Your search keyword '"Polhemus Mark"' showing total 210 results

1. Results from tandem Phase 1 studies evaluating the safety, reactogenicity and immunogenicity of the vaccine candidate antigen Plasmodium falciparum FVO merozoite surface protein-1 (MSP142) administered intramuscularly with adjuvant system AS01

Author

Otsyula Nekoye, Angov Evelina, Bergmann-Leitner Elke, Koech Margaret, Khan Farhat, Bennett Jason, Otieno Lucas, Cummings James, Andagalu Ben, Tosh Donna, Waitumbi John, Richie Nancy, Shi Meng, Miller Lori, Otieno Walter, Otieno Godfrey Allan, Ware Lisa, House Brent, Godeaux Olivier, Dubois Marie-Claude, Ogutu Bernhards, Ballou W Ripley, Soisson Lorraine, Diggs Carter, Cohen Joe, Polhemus Mark, Heppner D Gray, Ockenhouse Christian F, and Spring Michele D

Subjects

Malaria, Vaccine, Merozoite surface protein-1, Plasmodium, Arctic medicine. Tropical medicine, RC955-962, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background The development of an asexual blood stage vaccine against Plasmodium falciparum malaria based on the major merozoite surface protein-1 (MSP1) antigen is founded on the protective efficacy observed in preclinical studies and induction of invasion and growth inhibitory antibody responses. The 42 kDa C-terminus of MSP1 has been developed as the recombinant protein vaccine antigen, and the 3D7 allotype, formulated with the Adjuvant System AS02A, has been evaluated extensively in human clinical trials. In preclinical rabbit studies, the FVO allele of MSP142 has been shown to have improved immunogenicity over the 3D7 allele, in terms of antibody titres as well as growth inhibitory activity of antibodies against both the heterologous 3D7 and homologous FVO parasites. Methods Two Phase 1 clinical studies were conducted to examine the safety, reactogenicity and immunogenicity of the FVO allele of MSP142 in the adjuvant system AS01 administered intramuscularly at 0-, 1-, and 2-months: one in the USA and, after evaluation of safety data results, one in Western Kenya. The US study was an open-label, dose escalation study of 10 and 50 μg doses of MSP142 in 26 adults, while the Kenya study, evaluating 30 volunteers, was a double-blind, randomized study of only the 50 μg dose with a rabies vaccine comparator. Results In these studies it was demonstrated that this vaccine formulation has an acceptable safety profile and is immunogenic in malaria-naïve and malaria-experienced populations. High titres of anti-MSP1 antibodies were induced in both study populations, although there was a limited number of volunteers whose serum demonstrated significant inhibition of blood-stage parasites as measured by growth inhibition assay. In the US volunteers, the antibodies generated exhibited better cross-reactivity to heterologous MSP1 alleles than a MSP1-based vaccine (3D7 allele) previously tested at both study sites. Conclusions Given that the primary effector mechanism for blood stage vaccine targets is humoral, the antibody responses demonstrated to this vaccine candidate, both quantitative (total antibody titres) and qualitative (functional antibodies inhibiting parasite growth) warrant further consideration of its application in endemic settings. Trial registrations Clinical Trials NCT00666380

Published

2013

2. A Global Map of Suitability for Coastal Vibrio cholerae Under Current and Future Climate Conditions

Author

Escobar, Luis E., Ryan, Sadie J., Stewart-Ibarra, Anna M., Finkelstein, Julia L., King, Christine A., Qiao, Huijie, and Polhemus, Mark E.

Subjects

Quantitative Biology - Populations and Evolution

Abstract

Vibrio cholerae is a globally distributed water-borne pathogen that causes severe diarrheal disease and mortality, with current outbreaks as part of the seventh pandemic. Further understanding of the role of environmental factors in potential pathogen distribution and corresponding V. cholerae disease transmission over time and space is urgently needed to target surveillance of cholera and other climate and water-sensitive diseases. We used an ecological niche model (ENM) to identify environmental variables associated with V. cholerae presence in marine environments, to project a global model of V. cholerae distribution in ocean waters under current and future climate scenarios. We generated an ENM using published reports of V. cholerae in seawater and freely available remotely sensed imagery. Models indicated that factors associated with V. cholerae presence included chlorophyll-a, pH, and sea surface temperature (SST), with chlorophyll-a demonstrating the greatest explanatory power from variables selected for model calibration. We identified specific geographic areas for potential V. cholerae distribution. Coastal Bangladesh, where cholera is endemic, was found to be environmentally similar to coastal areas in Latin America. In a conservative climate change scenario, we observed a predicted increase in areas with environmental conditions suitable for V. cholerae. Findings highlight the potential for vulnerability maps to inform cholera surveillance, early warning systems, and disease prevention and control., Comment: This manuscript was accepted by Acta Tropica. Please cite as Escobar, L.E., et al., A global map of suitability for coastal Vibrio cholerae under current and future climate conditions. Acta Trop. (2015), http://dx.doi.org/10.1016/j.actatropica.2015.05.028

Published

2015

3. Allergies, body mass and hospitalization due to arbovirus infection: A prospective surveillance study in Machala, Ecuador

Author

Hargrave, Anita S., primary, Sippy, Rachel, additional, Cueva, Cinthya, additional, Polhemus, Mark, additional, Beltran, Efrain, additional, Abbott, Mark A., additional, and Stewart-Ibarra, Anna M., additional

