sharma, Piyush, Deenen, Rene, Koehrer, Karl, Rahbar, Ramtin, Diefenbach, Andreas, Gibbert, Kathrin, Loehning, Max, Hoecker, Lena, Waibler, Zoe, Haeussinger, Dieter, Mak, Tak W., Ohashi, Pamela S., Lang, Karl S., Lang, Philipp A., Xu, Haifeng C., Grusdat, Melanie, Pandyra, Aleksandra A., Polz, Robin, Huang, Jun, Sharma, Piyush, Deenen, Rene, Koehrer, Karl, Rahbar, Ramtin, Diefenbach, Andreas, Gibbert, Kathrin, Loehning, Max, Hoecker, Lena, Waibler, Zoe, Haeussinger, Dieter, Mak, Tak W., Ohashi, Pamela S., Lang, Karl S., and Lang, Philipp A.

Abstract

Despite development of new antiviral drugs, viral infections are still a major health problem. The most potent antiviral defense mechanism is the innate production of type I interferon (IFN-I), which not only limits virus replication but also promotes antiviral T cell immunity through mechanisms, which remain insufficiently studied. Using the murine lymphocytic choriomeningitis virus model system, we show here that IFN-I signaling on T cells prevented their rapid elimination in vivo. Microarray analyses uncovered that IFN-I triggered the expression of selected inhibitory NK-cell-receptor ligands. Consequently, T cell immunity of IFN-I receptor (IFNAR)-deficient T cells could be restored by NK cell depletion or in NK-cell-deficient hosts (Nfil3(-/-)).The elimination of Ifnar1(-/-) T cells was dependent on NK-cell-mediated perforin expression. In summary, we identified IFN-I as a key player regulating the protection of T cells against regulatory NK cell function.

Published

2014

30. Ambulatory care for HIV-infected patients: differences in outcomes between hospital-based units and private practices: analysis of the RESINA cohort

Author

Oette, Mark, Reuter, Stefan, Kaiser, Rolf, Jensen, Bjoern, Lengauer, Thomas, Faetkenheuer, Gerd, Knechten, Heribert, Hower, Martin, Sagir, Abdurrahman, Pfister, Herbert, Haeussinger, Dieter, Oette, Mark, Reuter, Stefan, Kaiser, Rolf, Jensen, Bjoern, Lengauer, Thomas, Faetkenheuer, Gerd, Knechten, Heribert, Hower, Martin, Sagir, Abdurrahman, Pfister, Herbert, and Haeussinger, Dieter

Abstract

Background: The efficacy of highly active antiretroviral therapy (HAART) in the treatment of HIV infection is influenced by factors such as potency of applied drugs, adherence of the patient, and resistance-associated mutations. Up to now, there is insufficient data on the impact of the therapeutic setting. Methods: Since 2001, the prospective multicenter RESINA study has examined the epidemiology of transmitted HIV drug resistance in Nordrhein-Westfalen, the largest federal state of Germany by population. Characteristics of patients treated in hospital-based outpatient units were compared to those of patients treated in medical practices. Longitudinal data of all participants are being followed in a cohort study. Results: Overall, 1,591 patients were enrolled between 2001 and 2009 with follow-up until the end of 2010. Of these, 1,099 cases were treated in hospital-based units and 492 in private practices. Significant differences were found with respect to baseline characteristics. A higher rate of patients with advanced disease and non-European nationality were cared for in hospital units. Patients in medical practices were predominantly Caucasian men who have sex with men (MSM) harboring HIV-1 subtype B, with lower CDC stage and higher CD4 cell count. Median viral load was 68,828 c/mL in hospital-based units and 100,000 c/mL in private practices (P = 0.041). Only median age and rate of transmitted drug resistance were not significantly different. After 48 weeks, 81.9% of patients in hospital units and 85.9% in private practices had a viral load below the limit of detection (P = 0.12). A similar result was seen after 96 weeks (P = 0.54). Although the baseline CD4 cell count was different (189.5/mu L in hospital units and 246.5/mu L in private practices, P < 0.001), a consistent and almost identical increase was determined in both groups. Conclusions: The RESINA study covers a large HIV-infected patient cohort cared for in specialized facilities in Germany. Despite

