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Dive into the research topics where Charmagne G. Beckett is active.

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Featured researches published by Charmagne G. Beckett.


Vaccine | 2011

Evaluation of a prototype dengue-1 DNA vaccine in a Phase 1 clinical trial.

Charmagne G. Beckett; Jeffrey A. Tjaden; Timothy Burgess; Janine R. Danko; Cindy Tamminga; Monika Simmons; Shuenn-Jue Wu; Peifang Sun; Tadeusz J. Kochel; Kanakatte Raviprakash; Curtis G. Hayes; Kevin R. Porter

Candidate dengue DNA vaccine constructs for each dengue serotype were developed by incorporating pre-membrane and envelope genes into a plasmid vector. A Phase 1 clinical trial was performed using the dengue virus serotype-1 (DENV-1) vaccine construct (D1ME(100)). The study was an open-label, dose-escalation, safety and immunogenicity trial involving 22 healthy flavivirus-naïve adults assigned to one of two groups. Each group received three intramuscular injections (0, 1, and 5 months) of either a high dose (5.0mg, n=12) or a low dose (1.0mg, n=10) DNA vaccine using the needle-free Biojector(®) 2000. The most commonly reported solicited signs and symptoms were local mild pain or tenderness (10/22, 45%), local mild swelling (6/22, 27%), muscle pain (6/22, 27%) and fatigue (6/22, 27%). Five subjects (41.6%) in the high dose group and none in the low dose group developed detectable anti-dengue neutralizing antibodies. T-cell IFN gamma responses were detected in 50% (4/8) and 83.3% (10/12) of subjects in the low and high dose groups, respectively. The safety profile of the DENV-1 DNA vaccine is acceptable at both doses administered in the study. These results demonstrate a favorable reactogenicity and safety profile of the first in human evaluation of a DENV-1 DNA vaccine.


Clinical Infectious Diseases | 2004

Influenza Surveillance in Indonesia: 1999–2003

Charmagne G. Beckett; Herman Kosasih; Chairin Nisa Ma'roef; Erlin Listiyaningsih; Iqbal Elyazar; Suharyono Wuryadi; Djoko Yuwono; James L. Mcardle; Andrew L. Corwin; Kevin R. Porter

Although influenza is recognized for its worldwide importance, little is known about the disease from tropical countries like Indonesia. From August 1999 through January 2003, a surveillance study was conducted in clinics at 6 sentinel locations. Adults (age, >14 years) and children (age, 4-14 years) presenting with respiratory symptoms suggestive of influenza were asked to enroll in the study. Nasal and pharyngeal swabs were examined by virus isolation, polymerase chain reaction, and rapid immunochromatographic tests. A total of 3079 specimens were collected from 1544 participants. Influenza infection was confirmed in 172 volunteers (11.1%) presenting with influenza-like illness. Influenza A (H1N1 and H3N2) and B viruses were detected at all sites. Peak prevalence tended to coincide with the respective rainy seasons, regardless of location. In light of the recent epidemic of severe acute respiratory syndrome, continued influenza surveillance would be useful in strengthening the infrastructure of the Indonesian public health system.


Virology | 2011

Infection and activation of human peripheral blood monocytes by dengue viruses through the mechanism of antibody-dependent enhancement ☆ , ☆☆ , ★, ★★

Peifang Sun; Karolis Bauza; Subhamoy Pal; Zhaodong Liang; Shuenn-Jue Wu; Charmagne G. Beckett; Timothy Burgess; Kevin R. Porter

Human monocytes are susceptible to dengue virus (DV) infection through an FcR-dependent pathway known as antibody-dependent enhancement (ADE). In this study, infection enhancement was observed when purified monocytes were infected with DV serotypes in the presence of serially diluted immune serum antibodies. Analyzing binding of the DV-antibody immune complexes to monocytes by quantifying the amount of viruses attached to monocytes, we found that binding did not correlate with the input amount of antibodies; rather, it peaked at suboptimal antibody concentrations, correlating with the observed infection enhancement. These results suggested that immune complexes are involved in hindering DV from binding to FcR-bearing cells; when such a protective feature is weakened, enhancement of viral attachment and ADE are observed. Further, increased cytokine production (TNF-alpha and IFN-alpha), and costimulatory marker expression (CD86 and CD40), were found to be associated with infection enhancement, suggesting a pathological role of ADE-affected monocytes in dengue hemorrhagic diseases.


