<i>HLA-DP</i>Polymorphisms Affect the Outcomes of Chronic Hepatitis B Virus Infections, Possibly through Interacting with Viral Mutations

Zhang, Qi; Yin, Jianhua; Zhang, Yuwei; Deng, Yang; Du, Yan; Pu, Rui; Han, Yaling; Zhao, Jingbo; Han, Xue; Zhang, Hongwei; Cao, Guangwen

doi:10.1128/jvi.02073-13

Cited by 56 publications

(75 citation statements)

References 53 publications

(79 reference statements)

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“…Virus mutations related to advanced liver disease seem to accumulate along the course of CHB Many of the virus mutations identified here affected genomic positions frequently associated with chronic hepatitis, liver cirrhosis and hepatocellular carcinoma (Table 2) (Yin et al, 2011;Zhang et al, 2013). Remarkably, such mutations were present in both the inactive carrier patient and the immunotolerant ones, supporting the idea of a continuous diversification along the course of CHB, accompanied by the emergence of mutants associated with serious liver conditions.…”

Section: T-cell Epitopessupporting

confidence: 62%

“…Furthermore, all the study patients presented virus mutations, many of which have been shown recently to correlate with serious liver conditions (Table 2) (Yin et al, 2011;Zhang et al, 2013). The discovery of such mutations in immune-tolerant patients is novel and possibly has been hampered to date due to the limited sensitivity of traditional genotyping approaches (i.e.…”

Section: Discussionmentioning

confidence: 99%

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Virus evolution during chronic hepatitis B virus infection as revealed by ultradeep sequencing data

Jones

Sede

Manrique

et al. 2016

Journal of General Virology

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Despite chronic hepatitis B virus (HBV) infection (CHB) being a leading cause of liver cirrhosis and cancer, HBV evolution during CHB is not fully understood. Recent studies have indicated that virus diversity progressively increases along the course of CHB and that some virus mutations correlate with severe liver conditions such as chronic hepatitis, cirrhosis and hepatocellular carcinoma. Using ultradeep sequencing (UDS) data from an intrafamilial case, we detected such mutations at low frequencies among three immunotolerant patients and at high frequencies in an inactive carrier. Furthermore, our analyses indicated that the HBV population from the seroconverter patient underwent many genetic changes in response to virus clearance. Together, these data indicate a potential use of UDS for developing non-invasive biomarkers for monitoring disease changes over time or in response to specific therapies. In addition, our analyses revealed that virus clearance seemed not to require the virus effective population size to decline. A detailed genetic analysis of the viral lineages arising during and after the clearance suggested that mutations at or close to critical elements of the core promoter (enhancer II, epsilon encapsidation signal, TA2, TA3 and direct repeat 1-hormone response element) might be responsible for a sustained replication. This hypothesis requires the decline in virus load to be explained by constant clearance of virus-producing hepatocytes, consistent with the sustained progress towards serious liver conditions experienced by many CHB patients.

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Section: T-cell Epitopessupporting

confidence: 62%

Section: Discussionmentioning

confidence: 99%

Virus evolution during chronic hepatitis B virus infection as revealed by ultradeep sequencing data

Jones

Sede

Manrique

et al. 2016

Journal of General Virology

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“…Of these mutations, A1762T/G1764A has been prospectively shown to be an independent risk factor of HCC (15,26). A1762T/ G1764A and A1762T/G1764A-based combo mutants are potentially selected by the immunocompromised microenvironment predisposed by genetic polymorphisms of key immune and proinflammatory molecules, and in turn promote an aggressive phenotype of HCC, as well as the recurrence of HCC after curative surgery (27)(28)(29)(30). The objective of this study was to clarify whether the baseline HBV mutations can predict the outcome of HBVinfected patients and whether HCC risk contributed by the HBV mutations can be selectively reduced by antiviral treatment.…”

Section: Introductionmentioning

confidence: 99%

Hepatitis B Virus Combo Mutations Improve the Prediction and Active Prophylaxis of Hepatocellular Carcinoma: A Clinic-Based Cohort Study

Yin

Wang

et al. 2015

Cancer Prevention Research

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We aimed to evaluate whether hepatitis B virus (HBV) mutations at the core promoter region could improve the prediction and specific prophylaxis of hepatocellular carcinoma (HCC) in chronic HBV-infected patients. A total of 2,114 HBV-infected patients enrolled between August 1998 and December 2007 were followed-up for 18,406 person-years. Of those, 612 received !48 week treatments with nucleos(t)ide analogue (NA) and/or IFNa.

