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3. Uncoupling immune trajectories of response and adverse events from anti-PD-1 immunotherapy in hepatocellular carcinoma

Author

Chuah, Samuel, Lee, Joycelyn, Song, Yuan, Kim, Hyung-Don, Wasser, Martin, Kaya, Neslihan A., Bang, Kyunghye, Lee, Yong Joon, Jeon, Seung Hyuck, Suthen, Sheena, A’Azman, Shamirah, Gien, Gerald, Lim, Chun Jye, Chua, Camillus, Hazirah, Sharifah Nur, Lee, Hong Kai, Lim, Jia Qi, Lim, Tony K.H., Yeong, Joe, Chen, Jinmiao, Shin, Eui-Cheol, Albani, Salvatore, Zhai, Weiwei, Yoo, Changhoon, Liu, Haiyan, Choo, Su Pin, Tai, David, and Chew, Valerie

Published
2022
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7. The third dose of measles-containing vaccine induces robust immune responses against measles in young seronegative healthcare workers who had previous two-dose measles vaccination.

Author

Kim, Yong Chan, Nam, Heejin, Choi, Jun Yong, Shin, Eui-Cheol, and Choi, Young Hwa

Abstract

Despite the low measles antibody positivity rate among young healthcare workers (HCWs) who have previously received two doses of a measles-containing vaccine (MCV), whether an additional dose of MCV acts as a booster remains unknown. Thus, we aimed to evaluate the immune responses to a third dose of MCV in young HCWs. Hospital-wide measles seroprevalence was assessed using enzyme-linked immunosorbent assay (ELISA). The immunogenicity of a third dose of MCV was determined in young seronegative HCWs (born between 1986 and 1997) who had previously received a two-dose measles vaccination. A total of 3033 (92.6%) HCWs had anti-measles immunoglobulin G. The lowest seropositivity rate was observed in HCWs aged 20–24 years (87.7%). In this group, HCWs who received a third dose of MCV had higher seropositivity than those who received a second dose (89.5% vs. 75.4%). A third dose of MCV was administered to 18 HCWs who did not have anti-measles IgG despite two doses. Neutralizing antibody titers increased significantly 4 weeks after the third vaccination. Although neutralizing antibody titers decreased 1 year post vaccination, 17 (94.4%) HCWs had medium (121–900 mIU/mL) or high (>900 mIU/mL) levels. Furthermore, the third dose of MCV increased the measles virus-specific T-cell effector function. The third dose of MCV induced a strong immune response against measles in young seronegative HCWs who had previously received a two-dose measles vaccination. [Display omitted] [ABSTRACT FROM AUTHOR]

Published
2023
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10. Exploration of basil (Ocimum basilicum) essential oil profiles using E-nose and GC–MS combined with GC-O and inhalation effects on the human EEG topography and tomography (s-LORETA) and blood pressure.

Author

Hong, Seong Jun, Kim, Da-Som, Jo, Seong Min, Yoon, Sojeong, Jeong, Hyangyeon, Yoon, Moon Yeon, Kim, Jae Kyeom, Kim, Young Jun, and Shin, Eui-Cheol

Abstract

[Display omitted] • Volatile compounds and odor-active compounds were detected in basil essential oil by GC–MS-O combined with electronic nose, and linalool (668.43 ± 338.82 ug/100 g) was identified as a key volatile compound. • Inhalation of basil essential oil decreased blood pressure and pulse levels of participants. • Beta waves Brodmann 38 area were activated by inhalation of basil essential oil. This study aimed to investigate the changes in human EEG activity, Brodmann area, and blood pressure during basil essential oil inhalation. Seven odor-active compounds were detected by GC–MS combined with GC–olfactometry, and three abundant volatile compounds were detected by electronic nose. Linalool was simultaneously regarded as a major volatile compound. The systolic and diastolic blood pressures and pulse levels showed a decreasing trend during BEO inhalation. The relative beta and gamma waves in most brain regions changed during BEO inhalation. The gamma waves decreased, whereas the beta waves increased during BEO inhalation. In particular, the beta waves in the left frontal and right parietal regions and Brodmann area 38 significantly increased during inhalation using sLORETA. Accordingly, these results were highly associated with reduced stress responses by decreased gamma waves, blood pressures, and pulse levels and improved language-related functions by the increased beta wave at Brodmann area 38. [ABSTRACT FROM AUTHOR]

Published
2024
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12. Tumor Necrosis Factor-producing T-regulatory Cells Are Associated With Severe Liver Injury in Patients With Acute Hepatitis A.

Author

Choi, Yoon Seok, Jung, Min Kyung, Lee, Jeewon, Choi, Seong Jin, Choi, Sung Hoon, Lee, Hyun Woong, Lee, Jong-Joo, Kim, Hyung Joon, Ahn, Sang Hoon, Lee, Dong Hyeon, Kim, Won, Park, Su-Hyung, Huh, Jun R., Kim, Hyoung-Pyo, Park, Jun Yong, and Shin, Eui-Cheol

Abstract

Background and Aims CD4 + CD25 + Foxp3 + T-regulatory (Treg) cells control immune responses and maintain immune homeostasis. However, under inflammatory conditions, Treg cells produce cytokines that promote inflammation. We investigated production of tumor necrosis factor (TNF) by Treg cells in patients with acute hepatitis A (AHA), and examined the characteristics of these cells and association with clinical factors. Methods We analyzed blood samples collected from 63 patients with AHA at the time of hospitalization (and some at later time points) and 19 healthy donors in South Korea. Liver tissues were collected from patients with fulminant AHA during liver transplantation. Peripheral blood mononuclear cells were isolated from whole blood and lymphocytes were isolated from liver tissues and analyzed by flow cytometry. Cytokine production from Treg cells (CD4 + CD25 + Foxp3 + ) was measured by immunofluorescence levels following stimulation with anti-CD3 and anti-CD28. Epigenetic stability of Treg cells was determined based on DNA methylation patterns. Phenotypes of Treg cells were analyzed by flow cytometry and an RORγt inhibitor, ML-209, was used to inhibit TNF production. Treg cell suppression assay was performed by co-culture of Treg-depleted peripheral blood mononuclear cells s and isolated Treg cells. Results A higher proportion of CD4 + CD25 + Foxp3 + Treg cells from patients with AHA compared with controls produced TNF upon stimulation with anti-CD3 and anti-CD28 (11.2% vs 2.8%). DNA methylation analysis confirmed the identity of the Treg cells. TNF-producing Treg cells had features of T-helper 17 cells, including up-regulation of RORγt, which was required for TNF production. The Treg cells had reduced suppressive functions compared with Treg cells from controls. The frequency of TNF-producing Treg cells in AHA patients’ blood correlated with their serum level of alanine aminotransferase. Conclusions Treg cells from patients with AHA have altered functions compared with Treg cells from healthy individuals. Treg cells from patients with AHA produce higher levels of TNF, gain features of T-helper 17 cells, and have reduced suppressive activity. The presence of these cells is associated with severe liver injury in patients with AHA. [ABSTRACT FROM AUTHOR]

Published
2018
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13. KIR+CD8+ and NKG2A+CD8+ T cells are distinct innate-like populations in humans.

Author

Choi, Seong Jin, Koh, June-Young, Rha, Min-Seok, Seo, In-Ho, Lee, Hoyoung, Jeong, Seongju, Park, Su-Hyung, and Shin, Eui-Cheol

Abstract

Subsets of the human CD8+ T cell population express inhibitory NK cell receptors, such as killer immunoglobulin-like receptors (KIRs) and NKG2A. In the present study, we examine the phenotypic and functional characteristics of KIR+CD8+ T cells and NKG2A+CD8+ T cells. KIRs and NKG2A tend to be expressed by human CD8+ T cells in a mutually exclusive manner. In addition, TCR clonotypes of KIR+CD8+ T cells barely overlap with those of NKG2A+CD8+ T cells, and KIR+CD8+ T cells are more terminally differentiated and replicative senescent than NKG2A+CD8+ T cells. Among cytokine receptors, IL12Rβ1, IL12Rβ2, and IL18Rβ are highly expressed by NKG2A+CD8+ T cells, whereas IL2Rβ is expressed by KIR+CD8+ T cells. IL-12/IL-18-induced production of IFN-γ is prominent in NKG2A+CD8+ T cells, whereas IL-15-induced NK-like cytotoxicity is prominent in KIR+CD8+ T cells. These findings suggest that KIR+CD8+ and NKG2A+CD8+ T cells are distinct innate-like populations with different cytokine responsiveness. [Display omitted] • TCR clonotypes of KIR+CD8+ T cells barely overlap with those of NKG2A+CD8+ T cells • KIR+CD8+ T cells are terminally differentiated with replicative senescence • NKG2A+CD8+ T cells exhibit IL-12/IL-18-induced IFN-γ production • KIR+CD8+ T cells exert IL-15-induced NK-like cytotoxicity Choi et al. examined the heterogeneity among human KIR/NKG2A+CD8+ T cells and found that KIRs and NKG2A are expressed by human CD8+ T cells in a mutually exclusive manner. NKG2A+CD8+ T cells express PLZF and exhibit IL-12/IL-18-induced IFN-γ production. In contrast, KIR+CD8+ T cells exert IL-15-induced cytotoxic activity. [ABSTRACT FROM AUTHOR]

Published
2023
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14. Evaluation of hyaluronic acid-based combination adjuvant containing monophosphoryl lipid A and aluminum salt for hepatitis B vaccine.