Published

2013

31. Ambulatory care for HIV-infected patients: differences in outcomes between hospital-based units and private practices: analysis of the RESINA cohort

Author

Oette, Mark, Reuter, Stefan, Kaiser, Rolf, Jensen, Bjoern, Lengauer, Thomas, Faetkenheuer, Gerd, Knechten, Heribert, Hower, Martin, Sagir, Abdurrahman, Pfister, Herbert, Haeussinger, Dieter, Oette, Mark, Reuter, Stefan, Kaiser, Rolf, Jensen, Bjoern, Lengauer, Thomas, Faetkenheuer, Gerd, Knechten, Heribert, Hower, Martin, Sagir, Abdurrahman, Pfister, Herbert, and Haeussinger, Dieter

Abstract

Background: The efficacy of highly active antiretroviral therapy (HAART) in the treatment of HIV infection is influenced by factors such as potency of applied drugs, adherence of the patient, and resistance-associated mutations. Up to now, there is insufficient data on the impact of the therapeutic setting. Methods: Since 2001, the prospective multicenter RESINA study has examined the epidemiology of transmitted HIV drug resistance in Nordrhein-Westfalen, the largest federal state of Germany by population. Characteristics of patients treated in hospital-based outpatient units were compared to those of patients treated in medical practices. Longitudinal data of all participants are being followed in a cohort study. Results: Overall, 1,591 patients were enrolled between 2001 and 2009 with follow-up until the end of 2010. Of these, 1,099 cases were treated in hospital-based units and 492 in private practices. Significant differences were found with respect to baseline characteristics. A higher rate of patients with advanced disease and non-European nationality were cared for in hospital units. Patients in medical practices were predominantly Caucasian men who have sex with men (MSM) harboring HIV-1 subtype B, with lower CDC stage and higher CD4 cell count. Median viral load was 68,828 c/mL in hospital-based units and 100,000 c/mL in private practices (P = 0.041). Only median age and rate of transmitted drug resistance were not significantly different. After 48 weeks, 81.9% of patients in hospital units and 85.9% in private practices had a viral load below the limit of detection (P = 0.12). A similar result was seen after 96 weeks (P = 0.54). Although the baseline CD4 cell count was different (189.5/mu L in hospital units and 246.5/mu L in private practices, P < 0.001), a consistent and almost identical increase was determined in both groups. Conclusions: The RESINA study covers a large HIV-infected patient cohort cared for in specialized facilities in Germany. Despite

Published

2013

32. Recent advances in 2D and 3D in vitro systems using primary hepatocytes, alternative hepatocyte sources and non-parenchymal liver cells and their use in investigating mechanisms of hepatotoxicity, cell signaling and ADME

