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Featured researches published by Dong-Un Han.


American Journal of Pathology | 2010

A Mouse Model of Lethal Synergism Between Influenza Virus and Haemophilus influenzae

Lian Ni Lee; Peter Dias; Dong-Un Han; So-Rah Yoon; Ashley Shea; Vladislav Zakharov; David M. Parham; Sally Sarawar

Secondary bacterial infections that follow infection with influenza virus result in considerable morbidity and mortality in young children, the elderly, and immunocompromised individuals and may also significantly increase mortality in normal healthy adults during influenza pandemics. We herein describe a mouse model for investigating the interaction between influenza virus and the bacterium Haemophilus influenzae. Sequential infection with sublethal doses of influenza and H. influenzae resulted in synergy between the two pathogens and caused mortality in immunocompetent adult wild-type mice. Lethality was dependent on the interval between administration of the bacteria and virus, and bacterial growth was prolonged in the lungs of dual-infected mice, although influenza virus titers were unaffected. Dual infection induced severe damage to the airway epithelium and confluent pneumonia, similar to that observed in victims of the 1918 global influenza pandemic. Increased bronchial epithelial cell death was observed as early as 1 day after bacterial inoculation in the dual-infected mice. Studies using knockout mice indicated that lethality occurs via a mechanism that is not dependent on Fas, CCR2, CXCR3, interleukin-6, tumor necrosis factor, or Toll-like receptor-4 and does not require T or B cells. This model suggests that infection with virulent strains of influenza may predispose even immunocompetent individuals to severe illness on secondary infection with H. influenzae by a mechanism that involves innate immunity, but does not require tumor necrosis factor, interleukin-6, or signaling via Toll-like receptor-4.


Journal of General Virology | 2010

Genomic expression profiling in lymph nodes with lymphoid depletion from porcine circovirus 2-infected pigs.

Garam Lee; Dong-Un Han; Jae-Young Song; Yong-Soon Lee; Kyung-Sun Kang; Sorah Yoon

Porcine circovirus type 2 (PCV2) is the main causative agent of porcine circovirus-associated disease, such as post-weaning multisystemic wasting syndrome, which involves lymphocyte depletion. However, little is known about the molecular mechanisms of lymphoid depletion. To gain insight into the interaction between virus and host cells, microarrays were used to analyse changes in genomic expression in lymph nodes following PCV2 infection of pigs, together with negative controls. Total RNA was subjected to microarray analysis with an Affymetrix Porcine Genome Array GeneChip. Of the 23,256 pig genes arrayed on a chip, 160 genes showed altered expression after infection (upregulated, 64; downregulated, 96). The altered genomic expression of 18 selected genes was confirmed by quantitative real-time PCR. The expression changes of numerous genes involved in innate immune defence (TLR1, CD14 and CD180), immunosuppressed responses (FGL2 and GPNMB), pro-inflammatory signals (galectin-3) and fasting processes (ANGPTL-4) indicate that PCV2 has developed an intricate mechanism to cause immunosuppression, inflammatory cell infiltration and weight loss in pigs. The results of this study provide a basis for understanding the molecular pathogenesis of PCV2 infection.


Journal of Virology | 2010

CD4 T-Cell Help Programs a Change in CD8 T-Cell Function Enabling Effective Long-Term Control of Murine Gammaherpesvirus 68: Role of PD-1-PD-L1 Interactions

Peter Dias; Francesca Giannoni; Lian Ni Lee; Dong-Un Han; So-Rah Yoon; Hideo Yagita; Miyuki Azuma; Sally R. Sarawar