Author

Moon, Se-hee, Shin, Eui-Cheol, Noh, Young-Woock, and Lim, Yong Taik

Subjects
*HYALURONIC acid, *IMMUNOLOGICAL adjuvants, *PHOSPHORYL group, *HEPATITIS B vaccines, *HUMORAL immunity
Abstract

Here, monophosphoryl lipid A (MPLA) and aluminum salt (Alum) were introduced into a hyaluronic acid (HA)-based combination vaccine adjuvant for hepatitis B vaccine (HBV). Although Alum is a well-known hepatitis B vaccine adjuvant that induces an enhanced humoral immune response, it cannot induce the cellular immune responses. On the other hand, MPLA has been generally reported to promote IFN-γ production via antigen-specific CD4 + T cells, but it is not water soluble as a result of its long hydrophobic alkyl chains. To this end, water insoluble MPLA could be solubilized in an aqueous solution with the help of HA, which contains many carboxyl and hydroxyl groups that can be used to attach to the hydroxyl head groups of MPLA via hydrogen bonds. Three groups of mice were treated with either hepatitis B surface antigen (HBsAg) alone, HBsAg_Alum complex, or HBsAg_Alum_MPLA/HA complex. The group immunized with the HBsAg_Alum_MPLA/HA complex exhibited a high increase in cellular immune response as well as in humoral immune response relative to the other two groups. The antibody, cytokine and T cell levels were most elevated in the group of mice immunized with HBsAg_Alum_MPLA/HA complex, even at a 1 μg/mice dose, and the magnitude was still maintained even after 8 weeks. Specifically, the antibody value was 120 times larger in mice vaccinated with HBsAg_Alum_MPLA/HA complex than in mice vaccinated with HBsAg_Alum complex designed similar to commercially available hepatitis B vaccine, Engerix B. The cytokine and T cell proliferation levels were 2 times and 6 times larger in mice adjuvanted with HBsAg_Alum_MPLA/HA complex than in those vaccinated with HBsAg_Alum. The results therefore indicate that incorporating MPLA and Alum with HA can be a potent strategy to increase both the magnitude and the persistence of HBsAg-specific immune responses to protect hosts against hepatitis B virus infection. [ABSTRACT FROM AUTHOR]

Published
2015
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15. The generation of stem cell-like memory cells early after BNT162b2 vaccination is associated with durability of memory CD8+ T cell responses.

Author

Jung, Sungmin, Jung, Jae Hyung, Noh, Ji Yun, Kim, Woo-Joong, Yoon, Soo-Young, Jung, Jongtak, Kim, Eu Suk, Kim, Hong Bin, Cheong, Hee Jin, Kim, Woo Joo, Park, Su-Hyung, Song, Kyoung-Ho, Song, Joon Young, and Shin, Eui-Cheol

Abstract

COVID-19 vaccines elicit humoral and cellular immune responses. Durable maintenance of vaccine-induced immunity is required for long-term protection of the host. Here, we examine activation and differentiation of vaccine-induced CD8+ T cells using MHC class I (MHC-I) multimers and correlations between early differentiation and the durability of CD8+ T cell responses among healthcare workers immunized with two doses of BNT162b2. The frequency of MHC-I multimer+ cells is robustly increased by BNT162b2 but decreases 6 months post-second vaccination to 2.4%–65.6% (23.0% on average) of the peak. MHC-I multimer+ cells dominantly exhibit phenotypes of activated effector cells 1–2 weeks post-second vaccination and gradually acquire phenotypes of long-term memory cells, including stem cell-like memory T (T SCM) cells. Importantly, the frequency of T SCM cells 1–2 weeks post-second vaccination significantly correlates with the 6-month durability of CD8+ T cells, indicating that early generation of T SCM cells determines the longevity of vaccine-induced memory CD8+ T cell responses. [Display omitted] • Spike-specific CD8+ T cells quantitatively decrease 6 months after BNT162b2 vaccination • CD8+ T SCM cells are successfully generated by BNT162b2 vaccination • T SCM cell generation significantly correlates with the durability of CD8+ T cells • T SCM cell generation inversely correlates with the age of vaccinated individuals The longevity of SARS-CoV-2-specific CD8+ T cells elicited by BNT162b2 has yet to be fully understood. Jung et al. demonstrate that early generation of T SCM cells after vaccination determines the durability of spike-specific memory CD8+ T cells. This early generation of T SCM cells negatively correlates with age. [ABSTRACT FROM AUTHOR]

Published
2022
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16. CD8α− Dendritic Cells Induce Antigen-Specific T Follicular Helper Cells Generating Efficient Humoral Immune Responses.

Author

Shin, Changsik, Han, Jae-A, Koh, Hyein, Choi, Bongseo, Cho, Yongbin, Jeong, Hyeongmin, Ra, Jea-Sun, Sung, Pil Soo, Shin, Eui-Cheol, Ryu, Seongho, and Do, Yoonkyung

Abstract

Summary Recent studies on T follicular helper (Tfh) cells have significantly advanced our understanding of T cell-dependent B cell responses. However, little is known about the early stage of Tfh cell commitment by dendritic cells (DCs), particularly by the conventional CD8α + and CD8α − DC subsets. We show that CD8α − DCs localized at the interfollicular zone play a pivotal role in the induction of antigen-specific Tfh cells by upregulating the expression of Icosl and Ox40l through the non-canonical NF-κB signaling pathway. Tfh cells induced by CD8α − DCs function as true B cell helpers, resulting in significantly increased humoral immune responses against various human pathogenic antigens, including Yersinia pestis LcrV, HIV Gag, and hepatitis B surface antigen. Our findings uncover a mechanistic role of CD8α − DCs in the initiation of Tfh cell differentiation and thereby provide a rationale for investigating CD8α − DCs in enhancing antigen-specific humoral immune responses for improving vaccines and therapeutics. [ABSTRACT FROM AUTHOR]

Published
2015
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17. IL-17A–producing sinonasal MAIT cells in patients with chronic rhinosinusitis with nasal polyps.

Author

Rha, Min-Seok, Yoon, Young Hoon, Koh, June-Young, Jung, Jae Hyung, Lee, Ha Seok, Park, Soo Kyoung, Park, Su-Hyung, Kim, Yong Min, Rha, Ki-Sang, and Shin, Eui-Cheol

Abstract

Diverse immune cells contribute to the pathogenesis of chronic rhinosinusitis (CRS), an inflammatory disease of the nasal cavity and paranasal sinuses. However, whether mucosal-associated invariant T (MAIT) cells are present in human sinonasal tissues remains unclear. Furthermore, the characteristics of sinonasal MAIT cells have not been studied in patients with CRS. We investigated the phenotype, function, and clinical implications of MAIT cells in patients with CRS. Peripheral blood and sinonasal tissue were obtained from patients with CRS with (CRSwNP) or without nasal polyps (CRSsNP) and healthy controls. MAIT cells were analyzed by flow cytometry. We found that MAIT cells are present in human sinonasal tissues from healthy controls and patients with CRS. The sinonasal MAIT cell population, but not peripheral blood MAIT cells, from patients with CRSsNP, noneosinophilic CRSwNP (NE-NP), or eosinophilic CRSwNP (E-NP) had a significantly higher frequency of activated cells marked by CD38 expression. In functional analysis, the sinonasal MAIT cell population from NE-NP and E-NP had a significantly higher frequency of IL-17A+ cells but lower frequency of IFN-γ+ or TNF+ cells than control sinonasal tissues. Furthermore, CD38 expression and IL-17A production by sinonasal MAIT cells significantly correlated with disease extent evaluated by the Lund-Mackay computed tomography score in patients with E-NP. Sinonasal MAIT cells exhibit an activated phenotype and produce higher levels of IL-17A in patients with CRSwNP. These alterations are associated with the extent of disease in patients with E-NP. [Display omitted] [ABSTRACT FROM AUTHOR]

Published
2022
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18. Chemometric approach to fatty acid profiles in Runner-type peanut cultivars by principal component analysis (PCA)

Author

Shin, Eui-Cheol, Craft, Brian D., Pegg, Ronald B., Phillips, R. Dixon, and Eitenmiller, Ronald R.

Subjects
*CHEMOMETRICS, *FATTY acids, *PEANUT varieties, *PRINCIPAL components analysis, *GAS chromatography, *PALMITIC acid, *STEARIC acid
Abstract

Abstract: The fatty acid profiles of commercially-grown Runner-type peanut cultivars (i.e., 10 cultivars, n =151) collected over two production years (2005 and 2006) were determined by gas–liquid chromatography. Eight major fatty acids were identified in the sample set including palmitic (C16:0), stearic (C18:0), oleic (C18:1, ω9), linoleic (C18:2, ω6), arachidic (C20:0), gondoic (C20:1, ω9), behenic (C22:0), and lignoceric (C24:0) acids. Based on the oleic to linoleic acid (O/L) ratio, these cultivars were denoted as normal, mid-, and high-oleic peanut types. Correlation coefficients (r) between the eight major fatty acids identified were generated and revealed an inverse association between oleic and linoleic acids (r =–0.997, P <0.001), while oleic acid and linoleic acid were positively correlated to gondoic acid (r =0.818, P <0.001) and palmitic acid (r =0.967, P <0.001), respectively. Principal component analysis (PCA) of the fatty acid data yielded three significant PCs (i.e., eigenvalues⩾1), which together account for 87.18% of the total variance in the data set; with PC1 contributing 60.45% of the total. Eigen analysis of the correlation matrix loadings of the three significant PCs revealed that PC1 was mainly contributed to by palmitic, oleic, linoleic, and gondoic acids; PC2, by behenic acid; and PC3, by lignoceric acid. The score plot generated between PC1 and PC2 successfully segregated normal, mid- and high-oleic peanut cultivars, while the PC1–PC3 plot segregated normal and the combination of mid- and high-oleic acid cultivars. [Copyright &y& Elsevier]

Published
2010
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19. Identification of CD4 T-Cell Epitopes in Soluble Liver Antigen/Liver Pancreas Autoantigen in Autoimmune Hepatitis.