Author

Godoy, Patricio, Hewitt, Nicola J., Albrecht, Ute, Andersen, Melvin E., Ansari, Nariman, Bhattacharya, Sudin, Bode, Johannes Georg, Bolleyn, Jennifer, Borner, Christoph, Boettger, Jan, Braeuning, Albert, Budinsky, Robert A., Burkhardt, Britta, Cameron, Neil R., Camussi, Giovanni, Cho, Chong-Su, Choi, Yun-Jaie, Rowlands, J. Craig, Dahmen, Uta, Damm, Georg, Dirsch, Olaf, Teresa Donato, Maria, Dong, Jian, Dooley, Steven, Drasdo, Dirk, Eakins, Rowena, Ferreira, Karine Sa, Fonsato, Valentina, Fraczek, Joanna, Gebhardt, Rolf, Gibson, Andrew, Glanemann, Matthias, Goldring, Chris E. P., Jose Gomez-Lechon, Maria, Groothuis, Geny M. M., Gustavsson, Lena, Guyot, Christelle, Hallifax, David, Hammad, Seddik, Hayward, Adam, Haeussinger, Dieter, Hellerbrand, Claus, Hewitt, Philip, Hoehme, Stefan, Holzhuetter, Hermann-Georg, Houston, J. Brian, Hrach, Jens, Ito, Kiyomi, Jaeschke, Hartmut, Keitel, Verena, Kelm, Jens M., Park, B. Kevin, Kordes, Claus, Kullak-Ublick, Gerd A., LeCluyse, Edward L., Lu, Peng, Luebke-Wheeler, Jennifer, Lutz, Anna, Maltman, Daniel J., Matz-Soja, Madlen, McMullen, Patrick, Merfort, Irmgard, Messner, Simon, Meyer, Christoph, Mwinyi, Jessica, Naisbitt, Dean J., Nussler, Andreas K., Olinga, Peter, Pampaloni, Francesco, Pi, Jingbo, Pluta, Linda, Przyborski, Stefan A., Ramachandran, Anup, Rogiers, Vera, Rowe, Cliff, Schelcher, Celine, Schmich, Kathrin, Schwarz, Michael, Singh, Bijay, Stelzer, Ernst H. K., Stieger, Bruno, Stoeber, Regina, Sugiyama, Yuichi, Tetta, Ciro, Thasler, Wolfgang E., Vanhaecke, Tamara, Vinken, Mathieu, Weiss, Thomas S., Widera, Agata, Woods, Courtney G., Xu, Jinghai James, Yarborough, Kathy M., Hengstler, Jan G., Godoy, Patricio, Hewitt, Nicola J., Albrecht, Ute, Andersen, Melvin E., Ansari, Nariman, Bhattacharya, Sudin, Bode, Johannes Georg, Bolleyn, Jennifer, Borner, Christoph, Boettger, Jan, Braeuning, Albert, Budinsky, Robert A., Burkhardt, Britta, Cameron, Neil R., Camussi, Giovanni, Cho, Chong-Su, Choi, Yun-Jaie, Rowlands, J. Craig, Dahmen, Uta, Damm, Georg, Dirsch, Olaf, Teresa Donato, Maria, Dong, Jian, Dooley, Steven, Drasdo, Dirk, Eakins, Rowena, Ferreira, Karine Sa, Fonsato, Valentina, Fraczek, Joanna, Gebhardt, Rolf, Gibson, Andrew, Glanemann, Matthias, Goldring, Chris E. P., Jose Gomez-Lechon, Maria, Groothuis, Geny M. M., Gustavsson, Lena, Guyot, Christelle, Hallifax, David, Hammad, Seddik, Hayward, Adam, Haeussinger, Dieter, Hellerbrand, Claus, Hewitt, Philip, Hoehme, Stefan, Holzhuetter, Hermann-Georg, Houston, J. Brian, Hrach, Jens, Ito, Kiyomi, Jaeschke, Hartmut, Keitel, Verena, Kelm, Jens M., Park, B. Kevin, Kordes, Claus, Kullak-Ublick, Gerd A., LeCluyse, Edward L., Lu, Peng, Luebke-Wheeler, Jennifer, Lutz, Anna, Maltman, Daniel J., Matz-Soja, Madlen, McMullen, Patrick, Merfort, Irmgard, Messner, Simon, Meyer, Christoph, Mwinyi, Jessica, Naisbitt, Dean J., Nussler, Andreas K., Olinga, Peter, Pampaloni, Francesco, Pi, Jingbo, Pluta, Linda, Przyborski, Stefan A., Ramachandran, Anup, Rogiers, Vera, Rowe, Cliff, Schelcher, Celine, Schmich, Kathrin, Schwarz, Michael, Singh, Bijay, Stelzer, Ernst H. K., Stieger, Bruno, Stoeber, Regina, Sugiyama, Yuichi, Tetta, Ciro, Thasler, Wolfgang E., Vanhaecke, Tamara, Vinken, Mathieu, Weiss, Thomas S., Widera, Agata, Woods, Courtney G., Xu, Jinghai James, Yarborough, Kathy M., and Hengstler, Jan G.