Published

2023

4. Adenovirus type 35-vectored tuberculosis vaccine has an acceptable safety and tolerability profile in healthy, BCG-vaccinated, QuantiFERON®-TB Gold (+) Kenyan adults without evidence of tuberculosis

Author

Walsh, Douglas S., Owira, Victorine, Polhemus, Mark, Otieno, Lucas, Andagalu, Ben, Ogutu, Bernhards, Waitumbi, John, Hawkridge, Anthony, Shepherd, Barbara, Pau, Maria Grazia, Sadoff, Jerald, Douoguih, Macaya, and McClain, J. Bruce

Published

2016

5. Klebsiella pneumoniae Liver Abscess: An Emerging Disease

Author

Fazili, Tasaduq, Sharngoe, Calden, Endy, Timothy, Kiska, Deana, Javaid, Waleed, and Polhemus, Mark

Published

2016

6. 1171. Epidemiology of Old World Cutaneous Leishmaniasis among Members of the U.S. Military

Author

Cebula, Brenan R, primary, Porter, William D, additional, Wortmann, Glenn, additional, Byrne, William R, additional, Polhemus, Mark, additional, Billick, Kendall, additional, Bernstein, Wendy B, additional, Hawkes, Cliffton, additional, Marovich, Mary, additional, and Aronson, Naomi E, additional

Published

2022

7. Controlled Human Malaria Infection

Author

Spring, Michele, Polhemus, Mark, and Ockenhouse, Christian

Published

2014

8. Infections

Author

Polhemus, Mark E., Kester, Kent E., Tsokos, George C., editor, and Atkins, James L., editor

Published

2003

9. Persistence of Vaccinia at the Site of Smallpox Vaccination

Author

Cummings, James F., Polhemus, Mark E., Hawkes, Clifton, Klote, Mary, Ludwìg, George V., and Wortmann, Glenn

Published

2008

10. Exploring the utility of social-ecological and entomological risk factors for dengue infection as surveillance indicators in the dengue hyper-endemic city of Machala, Ecuador

Author

Lippi, Catherine A., primary, Stewart-Ibarra, Anna M., additional, Endy, Timothy P., additional, Abbott, Mark, additional, Cueva, Cinthya, additional, Heras, Froilán, additional, Polhemus, Mark, additional, Beltrán-Ayala, Efraín, additional, and Ryan, Sadie J., additional

Published

2021

11. Phase I dose escalation safety and immunogenicity trial of Plasmodium falciparum apical membrane protein (AMA-1) FMP2.1, adjuvanted with AS02A, in malaria-naïve adults at the Walter Reed Army Institute of Research

Author

Polhemus, Mark E., Magill, Alan J., Cummings, James F., Kester, Kent E., Ockenhouse, Chris F., Lanar, David E., Dutta, Sheetij, Barbosa, Arnoldo, Soisson, Lorraine, Diggs, Carter L., Robinson, Sally A., Haynes, John D., Stewart, V. Ann, Ware, Lisa A., Brando, Clara, Krzych, Urszula, Bowden, Robert A., Cohen, Joe D., Dubois, Marie-Claude, Ofori-Anyinam, Opokua, De-Kock, Els, Ballou, W. Ripley, and Heppner, D. Gray, Jr.

Published

2007

12. Old world leishmaniasis: an emerging infection among deployed US military and civilian workers

Author

Weina, Peter J., Neafie, Ronald C., Wortmann, Glenn, Polhemus, Mark, and Aronson, Naomi E.

Subjects

Veterans -- Health aspects, Leishmaniasis -- Diagnosis, Leishmaniasis -- Care and treatment, Health, Health care industry

Published

2004

13. Malaria prevalence defined by microscopy, antigen detection, DNA amplification and total nucleic acid amplification in a malaria-endemic region during the peak malaria transmission season

Author

Waitumbi, John N., Gerlach, Jay, Afonina, Irina, Anyona, Samuel B., Koros, Joseph N., Siangla, Joram, Ankoudinova, Irina, Singhal, Mitra, Watts, Kate, Polhemus, Mark E., Vermeulen, Nicolaas M., Mahoney, Walt, Steele, Matt, and Domingo, Gonzalo J.

Published

2011

14. Exploring the utility of social-ecological and entomological risk factors for dengue infection as surveillance indicators in the dengue hyper-endemic city of Machala, Ecuador

Author

Lippi, Catherine A., primary, Stewart-Ibarra, Anna M., additional, Endy, Timothy P., additional, Abbott, Mark, additional, Cueva, Cinthya, additional, Heras, Froilán, additional, Polhemus, Mark, additional, Beltrán-Ayala, Efraín, additional, and Ryan, Sadie J., additional

Published

2020

15. A Phase 1, Open-Label Assessment of a Dengue Virus-1 Live Virus Human Challenge Strain

Author

Endy, Timothy P, primary, Wang, Dongliang, additional, Polhemus, Mark E, additional, Jarman, Richard G, additional, Jasper, Louis E, additional, Gromowski, Greg, additional, Lin, Leyi, additional, De La Barra, Rafael A, additional, Friberg, Heather, additional, Currier, Jeffrey R, additional, Abbott, Mark, additional, Ware, Lisa, additional, Klick, Michelle, additional, Paolino, Kristopher M, additional, Blair, Donald C, additional, Eckels, Kenneth, additional, Rutvisuttinunt, Wiriya, additional, and Thomas, Stephen J, additional

