2022
DOI: 10.1371/journal.pone.0264266
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Protocol for chronic hepatitis B virus infection mouse model development by patient-derived orthotopic xenografts

Abstract: Background According to the World Health Organization, more than 250 million people worldwide are chronically infected with the hepatitis B virus, and almost 800.000 patients die annually of mediated liver disorders. Therefore, adequate biological test systems are needed that could fully simulate the course of chronic hepatitis B virus infection, including in patients with hepatocellular carcinoma. Methods In this study, we will assess the effectiveness of existing protocols for isolation and cultivation of … Show more

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Cited by 3 publications
(4 citation statements)
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“…TLR response to HBV infection in many animal models has been well investigated ( 46 , 47 ). In animal models, TLR2 activation has been shown to expedite HBV clearance and improve HBV-specific T-cell responses ( 48 ).…”
Section: Tlr Response To Hbv Infection In Humanmentioning
confidence: 99%
“…TLR response to HBV infection in many animal models has been well investigated ( 46 , 47 ). In animal models, TLR2 activation has been shown to expedite HBV clearance and improve HBV-specific T-cell responses ( 48 ).…”
Section: Tlr Response To Hbv Infection In Humanmentioning
confidence: 99%
“…Lastly, TK-NOG mice were developed by expressing herpes simplex virus thymidine kinase (HSV-tk) driven by mouse liver protein promoters. This enzyme phosphorylates nontoxic ganciclovir (GCV) into a highly toxic metabolite, effectively eliminating mouse hepatocytes . Among these models, uPA mice support HBV replication, facilitating antiviral testing, immunotherapy engineering, analysis of genotype-specific antigen expression, and investigations into innate immunity .…”
Section: Infection and Replication System Of Hbvmentioning
confidence: 99%
“…This enzyme phosphorylates nontoxic ganciclovir (GCV) into a highly toxic metabolite, effectively eliminating mouse hepatocytes. 45 Among these models, uPA mice support HBV replication, facilitating antiviral testing, immunotherapy engineering, analysis of genotype-specific antigen expression, and investigations into innate immunity. 7 However, due to hepatotoxicity or uPA gene overexpression, newborn mice exhibit hemolysis, chronic liver agenesis, or hypofibrinogenemia 4 days after delivery, and are prone to complement reaction after human hepatocyte transplantation, resulting in kidney function impairment and elevated mortality.…”
Section: ■ Infection and Replication System Of Hbvmentioning
confidence: 99%
“…It depends on the interaction among virus, host and environmental factors when HCV carriers developed into HCC. The HCV genome cannot be integrated into the host genome, but it can damage the host liver cells DNA through viral proteins and ROS producing by some certain carcinogenesis pathways, causing gene mutation and HCC occurrence 180 . It is possible for HBV carriers or HCV carriers to develop cancer due to some certain factors, such as sex, age, family history, viral load, infection time, coinfection with other virus (HDV, HIV, HBV/HDV), environmental factors, and so on 181 .…”
Section: Human Carcinogenic or Cancer‐promoting Microbiomesmentioning
confidence: 99%