ABSTRACT We previously showed that agonistic antibodies to CD40 could substitute for CD4 T-cell help and prevent reactivation of murine gammaherpesvirus 68 (MHV-68) in the lungs of major histocompatibility complex (MHC) class II−/− (CII−/−) mice, which are CD4 T cell deficient. Although CD8 T cells were required for this effect, no change in their activity was detected in vitro. A key question was whether anti-CD40 treatment (or CD4 T-cell help) changed the function of CD8 T cells or another cell type in vivo. To address this question, in the present study, we showed that adoptive transfer of CD8 T cells from virus-infected wild-type mice or anti-CD40-treated CII−/− mice caused a significant reduction in lung viral titers, in contrast to those from control CII−/− mice. Anti-CD40 treatment also greatly prolonged survival of infected CII−/− mice. This confirms that costimulatory signals cause a change in CD8 T cells enabling them to maintain effective long-term control of MHV-68. We investigated the nature of this change and found that expression of the inhibitory receptor PD-1 was significantly increased on CD8 T cells in the lungs of MHV-68-infected CII−/−, CD40−/−, or CD80/86−/− mice, compared with that in wild-type or CD28/CTLA4−/− mice, correlating with the level of viral reactivation. Furthermore, blocking PD-1-PD-L1 interactions significantly reduced viral reactivation in CD4 T-cell-deficient mice. In contrast, the absence of another inhibitory receptor, NKG2A, had no effect. These data suggest that CD4 T-cell help programs a change in CD8 T-cell function mediated by altered PD-1 expression, which enables effective long-term control of MHV-68.


Fems Immunology and Medical Microbiology | 2011

Proteomic analysis of swine hepatitis E virus (sHEV)-infected livers reveals upregulation of apolipoprotein and downregulation of ferritin heavy chain

Garam Lee; Dong-Un Han; Jae-Young Song; Jae-Hoon Kim; So-Rah Yoon

Swine hepatitis E virus (sHEV) has been discovered to be almost ubiquitous in pigs, and is antigenically and genetically related to human HEV. Proteomic analysis was used to identify altered protein expression in swine liver, using two-dimensional electrophoresis and peptide mass fingerprinting. A total of 10 protein spots exhibited significant alterations in the sHEV-infected organ. The upregulation of apolipoprotein E (Apo E) and downregulation of ferritin heavy chain were confirmed by Western analysis and by semi-quantitative reverse transcription-PCR. The elevated expression of Apo E may provide a novel insight into molecular responses to HEV infection in swine.


Journal of Veterinary Medical Science | 2010

Immune-enhancing effect of fermented Maesil (Prunus mume Siebold & Zucc.) with probiotics against Bordetella bronchiseptica in mice.

Bock-Gie Jung; Jae-Hyung Ko; Sun-Ju Cho; Hong-Bum Koh; So-Rah Yoon; Dong-Un Han; Bong-Joo Lee


Korean Journal of Food Science and Technology | 2007

Effects of Fermented Milk with Hot Water Extract from Acanthopanax senticosus and Codonopsis lanceolata on the Immune Status of Mouse

Sang-Dong Lim; Ki-Seung Seong; Kee-Sung Kim; Dong-Un Han


Antiviral Research | 2010

Neutralization of infectivity of porcine circovirus type 2 (PCV2) by capsid-binding 2′F-RNA aptamers

Sorah Yoon; Garam Lee; Dong-Un Han; Jae-Young Song; Kyung-Sun Kang; Yong-Soon Lee


Korean Journal for Food Science of Animal Resources | 2007

Effects of Fermented Milk Containing Herb Extract from Acanthopanax divaricatus var. albeofructus and Codonopsis Ianceolata on the Immune Status of Mouse

Sang-Dong Lim; Ki-Seung Seong; Kee-Sung Kim; Dong-Un Han


Journal of The Korean Society of Food Science and Nutrition | 2005

Protective Effects of Welsh Onion (Allium fistulosum L.) on Drug-induced Hepatotoxicity in Rats

Hwan-Soo Cha; Ki-Seung Seong; Sung-Ho Kim; Ji-Woo Seo; Sun-Joo Park; Soon-Im Kim; Kyung-Won Lee; So-Rah Yoon; Dong-Un Han


Korean Journal of Veterinary Service | 2007

Epidemiological study of bovine neosporosis in Gyeonggi province

Yeon-Seok Chae; Jong-Tae Woo; So-Rah Yoon; Dong-Un Han; Bong-Joo Lee

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So-Rah Yoon

Torrey Pines Institute for Molecular Studies

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Chai-Yong Lee

Chonnam National University

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Mun-Il Kang

Chonnam National University

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Lian Ni Lee

Torrey Pines Institute for Molecular Studies

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Peter Dias

Torrey Pines Institute for Molecular Studies

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Bong-Joo Lee

Chonnam National University

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Kyung-Sun Kang

Seoul National University

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Sorah Yoon

Seoul National University

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Yong-Soon Lee

Seoul National University

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Ashley Shea

Torrey Pines Institute for Molecular Studies

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