Author

Mix, Heiko, Weiler–Normann, Christina, Thimme, Robert, Ahlenstiel, Golo, Shin, Eui–Cheol, Herkel, Johannes, David, Chella S., Lohse, Ansgar W., and Rehermann, Barbara

Subjects
CHRONIC active hepatitis, T cells, EPITOPES, TRANSGENIC mice, LIVER diseases, AUTOANTIBODIES, LYMPHOCYTES, DISEASE susceptibility
Abstract

Background & Aims: Autoimmune hepatitis (AIH) is a chronic inflammatory liver disease associated with autoantibodies and liver-infiltrating lymphocytes. Although autoantibodies are tested routinely to diagnose and classify AIH, liver-infiltrating lymphocytes are regarded as the primary factor for disease pathogenesis. The purpose of this study was to identify and characterize autoantigenic peptides within human AIH-specific soluble liver antigen/liver pancreas antigen (SLA/LP) that are targeted by CD4+ T cells and restricted by the disease susceptibility gene HLA-DRB1*0301. Methods: HLA-DRB1*0301 transgenic mice were immunized with SLA/LP. Antibody and T-cell responses were analyzed with SLA/LP-overlapping peptides in enzyme immunoassay, proliferation, and enzyme-linked immunospot (ELISpot) assays. Minimal optimal T-cell epitopes were identified, characterized with cloned T-cell hybridomas, and confirmed in tetramer and ELISpot assays with AIH patients'' peripheral blood mononuclear cells. Results: All mice developed SLA/LP-specific IgG1/IgG2a antibodies against the same SLA/LP peptides as human beings. T cells targeted several peptides within SLA/LP, 2 of which were DR3-restricted and one overlapped the sequence recognized by human autoantibodies. Minimal optimal epitopes were mapped, DRB1*0301/epitope-tetramers were generated, and the frequency and function of HLA-DRB1*0301-restricted autoantigen-specific T cells in AIH patients were analyzed with tetramer and interferon-γ ELISpot assays. Conclusions: This study identified T-cell epitopes within SLA/LP, restricted by the disease susceptibility gene DRB1*0301 and in close proximity to the human autoantibody epitope. These results and the generated reagents now provide the opportunity to directly monitor autoreactive T cells in AIH patients in clinical studies. [Copyright &y& Elsevier]

Published
2008
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20. Abnormality in the NK-cell population is prolonged in severe COVID-19 patients.

Author

Leem, Galam, Cheon, Shinhye, Lee, Hoyoung, Choi, Seong Jin, Jeong, Seongju, Kim, Eui-Soon, Jeong, Hye Won, Jeong, Hyeongseok, Park, Su-Hyung, Kim, Yeon-Sook, and Shin, Eui-Cheol

Abstract

Our understanding of adaptive immune responses in patients with coronavirus disease 2019 (COVID-19) is rapidly evolving, but information on the innate immune responses by natural killer (NK) cells is still insufficient. We aimed to examine the phenotypic and functional status of NK cells and their changes during the course of mild and severe COVID-19. We performed RNA sequencing and flow cytometric analysis of NK cells from patients with mild and severe COVID-19 at multiple time points in the course of the disease using cryopreserved PBMCs. In RNA-sequencing analysis, the NK cells exhibited distinctive features compared with healthy donors, with significant enrichment of proinflammatory cytokine-mediated signaling pathways. Intriguingly, we found that the unconventional CD56dimCD16neg NK-cell population expanded in cryopreserved PBMCs from patients with COVID-19 regardless of disease severity, accompanied by decreased NK-cell cytotoxicity. The NK-cell population was rapidly normalized alongside the disappearance of unconventional CD56dimCD16neg NK cells and the recovery of NK-cell cytotoxicity in patients with mild COVID-19, but this occurred slowly in patients with severe COVID-19. The current longitudinal study provides a deep understanding of the NK-cell biology in COVID-19. [Display omitted] [ABSTRACT FROM AUTHOR]

Published
2021
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22. IL-15 enhances CCR5-mediated migration of memory CD8+ T cells by upregulating CCR5 expression in the absence of TCR stimulation.

Author

Seo, In-Ho, Eun, Hyuk Soo, Kim, Ja Kyung, Lee, Hoyoung, Jeong, Seongju, Choi, Seong Jin, Lee, Jeewon, Lee, Byung Seok, Kim, Seok Hyun, Rou, Woo Sun, Lee, Dong Hyeon, Kim, Won, Park, Su-Hyung, and Shin, Eui-Cheol

Abstract

During microbial infection, bystander CD8+ T cells that are not specific to infecting pathogens can be activated by interleukin (IL)-15. However, the tissue-homing properties of bystander-activated CD8+ T cells have not been elucidated. Here, we examine the effects of IL-15 on the expression of chemokine receptors on CD8+ T cells and their migration. IL-15 upregulates CCR5 in memory CD8+ T cells in the absence of T cell receptor (TCR) stimulation and enhances CCR5-dependent migration. IL-15-induced CCR5 upregulation is abrogated by TCR stimulation, indicating that CCR5 is upregulated in bystander-activated CD8+ T cells. Moreover, CCR5 signals increase proliferation and cytotoxic protein expression in IL-15-treated memory CD8+ T cells, although the increase has a small extent. CCR5 upregulation in bystander-activated CD8+ T cells is associated with severe liver injury in patients with acute hepatitis A. Altogether, the results indicate that CCR5 upregulation by IL-15 mediates the migration of bystander-activated CD8+ T cells. [Display omitted] • IL-15 upregulates CCR5 in memory CD8+ T cells in the absence of TCR stimulation • CCR5 is upregulated in IL-15-induced bystander-activated CD8+ T cells • IL-15-treated CD8+ T cells migrate in a CCR5-dependent manner • CCR5 upregulation is associated with liver injury during acute hepatitis A IL-15 induces TCR-independent bystander activation of memory CD8+ T cells. Seo et al. demonstrate that IL-15 upregulates CCR5 expression on memory CD8+ T cells and enhances CCR5-mediated migration. During acute hepatitis A, CCR5 is upregulated in bystander-activated CD8+ T cells and associated with liver injury. [ABSTRACT FROM AUTHOR]

Published
2021
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23. Targeting inducible costimulator expressed on CXCR5+PD-1+ TH cells suppresses the progression of pemphigus vulgaris.

Author

Kim, A Reum, Han, Dawoon, Choi, Ji Young, Seok, Joon, Kim, Song-Ee, Seo, Seong-Hoon, Takahashi, Hayato, Amagai, Masayuki, Park, Su-Hyung, Kim, Soo-Chan, Shin, Eui-Cheol, and Kim, Jong Hoon

Abstract

Pemphigus vulgaris (PV) is an autoimmune bullous disease mediated by autoantibodies against desmoglein 3 (DSG3). Inducible costimulator (ICOS) is a costimulatory receptor expressed on T cells and influences the activity of T follicular helper (T FH) cells in various autoimmune diseases, but the roles of ICOS and T FH cells in PV remain unclear. We examined the immunological characteristics, antigen specificity, and pathogenicity of CD4+ T-cell subpopulations, as well as the therapeutic effect of anti-ICOS blocking antibodies in PV. A mouse model of PV was established by adoptive transfer of immune cells from the skin-draining lymph nodes or spleens of DSG3-expressing skin-grafted Dsg3 –/– mice into Rag1 –/– mice. The T FH cells and CD4+ T cells in PBMCs from PV patients were examined by flow cytometry. Among CD4+ T cells from the mouse model, ICOS-positive T FH cells were associated with B-cell differentiation and were required for disease induction. Using an MHC class II tetramer, DSG3-specific ICOS+ T FH cells were found to be associated with anti-DSG3 antibody production and expanded in the absence of B cells. In human PV, the frequency of ICOS+CXCR5+PD-1+ memory CD4+ T cells correlated with the autoantibody level. Treatment with anti-ICOS blocking antibodies targeting ICOS+ T FH cells decreased the anti-DSG3 antibody level and delayed disease progression in vivo. Mouse Dsg3-specific ICOS+ T FH cells and human ICOS+CXCR5+PD-1+ T H cells are associated with the anti-DSG3 antibody response in PV. ICOS expressed on CXCR5+PD-1+ T H cells may be a therapeutic target for PV. [ABSTRACT FROM AUTHOR]

Published
2020
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24. Superantigen-related TH2 CD4+ T cells in nonasthmatic chronic rhinosinusitis with nasal polyps.

Author

Rha, Min-Seok, Kim, Sang-Wook, Chang, Dong-Yeop, Lee, Jin-Ku, Kim, Jihye, Park, Su-Hyung, Khalmuratova, Roza, Lim, Hee-Suk, Eun, Kyoung Mi, Hong, Seung-No, Kim, Dae Woo, and Shin, Eui-Cheol

Abstract

Staphylococcus aureus enterotoxin (SAE) superantigens are detected in nasal polyps (NPs), and SAE-specific IgE predicts asthma comorbidity in patients with NPs. However, roles of SAE superantigens and superantigen-related T-cell responses remain to be elucidated in nonasthmatic patients. We investigated the presence of SAEs and SAE-related T-cell receptor (TCR) Vβ (TCRVβ) in nonasthmatic NPs, the phenotypes and functions of SAE-related T cells, and the clinical implication of SAE-related T-cell expansion. Sinonasal tissue samples were obtained from patients with nonasthmatic chronic rhinosinusitis (CRS) with NPs (CRSwNP), patients with CRS without NPs (CRSsNP), and control subjects. SAE genes were detected by PCR, and the TCRVβ distribution and T-cell phenotypes were examined by flow cytometry. Various SAE genes were detected not only in NPs but also in sinonasal mucosa from patients with CRSsNP and from controls. The S aureus enterotoxin I (SEI) gene was detected in all NPs. The fraction of SEI–responsive TCRVβ+ (TCRVβ1+ and Vβ5.1+) CD4+ T cells was significantly increased only in NPs and the ethmoidal mucosa of patients with CRSwNP, indicating superantigen-induced expansion. The expanded TCRVβ5.1+ CD4+ T cells expressed proliferation marker Ki-67 and the T H 2 transcription factor GATA3. Furthermore, TCRVβ5.1+ CD4+ T cells in NPs highly expressed T H 2 markers, including IL-17RB, thymic stromal lymphoprotein receptor, and chemoattractant receptor–homologous molecule expressed on T H 2 cells, with a potent T H 2 cytokine–producing ability. Moreover, the expansion of TCRVβ1+ or Vβ5.1+ CD4+ T cells was associated with the Lund-Mackay computed tomography score, indicating disease extent. In nonasthmatic patients with CRSwNP, superantigen-related expansion of CD4+ T cells with T H 2 differentiation was associated with the disease extent. [ABSTRACT FROM AUTHOR]

Published
2020
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26. Dynamic Responses of Circulating T Cells After Stereotactic Body Radiation Therapy for Bone Metastasis in Patients With Breast Cancer.