Influenza and Other Respiratory Viruses | 2013

Surveillance of Influenza in Indonesia, 2003–2007

Herman Kosasih; Roselinda; Nurhayati; Alexander Klimov; Xu Xiyan; Stephen Lindstrom; Frank Mahoney; Charmagne G. Beckett; Timothy Burgess; Patrick J. Blair; Timothy M. Uyeki; Endang R. Sedyaningsih

Background  Longitudinal data are limited about the circulating strains of influenza viruses and their public health impact in Indonesia. We conducted influenza surveillance among outpatients and hospitalized patients with influenza‐like illness (ILI) across the Indonesian archipelago from 2003 through 2007.


PLOS Neglected Tropical Diseases | 2016

The Epidemiology, Virology and Clinical Findings of Dengue Virus Infections in a Cohort of Indonesian Adults in Western Java

Herman Kosasih; Bachti Alisjahbana; Nurhayati; Quirijn de Mast; Irani Rudiman; Susana Widjaja; Ungke Antonjaya; Harli Novriani; Nugroho Harry Susanto; Hadi Jusuf; Andre van der Ven; Charmagne G. Beckett; Patrick J. Blair; Timothy Burgess; Maya Williams; Kevin R. Porter

Background Dengue has emerged as one of the most important infectious diseases in the last five decades. Evidence indicates the expansion of dengue virus endemic areas and consequently the exponential increase of dengue virus infections across the subtropics. The clinical manifestations of dengue virus infection include sudden fever, rash, headache, myalgia and in more serious cases, spontaneous bleeding. These manifestations occur in children as well as in adults. Defining the epidemiology of dengue in a given area is critical to understanding the disease and devising effective public health strategies. Methodology/Principal Findings Here, we report the results from a prospective cohort study of 4380 adults in West Java, Indonesia, from 2000–2004 and 2006–2009. A total of 2167 febrile episodes were documented and dengue virus infections were confirmed by RT-PCR or serology in 268 cases (12.4%). The proportion ranged from 7.6 to 41.8% each year. The overall incidence rate of symptomatic dengue virus infections was 17.3 cases/1,000 person years and between September 2006 and April 2008 asymptomatic infections were 2.6 times more frequent than symptomatic infections. According to the 1997 WHO classification guidelines, there were 210 dengue fever cases, 53 dengue hemorrhagic fever cases (including one dengue shock syndrome case) and five unclassified cases. Evidence for sequential dengue virus infections was seen in six subjects. All four dengue virus serotypes circulated most years. Inapparent dengue virus infections were predominantly associated with DENV-4 infections. Conclusions/Significance Dengue virus was responsible for a significant percentage of febrile illnesses in an adult population in West Java, Indonesia, and this percentage varied from year to year. The observed incidence rate during the study period was 43 times higher than the reported national or provincial rates during the same time period. A wide range of clinical severity was observed with most infections resulting in asymptomatic disease. The circulation of all four serotypes of dengue virus was observed in most years of the study.


Journal of Virological Methods | 2011

A dendritic cell-based assay for measuring memory T cells specific to dengue envelope proteins in human peripheral blood

Peifang Sun; Charmagne G. Beckett; Janine R. Danko; Timothy Burgess; Zhaodong Liang; Tadeusz J. Kochel; Kevin R. Porter

