Your search keyword '"Polhemus ME"' showing total 33 results

1. Dietary and socio-economic correlates of nutritional status in a rural adult Kenyan population

Author

Jayne, J, Scrimgeour, AG, Polhemus, ME, Otieno, L, and Bovill, ME

Subjects

Nutrition Transition, Malnutrition, Adults, Overweight, Kenya

Abstract

There is a lack of data on trends in body composition among developing countries and the distribution of malnutrition among adults is poorly understood. Thus, the objective was to establish nutritional status, demographic make-up, dietary habits, and to determine if socioeconomic variables or dietary habits are associated withnutritional status in a rural adult Kenyan population. Five hundred Kenyan adults ages 18-55 years were recruited from the Kombewa division, located 40 km west of Kisumu, Kenya. The proportion of underweight and overweight adults is consistent with developing countries in nutrition transition. Using standard body mass index (BMI) classifications, 9.8% of the study population was underweight, 76.0% were normal weight, and 14.2% were overweight or obese. Significantly more females (20.7%) were overweight or obese than males (4.1%) (P=0.001). Iron deficiency was a significant issue, with 21.4% of females classified as anemic (Hb

Published

2011

2. A phase IIa, randomized, double-blind, safety, immunogenicity and efficacy trial of Plasmodium falciparum vaccine antigens merozoite surface protein 1 and RTS,S formulated with AS02 adjuvant in healthy, malaria-naïve adults.

Author

Cummings JF, Polhemus ME, Kester KE, Ockenhouse CF, Gasser RA Jr, Coyne P, Wortmann G, Nielsen RK, Schaecher K, Holland CA, Krzych U, Tornieporth N, Soisson LA, Angov E, and Heppner DG

Subjects

Adult, Child, Humans, Adjuvants, Immunologic, Antibodies, Protozoan, Antigens, Protozoan, Merozoite Surface Protein 1, Parasitemia, Plasmodium falciparum, Protozoan Proteins, Double-Blind Method, Malaria prevention & control, Malaria Vaccines, Malaria, Falciparum prevention & control

Abstract

Background: To improve the efficacy of Plasmodium falciparum malaria vaccine RTS,S/AS02, we conducted a study in 2001 in healthy, malaria-naïve adults administered RTS,S/AS02 in combination with FMP1, a recombinant merozoite surface-protein-1, C-terminal 42kD fragment., Methods: A double-blind Phase I/IIa study randomized N = 60 subjects 1:1:1:1 to one of four groups, N = 15/group, to evaluate safety, immunogenicity, and efficacy of intra-deltoid half-doses of RTS,S/AS02 and FMP1/AS02 administered in the contralateral (RTS,S + FMP1-separate) or same (RTS,S + FMP1-same) sites, or FMP1/AS02 alone (FMP1-alone), or RTS,S/AS02 alone (RTS,S-alone) on a 0-, 1-, 3-month schedule. Subjects receiving three doses of vaccine and non-immunized controls (N = 11) were infected with homologous P. falciparum 3D7 sporozoites by Controlled Human Malaria Infection (CHMI)., Results: Subjects in all vaccination groups experienced mostly mild or moderate local and general adverse events that resolved within eight days. Anti-circumsporozoite antibody levels were lower when FMP1 and RTS,S were co-administered at the same site (35.0 µg/mL: 95 % CI 20.3-63), versus separate arms (57.4 µg/mL: 95 % CI 32.3-102) or RTS,S alone (62.0 µg/mL: 95 % CI: 37.8-101.8). RTS,S-specific lymphoproliferative responses and ex vivo ELISpot CSP-specific interferon-gamma (IFN-γ) responses were indistinguishable among groups receiving RTS,S/AS02. There was no difference in antibody to FMP1 among groups receiving FMP1/AS02. After CHMI, groups immunized with a RTS,S-containing regimen had ∼ 30 % sterile protection against parasitemia, and equivalent delays in time-to-parasitemia. The FMP1/AS02 alone group showed no sterile immunity or delay in parasitemia., Conclusion: Co-administration of RTS,S and FMP1/AS02 reduced anti-RTS,S antibody, but did not affect tolerability, cellular immunity, or efficacy in a stringent CHMI model. Absence of efficacy or delay of patency in the sporozoite challenge model in the FMP1/AS02 group did not rule out efficacy of FMP1/AS02 in an endemic population. However, a Phase IIb trial of FMP1/AS02 in children in malaria-endemic Kenya did not demonstrate efficacy against natural infection., Clinicaltrials: gov identifier: NCT01556945., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Evelina Angov has patent #7,550275 issued to United States Government. Evelina Angov has patent #7,595,191 issued to United States Government. Coauthor, Nadia Tornieporth, previously employee of GlaxoSmithKline Biologics., (Published by Elsevier India Pvt Ltd.)