Author

Jeon, Seung Hyuck, Jang, Bum-Sup, Kim, Dong-Yun, Kim, Jin Ho, Shin, Eui-Cheol, and Kim, In Ah

Subjects
*STEREOTACTIC radiotherapy, *T cells, *REGULATORY T cells, *BONE metastasis, *CANCER radiotherapy, *CELLS
Abstract

Preclinical studies have shown that radiation therapy modulates antitumor immune responses. However, circulating T-cell responses after radiation therapy in patients with cancer have been poorly characterized. This study aims to explore the changes in circulating T cells after stereotactic body radiation therapy (SBRT). Peripheral blood samples of 30 patients with breast cancer who underwent SBRT for bone metastasis were analyzed using multicolor flow cytometry. Phenotypes of PD-1+ CD8+ T cells and regulatory T (T REG) cells were examined. Additionally, plasma protein levels were analyzed using a bead-based immunoassay. Circulating PD-1+ CD8+ T cells, which are enriched for tumor-specific clonotypes, were activated at 1 week after SBRT. However, circulating T REG cells were also activated after SBRT; this pattern was also evident among effector Foxp3hiCD45RA− T REG cells. We observed no difference in T-cell responses according to the fraction size and number. Notably, activation of T REG cells was more prominent in patients who experienced greater activation of PD-1+ CD8+ T cells. Plasma level changes in TGF-β1, soluble CTLA-4, and soluble 4-1BB at 1 week after SBRT were associated with PD-1+ CD8+ T-cell responses. Activation of T REG cells at 1 week after SBRT was associated with worse progression-free survival. Clinical factors including molecular subtype were not associated with the T-cell responses. SBRT induced activation of both potentially tumor-specific CD8+ T cells and T REG cells, which were tightly associated with each other. These results may support the use of T REG cell-modulating strategies with SBRT to improve the antitumor immune response. [ABSTRACT FROM AUTHOR]

Published
2024
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27. Association Between Expression Level of PD1 by Tumor-Infiltrating CD8+ T Cells and Features of Hepatocellular Carcinoma.

Author

Kim, Hyung-Don, Song, Gi-Won, Park, Seongyeol, Jung, Min Kyung, Kim, Min Hwan, Kang, Hyo Jeong, Yoo, Changhoon, Yi, Kijong, Kim, Kyung Hwan, Eo, Sukyeong, Moon, Deok-Bog, Hong, Seung-Mo, Ju, Young Seok, Shin, Eui-Cheol, Hwang, Shin, and Park, Su-Hyung

Abstract

Background & Aims T-cell exhaustion, or an impaired capacity to secrete cytokines and proliferate with overexpression of immune checkpoint receptors, occurs during chronic viral infections but has also been observed in tumors, including hepatocellular carcinomas (HCCs). We investigated features of exhaustion in CD8+ T cells isolated from HCC specimens. Methods We obtained HCC specimens, along with adjacent nontumor tissues and blood samples, from 90 patients who underwent surgical resection at Asan Medical Center (Seoul, Korea) from April 2016 through April 2018. Intrahepatic lymphocytes and tumor-infiltrating T cells were analyzed by flow cytometry. Tumor-infiltrating CD8+ T cells were sorted by flow cytometry into populations based on expression level of programmed cell death 1 (PDCD1 or PD1): PD1-high, PD1-intermediate, and PD1-negative. Sorted cells were analyzed by RNA sequencing. Proliferation and production of interferon gamma (IFNG) and tumor necrosis factor (TNF) by CD8+ T cells were measured in response to anti-CD3 and antibodies against immune checkpoint receptors including PD1, hepatitis A virus cellular receptor 2 (HAVCR2 or TIM3), lymphocyte activating 3 (LAG3), or isotype control. Tumor-associated antigen-specific CD8+ T cells were identified using HLA-A*0201 dextramers. PDL1 expression on tumor tissue was assessed by immunohistochemistry. Results PD1-high, PD1-intermediate, and PD1-negative CD8+ T cells from HCCs had distinct gene expression profiles. PD1-high cells expressed higher levels of genes that regulate T-cell exhaustion than PD1-intermediate cells. PD1-high cells expressed TIM3 and LAG3, and low proportions of TCF1+, TBEThigh/eomesoderminlow, and CD127+. PD1-high cells produced the lowest amounts of IFNG and TNF upon anti-CD3 stimulation. Differences in the PD1 expression patterns of CD8+ T cells led to the identification of 2 subgroups of HCCs: HCCs with a discrete population of PD1-high cells were more aggressive than HCCs without a discrete population of PD1-high cells. HCCs with a discrete population of PD1-high cells had higher levels of predictive biomarkers of response to anti-PD1 therapy. Incubation of CD8+ T cells from HCCs with a discrete population of PD1-high cells with antibodies against PD1 and TIM3 or LAG3 further restored proliferation and production of IFNG and TNF in response to anti-CD3. Conclusions We found HCC specimens to contain CD8+ T cells that express different levels of PD1. HCCs with a discrete population of PD1-high CD8+ T cells express TIM3 and/or LAG3 and produce low levels of IFNG and TNF in response to anti-CD3. Incubation of these cells with antibodies against PD1 and TIM3 or LAG3 further restore proliferation and production of cytokines; HCCs with a discrete population of PD1-high CD8+ T cells might be more susceptible to combined immune checkpoint blockade–based therapies. Graphical abstract [ABSTRACT FROM AUTHOR]

Published
2018
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28. Programmed cell death ligand 1 alleviates psoriatic inflammation by suppressing IL-17A production from programmed cell death 1–high T cells.

Author

Kim, Jong Hoon, Choi, Young Joon, Lee, Byung Ha, Song, Mi-Young, Ban, Chae Yeon, Kim, Jihye, Park, Junsik, Kim, Song-Ee, Kim, Tae-Gyun, Park, Su-Hyung, Kim, Hyoung-Pyo, Sung, Young-Chul, Kim, Soo-Chan, and Shin, Eui-Cheol

Abstract

Background Psoriasis is one of the most common chronic inflammatory diseases of the skin. Recently, IL-17–producing T cells have been shown to play a critical role in psoriatic inflammation. Programmed cell death 1 (PD-1) is a coinhibitory receptor expressed on T cells in various chronic inflammatory diseases; however, the expression and function of PD-1 during psoriatic inflammation have not previously been characterized. Objective We examined PD-1 expression on IL-17A–producing T cells from imiquimod-treated mice and patients with psoriasis. Additionally, we investigated the therapeutic effect of recombinant programmed cell death ligand 1 (PD-L1) protein on imiquimod-induced psoriatic inflammation. Methods PD-1 expression on IL-17A–producing γδ T cells from imiquimod-treated mice was examined by means of multicolor flow cytometric analysis. In the psoriatic skin of patients, PD-1 and IL-17A expression was analyzed by using immunofluorescence. The therapeutic effect of PD-L1–Fc fusion protein (PD-L1-Fc) was assessed in imiquimod-treated mice ex vivo and in vivo . Results During imiquimod-induced psoriatic inflammation, PD-1 is overexpressed on CD27 − Vγ1 − γδ T cells. Furthermore, PD-1 expression on IL-17A + T cells was confirmed in psoriatic skin tissues from patients and imiquimod-treated mice. In the CD27 − Vγ1 − γδ T-cell population, Vγ4 − γδ T cells with Vγ6 mRNA expression showed a high level of PD-1 expression. Furthermore, these PD-1 hi Vγ4 − (Vγ6 + ) γδ T cells were specialized for anti-CD3–induced IL-17A production, which was inhibited by PD-L1-Fc treatment. In imiquimod-treated mice PD-L1-Fc reduced psoriatic inflammation when given alone and enhanced the therapeutic effect of anti-p40 when given in combination. Conclusion PD-1 is overexpressed in IL-17A–producing T cells in both imiquimod-treated mice and patients with psoriasis. Moreover, recombinant PD-L1-Fc alleviates psoriatic inflammation in imiquimod-treated mice. [ABSTRACT FROM AUTHOR]

Published
2016
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29. Hepatitis C Virus Attenuates Interferon-Induced Major Histocompatibility Complex Class I Expression and Decreases CD8+ T Cell Effector Functions.

