14 results on '"Ahn CD"'
Search Results
2. Comparison of Prevalence and Ultrasonography Features of Thyroglossal Duct Cyst in Adults According to Radioactive Iodine Ablation.
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Yoo Jin Lee, Dong Wook Kim, Gi Won Shin, Jin Young Park, Hye Jung Choo, Ha Kyoung Park, Tae Kwun Ha, Do Hun Kim, Soo Jin Jung, Ji Sun Park, Sung Ho Moon, Ki Jung Ahn, and Hye Jin Baek
- Published
- 2019
- Full Text
- View/download PDF
3. Utility of Preoperative Ultrasonography in Transferred Patients with Suspicious Malignancy on Ultrasonography-Guided Fine-Needle Aspiration Cytology of Thyroid Nodules: A Single-Center Retrospective Study.
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Taewoo Kang, Dong Wook Kim, Gi Won Shin, Jin Young Park, Yoo Jin Lee, Hye Jung Choo, Young Jun Cho, Soo Jin Jung, Ha Kyoung Park, Tae Kwun Ha, Do Hun Kim, Ji Sun Park, Sung Ho Moon, Ki Jung Ahn, and Hye Jin Baek
- Published
- 2019
- Full Text
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4. Features of effective T Cell-inducing vaccines against Chronic viral infections.
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Panagioti, Eleni, Klenerman, Paul, Lee, Lian N., van der Burg, Sjoerd H., and Arens, Ramon
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T cells ,VIRUS diseases ,VIRAL vaccines - Abstract
For many years, the focus of prophylactic vaccines was to elicit neutralizing antibodies, but it has become increasingly evident that T cell-mediated immunity plays a central role in controlling persistent viral infections such as with human immunodeficiency virus, cytomegalovirus, and hepatitis C virus. Currently, various promising prophylactic vaccines, capable of inducing substantial vaccine-specific T cell responses, are investigated in preclinical and clinical studies. There is compelling evidence that protection by T cells is related to the magnitude and breadth of the T cell response, the type and homing properties of the memory T cell subsets, and their cytokine polyfunctionality and metabolic fitness. In this review, we evaluated these key factors that determine the qualitative and quantitative properties of CD4
+ and CD8+ T cell responses in the context of chronic viral disease and prophylactic vaccine development. Elucidation of the mechanisms underlying T cell-mediated protection against chronic viral pathogens will facilitate the development of more potent, durable and safe prophylactic T cell-based vaccines. [ABSTRACT FROM AUTHOR]- Published
- 2018
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- View/download PDF
5. Fighting Napoleon in Totonicapán.
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Hawkins, Timothy
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IMPERIALISM ,BUREAUCRACY ,SPANISH monarchy ,POLITICAL autonomy - Published
- 2017
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6. The role of MHC class I gene products in SIV infection of macaques.
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Silver, Zachary and Watkins, David
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HIV ,PUBLIC health ,GENOTYPES ,EPITOPES ,VIRAL replication - Abstract
Human immunodeficiency virus (HIV) remains among the most significant public health threats worldwide. Despite three decades of research following the discovery of HIV, a preventive vaccine remains elusive. The study of HIV elite controllers has been crucial to elaborate the genetic and immunologic determinants that underlie control of HIV replication. Coordinated studies of elite control in humans have, however, been limited by variability among infecting viral strains, host genotype, and the uncertainty of the timing and route of infection. In this review, we discuss the role of nonhuman primate (NHP) models for the elucidation of the immunologic correlates that underlie control of AIDS virus replication. We discuss the importance of major histocompatibility complex class I (MHC-I) alleles in activating CD8+ T-cell populations that promote control of both HIV and simian immunodeficiency virus (SIV) replication. Provocatively, we make the argument that T-cell subsets recognizing the HIV/SIV viral infectivity factor (Vif) protein may be crucial for control of viral replication. We hope that this review demonstrates how an in-depth understanding of the MHC-I gene products associated with elite control of HIV/SIV, and the epitopes that they present, can provide researchers with a glimpse into the protective immune responses that underlie AIDS nonprogression. [ABSTRACT FROM AUTHOR]
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- 2017
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7. Dendritic Cell Targeting Effectively Boosts T Cell Responses Elicited by an HIV Multiepitope DNA Vaccine.