Published

2020

16. Serologic Response of 2 Versus 3 Doses and Intradermal Versus Intramuscular Administration of a Licensed Rabies Vaccine for Preexposure Prophylaxis

Author

Endy, Timothy P, primary, Keiser, Paul B, additional, Wang, Dongliang, additional, Jarman, Richard G, additional, Cibula, Don, additional, Fang, Hengsheng, additional, Ware, Lisa, additional, Abbott, Mark, additional, Thomas, Stephen J, additional, and Polhemus, Mark E, additional

Published

2019

17. Towards an RTS,S-based, multi-stage, multi-antigen vaccine against falciparum malaria: progress at the Walter Reed Army Institute of Research

Author

Heppner, D. Gray, Jr., Kester, Kent E., Ockenhouse, Christian F., Tornieporth, Nadia, Ofori, Opokua, Lyon, Jeffrey A., Stewart, V. Ann, Dubois, Patrice, Lanar, David E., Krzych, Urszula, Moris, Philippe, Angov, Evelina, Cummings, James F., Leach, Amanda, Hall, B. Ted, Dutta, Sheetij, Schwenk, Robert, Hillier, Collette, Barbosa, Arnoldo, Ware, Lisa A., Nair, Lalitha, Darko, Christian A., Withers, Mark R., Ogutu, Bernhards, Polhemus, Mark E., Fukuda, Mark, Pichyangkul, Sathit, Gettyacamin, Montip, Diggs, Carter, Soisson, Lorraine, Milman, Jessica, Dubois, Marie-Claude, Garçon, Nathalie, Tucker, Kathryn, Wittes, Janet, Plowe, Christopher V., Thera, Mahamadou A., Duombo, Ogobara K., Pau, Maria G., Goudsmit, Jaap, Ballou, W. Ripley, and Cohen, Joe

Published

2005

18. Hb G-Philadelphia or Stanleyville II? When the phenotype and genotype do not agree

Author

Waitumbi, John N., Kifude, Carolyne M., Withers, Mark R., Polhemus, Mark E., Heppner, D. Gray, Jr, and Ogutu, Bernhards R.

Published

2007

19. Molecular epidemiology of chikungunya virus from Ecuador demonstrates two introductions and the E1-K211E mutation suggesting presence of enhanced fitness to Aedes aegypti

Author

Berry, Irina Maljkovic, Ibarra, Anna M. Stewart, Wiriya Rutvisuttinunt, Ayala, Felix Efrain Beltran, Figueroa, Katherine, Abhinaya Srikanth, Washington B Cárdenas, Cueva, Cinthya, Polhemus, Mark, Ryan, Sadie Jane, Endy, Timothy P, and Jarman, Richard G

Published

2018

20. The Effects of Japanese Encephalitis Vaccine and Accelerated Dosing Scheduling on the Immunogenicity of the Chimeric Yellow Fever Derived Tetravalent Dengue Vaccine: A Phase II, Randomized, Open-Label, Single-Center Trial in Adults Aged 18 to 45 Years in the United States

Author

Glass, Aaron, primary, Polhemus, Mark, additional, Wang, Dongliang, additional, Jarman, Richard G, additional, Thomas, Stephen J, additional, Friberg, Heather, additional, Currier, Jeffrey R, additional, Bonaparte, Matthew, additional, De La Barra, Rafael, additional, Princiotta, Michael F, additional, Abbott, Mark, additional, Cuzzo, Brian, additional, Machabert, Tifany, additional, Sridhar, Saranya, additional, and Endy, Timothy P, additional

Published

2019

21. Effect of Antimalarial Drugs on the Immune Response to Intramuscular Rabies Vaccination Using a Postexposure Prophylaxis Regimen

Author

Endy, Timothy P, primary, Keiser, Paul B, primary, Cibula, Don, primary, Abbott, Mark, primary, Ware, Lisa, primary, Thomas, Stephen J, primary, and Polhemus, Mark E, primary

Published

2019

22. Micronutrients, Immunological Parameters, and Dengue Virus Infection in Coastal Ecuador: A Nested Case-Control Study in an Infectious Disease Surveillance Program

Author

Finkelstein, Julia L, primary, Colt, Susannah, additional, Layden, Alexander J, additional, Krisher, Jesse T, additional, Stewart-Ibarra, Anna M, additional, Polhemus, Mark, additional, Beltrán-Ayala, Efraín, additional, Tedesco, Julia M, additional, Cárdenas, Washington B, additional, Endy, Timothy, additional, and Mehta, Saurabh, additional

Published

2019

23. Assessing the Diversity and Stability of Cellular Immunity Generated in Response to the Candidate Live-Attenuated Dengue Virus Vaccine TAK-003

Author

Waickman, Adam T., primary, Friberg, Heather, additional, Gargulak, Morgan, additional, Kong, Amanda, additional, Polhemus, Mark, additional, Endy, Timothy, additional, Thomas, Stephen J., additional, Jarman, Richard G., additional, and Currier, Jeffrey R., additional