Published

2024

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

Author

Endy TP, Wang D, Polhemus ME, Jarman RG, Jasper LE, Gromowski G, Lin L, De La Barra RA, Friberg H, Currier JR, Abbott M, Ware L, Klick M, Paolino KM, Blair DC, Eckels K, Rutvisuttinunt W, and Thomas SJ

Subjects

Dengue immunology, Dengue virology, Dengue Vaccines administration & dosage, Dengue Vaccines adverse effects, Healthy Volunteers, Humans, Outcome Assessment, Health Care, Vaccination, Vaccines, Virus-Like Particle administration & dosage, Vaccines, Virus-Like Particle adverse effects, Viremia immunology, Viremia prevention & control, Viremia virology, Dengue prevention & control, Dengue Vaccines immunology, Dengue Virus immunology, Vaccines, Virus-Like Particle immunology

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., (© The Author(s) 2020. Published by Oxford University Press for the Infectious Diseases Society of America. All rights reserved. For permissions, e-mail: journals.permissions@oup.com.)

Published

2021

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

Author

Endy TP, Keiser PB, Wang D, Jarman RG, Cibula D, Fang H, Ware L, Abbott M, Thomas SJ, and Polhemus ME

Subjects

Adolescent, Adult, Antibodies, Viral immunology, Female, Humans, Immunization Schedule, Immunization, Secondary, Injections, Intradermal, Injections, Intramuscular, Linear Models, Male, Middle Aged, Post-Exposure Prophylaxis, Pre-Exposure Prophylaxis methods, Rabies Vaccines adverse effects, Rabies virus immunology, Vaccination, Young Adult, Antibodies, Neutralizing blood, Immunogenicity, Vaccine, Rabies prevention & control, Rabies Vaccines administration & dosage, Rabies Vaccines immunology

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 antibody titers at a fraction of the dose., Clinical Trials Registration: NCT02374814., (© The Author(s) 2019. Published by Oxford University Press for the Infectious Diseases Society of America. All rights reserved. For permissions, e-mail: journals.permissions@oup.com.)

Published

2020

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

Author

Endy TP, Keiser PB, Cibula D, Abbott M, Ware L, Thomas SJ, and Polhemus ME

Subjects

Adolescent, Adult, Antibodies, Neutralizing, Antimalarials administration & dosage, Drug Interactions, Female, Humans, Immunization Schedule, Male, Middle Aged, Post-Exposure Prophylaxis, Rabies Vaccines administration & dosage, Rabies virus immunology, Vaccination, Young Adult, Antibodies, Viral blood, Antimalarials pharmacology, Rabies prevention & control, Rabies Vaccines immunology

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., (© The Author(s) 2019. Published by Oxford University Press for the Infectious Diseases Society of America. All rights reserved. For permissions, e-mail: journals.permissions@oup.com.)

Published

2020

6. 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 A, Beltrán-Ayala E, Borbor-Cordova MJ, Polhemus ME, Ryan SJ, Endy TP, and Stewart-Ibarra AM

Subjects

Adult, Animals, Dengue epidemiology, Dengue virology, Disease Outbreaks, Ecuador epidemiology, Epidemiological Monitoring, Family Characteristics, Female, Housing, Humans, Logistic Models, Male, Middle Aged, Prospective Studies, Risk Factors, Social Environment, Aedes virology, Dengue prevention & control, Dengue Virus physiology, Insect Vectors virology, Mosquito Control

