The Inside-Out of End-Stage Liver Disease: Hepatocytes are the Keystone

Haep, Nils; Florentino, Rodrigo M.; Squires, James E.; Bell, Aaron; Soto-Gutiérrez, Alejandro

doi:10.1055/s-0041-1725023

Cited by 17 publications

(5 citation statements)

References 116 publications

(156 reference statements)

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“…However, evidence accumulated over the past two decades indicates that breakdown of hepatic function cannot be simply ascribed to reduced parenchymal mass. Functional deficiencies of chronically injured and regenerating hepatocytes may underlie liver failure in cirrhosis, and these can be related to an impairment in the expression of genes that typify the mature hepatocyte phenotype [20,21]. Herein, after summarizing the current understanding of how hepatocellular differentiation occurs during development, we will discuss mechanisms leading to the loss of hepatocellular identity and organ dysfunction in chronic liver injury.…”

Section: Introductionmentioning

confidence: 99%

Loss of liver function in chronic liver disease: An identity crisis

Berasain¹,

Arechederra²,

Argemí³

et al. 2023

Journal of Hepatology

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Section: Introductionmentioning

confidence: 99%

Loss of liver function in chronic liver disease: An identity crisis

Berasain¹,

Arechederra²,

Argemí³

et al. 2023

Journal of Hepatology

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“…These hepatocytes may therefore have different gene expression than what would be expected in early disease, as supported by published reports describing altered gene expression and immune dysfunction in advanced stages of liver disease. 19 , 28 , 29 Additionally, there may also be an association with paradoxical expression of these genes and advanced disease progression, which we may be inadvertently selecting due to our samples being exclusively from end-stage, transplant patients with PBC and PSC.…”

Section: Discussionmentioning

confidence: 99%

Human Hepatocellular response in Cholestatic Liver Diseases

Ortiz,

Cetin,

Sun

et al. 2023

Organogenesis

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Primary biliary cholangitis (PBC) and primary sclerosing cholangitis (PSC), the most common types of cholestatic liver disease (CLD), result in enterohepatic obstruction, bile acid accumulation, and hepatotoxicity. The mechanisms by which hepatocytes respond to and cope with CLD remain largely unexplored. This study includes the characterization of hepatocytes isolated from explanted livers of patients with PBC and PSC. We examined the expression of hepatocyte-specific genes, intracellular bile acid (BA) levels, and oxidative stress in primary-human-hepatocytes (PHHs) isolated from explanted livers of patients with PBC and PSC and compared them with control normal human hepatocytes. Our findings provide valuable initial insights into the hepatocellular response to cholestasis in CLD and help support the use of PHHs as an experimental tool for these diseases.

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“…As cirrhosis advances, complications such as portal hypertension develop, and there is an escalated risk of HCC due to neoplastic transformations within the hepatic parenchyma [ 255 , 256 ]. Understanding this pathophysiological process that culminates in end-stage liver disease is necessary for timely and effective therapeutic interventions to halt or reverse the fibrosis processes in chronic HCV infection [ 257 , 258 ].…”

Section: Clinical and Histopathologic Features Of Hepatitis Cmentioning

confidence: 99%

Contemporary Insights into Hepatitis C Virus: A Comprehensive Review

Sallam,

Khalil

2024

Microorganisms

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Hepatitis C virus (HCV) remains a significant global health challenge. Approximately 50 million people were living with chronic hepatitis C based on the World Health Organization as of 2024, contributing extensively to global morbidity and mortality. The advent and approval of several direct-acting antiviral (DAA) regimens significantly improved HCV treatment, offering potentially high rates of cure for chronic hepatitis C. However, the promising aim of eventual HCV eradication remains challenging. Key challenges include the variability in DAA access across different regions, slightly variable response rates to DAAs across diverse patient populations and HCV genotypes/subtypes, and the emergence of resistance-associated substitutions (RASs), potentially conferring resistance to DAAs. Therefore, periodic reassessment of current HCV knowledge is needed. An up-to-date review on HCV is also necessitated based on the observed shifts in HCV epidemiological trends, continuous development and approval of therapeutic strategies, and changes in public health policies. Thus, the current comprehensive review aimed to integrate the latest knowledge on the epidemiology, pathophysiology, diagnostic approaches, treatment options and preventive strategies for HCV, with a particular focus on the current challenges associated with RASs and ongoing efforts in vaccine development. This review sought to provide healthcare professionals, researchers, and policymakers with the necessary insights to address the HCV burden more effectively. We aimed to highlight the progress made in managing and preventing HCV infection and to highlight the persistent barriers challenging the prevention of HCV infection. The overarching goal was to align with global health objectives towards reducing the burden of chronic hepatitis, aiming for its eventual elimination as a public health threat by 2030.

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The Inside-Out of End-Stage Liver Disease: Hepatocytes are the Keystone

Cited by 17 publications

References 116 publications

Loss of liver function in chronic liver disease: An identity crisis

Loss of liver function in chronic liver disease: An identity crisis

Human Hepatocellular response in Cholestatic Liver Diseases

Contemporary Insights into Hepatitis C Virus: A Comprehensive Review

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