Published

2019

24. Lack of vaccinia viremia after smallpox vaccination

Author

Cummings, James F., Polhemus, Mark E., Hawkes, Clifton, Klote, Mary, Ludwig, George V., and Wortmann, Glenn

Subjects

Health, Health care industry

Published

2004

25. Spatiotemporal Variation in Environmental Vibrio cholerae in an Estuary in Southern Coastal Ecuador

Author

Fish and Wildlife Conservation, Ryan, Sadie J., Stewart-Ibarra, Anna M., Ordóñez-Enireb, Eunice, Chu, Winnie, Finkelstein, Julia L., King, Christine A., Escobar, Luis E., Lupone, Christina, Heras, Froilan, Tauzer, Erica, Waggoner, Egan, James, Tyler G., Cárdenas, Washington B., Polhemus, Mark, Fish and Wildlife Conservation, Ryan, Sadie J., Stewart-Ibarra, Anna M., Ordóñez-Enireb, Eunice, Chu, Winnie, Finkelstein, Julia L., King, Christine A., Escobar, Luis E., Lupone, Christina, Heras, Froilan, Tauzer, Erica, Waggoner, Egan, James, Tyler G., Cárdenas, Washington B., and Polhemus, Mark

Abstract

Cholera emergence is strongly linked to local environmental and ecological context. The 1991–2004 pandemic emerged in Perú and spread north into Ecuador’s El Oro province, making this a key site for potential re-emergence. Machala, El Oro, is a port city of 250,000 inhabitants, near the Peruvian border. Many livelihoods depend on the estuarine system, from fishing for subsistence and trade, to domestic water use. In 2014, we conducted biweekly sampling for 10 months in five estuarine locations, across a gradient of human use, and ranging from inland to ocean. We measured water-specific environmental variables implicated in cholera growth and persistence: pH, temperature, salinity, and algal concentration, and evaluated samples in five months for pathogenic and non-pathogenic Vibrio cholerae, by polymerase chain reaction (PCR). We found environmental persistence of pandemic strains O1 and O139, but no evidence for toxigenic strains. Vibrio cholerae presence was coupled to algal and salinity concentration, and sites exhibited considerable seasonal and spatial heterogeneity. This study indicates that environmental conditions in Machala are optimal for cholera re-emergence, with risk peaking during September, and higher risk near urban periphery low-income communities. This highlights a need for surveillance of this coupled cholera–estuarine system to anticipate potential future cholera outbreaks.

Published

2018

26. A Phase 1, Open-Label Assessment of a Dengue Virus-1 Live Virus Human Challenge Strain.

Author

Endy, Timothy P, Wang, Dongliang, Polhemus, Mark E, Jarman, Richard G, Jasper, Louis E, Gromowski, Greg, Lin, Leyi, Barra, Rafael A De La, Friberg, Heather, Currier, Jeffrey R, Abbott, Mark, Ware, Lisa, Klick, Michelle, Paolino, Kristopher M, Blair, Donald C, Eckels, Kenneth, Rutvisuttinunt, Wiriya, Thomas, Stephen J, and De La Barra, Rafael A

Subjects

DENGUE, CLINICAL trial registries, VIRUSES, COMMERCIAL product testing, DENGUE viruses, RESEARCH, VIRAL vaccines, HUMAN research subjects, IMMUNIZATION, CLINICAL trials, FLAVIVIRUSES, RESEARCH methodology, MEDICAL cooperation, EVALUATION research, COMPARATIVE studies, VIREMIA

Abstract

Background: Dengue human infection models (DHIM) have been used as a safe means to test the viability of prophylaxis and therapeutics.Methods: A phase 1 study of 12 healthy adult volunteers using a challenge virus, DENV-1-LVHC strain 45AZ5, was performed. A dose escalating design was used to determine the safety and performance profile of the challenge virus. Subjects were evaluated extensively until 28 days and then out to 6 months.Results: Twelve subjects received the challenge virus: 6 with 0.5 mL of 6.5 × 103 plaque-forming units (PFU)/mL (low-dose group) and 6 with 0.5 mL of 6.5 × 104 PFU/mL (mid-dose group). All except 1 in the low-dose group developed detectable viremia. For all subjects the mean incubation period was 5.9 days (range 5-9 days) and mean time of viremia was 6.8 days (range 3-9 days). Mean peak for all subjects was 1.6 × 107 genome equivalents (GE)/mL (range 4.6 × 103 to 5 × 107 GE/mL). There were no serious adverse events or long-term safety signals noted.Conclusions: We conclude that DENV-1-LVHC was well-tolerated, resulted in an uncomplicated dengue illness, and may be a suitable DHIM for therapeutic and prophylactic product testing.Clinical Trials Registration: NCT02372175. [ABSTRACT FROM AUTHOR]

Published

2021

27. Spread of dengue 1 and 2 in Machala, Ecuador: Evidence of a dynamic epidemic genetically related to those of surrounding countries of Colombia, Venezuela and Peru Data and Analyses Dengue 1 Dengue 2

Author

Berry, Irina Maljkovic, Stewart-Ibarra, Anna M, Wiriya Rutvisuttinunt, Beltrán-Ayala, Efraín, Washington B Cárdenas, Cueva, Cinthya, Polhemus, Mark, Ryan, Sadie J, Endy, Timothy P, and Jarman, Richard G

Published

2017

28. Serologic Response of 2 Versus 3 Doses and Intradermal Versus Intramuscular Administration of a Licensed Rabies Vaccine for Preexposure Prophylaxis.