Author

Kang, Wonseok, Sung, Pil Soo, Park, Su-Hyung, Yoon, Sarah, Chang, Dong-Yeop, Kim, Seungtaek, Han, Kwang Hyub, Kim, Ja Kyung, Rehermann, Barbara, Chwae, Yong-Joon, and Shin, Eui-Cheol

Abstract

Background & Aims: Major histocompatibility complex (MHC) class I−restricted CD8+ T cells are required for clearance of hepatitis C virus (HCV) infection. MHC class I expression is up-regulated by type I and II interferons (IFNs). However, little is known about the effects of HCV infection on IFN-induced expression of MHC class I. Methods: We used the HCV cell culture system (HCVcc) with the genotype 2a Japanese fulminant hepatitis-1 strain to investigate IFN-induced expression of MHC class I and its regulatory mechanisms. HCVcc-infected Huh-7.5 cells were analyzed by flow cytometry, metabolic labeling, immunoprecipitation, and immunoblotting analyses. Protein kinase R (PKR) was knocked down with lentiviruses that express small hairpin RNAs. The functional effects of MHC class I regulation by HCV were demonstrated in co-culture studies, using HCV-specific CD8+ T cells. Results: Although the baseline level of MHC class I was not affected by HCV infection, IFN-induced expression of MHC class I was notably attenuated in HCV-infected cells. This was associated with replicating HCV RNA, not with viral protein. HCV infection reduced IFN-induced synthesis of MHC class I protein and induced phosphorylation of PKR and eIF2α. IFN-induced MHC class I expression was restored by small hairpin RNA-mediated knockdown of PKR in HCV-infected cells. Co-culture of HCV-specific CD8+ T cells and HCV-infected cells that expressed HLA-A2 demonstrated that HCV infection reduced the effector functions of HCV-specific CD8+ T cells; these functions were restored by small hairpin RNA-mediated knockdown of PKR. Conclusions: IFN-induced expression of MHC class I is attenuated in HCV-infected cells by activation of PKR, which reduces the effector functions of HCV-specific CD8+ T cells. This appears to be an important mechanism by which HCV circumvents antiviral adaptive immune responses. [Copyright &y& Elsevier]

Published
2014
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30. A heterologous AZD1222 priming and BNT162b2 boosting regimen more efficiently elicits neutralizing antibodies, but not memory T cells, than the homologous BNT162b2 regimen.

Author

Baek, Yae Jee, Kim, Woo-Joong, Ko, Jae-Hoon, Lee, Youn-Jung, Ahn, Jin Young, Kim, Jung Ho, Jang, Ho Cheol, Jeong, Hye Won, Kim, Yong Chan, Park, Yoon Soo, Kim, Sung-Han, Peck, Kyong Ran, Shin, Eui-Cheol, and Choi, Jun Yong

Subjects
*IMMUNOLOGIC memory, *T cells, *COVID-19 vaccines, *SARS-CoV-2 Delta variant, *IMMUNOGLOBULINS, *IMMUNOGLOBULIN G
Abstract

Comparative analyses of SARS-CoV-2-specific immune responses elicited by diverse prime-boost regimens are required to establish efficient regimens for the control of COVID-19. In this prospective observational cohort study, spike-specific immunoglobulin G (IgG) and neutralizing antibodies (nAbs) alongside spike-specific T -cell responses in age-matched groups of homologous BNT162b2/BNT162b2 or AZD1222/AZD1222 vaccination, heterologous AZD1222/BNT162b2 vaccination, and prior wild-type SARS-CoV-2 infection/vaccination were evaluated. Peak immune responses were achieved after the second vaccine dose in the naïve vaccinated groups and after the first dose in the prior infection/vaccination group. Peak titers of anti-spike IgG and nAb were significantly higher in the AZD1222/BNT162b2 vaccination and prior infection/vaccination groups than in the BNT162b2/BNT162b2 or AZD1222/AZD1222 groups. However, the frequency of interferon-γ-producing CD4+ T cells was highest in the BNT162b2/BNT162b2 vaccination group. Similar results were observed in the analysis of polyfunctional T cells. When nAb and CD4+ T -cell responses against the Delta variant were analyzed, the prior infection/vaccination group exhibited higher responses than the groups of other homologous or heterologous vaccination regimens. nAbs are efficiently elicited by heterologous AZD1222/BNT162b2 vaccination, as well as prior infection/vaccination, whereas spike-specific CD4+ T -cell responses are efficiently elicited by homologous BNT162b2 vaccination. Variant-recognizing immunity is more efficiently generated by prior infection/vaccination than the other homologous or heterologous vaccination regimens. [ABSTRACT FROM AUTHOR]

Published
2023
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31. Association of T Cell Senescence with Radiation Pneumonitis in Patients with Non-small Cell Lung Cancer.

Author

Kim, Kyung Hwan, Pyo, Hongryull, Lee, Hoyoung, Oh, Dongryul, Noh, Jae Myoung, Ahn, Yong Chan, Kim, Chang Gon, Yoon, Hong In, Lee, Jiyun, Park, Sehhoon, Jung, Hyun-Ae, Sun, Jong-Mu, Lee, Se-Hoon, Ahn, Jin Seok, Park, Keunchil, Ku, Bo mi, Shin, Eui-Cheol, and Ahn, Myung-Ju

Subjects
*NON-small-cell lung carcinoma, *CELLULAR aging, *T cells, *RADIATION pneumonitis, *RECURSIVE partitioning
Abstract

Associations between immunosenescence and radiation pneumonitis (RP) are largely unknown. We aimed to identify a peripheral blood T cell senescence biomarker to predict RP in patients with non-small cell lung cancer (NSCLC). Patients with locally advanced NSCLC who received definitive concurrent chemoradiotherapy (dCRT) were prospectively registered (cohort 1, n=23; cohort 2, n=31). Peripheral blood was collected at baseline, during dCRT, and at 1 month post-dCRT. Patients were dichotomized to grade ≥2 (G2+) RP and grade 0-1 (G0-1) RP. Flow cytometry was performed to assess phenotypes and functional properties of T cell subsets. RP incidence was estimated via competing risk analysis. Five and six patients exhibited G2+ RP following dCRT in cohorts 1 and 2, respectively. Patients with G2+ RP exhibited a more aged T cell pool and higher frequencies of senescent CD57+CD28−CD8+ T cells than patients with G0-1 RP at baseline, during dCRT, and at 1 month post-dCRT. These senescent cells exhibited increased granzyme B, IFN-γ, and TNF-α production. Higher baseline frequency of CD57+CD28−CD8+ T cells was an independent predictor of G2+ RP (hazard ratio, 8.42; 95% confidence interval, 2.58–27.45; P<0.001). Recursive partitioning analysis revealed three distinct risk groups stratified by baseline CD57+CD28−CD8+ T cell frequency and lung V 20 Gy , with 1-year cumulative G2+ RP incidences of 50.0%, 16.7%, and 0% for high-, intermediate-, and low-risk groups, respectively (P=0.002). Higher baseline frequencies of CD57+CD28−CD8+ T cells correlated with increased G2+ RP risks. Our results suggest the need for further investigation of the role of T cell senescence on radiation-induced organ damage. [ABSTRACT FROM AUTHOR]

Published
2023
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32. Successful Vaccination Induces Multifunctional Memory T-Cell Precursors Associated With Early Control of Hepatitis C Virus.

Author

Park, Su–Hyung, Shin, Eui–Cheol, Capone, Stefania, Caggiari, Laura, Re, Valli De, Nicosia, Alfredo, Folgori, Antonella, and Rehermann, Barbara

Subjects
HEPATITIS C virus, VIRAL vaccines, T cells, HEPATITIS C vaccines, DRUG development, COMPARATIVE studies, PHENOTYPES, POLYMERASE chain reaction
Abstract

Background & Aims: T cells are an important component for development of a vaccine against hepatitis C virus (HCV), but little is known about the features of successful vaccine-induced T cells. Methods: We compared the phenotype, function, and kinetics of vaccine-induced and infection-induced T cells in chimpanzees with HCV infection using multicolor flow cytometry and real-time polymerase chain reaction. Results: In chimpanzees successfully vaccinated with recombinant adenovirus and DNA against HCV NS3-5, HCV-specific T cells appeared earlier, maintained better functionality, and persisted at higher frequencies for a longer time after HCV challenge, than those of mock-vaccinated chimpanzees. Vaccine-induced T cells displayed higher levels of CD127, a marker of memory precursors, and lower levels of programmed death-1 (PD-1) than infection-induced T cells. Vaccine-induced, but not infection-induced, T cells were multifunctional; their ability to secrete interferon gamma and tumor necrosis factor α correlated with early expression of CD127 but not PD-1. Based on a comparison of vaccine-induced and infection-induced T cells from the same chimpanzee, the CD127+ memory precursor phenotype was induced by the vaccine itself rather than by low viremia. In contrast, induction of PD-1 correlated with viremia, and levels of intrahepatic PD-1, PD-L1, and 2,5-OAS-1 messenger RNAs correlated with peak titers of HCV. Conclusions: Compared with infection, vaccination-induced HCV-specific CD127+ T cells with high functionality that persisted at higher levels for a longer time. Control of viremia prevented up-regulation of PD-1 on T cells and induction of PD-1, PD-L1, and 2,5-OAS-1 in the liver. Early development of a memory T-cell phenotype and, via control of viremia, attenuation of the inhibitory PD1–PD–L1 pathway might be necessary components of successful vaccine-induced protection against HCV. [ABSTRACT FROM AUTHOR]

Published
2012
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33. Delayed Induction, Not Impaired Recruitment, of Specific CD8+ T Cells Causes the Late Onset of Acute Hepatitis C.

Author

Shin, Eui–Cheol, Park, Su–Hyung, DeMino, Mary, Nascimbeni, Michelina, Mihalik, Kathleen, Major, Marian, Veerapu, Naga S., Heller, Theo, Feinstone, Stephen M., Rice, Charles M., and Rehermann, Barbara

Subjects
HEPATITIS C, T cells, CHEMOKINES, IMMUNE response, MEDICAL virology, CHIMPANZEES as laboratory animals, CELL adhesion molecules, INTERFERONS
Abstract

Background & Aims: Hepatitis C virus (HCV) infection is characterized by lack of immune-mediated liver injury despite a high level of HCV replication during the incubation phase, which lasts about 8 weeks. We investigated whether this results from delayed recruitment of HCV-specific T cells and whether it facilitates HCV persistence. Methods: Six chimpanzees were infected with HCV; blood and liver samples were collected for 28 weeks and analyzed for immune cells and chemokines. Results: Two chimpanzees developed self-limited infections, whereas the remaining 4 developed chronic infections. Levels of the chemokines CXCL10, CXCL11, CCL4, and CCL5 increased in blood and liver samples from all chimpanzees within 1 month of HCV infection. Chemokine induction correlated with intrahepatic type I interferon (IFN) responses in vivo and was blocked by neutralizing antibodies against IFN-β in vitro. Despite the early-stage induction of chemokines, the intrahepatic lymphocytic infiltrate started to increase no earlier than 8 weeks after HCV infection, when HCV-specific, tetramer-positive CD8+ T cells appeared in the circulation. The HCV-specific CD8+ T cells expressed chemokine receptors when they were initially detected in blood samples, so they could be recruited to the liver as soon as they entered the circulation. Conclusions: Chemokines are induced during early stages of HCV infection, which requires a type I IFN–mediated response. The delayed onset of acute hepatitis does not result from delayed recruitment of HCV-specific T cells, but could instead be related to a primary delay in the induction of HCV-specific T cells. Divergent outcomes occur without evident differences in chemokine induction and T-cell recruitment. [ABSTRACT FROM AUTHOR]

Published
2011
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34. Physicochemical and chemosensory properties of pomegranate (Punica granatum L.) seeds under various oven-roasting conditions.

