Your search keyword '"Roca Suarez, Armando Andres"' showing total 9 results

1. Interspecies comparison of the early transcriptomic changes associated with hepatitis B virus exposure in human and macaque immune cell populations.

Author

Roca Suarez, Armando Andres, Planel, Séverine, Grand, Xavier, Couturier, Céline, Trang Tran, Porcheray, Fabrice, Becker, Jérémie, Reynier, Frédéric, Delgado, Ana, Cascales, Elodie, Peyrot, Loïc, Tamellini, Andrea, Saliou, Adrien, Elie, Céline, Baum, Chloé, Bao Quoc Vuong, Testoni, Barbara, Roques, Pierre, Zoulim, Fabien, and Hasan, Uzma

Subjects

HEPATITIS B virus, B cells, CELL populations, MACAQUES, TRANSCRIPTOMES, INTERFERON gamma

Abstract

Background and aims: Hepatitis B virus (HBV) infection affects 300 million individuals worldwide, representing a major factor for the development of hepatic complications. Although existing antivirals are effective in suppressing replication, eradication of HBV is not achieved. Therefore, a multi-faceted approach involving antivirals and immunomodulatory agents is required. Non-human primates are widely used in pre-clinical studies due to their close evolutionary relationship to humans. Nonetheless, it is fundamental to identify the differences in immune response between humans and these models. Thus, we performed a transcriptomic characterization and interspecies comparison of the early immune responses to HBV in human and cynomolgus macaques. Methods: We characterized early transcriptomic changes in human and cynomolgus B cells, T cells, myeloid and plasmacytoid dendritic cells (pDC) exposed to HBV ex vivo for 2 hours. Differentially-expressed genes were further compared to the profiles of HBV-infected patients using publicly-available single-cell data. Results: HBV induced a wide variety of transcriptional changes in all cell types, with common genes between species representing only a small proportion. In particular, interferon gamma signaling was repressed in human pDCs. At the gene level, interferon gamma inducible protein 16 (IFI16) was upregulated in macaque pDCs, while downregulated in humans. Moreover, IFI16 expression in pDCs from chronic HBV-infected patients anti-paralleled serum HBsAg levels. Conclusion: Our characterization of early transcriptomic changes induced by HBV in humans and cynomolgus macaques represents a useful resource for the identification of shared and divergent host responses, as well as potential immune targets against HBV. [ABSTRACT FROM AUTHOR]

Published

2023

2. HBV 2021: New therapeutic strategies against an old foe.

Author

Roca Suarez, Armando Andres, Testoni, Barbara, and Zoulim, Fabien

Subjects

HEPATITIS B virus, HEPATITIS B, THERAPEUTICS, HEPATOCELLULAR carcinoma

Abstract

Hepatitis B virus (HBV) affects more than 250 million people worldwide, and is one of the major aetiologies for the development of cirrhosis and hepatocellular carcinoma (HCC). In spite of universal vaccination programs, HBV infection is still a public health problem, and the limited number of available therapeutic approaches complicates the clinical management of these patients. Thus, HBV infection remains an unmet medical need that requires a continuous effort to develop new individual molecules, treatment combinations and even completely novel therapeutic strategies to achieve the goal of HBV elimination. The following review provides an overview of the current situation in chronic HBV infection, with an analysis of the scientific rationale of certain clinical interventions and, more importantly, explores the most recent developments in the field of HBV drug discovery. [ABSTRACT FROM AUTHOR]

Published

2021

3. Nucleic Acid-Induced Signaling in Chronic Viral Liver Disease.

Author

Roca Suarez, Armando Andres, Testoni, Barbara, Baumert, Thomas F., and Lupberger, Joachim

Subjects

VIRUS diseases, LIVER diseases, HEPATITIS C virus, HEPATITIS B virus, HEPATIC fibrosis