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“…In our previous epidemiological studies, we found that the HLA-II genetic polymorphisms are statistically associated with the generation of the liver diseasesassociated HBV mutations. The HLA-DP polymorphisms rs3077 (CT + TT vs. CC), rs3135021 (GA + AA vs. GG), rs9277535 (GA + AA vs. GG), and rs2281388 (CC vs. CT + TT) significantly decrease HBV persistence in genotype B HBV-infected subjects; HLA-DP genotypes that promote HBV clearance are associated with a lower prevalence of HBV mutations increasing HCC risk (C1653T, T1674C/G, A1846T, G1896A, preS2 mutations, and preS deletion in genotype C) and a higher prevalence of HBV mutations decreasing HCC risk (G1652A, T1673C, T1674C, G1719T, G1730C, and G1799C in genotype B and A1727T in genotype C); furthermore, significant effects of HBV mutations on cirrhosis and HCC are selectively evident in those with the HLA-DP genotypes that promote HBV persistence [61] . Thus, the HLA-DP polymorphisms affect genotype B HBV clearance, regulate immune selection of viral mutations, and influence cirrhosis and HCC risks contributed by the HBV mutations.…”

Section: Interaction Of Genetic Predispositions Of Immune or Inflammamentioning

confidence: 99%

Cancer Evo-Dev, a novel hypothesis derived from studies on hepatitis B virus-induced carcinogenesis

Cao¹

2017

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How to cite this article: Cao GW. Cancer Evo-Dev, a novel hypothesis derived from studies on hepatitis B virus-induced carcinogenesis. Hepatoma Res 2017;3:241-59.Non-resolving inflammation, which may be maintained by infection, pollution, and metabolic stimulants and their interactions with immunogenetic predisposition, provides a fertile field for cancer development. This is strongly evident in hepatocellular carcinoma. Here, the framework of a hypothesis called Cancer Evo-Dev is presented, based on the advances in hepatitis B virusinduced hepatocarcinogenesis. Several aspects central to this theory are as follows: (1) immune imbalance caused by the interaction of immunogenetic predispositions and hepatitis B virus infection maintains non-resolving inflammation; (2) active inflammation executants promote mutations in viral and host genomes via disbalancing mutagenic forces including cytidine deaminases and mutation-repairing forces including uracil-DNA glycosylases, thus promoting cancer-related somatic mutations and viral mutations; (3) a small percentage of the cells whose somatic mutations alter the survival signalling adapt to the inflammatory microenvironment, de-differentiate via demethylating role of cytidine deaminases, and reversely develop into tumor-initiating cells (TICs); (4) under the cultivation of some factors like POSTN from tumorinfiltrating fibroblasts and M2 macrophages, TICs acquire the stemness, cancer-stem cells obtain distinct metastatic and drug-resistant potentials under the selection pressure from distinct microenvironments; (5) glycolysis persistence in the presence of oxygen provides essential energy for cell survival and the raw material for DNA synthesis. Thus, cancer development is characterized by an evolutionary process of "mutation-selection-adaptation". The framework of Cancer Evo-Dev can be verified in other cancers. Cancer Evo-Dev lays theoretical foundation for understanding the mechanisms by which inflammation promotes cancer development, and it also plays a role in specific prophylaxis, prediction, and targeted treatment of cancers. Key words:Inflammation, hepatitis B virus, mutations, hepatoma, Cancer Evo-Dev ABSTRACTArticle history:

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HLA-DPPolymorphisms Affect the Outcomes of Chronic Hepatitis B Virus Infections, Possibly through Interacting with Viral Mutations

Cited by 56 publications

References 53 publications

Virus evolution during chronic hepatitis B virus infection as revealed by ultradeep sequencing data

Virus evolution during chronic hepatitis B virus infection as revealed by ultradeep sequencing data

Hepatitis B Virus Combo Mutations Improve the Prediction and Active Prophylaxis of Hepatocellular Carcinoma: A Clinic-Based Cohort Study

Cancer Evo-Dev, a novel hypothesis derived from studies on hepatitis B virus-induced carcinogenesis

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