Author

Yoon, Sojeong, Jeong, Hyangyeon, Jo, Seong Min, Hong, Seong Jun, Park, Hyeonjin, Ban, Younglan, Youn, Moon Yeon, and Shin, Eui-Cheol

Subjects
*POMEGRANATE, *SEEDS, *FURAN derivatives, *SULFUR compounds, *FLAVONOIDS, *OXIDANT status, *ELLAGITANNINS, *PYRAZINES
Abstract

• Excessive oven-roasting of pomegranate seeds breaks down the innate carotenoid pigments and reduces the a* (redness) value. • Oven roasting increases the total phenolic and flavonoid content of pomegranate seeds, which improves their antioxidant capacities. • Proper roasting conditions increase antioxidant properties and positive flavors such as furan derivatives, pyrazines. • Higher temperatures and a long roasting time increase the amounts of off-flavor such as sulfur compounds and amines. This study investigated the effects of oven-roasting temperature (160, 180, and 200 ℃) and time (5, 10, 15, and 20 min) on pomegranate seeds. Physicochemical properties, such as color (L*, a*, and b* values), browning index (BI), total phenolic and flavonoid contents, 2,2-diphenyl-1-picrylhydrazyl radical scavenging capacity, and chemosensory properties, including taste and volatile compounds, were analyzed. The L* and a* values, and level of sourness, umami, sweetness, and terpenes decreased, whereas the b* value, BI, and level of saltiness, bitterness, furan derivatives, pyrazines, and sulfur-containing compounds, increased with roasting time. The findings of this study showed that the positive roasting conditions for pomegranate seeds were 10–20 min at 160 ℃ and, 5–10 min at 180 ℃. This study is expected to be used as a primary reference for selecting the optimal oven-roasting conditions in which positive effects appear and for developing products utilizing pomegranate seeds. [ABSTRACT FROM AUTHOR]

Published
2024
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36. Dynamics of Circulating Immune Cells During Chemoradiotherapy in Patients with Non-Small Cell Lung Cancer Support Earlier Administration of Anti-PD-1/PD-L1 Therapy.

Author

Kim, Kyung Hwan, Pyo, Hongryull, Lee, Hoyoung, Oh, Dongryul, Noh, Jae Myoung, Ahn, Yong Chan, Yoon, Hong In, Moon, Hyowon, Lee, Jiyun, Park, Sehhoon, Jung, Hyun-Ae, Sun, Jong-Mu, Lee, Se-Hoon, Ahn, Jin Seok, Park, Keunchil, Ku, Bo Mi, Ahn, Myung-Ju, and Shin, Eui-Cheol

Subjects
*NON-small-cell lung carcinoma, *PEMBROLIZUMAB, *IMMUNE checkpoint inhibitors, *T cells, *CELL analysis, *CHEMORADIOTHERAPY, *LYMPHOPENIA
Abstract

Purpose: Chemoradiotherapy (CRT) followed by consolidation immune checkpoint inhibitors significantly improves survival in unresectable locally advanced non-small cell lung cancer. However, the optimal sequence for CRT and immune checkpoint inhibitors has not yet been established. We investigated the dynamics of peripheral blood immune cells during CRT to determine the best sequence for treatment.Methods and Materials: Peripheral blood samples were prospectively collected pretreatment, weekly during CRT for 6 weeks, and 1 month posttreatment in 24 patients with locally advanced non-small cell lung cancer who received definitive CRT. Immune cell analysis was performed by flow cytometry. Ex vivo PD-1 blockade assays were performed by IFN-γ intracellular cytokine staining.Results: Lymphopenia was prominently observed during CRT and mostly recovered 1 month post-CRT. Robust proliferation of CD8+ T cells was induced, peaking in the last week during CRT and decreasing post-CRT. The robust proliferation of CD8+ T cells led to an increase in the frequency of CD28-CD57+ replicative senescent and terminally differentiated cells post-CRT. Tumor-reactive CD8+ T cells increased during CRT and peaked in the last week. One month post-CRT, the frequency of tumor-reactive CD8+ T cells decreased and TOXhiTCF1lo terminally exhausted CD8+ T cells significantly increased. Anti-PD-1-induced functional restoration of PD-1+CD8+ T cells was maximized in the last week of CRT and significantly decreased post-CRT.Conclusions: The findings suggest that earlier administration of PD-1 blockade may be associated with superior efficacy compared with delayed administration after completion of CRT. These findings provide an immunologic rationale for optimal timing of combining immune checkpoint inhibitors with CRT in clinical trials. [ABSTRACT FROM AUTHOR]

Published
2022
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37. Hepatitis B virus X protein induced expression of interleukin 18 (IL-18): a potential mechanism for liver injury caused by hepatitis B virus (HBV) infection

Author

Lee, Mi-Ock, Choi, Youn-Hee, Shin, Eui-Cheol, Kang, Hyo-Jin, Kim, Young-Mee, Jeong, Su-Yon, Seong, Je Kyung, Yu, Dae-Yeul, Cho, Hyeseong, Park, Jeon Han, and Kim, Se Jong

Subjects
*HEPATITIS B virus, *INTERLEUKINS, *LIVER injuries
Abstract

Background/Aims: The hepatitis B virus X protein (HBx), a major viral transactivator, is implicated in hepatic inflammation, since it induces many pro-inflammatory cytokines at transcriptional level. The aim of this study was to investigate role of HBx in expression of interleukin 18 (IL-18), a newly identified cytokine that up-regulates Fas ligand (FasL) expression.Methods: Chang X-34 that expressing HBx under the control of a doxycycline-inducible promoter, and hepatitis B virus (HBV)-integrated hepatoma cell lines were examined for IL-18 expression by Northern and Western blotting analysis. To test the role of IL-18 produced by hepatoma cells, FasL expression was examined by flow cytometry after treatment with neutralizing anti-IL-18 antibodies. Further, IL-18 expression was examined in the liver tissues of HBx-transgenic mice.Results: Induction of IL-18 following HBx expression in Chang X-34 and the pattern of IL-18 expression in HBV-integrated cell lines, implicated that HBx transcriptionally induces IL-18 expression. Neutralizing anti-IL-18 antibodies blocked the expression of FasL, suggesting that IL-18 plays a critical role in FasL expression. Further, IL-18 expression in the HBx-transgenic liver, was correlated with the degree of hepatitis.Conclusions: Our results demonstrated that HBx induces IL-18 expression in liver, which may be associated with hepatic injury by amplifying FasL expression during HBV infection. [Copyright &y& Elsevier]

Published
2002
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38. TOX-expressing terminally exhausted tumor-infiltrating CD8+ T cells are reinvigorated by co-blockade of PD-1 and TIGIT in bladder cancer.

Author

Han, Hye Sook, Jeong, Seongju, Kim, Hyunglae, Kim, Hyung-Don, Kim, A.Reum, Kwon, Minsuk, Park, Su-Hyung, Woo, Chang Gok, Kim, Hee Kyung, Lee, Ki Hyeong, Seo, Sung Pil, Kang, Ho Won, Kim, Won Tae, Kim, Wun-Jae, Yun, Seok Joong, and Shin, Eui-Cheol

Subjects
*BLADDER cancer, *HIGH mobility group proteins, *T cells, *PROGRAMMED death-ligand 1, *PROGRAMMED cell death 1 receptors, *TUMOR antigens
Abstract

Exhausted T cells in the tumor microenvironment are major targets of immunotherapies. However, the exhaustion status of CD8+ tumor-infiltrating lymphocytes (TILs) in bladder cancer has not been comprehensively evaluated. Herein, we examined distinct exhaustion status of CD8+ TILs based on the level of programmed cell death-1 (PD-1) and thymocyte selection-associated high mobility group box protein (TOX) expression in urothelial bladder cancer. We also evaluated the reinvigoration of exhausted CD8+ TILs upon ex vivo treatment with inhibitory checkpoint blockers. TOX-expressing PD-1highCD8+ TILs had the highest expression of immune checkpoint receptors (ICRs), the most terminally exhausted features, and the highest tumor antigen reactivity among PD-1+CD8+ TILs. Bladder cancer patients with a high percentage of PD-1highTOX+CD8+ TILs had more progressed T-cell exhaustion features and higher programmed death-ligand 1 expression in tumor tissues. TIGIT was the most frequent co-expressed ICR on PD-1+CD8+ TILs, and TIGIT blockade enhanced the PD-1 blockade-mediated cytokine production by CD8+ TILs from bladder cancer patients. Our findings provide an improved understanding of the heterogeneous exhaustion status of CD8+ TILs and additional immunotherapy strategies to improve outcomes of bladder cancer patients. [ABSTRACT FROM AUTHOR]

Published
2021
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39. Hyperprogressive disease during PD-1 blockade in patients with advanced hepatocellular carcinoma.