Abstract

Background: In Ecuador, dengue virus (DENV) infections transmitted by the Aedes aegypti mosquito are among the greatest public health concerns in urban coastal communities. Community- and household-level vector control is the principal means of controlling disease outbreaks. This study aimed to assess the impact of knowledge, attitudes, and practices (KAPs) and social-ecological factors on the presence or absence of DENV infections in the household., Methods: In 2014 and 2015, individuals with DENV infections from sentinel clinics in Machala, Ecuador, were invited to participate in the study, as well as members of their household and members of four neighboring households located within 200 meters. We conducted diagnostic testing for DENV on all study participants; we surveyed heads of households (HOHs) regarding demographics, housing conditions and KAPs. We compared KAPs and social-ecological factors between households with (n = 139) versus without (n = 80) DENV infections, using bivariate analyses and multivariate logistic regression models with and without interactions., Results: Significant risk factors in multivariate models included proximity to abandoned properties, interruptions in piped water, and shaded patios (p<0.05). Significant protective factors included the use of mosquito bed nets, fumigation inside the home, and piped water inside the home (p<0.05). In bivariate analyses (but not multivariate modeling), DENV infections were positively associated with HOHs who were male, employed, and of younger age than households without infections (p<0.05). DENV infections were not associated with knowledge, attitude, or reported barriers to prevention activities., Discussion: Specific actions that can be considered to decrease the risk of DENV infections in the household include targeting vector control in highly shaded properties, fumigating inside the home, and use of mosquito bed nets. Community-level interventions include cleanup of abandoned properties, daily garbage collection, and reliable piped water inside houses. These findings can inform interventions to reduce the risk of other diseases transmitted by the Ae. aegypti mosquito, such as chikungunya and Zika fever.

Published

2017

7. 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 C, Mombo-Ngoma G, Kombila M, Ospina Salazar CL, Held J, Lell B, Cantalloube C, Djeriou E, Ogutu B, Waitumbi J, Otsula N, Apollo D, Polhemus ME, Kremsner PG, and Walsh DS

Subjects

Adult, Aged, Aged, 80 and over, Artesunate, Dose-Response Relationship, Drug, Gabon, Humans, Kenya, Male, Metallocenes, Middle Aged, Aminoquinolines therapeutic use, Amodiaquine therapeutic use, Antimalarials therapeutic use, Artemisinins therapeutic use, Drug Therapy, Combination, Ferrous Compounds therapeutic use, Malaria, Falciparum drug therapy

Abstract

Artemisinin-based combination therapies are recommended as first-line agents for treating uncomplicated Plasmodium falciparum malaria. Ferroquine, a 4-aminoquinolone, is a novel long-acting combination partner for fast-acting drugs like artesunate (AS). We did a small phase 2a, multicenter, open-label, safety-focused dose-ranging randomized study of ferroquine at three African hospitals: two Gabonese and one Kenyan. We recruited adult men with symptomatic uncomplicated P. falciparum monoinfection. Four escalating doses of ferroquine (100, 200, 400, and 600 mg) were assessed in sequence, versus an amodiaquine comparator. After a 2:1 randomization (block size three, equating to N = 12 for each ferroquine dose and N = 6 for each of four amodiaquine comparator groups) patients received daily for three consecutive days, either ferroquine + AS (200 mg/day) or amodiaquine (612 mg/day) + AS (200 mg/day). Safety, electrocardiograms, parasite clearance times, efficacy, and pharmacokinetics were assessed to day 28. Seventy-two patients were randomized. Ferroquine + AS showed generally mild increases (Grade 1 toxicity) in alanine aminotransferase (ALT) levels with a dose trend starting at 400 mg. There were two Grade 2 ALT events: one patient receiving 200 mg (3.8 upper limit of normal [ULN], day 7) and one receiving 600 mg (3.3 ULN, day 14), both without increased bilirubin. One ferroquine 100 mg + AS patient after one dose was withdrawn after developing a QTcF interval prolongation > 60 milliseconds over baseline. Parasitemias in all patients cleared quickly, with no recurrence through day 28. Hepatic, as well as cardiac, profiles should be monitored closely in future trials. (ClinicalTrials.gov: NCT00563914).

