Molecular Mechanism for Protection Against Liver Failure in Human Yellow Fever Infection
Yellow fever (YF) is a viral hemorrhagic fever that typically involves the liver. Brazil recently experienced its largest recorded YF outbreak, and the disease was fatal in more than a third of affected individuals, mostly because of acute liver failure. Affected individuals are generally treated on...
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| Format: | Article |
| Language: | English |
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Wiley
2020-05-01
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| Series: | Hepatology Communications |
| Online Access: | https://doi.org/10.1002/hep4.1504 |
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doaj-59d27a4e58c44022a13225226bebe6d8 |
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Article |
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DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Fernanda de Oliveira Lemos Andressa França Antônio Carlos Melo Lima Filho Rodrigo M. Florentino Marcone Loiola Santos Dabny G. Missiaggia Gisele Olinto Libanio Rodrigues Felipe Ferraz Dias Ingredy Beatriz Souza Passos Mauro M. Teixeira Antônio Márcio de Faria Andrade Cristiano Xavier Lima Paula Vieira Teixeira Vidigal Vivian Vasconcelos Costa Matheus Castro Fonseca Michael H. Nathanson M. Fatima Leite |
| spellingShingle |
Fernanda de Oliveira Lemos Andressa França Antônio Carlos Melo Lima Filho Rodrigo M. Florentino Marcone Loiola Santos Dabny G. Missiaggia Gisele Olinto Libanio Rodrigues Felipe Ferraz Dias Ingredy Beatriz Souza Passos Mauro M. Teixeira Antônio Márcio de Faria Andrade Cristiano Xavier Lima Paula Vieira Teixeira Vidigal Vivian Vasconcelos Costa Matheus Castro Fonseca Michael H. Nathanson M. Fatima Leite Molecular Mechanism for Protection Against Liver Failure in Human Yellow Fever Infection Hepatology Communications |
| author_facet |
Fernanda de Oliveira Lemos Andressa França Antônio Carlos Melo Lima Filho Rodrigo M. Florentino Marcone Loiola Santos Dabny G. Missiaggia Gisele Olinto Libanio Rodrigues Felipe Ferraz Dias Ingredy Beatriz Souza Passos Mauro M. Teixeira Antônio Márcio de Faria Andrade Cristiano Xavier Lima Paula Vieira Teixeira Vidigal Vivian Vasconcelos Costa Matheus Castro Fonseca Michael H. Nathanson M. Fatima Leite |
| author_sort |
Fernanda de Oliveira Lemos |
| title |
Molecular Mechanism for Protection Against Liver Failure in Human Yellow Fever Infection |
| title_short |
Molecular Mechanism for Protection Against Liver Failure in Human Yellow Fever Infection |
| title_full |
Molecular Mechanism for Protection Against Liver Failure in Human Yellow Fever Infection |
| title_fullStr |
Molecular Mechanism for Protection Against Liver Failure in Human Yellow Fever Infection |
| title_full_unstemmed |
Molecular Mechanism for Protection Against Liver Failure in Human Yellow Fever Infection |
| title_sort |
molecular mechanism for protection against liver failure in human yellow fever infection |
| publisher |
Wiley |
| series |
Hepatology Communications |
| issn |
2471-254X |
| publishDate |
2020-05-01 |
| description |
Yellow fever (YF) is a viral hemorrhagic fever that typically involves the liver. Brazil recently experienced its largest recorded YF outbreak, and the disease was fatal in more than a third of affected individuals, mostly because of acute liver failure. Affected individuals are generally treated only supportively, but during the recent Brazilian outbreak, selected patients were treated with liver transplant. We took advantage of this clinical experience to better characterize the clinical and pathological features of YF‐induced liver failure and to examine the mechanism of hepatocellular injury in YF, to identify targets that would be amenable to therapeutic intervention in preventing progression to liver failure and death. Patients with YF liver failure rapidly developed massive transaminase elevations, with jaundice, coagulopathy, thrombocytopenia, and usually hepatic encephalopathy, along with pathological findings that included microvesicular steatosis and lytic necrosis. Hepatocytes began to express the type 3 isoform of the inositol trisphosphate receptor (ITPR3), an intracellular calcium (Ca2+) channel that is not normally expressed in hepatocytes. Experiments in an animal model, isolated hepatocytes, and liver‐derived cell lines showed that this new expression of ITPR3 was associated with increased nuclear Ca2+ signaling and hepatocyte proliferation, and reduced steatosis and cell death induced by the YF virus. Conclusion: Yellow fever often induces liver failure characterized by massive hepatocellular damage plus steatosis. New expression of ITPR3 also occurs in YF‐infected hepatocytes, which may represent an endogenous protective mechanism that could suggest approaches to treat affected individuals before they progress to liver failure, thereby decreasing the mortality of this disease in a way that does not rely on the costly and limited resource of liver transplantation. |