Abstract

A hallmark for the development and progression of chronic liver diseases is the persistent dysregulation of signaling pathways related to inflammatory responses, which eventually promotes the development of hepatic fibrosis, cirrhosis and hepatocellular carcinoma (HCC). The two major etiological agents associated with these complications in immunocompetent patients are hepatitis B virus (HBV) and hepatitis C virus (HCV), accounting for almost 1.4 million liver disease-associated deaths worldwide. Although both differ significantly from the point of their genomes and viral life cycles, they exert not only individual but also common strategies to divert innate antiviral defenses. Multiple virus-modulated pathways implicated in stress and inflammation illustrate how chronic viral hepatitis persistently tweaks host signaling processes with important consequences for liver pathogenesis. The following review aims to summarize the molecular events implicated in the sensing of viral nucleic acids, the mechanisms employed by HBV and HCV to counter these measures and how the dysregulation of these cellular pathways drives the development of chronic liver disease and the progression toward HCC. [ABSTRACT FROM AUTHOR]

Published

2021

4. Targeting clinical epigenetic reprogramming for chemoprevention of metabolic and viral hepatocellular carcinoma.

Author

Jühling, Frank, Hamdane, Nourdine, Crouchet, Emilie, Li, Shen, Saghire, Houssein El, Mukherji, Atish, Fujiwara, Naoto, Oudot, Marine A., Thumann, Christine, Saviano, Antonio, Roca Suarez, Armando Andres, Goto, Kaku, Masia, Ricard, Sojoodi, Mozhdeh, Arora, Gunisha, Aikata, Hiroshi, Ono, Atsushi, Tabrizian, Parissa, Schwartz, Myron, and Polyak, Stephen J.

Subjects

HEPATOCELLULAR carcinoma, FATTY liver, HUMAN carcinogenesis, EPIGENETICS, MEDICAL sciences

Published

2021

5. Viral manipulation of STAT3: Evade, exploit, and injure.

Author

Roca Suarez, Armando Andres, Van Renne, Nicolaas, Baumert, Thomas F., and Lupberger, Joachim

Subjects

IMMUNE response, INFLAMMATION, ANTIVIRAL agents, CELLULAR signal transduction, STAT proteins

Abstract

Signal transducer and activator of transcription 3 (STAT3) is a key regulator of numerous physiological functions, including the immune response. As pathogens elicit an acute phase response with concerted activation of STAT3, they are confronted with two evolutionary options: either curtail it or employ it. This has important consequences for the host, since abnormal STAT3 function is associated with cancer development and other diseases. This review provides a comprehensive outline of how human viruses cope with STAT3-mediated inflammation and how this affects the host. Finally, we discuss STAT3 as a potential target for antiviral therapy. [ABSTRACT FROM AUTHOR]

Published

2018

6. GOLT1B Activation in Hepatitis C Virus-Infected Hepatocytes Links ER Trafficking and Viral Replication.

Author

Butterworth, Jacqueline, Gregoire, Damien, Peter, Marion, Roca Suarez, Armando Andres, Desandré, Guillaume, Simonin, Yannick, Virzì, Alessia, Zine El Aabidine, Amal, Guivarch, Marine, Andrau, Jean-Christophe, Bertrand, Edouard, Assenat, Eric, Lupberger, Joachim, and Hibner, Urszula

Subjects

VIRAL replication, CHRONIC hepatitis C, FROZEN tissue sections, UNFOLDED protein response, HEPATITIS C virus, VIRAL hepatitis, HEPATITIS C

Abstract

Chronic hepatitis C carries a high risk of development of hepatocellular carcinoma (HCC), triggered by both direct and indirect effects of the virus. We examined cell-autonomous alterations in gene expression profiles associated with hepatitis C viral presence. Highly sensitive single molecule fluorescent in situ hybridization applied to frozen tissue sections of a hepatitis C patient allowed the delineation of clusters of infected hepatocytes. Laser microdissection followed by RNAseq analysis of hepatitis C virus (HCV)-positive and -negative regions from the tumoral and non-tumoral tissues from the same patient revealed HCV-related deregulation of expression of genes in the tumor and in the non-tumoral tissue. However, there was little overlap between both gene sets. Our interest in alterations that increase the probability of tumorigenesis prompted the examination of genes whose expression was increased by the virus in the non-transformed cells and whose level remained high in the tumor. This strategy led to the identification of a novel HCV target gene: GOLT1B, which encodes a protein involved in ER-Golgi trafficking. We further show that GOLT1B expression is induced during the unfolded protein response, that its presence is essential for efficient viral replication, and that its expression is correlated with poor outcome in HCC. [ABSTRACT FROM AUTHOR]