Published

2017

8. Successful malaria elimination in the Ecuador-Peru border region: epidemiology and lessons learned.

Author

Krisher LK, Krisher J, Ambuludi M, Arichabala A, Beltrán-Ayala E, Navarrete P, Ordoñez T, Polhemus ME, Quintana F, Rochford R, Silva M, Bazo J, and Stewart-Ibarra AM

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Child, Child, Preschool, Ecuador epidemiology, Female, Humans, Infant, Infant, Newborn, International Cooperation, Male, Middle Aged, Peru epidemiology, Young Adult, Communicable Disease Control methods, Communicable Disease Control organization & administration, Disease Eradication, Malaria, Falciparum epidemiology, Malaria, Falciparum prevention & control, Malaria, Vivax epidemiology, Malaria, Vivax prevention & control

Abstract

Background: In recent years, malaria (Plasmodium vivax and Plasmodium falciparum) has been successfully controlled in the Ecuador-Peru coastal border region. The aim of this study was to document this control effort and to identify the best practices and lessons learned that are applicable to malaria control and to other vector-borne diseases. A proximal outcome evaluation was conducted of the robust elimination programme in El Oro Province, Ecuador, and the Tumbes Region, Peru. Data collection efforts included a series of workshops with local public health experts who played central roles in the elimination effort, review of epidemiological records from Ministries of Health, and a review of national policy documents. Key programmatic and external factors are identified that determined the success of this eradication effort., Case Description: From the mid 1980s until the early 2000s, the region experienced a surge in malaria transmission, which experts attributed to a combination of ineffective anti-malarial treatment, social-ecological factors (e.g., El Niño, increasing rice farming, construction of a reservoir), and political factors (e.g., reduction in resources and changes in management). In response to the malaria crisis, local public health practitioners from El Oro and Tumbes joined together in the mid-1990s to forge an unofficial binational collaboration for malaria control. Over the next 20 years, they effectively eradicated malaria in the region, by strengthening surveillance and treatment strategies, sharing of resources, operational research to inform policy, and novel interventions., Discussion and Evaluation: The binational collaboration at the operational level was the fundamental component of the successful malaria elimination programme. This unique relationship created a trusting, open environment that allowed for flexibility, rapid response, innovation and resilience in times of crisis, and ultimately a sustainable control programme. Strong community involvement, an extensive microscopy network and ongoing epidemiologic investigations at the local level were also identified as crucial programmatic strategies., Conclusion: The results of this study provide key principles of a successful malaria elimination programme that can inform the next generation of public health professionals in the region, and serve as a guide to ongoing and future control efforts of other emerging vector borne diseases globally.

Published

2016

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

Author

Bennett JW, Yadava A, Tosh D, Sattabongkot J, Komisar J, Ware LA, McCarthy WF, Cowden JJ, Regules J, Spring MD, Paolino K, Hartzell JD, Cummings JF, Richie TL, Lumsden J, Kamau E, Murphy J, Lee C, Parekh F, Birkett A, Cohen J, Ballou WR, Polhemus ME, Vanloubbeeck YF, Vekemans J, and Ockenhouse CF

Subjects

Adolescent, Adult, Antibodies, Protozoan immunology, Female, Humans, Malaria Vaccines administration & dosage, Malaria Vaccines adverse effects, Malaria, Vivax immunology, Malaria, Vivax parasitology, Male, Middle Aged, Protozoan Proteins administration & dosage, Protozoan Proteins adverse effects, Vaccination, Young Adult, Malaria Vaccines immunology, Malaria, Vivax prevention & control, Plasmodium vivax immunology, Protozoan Proteins immunology