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de Souza Apostólico, Juliana, Santos Lunardelli, Victória Alves, Yamamoto, Marcio Massao, Santos Souza, Higo Fernando, Cunha-Neto, Edecio, Boscardin, Silvia Beatriz, and Santoro Rosa, Daniela
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DNA vaccines ,DENDRITIC cells ,TARGETED drug delivery - Abstract
Despite several efforts in the last decades, an efficacious HIV-1 vaccine is still not available. Different approaches have been evaluated, such as recombinant proteins, viral vectors, DNA vaccines, and, most recently, dendritic cell (DC) targeting. This strategy is based on DC features that place them as central for induction of immunity. Targeting is accomplished by the use of chimeric monoclonal antibodies directed to DC surface receptors fused to the antigen of interest. In this work, we targeted eight promiscuous HIV-derived CD4
+ T cell epitopes (HIVBr8) to the DEC205+ DCs by fusing the multiepitope immunogen to the heavy chain of αDEC205 (αDECHIVBr8), in the presence of the TLR3 agonist poly (I:C). In addition, we tested a DNA vaccine encoding the same epitopes using homologous or heterologous prime-boost regimens. Our results showed that mice immunized with αDECHIVBr8 presented higher CD4+ and CD8+ T cell responses when compared to mice that received the DNA vaccine (pVAXHIVBr8). In addition, pVAXHIVBr8 priming followed by αDECHIVBr8 boosting induced higher polyfunctional proliferative and cytokine-producing T cell responses to HIV-1 peptides than homologous DNA immunization or heterologous αDEC prime/DNA boost. Based on these results, we conclude that homologous prime-boost and heterologous boosting immunization strategies targeting CD4+ epitopes to DCs are effective to improve HIV-specific cellular immune responses when compared to standalone DNA immunization. Moreover, our results indicate that antigen targeting to DC is an efficient strategy to boost immunity against a multiepitope immunogen, especially in the context of DNA vaccination. [ABSTRACT FROM AUTHOR]- Published
- 2017
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8. La La La.
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De Fazio, Veronica
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CHILDREN'S music - Published
- 2017
9. Mucosal B Cells Are Associated with Delayed SIV Acquisition in Vaccinated Female but Not Male Rhesus Macaques Following SIVmac251 Rectal Challenge.
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Tuero, Iskra, Mohanram, Venkatramanan, Musich, Thomas, Miller, Leia, Vargas-Inchaustegui, Diego A., Demberg, Thorsten, Venzon, David, Kalisz, Irene, Kalyanaraman, V. S., Pal, Ranajit, Ferrari, Maria Grazia, LaBranche, Celia, Montefiori, David C., Rao, Mangala, Vaccari, Monica, Franchini, Genoveffa, Barnett, Susan W., and Robert-Guroff, Marjorie
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GENETICS of virus diseases ,B cells ,SIMIAN immunodeficiency virus diseases ,MEDICAL genetics ,PATHOGENIC microorganisms - Abstract
Many viral infections, including HIV, exhibit sex-based pathogenic differences. However, few studies have examined vaccine-related sex differences. We compared immunogenicity and protective efficacy of monomeric SIV gp120 with oligomeric SIV gp140 in a pre-clinical rhesus macaque study and explored a subsequent sex bias in vaccine outcome. Each immunization group (16 females, 8 males) was primed twice mucosally with replication-competent Ad-recombinants encoding SIV
smH4 env/rev, SIV239 gag and SIV239 nefΔ1–13 and boosted twice intramuscularly with SIVmac239 monomeric gp120 or oligomeric gp140 in MF59 adjuvant. Controls (7 females, 5 males) received empty Ad and MF59. Up to 9 weekly intrarectal challenges with low-dose SIVmac251 were administered until macaques became infected. We assessed vaccine-induced binding, neutralizing, and non-neutralizing antibodies, Env-specific memory B cells and plasmablasts/plasma cells (PB/PC) in bone marrow and rectal tissue, mucosal Env-specific antibodies, and Env-specific T-cells. Post-challenge, only one macaque (gp140-immunized) remained uninfected. However, SIV