| url |
https://doi.org/10.1002/hep4.1504 |
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doaj-59d27a4e58c44022a13225226bebe6d82020-11-25T02:20:23ZengWileyHepatology Communications2471-254X2020-05-014565766910.1002/hep4.1504Molecular Mechanism for Protection Against Liver Failure in Human Yellow Fever InfectionFernanda de Oliveira Lemos0Andressa França1Antônio Carlos Melo Lima Filho2Rodrigo M. Florentino3Marcone Loiola Santos4Dabny G. Missiaggia5Gisele Olinto Libanio Rodrigues6Felipe Ferraz Dias7Ingredy Beatriz Souza Passos8Mauro M. Teixeira9Antônio Márcio de Faria Andrade10Cristiano Xavier Lima11Paula Vieira Teixeira Vidigal12Vivian Vasconcelos Costa13Matheus Castro Fonseca14Michael H. Nathanson15M. Fatima Leite16Department of Physiology and Biophysics Universidade Federal de Minas Gerais Belo Horizonte BrazilDepartment of Physiology and Biophysics Universidade Federal de Minas Gerais Belo Horizonte BrazilDepartment of Physiology and Biophysics Universidade Federal de Minas Gerais Belo Horizonte BrazilDepartment of Physiology and Biophysics Universidade Federal de Minas Gerais Belo Horizonte BrazilDepartment of Physiology and Biophysics Universidade Federal de Minas Gerais Belo Horizonte BrazilDepartment of Physiology and Biophysics Universidade Federal de Minas Gerais Belo Horizonte BrazilDepartment of Biochemistry and Immunology Universidade Federal de Minas Gerais Belo Horizonte BrazilCenter of Microscopy Universidade Federal de Minas Gerais Belo Horizonte BrazilDepartment of Morphology Universidade Federal de Minas Gerais Belo Horizonte BrazilDepartment of Biochemistry and Immunology Universidade Federal de Minas Gerais Belo Horizonte BrazilHepatic Transplant Service Hospital Felício Rocho Belo Horizonte BrazilHepatic Transplant Service Hospital Felício Rocho Belo Horizonte BrazilPathological Anatomy and Forensic Medicine Universidade Federal de Minas Gerais Belo Horizonte BrazilDepartment of Morphology Universidade Federal de Minas Gerais Belo Horizonte BrazilBrazilian Biosciences National Laboratory (LNBio) Brazilian Center for Research in Energy and Materials Rua Giuseppe Máximo Scolfaro Campinas BrazilSection of Digestive Diseases Department of Internal Medicine Yale University School of Medicine New Haven CTDepartment of Physiology and Biophysics Universidade Federal de Minas Gerais Belo Horizonte BrazilYellow fever (YF) is a viral hemorrhagic fever that typically involves the liver. Brazil recently experienced its largest recorded YF outbreak, and the disease was fatal in more than a third of affected individuals, mostly because of acute liver failure. Affected individuals are generally treated only supportively, but during the recent Brazilian outbreak, selected patients were treated with liver transplant. We took advantage of this clinical experience to better characterize the clinical and pathological features of YF‐induced liver failure and to examine the mechanism of hepatocellular injury in YF, to identify targets that would be amenable to therapeutic intervention in preventing progression to liver failure and death. Patients with YF liver failure rapidly developed massive transaminase elevations, with jaundice, coagulopathy, thrombocytopenia, and usually hepatic encephalopathy, along with pathological findings that included microvesicular steatosis and lytic necrosis. Hepatocytes began to express the type 3 isoform of the inositol trisphosphate receptor (ITPR3), an intracellular calcium (Ca2+) channel that is not normally expressed in hepatocytes. Experiments in an animal model, isolated hepatocytes, and liver‐derived cell lines showed that this new expression of ITPR3 was associated with increased nuclear Ca2+ signaling and hepatocyte proliferation, and reduced steatosis and cell death induced by the YF virus. Conclusion: Yellow fever often induces liver failure characterized by massive hepatocellular damage plus steatosis. New expression of ITPR3 also occurs in YF‐infected hepatocytes, which may represent an endogenous protective mechanism that could suggest approaches to treat affected individuals before they progress to liver failure, thereby decreasing the mortality of this disease in a way that does not rely on the costly and limited resource of liver transplantation.https://doi.org/10.1002/hep4.1504 |