Abstract

Background: A vaccine to prevent infection and disease caused by Plasmodium vivax is needed both to reduce the morbidity caused by this parasite and as a key component in efforts to eradicate malaria worldwide. Vivax malaria protein 1 (VMP001), a novel chimeric protein that incorporates the amino- and carboxy- terminal regions of the circumsporozoite protein (CSP) and a truncated repeat region that contains repeat sequences from both the VK210 (type 1) and the VK247 (type 2) parasites, was developed as a vaccine candidate for global use., Methods: We conducted a first-in-human Phase 1 dose escalation vaccine study with controlled human malaria infection (CHMI) of VMP001 formulated in the GSK Adjuvant System AS01B. A total of 30 volunteers divided into 3 groups (10 per group) were given 3 intramuscular injections of 15 μg, 30 μg, or 60 μg respectively of VMP001, all formulated in 500 μL of AS01B at each immunization. All vaccinated volunteers participated in a P. vivax CHMI 14 days following the third immunization. Six non-vaccinated subjects served as infectivity controls., Results: The vaccine was shown to be well tolerated and immunogenic. All volunteers generated robust humoral and cellular immune responses to the vaccine antigen. Vaccination did not induce sterile protection; however, a small but significant delay in time to parasitemia was seen in 59% of vaccinated subjects compared to the control group. An association was identified between levels of anti-type 1 repeat antibodies and prepatent period., Significance: This trial was the first to assess the efficacy of a P. vivax CSP vaccine candidate by CHMI. The association of type 1 repeat-specific antibody responses with delay in the prepatency period suggests that augmenting the immune responses to this domain may improve strain-specific vaccine efficacy. The availability of a P. vivax CHMI model will accelerate the process of P. vivax vaccine development, allowing better selection of candidate vaccines for advancement to field trials.

Published

2016

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

Author

Escobar LE, Ryan SJ, Stewart-Ibarra AM, Finkelstein JL, King CA, Qiao H, and Polhemus ME

Subjects

Bangladesh epidemiology, Chlorophyll, Chlorophyll A, Environment, Humans, Latin America epidemiology, Models, Theoretical, Risk Factors, Temperature, Cholera epidemiology, Climate, Climate Change, Disease Outbreaks, Oceans and Seas, Vibrio cholerae

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., (Copyright © 2015 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2015

11. Micronutrients and dengue.

Author

Ahmed S, Finkelstein JL, Stewart AM, Kenneth J, Polhemus ME, Endy TP, Cardenas W, and Mehta S

Subjects

Chromium administration & dosage, Dengue Virus, Dietary Supplements, Disease Progression, Humans, Iron, Dietary administration & dosage, Observational Studies as Topic, Randomized Controlled Trials as Topic, Vitamin A administration & dosage, Vitamin D administration & dosage, Vitamin E administration & dosage, Zinc administration & dosage, Dengue drug therapy, Dengue prevention & control, Micronutrients administration & dosage, Micronutrients deficiency

Abstract

Dengue virus infection is the most widespread mosquito-borne viral infection in humans and has emerged as a serious global health challenge. In the absence of effective treatment and vaccine, host factors including nutritional status, which may alter disease progression, need investigation. The interplay between nutrition and other infections is well-established, and modulation of nutritional status often presents a simple low-cost method of interrupting transmission, reducing susceptibility, and/or ameliorating disease severity. This review examines the evidence on the role of micronutrients in dengue virus infection. We found critical issues and often inconsistent results across studies; this finding along with the lack of sufficient literature in this field have limited our ability to make any recommendations. However, vitamins D and E have shown promise in small supplementation trials. In summary, the role of micronutrients in dengue virus infection is an exciting research area and needs to be examined in well-designed studies with larger samples., (© The American Society of Tropical Medicine and Hygiene.)

Published

2014

12. Evaluation of immune responses to a Plasmodium vivax CSP-based recombinant protein vaccine candidate in combination with second-generation adjuvants in mice.

Author

Lumsden JM, Nurmukhambetova S, Klein JH, Sattabongkot J, Bennett JW, Bertholet S, Fox CB, Reed SG, Ockenhouse CF, Howard RF, Polhemus ME, and Yadava A

Subjects

Animals, Antibodies, Protozoan blood, CD4-Positive T-Lymphocytes immunology, Emulsions administration & dosage, Enzyme-Linked Immunosorbent Assay, Female, Fluorescent Antibody Technique, Indirect, Immunoglobulin G blood, Injections, Subcutaneous, Interferon-gamma metabolism, Interleukin-2 metabolism, Malaria Vaccines administration & dosage, Mice, Mice, Inbred C57BL, Protozoan Proteins genetics, Recombinant Proteins genetics, Recombinant Proteins immunology, Tumor Necrosis Factor-alpha metabolism, Vaccines, Synthetic administration & dosage, Vaccines, Synthetic immunology, Adjuvants, Immunologic administration & dosage, Malaria Vaccines immunology, Plasmodium vivax immunology, Protozoan Proteins immunology