Dengue envelope (E) protein is a dominant immune inducer and E protein-based vaccines elicited partial to complete protection in non-human primates. To study the immunogenicity of these vaccines in humans, an enzyme linked immunospot (ELISPOT) assay for measuring interferon gamma (IFN-γ) production was developed. Cells from two subject groups, based on dengue-exposure, were selected for assay development. The unique feature of the IFN-γ ELISPOT assay is the utilization of dendritic cells pulsed with E proteins as antigen presenting cells. IFN-γ production, ranging from 53-513 spot forming units per million peripheral blood mononuclear cells (PBMCs), was observed in dengue-exposed subjects as compared to 0-45 IFN-γ spot forming units in dengue-unexposed subjects. Further, both CD4(+) and CD8(+) T cells, and cells bearing CD45RO memory marker, were the major sources of IFN-γ production. The assay allowed quantification of E-specific IFN-γ-secreting memory T cells in subjects 9 years after exposure to a live-attenuated virus vaccine and live-virus challenge. Results suggested that the dendritic cell-based IFN-γ assay is a useful tool for assessing immunological memory for clinical research.


Journal of Immunological Methods | 2017

NK cell degranulation as a marker for measuring antibody-dependent cytotoxicity in neutralizing and non-neutralizing human sera from dengue patients

Peifang Sun; Brian J. Morrison; Charmagne G. Beckett; Zhaodong Liang; Nishith Nagabhushana; An Li; Kevin R. Porter; Maya Williams

The study assessed antibody-dependent NK cell degranulation, a biomarker relevant to antibody-dependent cell cytotoxicity (ADCC), to analyze dengue immune sera. We first determined binding intensity of patient sera to the surface of DENV-infected cells and examined the types of antigens expressed on infected cells. Antigens from pre-membrane (PreM) and envelope (E), but not from NS proteins were detected on the surface of infected cells. After adding NK cells to infected target cells previously treated with patient sera, rapid NK cell degranulation was observed. Non-neutralizing patient sera generated comparable NK cell degranulation as that of neutralizing sera, suggesting ADCC may be a protective mechanism apart from Ab neutralization. The level of NK cell degranulation varied dramatically among human individuals and was associated with the level of CD16 expression on NK cells, informing on the complexity of ADCC among human population.


Transactions of The Royal Society of Tropical Medicine and Hygiene | 2005

Tracking the re-emergence of epidemic chikungunya virus in Indonesia

Kanti Laras; Nono Sukri; Ria Purwita Larasati; Michael J. Bangs; Rizal Kosim; Djauzi; Tony Wandra; John Master; Herman Kosasih; Sri Hartati; Charmagne G. Beckett; Endang R. Sedyaningsih; H. James Beecham; Andrew L. Corwin


American Journal of Tropical Medicine and Hygiene | 2005

Epidemiology of dengue and dengue hemorrhagic fever in a cohort of adults living in Bandung, West Java, Indonesia

Kevin R. Porter; Charmagne G. Beckett; Herman Kosasih; Ratna Tan; Bachti Alisjahbana; Pandji Irani Fianza Rudiman; Susana Widjaja; Erlin Listiyaningsih; Chairin Nisa Ma’roef; James L. Mcardle; Ida Parwati; Primal Sudjana; Hadi Jusuf; Djoko Yuwono; Suharyono Wuryadi


American Journal of Tropical Medicine and Hygiene | 2005

EARLY DETECTION OF DENGUE INFECTIONS USING CLUSTER SAMPLING AROUND INDEX CASES

Charmagne G. Beckett; Herman Kosasih; Indra Faisal; Nurhayati; Ratna Tan; Susana Widjaja; Erlin Listiyaningsih; Chairin Nisa Ma’roef; Suharyono Wuryadi; Michael J. Bangs; Tatang K. Samsi; Djoko Yuwono; Curtis G. Hayes; Kevin R. Porter

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Kevin R. Porter

Naval Medical Research Center

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Timothy Burgess

Uniformed Services University of the Health Sciences

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Peifang Sun

Naval Medical Research Center

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Ratna Tan

New Mexico State University

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Patrick J. Blair

Naval Medical Research Center

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Susana Widjaja

Naval Medical Research Center

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Zhaodong Liang

Henry M. Jackson Foundation for the Advancement of Military Medicine

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