Author

Endy, Timothy P., Keiser, Paul B., Wang, Dongliang, Jarman, Richard G., Cibula, Don, Fang, Hengsheng, Ware, Lisa, Abbott, Mark, Thomas, Stephen J., and Polhemus, Mark E.

Abstract

Background. The World Health Organization recommends intradermal (ID) administration of rabies vaccine for preexposure prophylaxis. Methods. In a randomized trial in adults assigned to 1 of 6 treatment groups (ID vs intramuscular [IM], 2 vs 3 doses, and controls), rabies neutralizing antibody titers were measured to 1 year postvaccination. Results. ID vaccination produced acceptable antibody levels in all subjects (2- and 3-dose groups). At day 365, acceptable levels were 40% for IM and 50% for ID 2-dose schedule, and 70% for IM and 60% for ID 3-dose schedule. Conclusions. ID rabies vaccination induces acceptable an- tibody titers at a fraction of the dose. [ABSTRACT FROM AUTHOR]

Published

2020

29. The Effects of Japanese Encephalitis Vaccine and Accelerated Dosing Scheduling on the Immunogenicity of the Chimeric Yellow Fever Derived Tetravalent Dengue Vaccine: A Phase II, Randomized, Open-Label, Single-Center Trial in Adults Aged 18 to 45 Years in the United States

Author

Glass, Aaron, Polhemus, Mark, Wang, Dongliang, Jarman, Richard G, Thomas, Stephen J, Friberg, Heather, Currier, Jeffrey R, Bonaparte, Matthew, Barra, Rafael De La, Princiotta, Michael F, Abbott, Mark, Cuzzo, Brian, Machabert, Tifany, Sridhar, Saranya, and Endy, Timothy P

Subjects

*JAPANESE B encephalitis, *YELLOW fever, *DENGUE, *VACCINES, *IMMUNIZATION of children, *DENGUE viruses

Abstract

Background Dengue is a global health problem requiring an effective, safe dengue vaccine. Methods We report the results of a phase II, randomized, open-label, single-center trial in adults aged 18 to 45 years in the United States designed to explore the effects of the Chimeric Yellow Fever Derived Tetravalent Dengue Vaccine (CYD-TDV, Dengvaxia) when administered on its designated schedule (months 0, 6, and 12) or on an accelerated dosing schedule (months 0, 2, and 6) and/or given before, or concomitantly with, a vaccine against Japanese encephalitis (JE). Results Based on dengue virus serotype-specific neutralizing antibody (NAb), the accelerated dosing schedule was comparable to the 0, 6, and 12-month schedule. Giving JE vaccine concurrently with CYD-TDV did not result in an increase in overall NAb titers. Immunophenotyping of peripheral blood mononuclear cells revealed an increase in activated CD8+ T cells after CYD-TDV vaccination, a phenomenon that was greatest for the JE vaccine primed. Conclusions We conclude that an accelerated dosing schedule of CYD-TDV results in essentially equivalent dengue serotype-specific NAb titers as the currently used schedule, and there may be an early benefit in antibody titers and activated CD8+ T cells by the administration of the JE vaccine before CYD-TDV vaccination. [ABSTRACT FROM AUTHOR]

Published

2020

30. Effect of Antimalarial Drugs on the Immune Response to Intramuscular Rabies Vaccination Using a Postexposure Prophylaxis Regimen.

Author

Endy, Timothy P, Keiser, Paul B, Cibula, Don, Abbott, Mark, Ware, Lisa, Thomas, Stephen J, and Polhemus, Mark E

Subjects

RABIES vaccines, PHARMACOLOGY, IMMUNE response, PREVENTIVE medicine, ANTIBODY formation, RABIES prevention, RESEARCH, IMMUNIZATION, IMMUNOGLOBULINS, RESEARCH methodology, EVALUATION research, MEDICAL cooperation, MEDICAL protocols, COMPARATIVE studies, DRUG interactions, ANTIMALARIALS, VIRAL antibodies, RNA viruses, PHARMACODYNAMICS

Abstract

Background: Chloroquine can impair the immune responses to intradermal rabies vaccination. Current guidelines recommend an extra intramuscular dose be given for postexposure prophylaxis in previously unvaccinated persons taking any antimalarial drug.Methods: We conducted a randomized, open-label, single-site study in 103 previously unvaccinated healthy adults age ≥18 to ≤60 years old to evaluate the effects of chloroquine, atovaquone/proguanil (Malarone), and doxycycline on the antibody response to a purified chick embryo cell vaccine, given on a postexposure prophylaxis schedule. All treatment groups received antimalarials 14 days prior to and during vaccination.Results: All subjects achieved accepted neutralizing antibody titers of ≥0.5 IU/mL following the second rabies vaccination dose and maintained this protection through the duration of the study. We observed a reduction in rabies antibody geometric mean titer in the chloroquine versus control groups 28 days after vaccination: 2.3 versus 6.87 IU/mL, respectively (P < .001, t test). A significant difference was not observed for those taking Malarone or doxycycline.Conclusions: We conclude that there is no reduction of rabies antibody response in subjects taking Malarone or doxycycline, but a significant reduction in those taking chloroquine; however, accepted antibody levels were achieved for all 3 antimalarials.Clinical Trials Registration: NCT02564471. [ABSTRACT FROM AUTHOR]

Published

2020

31. Micronutrients, Immunological Parameters, and Dengue Virus Infection in Coastal Ecuador: A Nested Case-Control Study in an Infectious Disease Surveillance Program.