Abstract

Plasmodium vivax is the major cause of malaria outside of sub-Saharan Africa and causes morbidity and results in significant economic impact in developing countries. In order to produce a P. vivax vaccine for global use, we have previously reported the development of VMP001, based on the circumsporozoite protein (CSP) of P. vivax. Our interest is to evaluate second-generation vaccine formulations to identify novel combinations of adjuvants capable of inducing strong, long-lasting immune responses. In this study, groups of C57BL/6J mice were immunized subcutaneously three times with VMP001 emulsified with synthetic TLR4 (GLA) or TLR7/8 (R848) agonist in stable emulsion (SE), a combination of the TLR4 and TLR7/8 agonists, or SE alone. Sera and splenocytes were tested for the presence of antigen-specific humoral and cellular responses, respectively. All groups of mice generated high titers of anti-P. vivax IgG antibodies as detected by ELISA and immunofluorescence assay. GLA-SE promoted a shift in the antibody response to a Th1 profile, as demonstrated by the change in IgG2c/IgG1 ratio. In addition, GLA-SE induced a strong cellular immune response characterized by multi-functional, antigen-specific CD4(+) T cells secreting IL-2, TNF and IFN-γ. In contrast, mice immunized with SE or R848-SE produced low numbers of antigen-specific CD4(+) T cells, and these T cells secreted IL-2 and TNF, but not IFN-γ. Finally, R848-SE did not enhance the immune response compared to GLA-SE alone. Based on these results, we conclude that the combination of VMP001 and GLA-SE is highly immunogenic in mice and may serve as a potential second-generation vaccine candidate against vivax malaria., (Published by Elsevier Ltd.)

Published

2012

13. Antigen-displaying lipid-enveloped PLGA nanoparticles as delivery agents for a Plasmodium vivax malaria vaccine.

Author

Moon JJ, Suh H, Polhemus ME, Ockenhouse CF, Yadava A, and Irvine DJ

Subjects

Animals, Malaria Vaccines chemistry, Mice, Polylactic Acid-Polyglycolic Acid Copolymer, Sporozoites immunology, Lactic Acid chemistry, Malaria Vaccines administration & dosage, Malaria, Vivax prevention & control, Nanoparticles chemistry, Plasmodium vivax immunology, Polyglycolic Acid chemistry

Abstract

The parasite Plasmodium vivax is the most frequent cause of malaria outside of sub-Saharan Africa, but efforts to develop viable vaccines against P. vivax so far have been inadequate. We recently developed pathogen-mimicking polymeric vaccine nanoparticles composed of the FDA-approved biodegradable polymer poly(lactide-co-glycolide) acid (PLGA) "enveloped" by a lipid membrane. In this study, we sought to determine whether this vaccine delivery platform could be applied to enhance the immune response against P. vivax sporozoites. A candidate malaria antigen, VMP001, was conjugated to the lipid membrane of the particles, and an immunostimulatory molecule, monophosphoryl lipid A (MPLA), was incorporated into the lipid membranes, creating pathogen-mimicking nanoparticle vaccines (VMP001-NPs). Vaccination with VMP001-NPs promoted germinal center formation and elicited durable antigen-specific antibodies with significantly higher titers and more balanced Th1/Th2 responses in vivo, compared with vaccines composed of soluble protein mixed with MPLA. Antibodies raised by NP vaccinations also exhibited enhanced avidity and affinity toward the domains within the circumsporozoite protein implicated in protection and were able to agglutinate live P. vivax sporozoites. These results demonstrate that these VMP001-NPs are promising vaccines candidates that may elicit protective immunity against P. vivax sporozoites.

Published

2012

14. Evaluation of the safety and immunogenicity in rhesus monkeys of a recombinant malaria vaccine for Plasmodium vivax with a synthetic Toll-like receptor 4 agonist formulated in an emulsion.