Abstract

This review encompasses the most important advances in liver functions and hepatotoxicity and analyzes which mechanisms can be studied in vitro. In a complex architecture of nested, zonated lobules, the liver consists of approximately 80 % hepatocytes and 20 % non-parenchymal cells, the latter being involved in a secondary phase that may dramatically aggravate the initial damage. Hepatotoxicity, as well as hepatic metabolism, is controlled by a set of nuclear receptors (including PXR, CAR, HNF-4 alpha, FXR, LXR, SHP, VDR and PPAR) and signaling pathways. When isolating liver cells, some pathways are activated, e.g., the RAS/MEK/ERK pathway, whereas others are silenced (e.g. HNF-4 alpha), resulting in up- and downregulation of hundreds of genes. An understanding of these changes is crucial for a correct interpretation of in vitro data. The possibilities and limitations of the most useful liver in vitro systems are summarized, including three-dimensional culture techniques, co-cultures with non-parenchymal cells, hepatospheres, precision cut liver slices and the isolated perfused liver. Also discussed is how closely hepatoma, stem cell and iPS cell-derived hepatocyte-like-cells resemble real hepatocytes. Finally, a summary is given of the state of the art of liver in vitro and mathematical modeling systems that are currently used in the pharmaceutical industry with an emphasis on drug metabolism, prediction of clearance, drug interaction, transporter studies and hepatotoxicity. One key message is that despite our enthusiasm for in vitro systems, we must never lose sight of the in vivo situation. Although hepatocytes have been isolated for decades, the hunt for relevant alternative systems has only just begun.

Published

2013

33. Sphingolipid subtypes differentially control proinsulin processing and systemic glucose homeostasis

Author

Griess, Kerstin, Rieck, Michael, Muller, Nadine, Karsai, Gergely, Hartwig, Sonja, Pelligra, Angela, Hardt, Robert, Schlegel, Caroline, Kuboth, Jennifer, Uhlemeyer, Celina, Trenkamp, Sandra, Jeruschke, Kay, Weiss, Jurgen, Peifer-Weiss, Leon, Xu, Weiwei, Cames, Sandra, Yi, Xiaoyan, Cnop, Miriam, Beller, Mathias, Stark, Holger, Kondadi, Arun Kumar, Reichert, Andreas S., Markgraf, Daniel, Wammers, Marianne, Haeussinger, Dieter, Kuss, Oliver, Lehr, Stefan, Eizirik, Decio, Lickert, Heiko, Lammert, Eckhard, Roden, Michael, Winter, Dominic, Al-Hasani, Hadi, Hoeglinger, Doris, Hornemann, Thorsten, Bruning, Jens C., Belgardt, Bengt-Frederik, Griess, Kerstin, Rieck, Michael, Muller, Nadine, Karsai, Gergely, Hartwig, Sonja, Pelligra, Angela, Hardt, Robert, Schlegel, Caroline, Kuboth, Jennifer, Uhlemeyer, Celina, Trenkamp, Sandra, Jeruschke, Kay, Weiss, Jurgen, Peifer-Weiss, Leon, Xu, Weiwei, Cames, Sandra, Yi, Xiaoyan, Cnop, Miriam, Beller, Mathias, Stark, Holger, Kondadi, Arun Kumar, Reichert, Andreas S., Markgraf, Daniel, Wammers, Marianne, Haeussinger, Dieter, Kuss, Oliver, Lehr, Stefan, Eizirik, Decio, Lickert, Heiko, Lammert, Eckhard, Roden, Michael, Winter, Dominic, Al-Hasani, Hadi, Hoeglinger, Doris, Hornemann, Thorsten, Bruning, Jens C., and Belgardt, Bengt-Frederik

Abstract

Impaired proinsulin-to-insulin processing in pancreatic beta-cells is a key defective step in both type 1 diabetes and type 2 diabetes (T2D) (refs. (1)(,)(2)), but the mechanisms involved remain to be defined. Altered metabolism of sphingolipids (SLs) has been linked to development of obesity, type 1 diabetes and T2D (refs. (3-8)); nonetheless, the role of specific SL species in beta-cell function and demise is unclear. Here we define the lipid signature of T2D-associated beta-cell failure, including an imbalance of specific very-long-chain SLs and long-chain SLs. beta-cell-specific ablation of CerS2, the enzyme necessary for generation of very-long-chain SLs, selectively reduces insulin content, impairs insulin secretion and disturbs systemic glucose tolerance in multiple complementary models. In contrast, ablation of long-chain-SL-synthesizing enzymes has no effect on insulin content. By quantitatively defining the SL-protein interactome, we reveal that CerS2 ablation affects SL binding to several endoplasmic reticulum-Golgi transport proteins, including Tmed2, which we define as an endogenous regulator of the essential proinsulin processing enzyme Pcsk1. Our study uncovers roles for specific SL subtypes and SL-binding proteins in beta-cell function and T2D-associated beta-cell failure.