Tolerizing CTL by Sustained Hepatic PD-L1 Expression Provides a New Therapy Approach in Mouse Sepsis.

von Knethen, Andreas; Schäfer, Anne; Kuchler, Laura; Knape, Tilo; Christen, Urs; Hintermann, Edith; Fißlthaler, Beate; Schröder, Katrin; Brandes, Ralf P; Genz, Berit; Abshagen, Kerstin; Pützer, Brigitte M; Sha, Lisa K; Weigert, Andreas; Syed, Shahzad N; Schulz, Martin; Shah, Ajay M; Ernst, Andreas; Putyrski, Mateusz; Finkelmeier, Fabian; Pesic, Marina; Greten, Florian; Hogardt, Michael; Kempf, Volkhard A J; Gunne, Sandra; Parnham, Michael J; Brüne, Bernhard

von Knethen, Andreas; Schäfer, Anne; Kuchler, Laura; Knape, Tilo; Christen, Urs; Hintermann, Edith; Fißlthaler, Beate; Schröder, Katrin; Brandes, Ralf P; Genz, Berit; Abshagen, Kerstin; Pützer, Brigitte M; Sha, Lisa K; Weigert, Andreas; Syed, Shahzad N; Schulz, Martin; Shah, Ajay M; Ernst, Andreas; Putyrski, Mateusz; Finkelmeier, Fabian; Pesic, Marina; Greten, Florian; Hogardt, Michael; Kempf, Volkhard A J; Gunne, Sandra; Parnham, Michael J; Brüne, Bernhard.

Afiliação

von Knethen A; Institute of Biochemistry I, Faculty of Medicine, Goethe-University Frankfurt, Frankfurt, Germany.
Schäfer A; Fraunhofer Institute for Molecular Biology and Applied Ecology IME, Project Group Translational Medicine & Pharmacology TMP, Frankfurt, Germany.
Kuchler L; Institute of Biochemistry I, Faculty of Medicine, Goethe-University Frankfurt, Frankfurt, Germany.
Knape T; Institute of Biochemistry I, Faculty of Medicine, Goethe-University Frankfurt, Frankfurt, Germany.
Christen U; Fraunhofer Institute for Molecular Biology and Applied Ecology IME, Project Group Translational Medicine & Pharmacology TMP, Frankfurt, Germany.
Hintermann E; Pharmazentrum/ZAFES Frankfurt, Faculty of Medicine, Goethe-University Frankfurt, Frankfurt, Germany.
Fißlthaler B; Pharmazentrum/ZAFES Frankfurt, Faculty of Medicine, Goethe-University Frankfurt, Frankfurt, Germany.
Schröder K; Institute for Vascular Signalling, Centre for Molecular Medicine, Goethe-University Frankfurt, Frankfurt, Germany.
Brandes RP; Institute for Cardiovascular Physiology, Faculty of Medicine, Goethe-University Frankfurt, Frankfurt, Germany.
Genz B; Institute for Cardiovascular Physiology, Faculty of Medicine, Goethe-University Frankfurt, Frankfurt, Germany.
Abshagen K; Institute for Experimental Surgery, Rostock University Medical Center, Rostock, Germany.
Pützer BM; Institute for Experimental Surgery, Rostock University Medical Center, Rostock, Germany.
Sha LK; Institute of Experimental Gene Therapy and Cancer Research, Rostock University Medical Center, Rostock, Germany.
Weigert A; Institute of Biochemistry I, Faculty of Medicine, Goethe-University Frankfurt, Frankfurt, Germany.
Syed SN; Institute of Biochemistry I, Faculty of Medicine, Goethe-University Frankfurt, Frankfurt, Germany.
Schulz M; Institute of Biochemistry I, Faculty of Medicine, Goethe-University Frankfurt, Frankfurt, Germany.
Shah AM; Institute of Biochemistry I, Faculty of Medicine, Goethe-University Frankfurt, Frankfurt, Germany.
Ernst A; King's College London, British Heart Foundation, Centre of Excellence, The James Black Centre, London, UK.
Putyrski M; Fraunhofer Institute for Molecular Biology and Applied Ecology IME, Project Group Translational Medicine & Pharmacology TMP, Frankfurt, Germany.
Finkelmeier F; Pharmazentrum/ZAFES Frankfurt, Faculty of Medicine, Goethe-University Frankfurt, Frankfurt, Germany.
Pesic M; Fraunhofer Institute for Molecular Biology and Applied Ecology IME, Project Group Translational Medicine & Pharmacology TMP, Frankfurt, Germany.
Greten F; Georg Speyer Haus, Institute for Tumor Biology and Experimental Therapy, Frankfurt, Germany.
Hogardt M; Georg Speyer Haus, Institute for Tumor Biology and Experimental Therapy, Frankfurt, Germany.
Kempf VAJ; Georg Speyer Haus, Institute for Tumor Biology and Experimental Therapy, Frankfurt, Germany.
Gunne S; Institute for Medical Microbiology and Infection Control, University Hospital Frankfurt, Paul-Ehrlich-Str. 40, Frankfurt am Main, Germany.
Parnham MJ; Institute for Medical Microbiology and Infection Control, University Hospital Frankfurt, Paul-Ehrlich-Str. 40, Frankfurt am Main, Germany.
Brüne B; Fraunhofer Institute for Molecular Biology and Applied Ecology IME, Project Group Translational Medicine & Pharmacology TMP, Frankfurt, Germany.