Author

Kim, Chang Gon, Kim, Chan, Yoon, Sang Eun, Kim, Kyung Hwan, Choi, Seong Jin, Kang, Beodeul, Kim, Hye Ryun, Park, Su-Hyung, Shin, Eui-Cheol, Kim, Yeun-Yoon, Kim, Dae Jung, Chung, Hyun Cheol, Chon, Hong Jae, Choi, Hye Jin, and Lim, Ho Yeong

Subjects
*HEPATOCELLULAR carcinoma, *PROGRAMMED cell death 1 receptors, *NEUTROPHILS, *IMMUNE checkpoint inhibitors, *PATIENT selection
Abstract

Programmed cell death-1 (PD-1) inhibitor treatment can cause hyperprogressive disease (HPD), but the incidence, outcome, and predictive factors of HPD are unknown in patients with hepatocellular carcinoma (HCC). Herein, we assessed the existence and factors predictive of HPD in patients with advanced HCC treated with nivolumab. We enrolled 189 patients with advanced HCC treated with nivolumab. Occurrence of HPD was investigated using tumour growth dynamics based on tumour growth kinetics (TGK) and tumour growth rate (TGR) before and after treatment, or time to treatment failure. We additionally analysed patients treated with regorafenib (n = 95) or best supportive care (BSC)/placebo (n = 103) after progression on sorafenib to compare tumour growth dynamics. Flare-up of tumour growth was observed in a fraction of patients upon PD-1 blockade, indicating the occurrence of HPD. Based on distinct patterns of disease progression exclusively observed in the nivolumab-treated cohort, but not in the regorafenib- or BSC/placebo-treated cohorts, 4-fold increases in TGK and TGR ratios as well as a 40% increase in TGR were the cut-off values used to define HPD; 12.7% of the patients (24/189) treated with nivolumab met all these criteria. Patients with HPD had worse progression-free survival (hazard ratio [HR] 2.194; 95% CI 1.214–3.964) and overall survival (HR 2.238; 95% CI 1.233–4.062) compared to patients with progressive disease without HPD. More than 90% of patients with HPD missed the opportunity for subsequent treatment because of rapid clinical deterioration. An elevated neutrophil-to-lymphocyte ratio (>4.125) was associated with HPD and an inferior survival rate. HPD occurs in a fraction of patients with HCC who receive PD-1 inhibitor treatment. Analyses of the baseline immune profile and on-treatment tumour growth dynamics could enable optimal patient selection and earlier identification of HPD. Hyperprogressive disease is an unexpected response pattern observed in patients treated with an immune checkpoint inhibitor. This study revealed that hyperprogressive disease occurs in a fraction of patients with advanced hepatocellular carcinoma treated with an anti-PD-1 antibody, providing evidence to encourage careful monitoring of patients to prevent clinical deterioration induced by PD-1 blockade. • HPD occurs in a fraction of patients with HCC treated with PD-1 inhibitors. • HPD is associated with worse PFS and OS, depriving patients of the chance to receive subsequent treatments. • Elevated neutrophil-to-lymphocyte ratio predicts the occurrence of HPD and inferior survival rate after PD-1 blockade. [ABSTRACT FROM AUTHOR]

Published
2021
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40. Dynamic changes in circulating PD-1+CD8+ T lymphocytes for predicting treatment response to PD-1 blockade in patients with non-small-cell lung cancer.

Author

Kim, Chang Gon, Hong, Min Hee, Kim, Kyung Hwan, Seo, In-Ho, Ahn, Beung-Chul, Pyo, Kyoung-Ho, Synn, Chun-Bong, Yoon, Hong In, Shim, Hyo Sup, Lee, Yong Il, Choi, Seong Jin, Lee, Yun Jeong, Kim, Ellen Janine, Kim, Youngun, Kwak, Jeong-Eun, Jung, Jaehyung, Park, Su-Hyung, Paik, Soonmyung, Shin, Eui-Cheol, and Kim, Hye Ryun

Subjects
*BIOMARKERS, *FLOW cytometry, *LONGITUDINAL method, *LUNG cancer, *MEMBRANE proteins, *HEALTH outcome assessment, *PROBABILITY theory, *SURVIVAL, *T cells, *TUMOR antigens, *PHENOTYPES, *PRE-tests & post-tests, *PREDICTIVE tests, *DESCRIPTIVE statistics
Abstract

The predictive value of immune monitoring with circulating CD8+ T lymphocytes for treatment response to programmed cell death protein 1 (PD-1) inhibitors has not been explored in non-small-cell lung cancer (NSCLC), prompting us to investigate whether dynamic changes in PD-1+CD8+ T lymphocytes have predictive value for durable clinical benefit (DCB) and survival after PD-1 blockade. Patients with recurrent and/or metastatic NSCLC treated with PD-1 inhibitors were enrolled (discovery cohort; n = 94). Peripheral blood was obtained immediately before and after one cycle of treatment with PD-1 blockade. Phenotyping of circulating CD8+ T lymphocytes was conducted using multi-colour flow cytometry. Predictive values of dynamic changes in circulating PD-1+CD8+ T lymphocytes during the first cycle were validated in an independent cohort (validation cohort; n = 54) of a prospective trial with a PD-1 inhibitor (NCT03486119). Circulating PD-1+CD8+ T lymphocytes were enriched with effector/memory populations with elevated expression of activation- and exhaustion-related markers. Reduction in the frequency of PD-1+ cells among CD8+ T lymphocytes after one cycle of treatment was associated with a higher probability of DCB and superior survival outcomes in the discovery cohort. Similar results were obtained in the analysis of tumour antigen NY-ESO-1-specific CD8+ T lymphocytes and the validation cohort. Mechanistically, PD-1 molecule expression on CD8+ T lymphocytes suppresses the effector functions of tumour antigen-specific CD8+ T lymphocytes. Dynamic changes in circulating PD-1+CD8+ T lymphocytes predict clinical, and survival benefit from PD-1 blockade treatment in NSCLC, providing a useful tool to identify patient subgroups who will optimally benefit from PD-1 inhibitors. • Current biomarkers for PD-1 blockade are suboptimal and require invasive procedures. • Reduction of PD-1+ cells in CD8+ T lymphocytes predicts favourable treatment outcomes. • Suppressive function of circulating PD-1+CD8+ T lymphocytes was uncovered. [ABSTRACT FROM AUTHOR]

Published
2021
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41. Human liver CD8+ MAIT cells exert TCR/MR1-independent innate-like cytotoxicity in response to IL-15.

Author

Rha, Min-Seok, Han, Ji Won, Kim, Jong Hoon, Koh, June-Young, Park, Hye Jung, Kim, Soon Il, Kim, Myoung Soo, Lee, Jae Geun, Lee, Hyun Woong, Lee, Dong Hyeon, Kim, Won, Park, Jun Yong, Joo, Dong Jin, Park, Su-Hyung, and Shin, Eui-Cheol

Subjects
*LIVER cells, *T cell receptors, *VIRAL hepatitis, *LIVER, *VIRUS diseases, *ALANINE aminotransferase, *GRANZYMES
Abstract

Mucosal-associated invariant T (MAIT) cells, the most abundant innate-like T cells in the human liver, can be activated by cytokines during viral infection without TCR stimulation. Here, we examined the mechanisms underlying TCR/MR1-independent innate-like cytotoxicity of cytokine-activated liver MAIT cells. We also examined the phenotype and function of MAIT cells from patients with acute viral hepatitis. We obtained liver sinusoidal mononuclear cells from donor liver perfusate during liver transplantation and examined the effect of various cytokines on liver MAIT cells using flow cytometry and in vitro cytotoxicity assays. We also obtained peripheral blood and liver-infiltrating T cells from patients with acute hepatitis A (AHA) and examined the phenotype and function of MAIT cells using flow cytometry. IL-15-stimulated MAIT cells exerted granzyme B-dependent innate-like cytotoxicity in the absence of TCR/MR1 interaction. PI3K–mTOR signaling, NKG2D ligation, and CD2-mediated conjugate formation were critically required for this IL-15-induced innate-like cytotoxicity. MAIT cells from patients with AHA exhibited activated and cytotoxic phenotypes with higher NKG2D expression. The innate-like cytotoxicity of MAIT cells was significantly increased in patients with AHA and correlated with serum alanine aminotransferase levels. Taken together, the results demonstrate that liver MAIT cells activated by IL-15 exert NKG2D-dependent innate-like cytotoxicity in the absence of TCR/MR1 engagement. Furthermore, the innate-like cytotoxicity of MAIT cells is associated with liver injury in patients with AHA, suggesting that MAIT cells contribute to immune-mediated liver injury. Immune-mediated liver injury commonly occurs during viral infections of the liver. Mucosal-associated invariant T (MAIT) cells are the most abundant innate-like T cells in the human liver. Herein, we have identified a mechanism by which MAIT cells circumvent conventional T cell receptor interactions to exert cytotoxicity. We show that this innate-like cytotoxicity is increased during acute hepatitis A virus infection and correlates with the degree of hepatocyte injury. • MAIT cells activated by IL-15 exert TCR/MR1-independent, innate-like cytotoxicity. • Innate-like cytotoxicity of MAIT cells is dependent on NKG2D, granzyme B, and CD2. • PI3K–mTOR signaling is required for innate-like cytotoxicity of MAIT cells. • MAIT cells exhibit activated and cytotoxic phenotypes during acute hepatitis A. • MAIT cells may contribute to liver injury during acute hepatitis A. [ABSTRACT FROM AUTHOR]

Published
2020
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42. Adjuvant Therapy Using Ex Vivo-Expanded Allogenic Natural Killer Cells in Hepatectomy Patients with Hepatitis B Virus Related Solitary Hepatocellular Carcinoma: MG4101 study.

