Aggravation of viral hepatitis by platelet-derived serotonin

Philipp A. Lang; Claudio Contaldo; Panco Georgiev; Ashraf Mohammad El-Badry; Mike Recher; Michael Kurrer; Luisa Cervantes-Barragan; Burkhard Ludewig; Thomas Calzascia; Beatrice Bolinger; Doron Merkler; Bernhard Odermatt; Michael Bader; Rolf Graf; Pierre Alain Clavien; Ahmed N. Hegazy; Max Löhning; Nicola L. Harris; Pamela S. Ohashi; Hans Hengartner; Rolf M. Zinkernagel; Karl S. Lang

doi:10.1038/nm1780

Aggravation of viral hepatitis by platelet-derived serotonin

Philipp A. Lang, Claudio Contaldo, Panco Georgiev, Ashraf Mohammad El-Badry, Mike Recher, Michael Kurrer, Luisa Cervantes-Barragan, Burkhard Ludewig, Thomas Calzascia, Beatrice Bolinger, Doron Merkler, Bernhard Odermatt, Michael Bader, Rolf Graf, Pierre Alain Clavien, Ahmed N. Hegazy, Max Löhning, Nicola L. Harris, Pamela S. Ohashi, Hans HengartnerRolf M. Zinkernagel, Karl S. Lang

Research output: Contribution to journal › Article › Research › peer-review

205 Citations (Scopus)

Abstract

More than 500 million people worldwide are persistently infected with hepatitis B virus or hepatitis C virus. Although both viruses are poorly cytopathic, persistence of either virus carries a risk of chronic liver inflammation, potentially resulting in liver steatosis, liver cirrhosis, end-stage liver failure or hepatocellular carcinoma. Virus-specific T cells are a major determinant of the outcome of hepatitis, as they contribute to the early control of chronic hepatitis viruses, but they also mediate immunopathology during persistent virus infection. We have analyzed the role of platelet-derived vasoactive serotonin during virus-induced CD8⁺ T cell-dependent immunopathological hepatitis in mice infected with the noncytopathic lymphocytic choriomeningitis virus. After virus infection, platelets were recruited to the liver, and their activation correlated with severely reduced sinusoidal microcirculation, delayed virus elimination and increased immunopathological liver cell damage. Lack of platelet-derived serotonin in serotonin-deficient mice normalized hepatic microcirculatory dysfunction, accelerated virus clearance in the liver and reduced CD8⁺ T cell-dependent liver cell damage. In keeping with these observations, serotonin treatment of infected mice delayed entry of activated CD8⁺ T cells into the liver, delayed virus control and aggravated immunopathological hepatitis. Thus, vasoactive serotonin supports virus persistence in the liver and aggravates virus-induced immunopathology.

Original language	English
Pages (from-to)	756-761
Number of pages	6
Journal	Nature Medicine
Volume	14
Issue number	7
DOIs	https://doi.org/10.1038/nm1780
Publication status	Published - 1 Jul 2008
Externally published	Yes

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Lang, P. A., Contaldo, C., Georgiev, P., El-Badry, A. M., Recher, M., Kurrer, M., Cervantes-Barragan, L., Ludewig, B., Calzascia, T., Bolinger, B., Merkler, D., Odermatt, B., Bader, M., Graf, R., Clavien, P. A., Hegazy, A. N., Löhning, M., Harris, N. L., Ohashi, P. S., ... Lang, K. S. (2008). Aggravation of viral hepatitis by platelet-derived serotonin. Nature Medicine, 14(7), 756-761. https://doi.org/10.1038/nm1780

@article{e6c8b48a81ce4b8f99c708231c946a84,

title = "Aggravation of viral hepatitis by platelet-derived serotonin",

abstract = "More than 500 million people worldwide are persistently infected with hepatitis B virus or hepatitis C virus. Although both viruses are poorly cytopathic, persistence of either virus carries a risk of chronic liver inflammation, potentially resulting in liver steatosis, liver cirrhosis, end-stage liver failure or hepatocellular carcinoma. Virus-specific T cells are a major determinant of the outcome of hepatitis, as they contribute to the early control of chronic hepatitis viruses, but they also mediate immunopathology during persistent virus infection. We have analyzed the role of platelet-derived vasoactive serotonin during virus-induced CD8+ T cell-dependent immunopathological hepatitis in mice infected with the noncytopathic lymphocytic choriomeningitis virus. After virus infection, platelets were recruited to the liver, and their activation correlated with severely reduced sinusoidal microcirculation, delayed virus elimination and increased immunopathological liver cell damage. Lack of platelet-derived serotonin in serotonin-deficient mice normalized hepatic microcirculatory dysfunction, accelerated virus clearance in the liver and reduced CD8+ T cell-dependent liver cell damage. In keeping with these observations, serotonin treatment of infected mice delayed entry of activated CD8+ T cells into the liver, delayed virus control and aggravated immunopathological hepatitis. Thus, vasoactive serotonin supports virus persistence in the liver and aggravates virus-induced immunopathology.",