Theranostics ; 9(7): 2003-2016, 2019.

Article em En | MEDLINE | ID: mdl-31037153

ABSTRACT

ABSTRACT

Cytotoxic T lymphocyte (CTL) activation contributes to liver damage during sepsis, but the mechanisms involved are largely unknown. Understanding the underlying principle will permit interference with CTL activation and thus, provide a new therapeutic option.

Methods:

To elucidate the mechanism leading to CTL activation we used the Hepa1-6 cell line in vitro and the mouse model of in vivo polymicrobial sepsis, following cecal-ligation and -puncture (CLP) in wildtype, myeloid specific NOX-2, global NOX2 and NOX4 knockout mice, and their survival as a final readout. In this in vivo setting, we also determined hepatic mRNA and protein expression as well as clinical parameters of liver damage - aspartate- and alanine amino-transaminases. Hepatocyte specific overexpression of PD-L1 was achieved in vivo by adenoviral infection and transposon-based gene transfer using hydrodynamic injection.

Results:

We observed downregulation of PD-L1 on hepatocytes in the murine sepsis model. Adenoviral and transposon-based gene transfer to restore PD-L1 expression, significantly improved survival and reduced the release of liver damage, as PD-L1 is a co-receptor that negatively regulates T cell function. Similar protection was observed during pharmacological intervention using recombinant PD-L1-Fc. N-acetylcysteine blocked the downregulation of PD-L1 suggesting the involvement of reactive oxygen species. This was confirmed in vivo, as we observed significant upregulation of PD-L1 expression in NOX4 knockout mice, following sham operation, whereas its expression in global as well as myeloid lineage NOX2 knockout mice was comparable to that in the wild type animals. PD-L1 expression remained high following CLP only in total NOX2 knockouts, resulting in significantly reduced release of liver damage markers.

Conclusion:

These results suggest that, contrary to common assumption, maintaining PD-L1 expression on hepatocytes improves liver damage and survival of mice during sepsis. We conclude that administering recombinant PD-L1 or inhibiting NOX2 activity might offer a new therapeutic option in sepsis.

Assuntos

Antígeno B7-H1/imunologia; Fígado/imunologia; Sepse/imunologia; Linfócitos T Citotóxicos/imunologia; Animais; Modelos Animais de Doenças; Regulação para Baixo/imunologia; Hepatopatias/imunologia; Ativação Linfocitária/imunologia; Camundongos; Camundongos Endogâmicos C57BL; Camundongos Knockout; Regulação para Cima/imunologia

Palavras-chave

PD-L1; cytotoxic T cells; liver; reactive oxygen species; sepsis

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Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Assunto principal: Linfócitos T Citotóxicos / Sepse / Antígeno B7-H1 / Fígado Limite: Animals Idioma: En Ano de publicação: 2019 Tipo de documento: Article

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