Published

2022

7. Hepatitis C Virus and Hepatocellular Carcinoma: When the Host Loses Its Grip.

Author

Goto, Kaku, Roca Suarez, Armando Andres, Wrensch, Florian, Baumert, Thomas F., and Lupberger, Joachim

Subjects

HEPATITIS C virus, HEPATOCELLULAR carcinoma, CHRONIC hepatitis C, VIRAL proteins, VIRUS diseases, LIVER diseases, HEPATITIS C

Abstract

Chronic infection with hepatitis C virus (HCV) is a major cause of hepatocellular carcinoma (HCC). Novel treatments with direct-acting antivirals achieve high rates of sustained virologic response; however, the HCC risk remains elevated in cured patients, especially those with advanced liver disease. Long-term HCV infection causes a persistent and accumulating damage of the liver due to a combination of direct and indirect pro-oncogenic mechanisms. This review describes the processes involved in virus-induced disease progression by viral proteins, derailed signaling, immunity, and persistent epigenetic deregulation, which may be instrumental to develop urgently needed prognostic biomarkers and as targets for novel chemopreventive therapies. [ABSTRACT FROM AUTHOR]

Published

2020

8. Tight Junction Proteins and the Biology of Hepatobiliary Disease.

Author

Roehlen, Natascha, Roca Suarez, Armando Andres, El Saghire, Houssein, Saviano, Antonio, Schuster, Catherine, Lupberger, Joachim, and Baumert, Thomas F.

Subjects

TIGHT junctions, BIOLOGY, MEMBRANE proteins, HEPATITIS C virus, ADAPTOR proteins, CELL adhesion

Abstract

Tight junctions (TJ) are intercellular adhesion complexes on epithelial cells and composed of integral membrane proteins as well as cytosolic adaptor proteins. Tight junction proteins have been recognized to play a key role in health and disease. In the liver, TJ proteins have several functions: they contribute as gatekeepers for paracellular diffusion between adherent hepatocytes or cholangiocytes to shape the blood-biliary barrier (BBIB) and maintain tissue homeostasis. At non-junctional localizations, TJ proteins are involved in key regulatory cell functions such as differentiation, proliferation, and migration by recruiting signaling proteins in response to extracellular stimuli. Moreover, TJ proteins are hepatocyte entry factors for the hepatitis C virus (HCV)—a major cause of liver disease and cancer worldwide. Perturbation of TJ protein expression has been reported in chronic HCV infection, cholestatic liver diseases as well as hepatobiliary carcinoma. Here we review the physiological function of TJ proteins in the liver and their implications in hepatobiliary diseases. [ABSTRACT FROM AUTHOR]

Published

2020

9. Oncogenic Signaling Induced by HCV Infection.

Author

Virzì, Alessia, Roca Suarez, Armando Andres, Baumert, Thomas F., and Lupberger, Joachim

Subjects

HEPATITIS C virus, HEPATITIS C, FLAVIVIRAL diseases, LIVER diseases, LIVER cancer, LIVER disease treatment

Abstract

The liver is frequently exposed to toxins, metabolites, and oxidative stress, which can challenge organ function and genomic stability. Liver regeneration is therefore a highly regulated process involving several sequential signaling events. It is thus not surprising that individual oncogenic mutations in hepatocytes do not necessarily lead to cancer and that the genetic profiles of hepatocellular carcinomas (HCCs) are highly heterogeneous. Long-term infection with hepatitis C virus (HCV) creates an oncogenic environment by a combination of viral protein expression, persistent liver inflammation, oxidative stress, and chronically deregulated signaling events that cumulate as a tipping point for genetic stability. Although novel direct-acting antivirals (DAA)-based treatments efficiently eradicate HCV, the associated HCC risk cannot be fully eliminated by viral cure in patients with advanced liver disease. This suggests that HCV may persistently deregulate signaling pathways beyond viral cure and thereby continue to perturb cancer-relevant gene function. In this review, we summarize the current knowledge about oncogenic signaling pathways derailed by chronic HCV infection. This will not only help to understand the mechanisms of hepatocarcinogenesis but will also highlight potential chemopreventive strategies to help patients with a high-risk profile of developing HCC. [ABSTRACT FROM AUTHOR]

Published

2018