author = "Lang, {Philipp A.} and Claudio Contaldo and Panco Georgiev and El-Badry, {Ashraf Mohammad} and Mike Recher and Michael Kurrer and Luisa Cervantes-Barragan and Burkhard Ludewig and Thomas Calzascia and Beatrice Bolinger and Doron Merkler and Bernhard Odermatt and Michael Bader and Rolf Graf and Clavien, {Pierre Alain} and Hegazy, {Ahmed N.} and Max L{\"o}hning and Harris, {Nicola L.} and Ohashi, {Pamela S.} and Hans Hengartner and Zinkernagel, {Rolf M.} and Lang, {Karl S.}",

year = "2008",

month = jul,

day = "1",

doi = "10.1038/nm1780",

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Lang, PA, Contaldo, C, Georgiev, P, El-Badry, AM, Recher, M, Kurrer, M, Cervantes-Barragan, L, Ludewig, B, Calzascia, T, Bolinger, B, Merkler, D, Odermatt, B, Bader, M, Graf, R, Clavien, PA, Hegazy, AN, Löhning, M, Harris, NL, Ohashi, PS, Hengartner, H, Zinkernagel, RM & Lang, KS 2008, 'Aggravation of viral hepatitis by platelet-derived serotonin', Nature Medicine, vol. 14, no. 7, pp. 756-761. https://doi.org/10.1038/nm1780

TY - JOUR

T1 - Aggravation of viral hepatitis by platelet-derived serotonin

AU - Lang, Philipp A.

AU - Contaldo, Claudio

AU - Georgiev, Panco

AU - El-Badry, Ashraf Mohammad

AU - Recher, Mike

AU - Kurrer, Michael

AU - Cervantes-Barragan, Luisa

AU - Ludewig, Burkhard

AU - Calzascia, Thomas

AU - Bolinger, Beatrice

AU - Merkler, Doron

AU - Odermatt, Bernhard

AU - Bader, Michael

AU - Graf, Rolf

AU - Clavien, Pierre Alain

AU - Hegazy, Ahmed N.

AU - Löhning, Max

AU - Harris, Nicola L.

AU - Ohashi, Pamela S.

AU - Hengartner, Hans

AU - Zinkernagel, Rolf M.

AU - Lang, Karl S.

PY - 2008/7/1

Y1 - 2008/7/1

N2 - More than 500 million people worldwide are persistently infected with hepatitis B virus or hepatitis C virus. Although both viruses are poorly cytopathic, persistence of either virus carries a risk of chronic liver inflammation, potentially resulting in liver steatosis, liver cirrhosis, end-stage liver failure or hepatocellular carcinoma. Virus-specific T cells are a major determinant of the outcome of hepatitis, as they contribute to the early control of chronic hepatitis viruses, but they also mediate immunopathology during persistent virus infection. We have analyzed the role of platelet-derived vasoactive serotonin during virus-induced CD8+ T cell-dependent immunopathological hepatitis in mice infected with the noncytopathic lymphocytic choriomeningitis virus. After virus infection, platelets were recruited to the liver, and their activation correlated with severely reduced sinusoidal microcirculation, delayed virus elimination and increased immunopathological liver cell damage. Lack of platelet-derived serotonin in serotonin-deficient mice normalized hepatic microcirculatory dysfunction, accelerated virus clearance in the liver and reduced CD8+ T cell-dependent liver cell damage. In keeping with these observations, serotonin treatment of infected mice delayed entry of activated CD8+ T cells into the liver, delayed virus control and aggravated immunopathological hepatitis. Thus, vasoactive serotonin supports virus persistence in the liver and aggravates virus-induced immunopathology.

AB - More than 500 million people worldwide are persistently infected with hepatitis B virus or hepatitis C virus. Although both viruses are poorly cytopathic, persistence of either virus carries a risk of chronic liver inflammation, potentially resulting in liver steatosis, liver cirrhosis, end-stage liver failure or hepatocellular carcinoma. Virus-specific T cells are a major determinant of the outcome of hepatitis, as they contribute to the early control of chronic hepatitis viruses, but they also mediate immunopathology during persistent virus infection. We have analyzed the role of platelet-derived vasoactive serotonin during virus-induced CD8+ T cell-dependent immunopathological hepatitis in mice infected with the noncytopathic lymphocytic choriomeningitis virus. After virus infection, platelets were recruited to the liver, and their activation correlated with severely reduced sinusoidal microcirculation, delayed virus elimination and increased immunopathological liver cell damage. Lack of platelet-derived serotonin in serotonin-deficient mice normalized hepatic microcirculatory dysfunction, accelerated virus clearance in the liver and reduced CD8+ T cell-dependent liver cell damage. In keeping with these observations, serotonin treatment of infected mice delayed entry of activated CD8+ T cells into the liver, delayed virus control and aggravated immunopathological hepatitis. Thus, vasoactive serotonin supports virus persistence in the liver and aggravates virus-induced immunopathology.

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U2 - 10.1038/nm1780

DO - 10.1038/nm1780

M3 - Article

C2 - 18516052

AN - SCOPUS:46749155479

SN - 1078-8956

VL - 14

SP - 756

EP - 761

JO - Nature Medicine

JF - Nature Medicine

IS - 7

ER -

Aggravation of viral hepatitis by platelet-derived serotonin

Abstract

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