acquisition was significantly delayed in vaccinated females but not males, correlated with Env-specific IgA in rectal secretions, rectal Env-specific memory B cells, and PC in rectal tissue. These results extend previous correlations of mucosal antibodies and memory B cells with protective efficacy. The gp140 regimen was more immunogenic, stimulating elevated gp140 and cyclic V2 binding antibodies, ADCC and ADCP activities, bone marrow Env-specific PB/PC, and rectal gp140-specific IgG. However, immunization with gp120, the form of envelope immunogen used in RV144, the only vaccine trial to show some efficacy, provided more significant acquisition delay. Further over 40 weeks of follow-up, no gp120 immunized macaques met euthanasia criteria in contrast to 7 gp140-immunized and 2 control animals. Although males had higher binding antibodies than females, ADCC and ADCP activities were similar. The complex challenge outcomes may reflect differences in IgG subtypes, Fc glycosylation, Fc-R polymorphisms, and/or the microbiome, key areas for future studies. This first demonstration of a sex-difference in SIV vaccine-induced protection emphasizes the need for sex-balancing in vaccine trials. Our results highlight the importance of mucosal immunity and memory B cells at the SIV exposure site for protection. [ABSTRACT FROM AUTHOR]- Published
- 2015
- Full Text
- View/download PDF
10. Plasmacytoid dendritic cell and functional HIV Gag p55-specific T cells before treatment interruption can inform set-point plasma HIV viral load after treatment interruption in chronically suppressed HIV-1+ patients.
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Papasavvas, Emmanouil, Foulkes, Andrea, Yin, Xiangfan, Joseph, Jocelin, Ross, Brian, Azzoni, Livio, Kostman, Jay R., Mounzer, Karam, Shull, Jane, and Montaner, Luis J.
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DENDRITIC cells ,STATISTICAL correlation ,T cells ,ANTIRETROVIRAL agents ,HIV infections ,THERAPEUTICS ,HIV-positive persons ,NATURAL immunity - Abstract
The identification of immune correlates of HIV control is important for the design of immunotherapies that could support cure or antiretroviral therapy ( ART) intensification-related strategies. ART interruptions may facilitate this task through exposure of an ART partially reconstituted immune system to endogenous virus. We investigated the relationship between set-point plasma HIV viral load ( VL) during an ART interruption and innate/adaptive parameters before or after interruption. Dendritic cell ( DC), natural killer ( NK) cell and HIV Gag p55-specific T-cell functional responses were measured in paired cryopreserved peripheral blood mononuclear cells obtained at the beginning (on ART) and at set-point of an open-ended interruption from 31 ART-suppressed chronically HIV-1
+ patients. Spearman correlation and linear regression modeling were used. Frequencies of plasmacytoid DC (p DC), and HIV Gag p55-specific CD3+ CD4− perforin+ IFN- γ+ cells at the beginning of interruption associated negatively with set-point plasma VL. Inclusion of both variables with interaction into a model resulted in the best fit (adjusted R2 = 0·6874). Frequencies of p DC or HIV Gag p55-specific CD3+ CD4− CSFElo CD107a+ cells at set-point associated negatively with set-point plasma VL. The dual contribution of p DC and anti- HIV T-cell responses to viral control, supported by our models, suggests that these variables may serve as immune correlates of viral control and could be integrated in cure or ART-intensification strategies. [ABSTRACT FROM AUTHOR]- Published
- 2015
- Full Text
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11. La La La. Performed by Priscilla Ahn
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De Fazio, Veronica
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La La La (Sound recording) -- Ahn, Priscilla -- Sound recording reviews ,Education ,Library and information science ,Publishing industry - Abstract
La La La. Performed by Priscilla Ahn. CD. 30 min. Produced by Priscilla Ahn. 2016. $16.99. PreS-Gr2--Ahn brings her unique brand of quiet folk pop with hints of jazz to [...]