Author

Finkelstein, Julia L, Colt, Susannah, Layden, Alexander J, Krisher, Jesse T, Stewart-Ibarra, Anna M, Polhemus, Mark, Beltrán-Ayala, Efraín, Tedesco, Julia M, Cárdenas, Washington B, Endy, Timothy, and Mehta, Saurabh

Subjects

VIRUS diseases, DENGUE viruses, COMMUNICABLE diseases, RETINOL-binding proteins, MICRONUTRIENTS, DENGUE hemorrhagic fever, PUBLIC health surveillance, INTERLEUKINS, C-reactive protein, RESEARCH, DENGUE, FEVER, FERRITIN, RESEARCH methodology, CASE-control method, EVALUATION research, MEDICAL cooperation, VITAMIN D, COMPARATIVE studies, RESEARCH funding, BODY mass index, NUTRITIONAL status, CARRIER proteins, BODY size

Abstract

Background: Micronutrients are known to modulate host immunity, and there is limited literature on this association in the context of dengue virus infection (DENV).Methods: Using a nested case-control design in a surveillance program, we measured the following: anthropometry; nutritional biomarkers including serum ferritin, soluble transferrin receptor, retinol-binding protein (RBP), 25-hydroxy vitamin D, folate, and vitamin B12; and a panel of immune response markers. We then compared these measures across 4 illness categories: healthy control, nonfebrile DENV, other febrile illness (OFI), and apparent DENV using multivariate polytomous logistic regression models.Results: Among 142 participants, serum ferritin (ng/mL) was associated with apparent DENV compared to healthy controls (odds ratio [OR], 2.66; confidence interval [CI], 1.53-4.62; P = .001), and RBP concentrations (µmol/L) were associated with apparent DENV (OR, 0.03; CI, 0.00-0.30; P = .003) and OFI (OR, 0.02; CI, 0.00-0.24; P = .003). In a subset of 71 participants, interleukin-15 levels (median fluorescent intensity) were positively associated with apparent DENV (OR, 1.09; CI, 1.03-1.14; P = .001) and negatively associated with nonfebrile DENV (OR, 0.89; CI, 0.80-0.99; P = .03) compared to healthy controls.Conclusions: After adjusting for the acute-phase response, serum ferritin and RBP concentrations were associated with apparent DENV and may represent biomarkers of clinical importance in the context of dengue illness. [ABSTRACT FROM AUTHOR]

Published

2020

32. The Burden of Dengue Fever and Chikungunya in Southern Coastal Ecuador: Epidemiology, Clinical Presentation, and Phylogenetics from the First Two Years of a Prospective Study

Author

Stewart-Ibarra, Anna M., primary, Ryan, Sadie J., additional, Kenneson, Aileen, additional, King, Christine A., additional, Abbott, Mark, additional, Barbachano-Guerrero, Arturo, additional, Beltrán-Ayala, Efraín, additional, Borbor-Cordova, Mercy J., additional, Cárdenas, Washington B., additional, Cueva, Cinthya, additional, Finkelstein, Julia L., additional, Lupone, Christina D., additional, Jarman, Richard G., additional, Maljkovic Berry, Irina, additional, Mehta, Saurabh, additional, Polhemus, Mark, additional, Silva, Mercy, additional, and Endy, Timothy P., additional

Published

2018

33. Spatiotemporal Variation in Environmental Vibrio cholerae in an Estuary in Southern Coastal Ecuador

Author

Ryan, Sadie, primary, Stewart-Ibarra, Anna, additional, Ordóñez-Enireb, Eunice, additional, Chu, Winnie, additional, Finkelstein, Julia, additional, King, Christine, additional, Escobar, Luis, additional, Lupone, Christina, additional, Heras, Froilan, additional, Tauzer, Erica, additional, Waggoner, Egan, additional, James, Tyler, additional, Cárdenas, Washington, additional, and Polhemus, Mark, additional

Published

2018

34. Case Report: An Acute Chikungunya Infection and a Recent Secondary Dengue Infection in a Peripartum Case in Ecuador

Author

Farrell, Daniel F., primary, Lupone, Christina D., additional, Kenneson, Aileen, additional, Cueva, Cinthya, additional, Heydari, Naveed, additional, Barzallo Aguilera, Julio H., additional, Polhemus, Mark, additional, Endy, Timothy P., additional, and Stewart-Ibarra, Anna M., additional

Published

2018

35. Social-ecological factors and preventive actions decrease the risk of dengue infection at the household-level: Results from a prospective dengue surveillance study in Machala, Ecuador

Author

Kenneson, Aileen, primary, Beltrán-Ayala, Efraín, additional, Borbor-Cordova, Mercy J., additional, Polhemus, Mark E., additional, Ryan, Sadie J., additional, Endy, Timothy P., additional, and Stewart-Ibarra, Anna M., additional

Published

2017

36. MOESM1 of Successful malaria elimination in the Ecuadorâ Peru border region: epidemiology and lessons learned

Author

Krisher, Lyndsay, Krisher, Jesse, Ambuludi, Mariano, Arichabala, Ana, BeltrĂĄn-Ayala, Efrain, Navarrete, Patricia, OrdoĂąez, Tania, Polhemus, Mark, Quintana, Fernando, Rochford, Rosemary, Mercy Silva, Bazo, Juan, and Stewart-Ibarra, Anna

Abstract

Additional file 1: Table S1. Table of key informant experts in the study and their position during the elimination period.