Author

Kim, Jong Man, Cho, Sung Yoo, Shin, Eui-Cheol, Choi, Gyu-Seong, and Joh, Jae-Won

Subjects
*KILLER cells, *HEPATITIS B virus, *HEPATOCELLULAR carcinoma, *HEPATECTOMY
Abstract

B Introduction: b There are few reports in hepatectomy patients with solitary hepatocellular carcinoma (HCC) who received immunotherapeutic agents as adjuvant therapy. Three recurrence-free patients showed higher ratio of CD8+ T lymphocyte populations before and after ex-vivo expanded allogenic NK cells administrations compared with the two patients without recurrence. [Extracted from the article]

Published
2019
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43. Acute alcohol consumption-induced let-7a inhibition exacerbates hepatic apoptosis by regulating Rb1 in mice.

Author

Pan, Jeong Hoon, Kim, Hyunjin, Tang, Jingsi, Beane, Kaleigh E., Park, Jeen-Woo, Kong, Seongbae, Kong, Byungwhi C., Kim, Young Jun, Shin, Eui-Cheol, Kim, Jun Ho, Zhao, Jiangchao, Lee, Jin Hyup, and Kim, Jae Kyeom

Subjects
*ALCOHOLIC liver diseases, *APOPTOSIS, *MICE, *ALCOHOL drinking, *FATTY liver
Abstract

Alcohol consumption is a critical risk factor for hepatic pathogenesis, including alcoholic liver diseases (ALD), but implications of alcohol-induced dysregulation of microRNA (miRNA) in ALD pathogenesis are not completely understood. In the present study, C57BL/6J male mice were treated with saline (CON; oral gavage; n = 8) or alcohol (EtOH; 3 g/kg body weight; oral gavage; n = 8) for 7 days. A total of 599 miRNAs and 158 key mRNAs related to fatty liver and hepatotoxicity pathways were assessed in mice liver tissues. The mRNA expression datasets were then utilized to predict interactions with miRNAs that were changed by alcohol consumption. Predicted miRNA-mRNA interactions were validated using in vitro miRNA transfection experiments. The results showed that let-7a was significantly decreased in the EtOH group and Rb1 mRNA was predicted as a target gene. This was further supported by an inverse correlation of RB1 and let-7a expression in mice liver tissue. Additionally, key protein expressions involved in RB1-apoptosis axis [i.e., p73, cleaved CASP-3 (cCASP-3), and cCASP-7] showed a trend of increase in the EtOH mice; this was also confirmed by capase-3 enzyme activity and terminal deoxynucleotidyl transferase-mediated dUTP nick-end labeling assay in livers of mice that had consumed alcohol. In line with our in vivo observations, alcohol treatment suppressed the let-7a expression and subsequently upregulated p73, cCASP-3, and cCASP-7 protein expressions in mice hepatocytes. Additional proteins in the apoptosis regulatory pathway (i.e., MDM2-p53 axis) were significantly changed in response to let-7a suppression in the cells. Taken together, the current study provides mechanistic evidence that alcohol consumption-induced let-7a suppression results in the upregulation of RB1, thereby promoting hepatic apoptosis through induction of pro-apoptotic proteins (e.g., p73), and by, at least in part, preventing MDM2-mediated p53 degradation. [ABSTRACT FROM AUTHOR]

Published
2020
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44. Immunogenicity and safety of a new live attenuated herpes zoster vaccine (NBP608) compared to Zostavax® in healthy adults aged 50 years and older.

Author

Choi, Won Suk, Choi, Jung Hyun, Jung, Dong Sik, Choi, Hee Jung, Kim, Yeon-Sook, Lee, Jacob, Jang, Hee-Chang, Shin, Eui-Cheol, Park, Jun-Sik, Kim, Hun, and Cheong, Hee Jin

Abstract

A multi-centre, randomised, double-blinded, active-controlled, parallel-group clinical trial was carried out to assess the immunogenicity and safety of NBP608—a newly developed live-attenuated zoster vaccine in Korea—relative to Zostavax® in healthy adults aged 50 years or older. Immune responses to the vaccine were evaluated by glycoprotein enzyme-linked immunosorbent assay (gpELISA) and enzyme-linked immunosorbent spot (ELISPOT) assays using the interferon (IFN)-γ and interleukin (IL)-2 FluoroSpot kit 6 weeks after vaccination. Safety was monitored for 26 weeks based on subjects' diaries, spontaneous reports from subjects, and history taking by the investigators. A total of 845 subjects participated in the screening, and 823 received the vaccination (413 in the NBP608 group and 411 in the comparator group). The gpELISA-determined geometric mean fold rise from baseline to post NBP608 vaccination was 2.75 [95% confidence interval, CI (2.57, 2.94)]. The gpELISA-determined adjusted geometric mean titers (GMTs) of NBP608 and the comparator were 1346.37 [95% CI (1273.99, 1422.87)] and 1674.94 [95% CI (1585.35, 1769.58)], respectively. The adjusted GMT ratio of NBP608 to the comparator was 0.80 [95% CI (0.75, 0.87)]. There was no statistically significant difference between two groups in terms of the geometric mean spot numbers determined by IFN-γ and IL-2 ELISPOT assays at 6 weeks post vaccination (P = 0.7232, 0.3844). The incidence of adverse events (AEs) within 6 weeks post vaccination was 49.82% overall (410/823, 941 cases), 50.73% (209/412, 474 cases) in the NBP608 group, and 48.91% (201/411, 467 cases) in the comparator group. The difference in AE rate between the two groups was not statistically significant (P = 0.6010). Most AEs were mild, with a rate of 83.12% in the NBP608 group and 75.37% in the comparator group. Thus, NBP608 is non-inferior to Zostavax® in terms of inducing the immune response and can be safely administered to adults aged 50 years or older. ClinicalTrials.gov Identifier: NCT03120364. [ABSTRACT FROM AUTHOR]

Published
2019
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45. Polymorphism near the IL28B gene in Korean hepatitis C virus-infected patients treated with peg-interferon plus ribavirin

Author

Lyoo, KwangSoo, Song, Myeong Jun, Hur, Wonhee, Choi, Jung Eun, Hong, Sung Woo, Kim, Chang Wook, Bae, Si Hyun, Choi, Jong Young, Choi, Sang Wook, Shin, Eui-Cheol, and Yoon, Seung Kew

Subjects
*HEPATITIS C virus, *GENETIC polymorphisms, *RIBAVIRIN, *ANTIVIRAL agents, *HEALTH outcome assessment, *POLYMERASE chain reaction, *HEPATITIS C treatment
Abstract

Abstract: Background: Single nucleotide polymorphisms (SNPs) near the IL28B gene have recently been described as predictors of antiviral therapy responses in patients with hepatitis C virus (HCV) genotype-1. Objectives: The aim of this study was to investigate the association between genetic variation near the IL28B gene and treatment outcome prediction in Korean patients receiving peg-interferon (PEG-IFN) plus ribavirin therapy. Study design: The allelic discrimination assay by Taqman real-time PCR was developed to determine genotypes of SNPs, rs12979860 and rs8099917, which were analyzed in 65 Korean patients with HCV genotype-1. Results: For rs12979860, the frequency of patients with sustained virological response (SVR) was 70.2% in those with the CC genotype and 25% in those with the CT genotype. Early virological response (EVR) in patients with the CC genotype (84.2%) was higher than in those with the CT genotype (25.0%). For rs8099917, patients with the TT genotype showed significantly higher in SVR and EVR than those with the TG/GG genotype (69.6% vs 33.3% and 82.1% vs 44.4%, respectively). With regards to the genotype frequency of the SNPs, the homozygous genotypes for rs12979860 (CC) or rs8099917 (TT) in Korean patients showed a significantly higher frequency as compared with other ethnicities; Caucasians, African-American, Hispanic, and Japanese. Conclusions: These results demonstrate that the genotypes rs12979860 CC and rs8099917 TT were more frequently observed in Korean patients compared to other ethnicities, and suggest that the genetic characteristics of patients may be prognostic factor that predicts antiviral response to PEG-IFN therapy for chronic hepatitis C. [Copyright &y& Elsevier]

Published
2011
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46. Adjuvant effect of bacterial outer membrane vesicles with penta-acylated lipopolysaccharide on antigen-specific T cell priming

Author

Lee, Dong Ho, Kim, Sang-Hyun, Kang, Wonseok, Choi, Yoon Seok, Lee, Sang-Ho, Lee, Sang-Rae, You, Sooseong, Lee, Heung Kyu, Chang, Kyu-Tae, and Shin, Eui-Cheol

Subjects
*IMMUNOLOGICAL adjuvants, *ENDOTOXINS, *T cells, *CYTOKINES, *VIRAL vaccines, *CANCER vaccines, *GRAM-negative bacteria, *ESCHERICHIA coli
Abstract

Abstract: Outer membrane vesicles (OMV) are nano-sized spherical blebs shed by Gram-negative bacteria and have been utilized in vaccine development. In the present study, we evaluated T cell adjuvant activity of OMV with strictly penta-acylated LPS produced by ΔmsbB/ΔpagP mutant of non-pathogenic Escherichia coli W3110 (mOMV) compared to OMV with hexa-acylated LPS produced by wild-type E. coli W3110 (wOMV). Penta-acylation of LPS renders mOMV less endotoxic than wOMV in in vitro and in vivo toxicity assays. In mice, mOMV has adjuvant activity on T cell priming not only in KLH protein immunization but also in SIINFEKL peptide immunization. The T-cell adjuvant activity of mOMV was comparable to that of wOMV and LPS and was abrogated in TLR4 K/O mice. In innate immunity, mOMV stimulated BMDCs to up-regulate co-stimulatory and antigen-presenting molecules and to produce pro-inflammatory cytokines in a TLR4-dependent manner. Of note, mOMV induced cytokine production at a significantly less extent compared with wOMV. Taken together, we propose that mOMV with penta-acylated LPS is a safe vaccine adjuvant for T cell priming and can be used in vaccine development against viral diseases and cancer. [Copyright &y& Elsevier]

Published
2011
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