- Published
- 2017
12. A Great Fear : Luís De Onís and the Shadow War Against Napoleon in Spanish America, 1808–1812
- Author
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Timothy Hawkins and Timothy Hawkins
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- Spain--History--Napoleonic Conquest, 1808-1813, Spain--Foreign relations--1808-1814, Oni´s, Luis de--1762-1827, Spain--Colonies--America
- Abstract
An exploration of the Spanish colonial reaction to the threat of Napoleonic subversion A Great Fear: Luís de Onís and the Shadow War against Napoleon in Spanish America, 1808–1812 explores why Spanish Americans did not take the opportunity to seize independence in this critical period when Spain was overrun by French armies and, arguably, in its weakest state. In the first years after his appointment as Spanish ambassador to the United States, Luís de Onís claimed the heavy responsibility of defending Spanish America from the wave of French spies, subversives, and soldiers whom he believed Napoleon was sending across the Atlantic to undermine the empire. As a leading representative of Spain's loyalist government in the Americas, Onís played a central role in identifying, framing, and developing what soon became a coordinated response from the colonial bureaucracy to this perceived threat. This crusade had important short-term consequences for the empire. Since it paralleled the emergence of embryonic independence movements against Spanish rule, colonial officials immediately conflated these dangers and attributed anti-Spanish sentiment to foreign conspiracies. Little direct evidence of Napoleon's efforts at subversion in Spanish America exists. However, on the basis of prodigious research, Hawkins asserts that the fear of French intervention mattered far more than the reality. Reinforced by detailed warnings from Ambassador Onís, who found the United States to be the staging ground for many of the French emissaries, colonial officials and their subjects became convinced that Napoleon posed a real threat. The official reaction to the threat of French intervention increasingly led Spanish authorities to view their subjects with suspicion, as potential enemies rather than allies in the struggle to preserve the empire. In the long term, this climate of fear eroded the legitimacy of the Spanish Crown among Spanish Americans, a process that contributed to the unraveling of the empire by the 1820s. This study draws on documents and official records from both sides of the Hispanic Atlantic, with extensive research conducted in Spain, Guatemala, Argentina, and the United States. Overall, it is a provocative interpretation of the repercussions of Napoleonic intrigue and espionage in the New World and a stellar examination of late Spanish colonialism in the Americas.
- Published
- 2019
13. Human Vaccines : Emerging Technologies in Design and Development
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Kayvon Modjarrad, Wayne C. Koff, Kayvon Modjarrad, and Wayne C. Koff
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- Vaccination, Vaccines--Biotechnology, Vaccines--Design
- Abstract
Human Vaccines: Emerging Technologies in Design and Development discusses the advances in molecular biology, biophysics, and informatics—among other disciplines—that have provided scientists with the tools to create new vaccines against emerging and re-emerging pathogens. For example, the virus-like particle technologies that led to licensing of highly efficacious HPV vaccines have only come into full realization in the last 10 years. Their success has, in turn, accelerated the pace with which nanoparticle vaccines are being developed Given the rapidity with which the field is changing and the absence of any text documenting this change, there is a need for a resource that surveys these new vaccine technologies, assesses their potential, and describes their applications. This book provides that resource and complements traditional vaccinology books, but also serves as an excellent standalone for researchers and students with basic knowledge in immunology. - Introduces new topics in vaccine immunology in the context vaccine design and production - Consolidates the growing body of knowledge on new vaccine technologies that have only emerged in the past 2 – 3 decades - Reviews the currently licensed vaccines that have utilized leading-edge technologies and how this has translated into improved efficacy and safety - Provides a broad overview of innovative vaccine technologies, including immunological aspects
- Published
- 2017
14. A History of Theology
- Author
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Congar, Yves M.J., Guthrie, Hunter, Translated and edited by, Congar, Yves M.J., and Guthrie, Hunter
- Published
- 2019
- Full Text
- View/download PDF
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