Published

2016

37. Phase 2a, Open-Label, 4-Escalating-Dose, Randomized Multicenter Study Evaluating the Safety and Activity of Ferroquine (SSR97193) Plus Artesunate, versus Amodiaquine Plus Artesunate, in African Adult Men with Uncomplicated Plasmodium falciparum Malaria

Author

Supan, Christian, primary, Walsh, Douglas S., additional, Lell, Bertrand, additional, Kombila, Maryvonne, additional, Polhemus, Mark E., additional, Ospina Salazar, Carmen L., additional, Kremsner, Peter G., additional, Cantalloube, Cathy, additional, Otsula, Nekoye, additional, Djeriou, Elhadj, additional, Apollo, Duncan, additional, Waitumbi, John, additional, Ogutu, Bernhards, additional, Mombo-Ngoma, Ghyslain, additional, and Held, Jana, additional

Published

2017

38. Spatial and seasonal dynamics of cholera (Vibrio cholerae) in an estuary in southern coastal Ecuador

Author

Ryan, Sadie J., primary, Stewart Ibarra, Anna M., additional, Ordóñez, Eunice, additional, Chu, Winnie, additional, Finkelstein, Julia L., additional, King, Christine A., additional, Escobar, Luis E., additional, Lupone, Christina, additional, Heras, Froilan, additional, Tauzer, Erica, additional, Waggoner, Egan, additional, James, Tyler G., additional, Cárdenas, Washington B., additional, and Polhemus, Mark, additional

Published

2017

39. The burden of dengue fever and chikungunya in southern coastal Ecuador: Epidemiology, clinical presentation, and phylogenetics from the first two years of a prospective study

Author

Stewart-Ibarra, Anna M., primary, Ryan, Sadie J., additional, Kenneson, Aileen, additional, King, Christine A., additional, Abbott, Mark, additional, Barbachano-Guerrero, Arturo, additional, Beltrán-Ayala, Efraín, additional, Borbor-Cordova, Mercy J., additional, Cárdenas, Washington B., additional, Cueva, Cinthya, additional, Finkelstein, Julia L., additional, Lupone, Christina D., additional, Jarman, Richard G., additional, Berry, Irina Maljkovic, additional, Mehta, Saurabh, additional, Polhemus, Mark, additional, Silva, Mercy, additional, and Endy, Timothy P., additional

Published

2017

40. A global map of suitability for coastal cholera under current and future climate conditions

Author

Escobar, Luis E., Ryan, Sadie J., Ibarra, Anna M. Stewart, Finkelstein, Julia, King, Christine A., Huijie Qiao, and Polhemus, Mark E.

Published

2014

41. Successful malaria elimination in the Ecuador–Peru border region: epidemiology and lessons learned

Author

Krisher, Lyndsay K., primary, Krisher, Jesse, additional, Ambuludi, Mariano, additional, Arichabala, Ana, additional, Beltrán-Ayala, Efrain, additional, Navarrete, Patricia, additional, Ordoñez, Tania, additional, Polhemus, Mark E., additional, Quintana, Fernando, additional, Rochford, Rosemary, additional, Silva, Mercy, additional, Bazo, Juan, additional, and Stewart-Ibarra, Anna M., additional

Published

2016

42. Phase 1/2a Trial of Plasmodium vivax Malaria Vaccine Candidate VMP001/AS01B in Malaria-Naive Adults: Safety, Immunogenicity, and Efficacy

Author

Bennett, Jason W., primary, Yadava, Anjali, additional, Tosh, Donna, additional, Sattabongkot, Jetsumon, additional, Komisar, Jack, additional, Ware, Lisa A., additional, McCarthy, William F., additional, Cowden, Jessica J., additional, Regules, Jason, additional, Spring, Michele D., additional, Paolino, Kristopher, additional, Hartzell, Joshua D., additional, Cummings, James F., additional, Richie, Thomas L., additional, Lumsden, Joanne, additional, Kamau, Edwin, additional, Murphy, Jittawadee, additional, Lee, Cynthia, additional, Parekh, Falgunee, additional, Birkett, Ashley, additional, Cohen, Joe, additional, Ballou, W. Ripley, additional, Polhemus, Mark E., additional, Vanloubbeeck, Yannick F., additional, Vekemans, Johan, additional, and Ockenhouse, Christian F., additional

Published

2016

43. A global map of suitability for coastal Vibrio cholerae under current and future climate conditions

Author

Escobar, Luis E., primary, Ryan, Sadie J., additional, Stewart-Ibarra, Anna M., additional, Finkelstein, Julia L., additional, King, Christine A., additional, Qiao, Huijie, additional, and Polhemus, Mark E., additional

