Tomoko Kiyohara scite author profile

Background: Cytokines and host factors triggering innate immunity against hepatitis B virus (HBV) are not well understood.Results: IL-1 and TNFα induced cytidine deaminase AID, an anti-HBV host factor, and reduced HBV infection into hepatocytes.Conclusion: IL-1/TNFα reduced host susceptibility to HBV infection through AID up-regulation.Significance: Proinflammatory cytokines modulate HBV infection through a novel innate immune pathway involving AID.

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A Hyperimmune Serum against a Synthetic Peptide Corresponding to the Hypervariable Region 1 of Hepatitis C Virus Can Prevent Viral Infection in Cell Cultures

Shimizu

et al. 1996

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To investigate whether a principal neutralization epitope exists in hypervariable region 1 (HVR1) within the putative envelope of hepatitis C virus (HCV), we generated a hyperimmune rabbit serum against a synthetic peptide corresponding to HVR1 of HCV isolate H77. The reactivity of the serum in the enzyme-linked immunosorbent assay was correlated with the 13 amino acids (position 398-410) in HVR1. The serum prevented infection with H77 virus in cell cultures but did not prevent infection with H90 virus, a genetically divergent isolate from the same patient. The study demonstrated that neutralization of HCV was mediated, in part, by isolate-specific antibody recognizing HVR1.

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Shifting Seroepidemiology of Hepatitis A in Japan, 1973–2003

Kiyohara

Sato

Totsuka

et al. 2007

Microbiology and Immunology

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Background. Hepatitis A infection is caused by hepatitis A virus (HAV) contracted through fecal‐oral transmission. Life‐long immunity is conferred after infection. Improved sanitary conditions have generally resulted in a significant decline in the incidence of hepatitis A. However, a low incidence of infection results in increased HAV susceptibility. The present study investigates the prevalence of anti‐HAV antibody and clarifies the current HAV status and HAV susceptibility in Japan at 2003. Methods. A total of 2,430 serum specimens collected during 2003 from Japanese individuals ranging in age from 0–92 years, were tested for anti‐HAV antibody using an inhibition enzyme linked immunosorbent assay. All specimens were obtained from the WHO and the National Serum Reference Bank/National Institute of Infectious Diseases, Tokyo, Japan. Results. The overall seroprevalence was 12.2%. Anti‐HAV antibodies were rarely detected in individuals between 0–44 years of age. Starting from the age of 45–49 years, seropositivity gradually increased through age 65 years and above. Seroprevalence was not affected by gender, and geographic distribution did not affect age‐specific seroprevalence until the age of 60 years. Conclusions. HAV susceptibility in Japan is increasing annually. Particularly, the prevalence of anti‐HAV antibody in individuals older than 50 years in 2003 was 50.3%, which is significantly lower than that of corresponding studies in 1994 (74.3%), 1984 (96.9%) and 1973 (96.9%). The growing susceptible population of advanced age results in more frequent HAV infection among them. The surveillance of anti‐HAV antibody prevalence is useful for implementing preventive measures and for controlling the spread of HAV.

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Epidemiological and genetic analyses of a diffuse outbreak of hepatitis A in Japan, 2010

Ishii

Kiyohara

Yoshizaki

et al. 2012

Journal of Clinical Virology

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Rapid and real-time detection of hepatitis A virus by reverse transcription loop-mediated isothermal amplification assay

Yoneyama

Kiyohara

Shimasaki

et al. 2007

Journal of Virological Methods

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Tomoko Kiyohara

Interleukin-1 and Tumor Necrosis Factor-α Trigger Restriction of Hepatitis B Virus Infection via a Cytidine Deaminase Activation-induced Cytidine Deaminase (AID)

A Hyperimmune Serum against a Synthetic Peptide Corresponding to the Hypervariable Region 1 of Hepatitis C Virus Can Prevent Viral Infection in Cell Cultures

Shifting Seroepidemiology of Hepatitis A in Japan, 1973–2003

Epidemiological and genetic analyses of a diffuse outbreak of hepatitis A in Japan, 2010

Rapid and real-time detection of hepatitis A virus by reverse transcription loop-mediated isothermal amplification assay

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