Published

2015

44. Therapeutic Failure in Returning Traveler With Falciparum Malaria Treated With Artemether-Lumefantrine: First Reported Case Report in United States

Author

Sharma, Amit M, primary, Amin, Mohsena, additional, Syed, Wajihuddin, additional, Gnanabakthan, Naveen, additional, Orellana, Cesar, additional, Sharma, Namita, additional, and Polhemus, Mark, additional

Published

2015

45. A US soldier who returned from Iraq with nonhealing sores

Author

Polhemus, Mark E., Aronson, Naomi, Weina, Pete, McEvoy, Pete, Neafi, Ronald, and Wortmann, Glenn

Subjects

Leishmaniasis, Cutaneous -- Causes of, Leishmaniasis, Cutaneous -- Research, Leishmaniasis -- Risk factors, Leishmaniasis -- Research, Health, Health care industry

Published

2004

46. Infections

Author

Polhemus, Mark E., primary and Kester, Kent E., additional

47. Micronutrients and Dengue

Author

Ahmed, Sundus, primary, Mehta, Saurabh, additional, Kenneth, John, additional, Polhemus, Mark E., additional, Cardenas, Washington, additional, Stewart, Anna M., additional, Endy, Timothy P., additional, and Finkelstein, Julia L., additional

Published

2014

48. Pharmacokinetic evaluation of intravenous artesunate in adults with uncomplicated falciparum malaria in Kenya: a phase II study

Author

Li, Qigui, primary, Remich, Shon, additional, Miller, Scott R, additional, Ogutu, Bernhards, additional, Otieno, Walter, additional, Melendez, Victor, additional, Teja-Isavadharm, Paktiya, additional, Weina, Peter J, additional, Hickman, Mark R, additional, Smith, Bryan, additional, and Polhemus, Mark, additional

Published

2014

49. 923Lactococcus garvieae infective endocarditis requiring valve replacement: First case in the United States

Author

Sharngoe, Calden, primary, Fazili, Tasaduq, additional, Javaid, Waleed, additional, Endy, Timothy, additional, and Polhemus, Mark, additional

Published

2014

50. DNA Prime/Adenovirus Boost Malaria Vaccine Encoding P. falciparum CSP and AMA1 Induces Sterile Protection Associated with Cell-Mediated Immunity

Author

WALTER REED ARMY INST OF RESEARCH SILVER SPRING MD MILITARY MALARIA VACCINE PROGRAM, Chuang, Ilin, Sedegah, Martha, Cicatelli, Susan, Spring, Michele, Polhemus, Mark, Tamminga, Cindy, Patterson, Noelle, Guerrero, Melanie, Bennett, Jason W, McGrath, Shannon, WALTER REED ARMY INST OF RESEARCH SILVER SPRING MD MILITARY MALARIA VACCINE PROGRAM, Chuang, Ilin, Sedegah, Martha, Cicatelli, Susan, Spring, Michele, Polhemus, Mark, Tamminga, Cindy, Patterson, Noelle, Guerrero, Melanie, Bennett, Jason W, and McGrath, Shannon

Abstract

Gene-based vaccination using prime/boost regimens protects animals and humans against malaria, inducing cell-mediated responses that in animal models target liver stage malaria parasites. We tested a DNA prime/adenovirus boost malaria vaccine in a Phase 1 clinical trial with controlled human malaria infection. The vaccine regimen was three monthly doses of two DNA plasmids (DNA) followed four months later by a single boost with two non-replicating human serotype 5 adenovirus vectors (Ad). The constructs encoded genes expressing P. falciparum circumsporozoite protein (CSP) and apical membrane antigen-1 (AMA1). The regimen was safe and well-tolerated, with mostly mild adverse events that occurred at the site of injection. Only one AE (diarrhea), possibly related to immunization, was severe (Grade 3), preventing daily activities. Four weeks after the Ad boost, 15 study subjects were challenged with P. falciparum sporozoites by mosquito bite, and four (27%) were sterilely protected. Antibody responses by ELISA rose after Ad boost but were low (CSP geometric mean titer 210, range 44 817; AMA1 geometric mean micrograms/milliliter 11.9, range 1.5 102) and were not associated with protection. Ex vivo IFN-c ELISpot responses after Ad boost were modest (CSP geometric mean spot forming cells/million peripheral blood mononuclear cells 86, range 13 408; AMA1 348, range 88 1270) and were highest in three protected subjects. ELISpot responses to AMA1 were significantly associated with protection (p = 0.019). Flow cytometry identified predominant IFN-c mono-secreting CD8+ T cell responses in three protected subjects. No subjects with high pre-existing anti-Ad5 neutralizing antibodies were protected but the association was not statistically significant. The DNA/Ad regimen provided the highest sterile immunity achieved against malaria following immunization with a gene-based subunit vaccine (27%)., Published in PLoS ONE, v8 n2 article ID e55571, 14 Feb 2013. Prepared in collaboration with the US Military Malaria Vaccine Program, Naval Medical Research Center, Silver Spring, MD. Prepared in cooperation with the Radboud University Nijmegen Medical Center, Nijmegen, The Netherlands, GenVec, Inc., Gaithersburg, MD, and USAID, Washington, D. C. The original document contains color images.

Published

2013