Author

Lumsden JM, Pichyangkul S, Srichairatanakul U, Yongvanitchit K, Limsalakpetch A, Nurmukhambetova S, Klein J, Bertholet S, Vedvick TS, Reed SG, Sattabongkot J, Bennett JW, Polhemus ME, Ockenhouse CF, Howard RF, and Yadava A

Subjects

Adjuvants, Immunologic, Animals, Antigens, Protozoan immunology, CD4-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes, Emulsions, Enzyme-Linked Immunosorbent Assay, Fluorescent Antibody Technique, Immunoglobulin G blood, Interferon-gamma biosynthesis, Interleukin-2 biosynthesis, Interleukin-2 metabolism, Lipid A immunology, Macaca mulatta, Malaria, Vivax immunology, Protozoan Proteins immunology, Toll-Like Receptor 4 immunology, Tumor Necrosis Factor-alpha biosynthesis, Vaccines, Synthetic immunology, Malaria Vaccines immunology, Malaria, Vivax prevention & control, Plasmodium vivax immunology, Toll-Like Receptor 4 agonists

Abstract

Plasmodium vivax is the major cause of malaria outside sub-Saharan Africa and inflicts debilitating morbidity and consequent economic impacts in developing countries. In order to produce a P. vivax vaccine for global use, we have previously reported the development of a novel chimeric recombinant protein, VMP001, based on the circumsporozoite protein (CSP) of P. vivax. Very few adjuvant formulations are currently available for human use. Our interest is to evaluate second-generation vaccine formulations to identify novel combinations of adjuvants capable of inducing strong, long-lasting immune responses. In this study rhesus monkeys were immunized intramuscularly three times with VMP001 in combination with a stable emulsion (SE) or a synthetic Toll-like receptor 4 (TLR4) agonist (glucopyranosyl lipid A [GLA]) in SE (GLA-SE). Sera and peripheral blood mononuclear cells (PBMCs) were tested for the presence of antigen-specific humoral and cellular responses, respectively. All groups of monkeys generated high titers of anti-P. vivax IgG antibodies, as detected by enzyme-linked immunosorbent assays (ELISAs) and immunofluorescence assays. In addition, all groups generated a cellular immune response characterized by antigen-specific CD4(+) T cells secreting predominantly interleukin-2 (IL-2) and lesser amounts of tumor necrosis factor (TNF). We conclude that the combination of VMP001 and GLA-SE is safe and immunogenic in monkeys and may serve as a potential second-generation vaccine candidate against P. vivax malaria.

Published

2011

15. 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 JN, Gerlach J, Afonina I, Anyona SB, Koros JN, Siangla J, Ankoudinova I, Singhal M, Watts K, Polhemus ME, Vermeulen NM, Mahoney W, Steele M, and Domingo GJ

Subjects

Child, Child, Preschool, Cross-Sectional Studies, Female, Fructose-Bisphosphate Aldolase immunology, Humans, Immunoenzyme Techniques, Kenya epidemiology, Malaria, Falciparum transmission, Male, Microscopy, Plasmodium falciparum genetics, Plasmodium falciparum immunology, Prevalence, RNA, Protozoan isolation & purification, Real-Time Polymerase Chain Reaction, Reverse Transcriptase Polymerase Chain Reaction, Antigens, Protozoan isolation & purification, DNA, Protozoan isolation & purification, Endemic Diseases, Malaria, Falciparum diagnosis, Malaria, Falciparum epidemiology, Nucleic Acid Amplification Techniques, Parasite Egg Count, Plasmodium falciparum isolation & purification, Protozoan Proteins isolation & purification

Abstract

Objectives: To determine the malaria prevalence by microscopy, antigen detection and nucleic acid detection in a defined subpopulation in a Plasmodium falciparum-endemic region during the peak transmission season., Methods: Blood specimens were collected in a cross-sectional study involving children aged 5-10 years (n = 195) presenting with acute fever to two clinics in Western Kenya. All specimens underwent microscopy, HRP2 and aldolase antigen detection by enzyme immunoassay (EIA), parasite-specific DNA and total nucleic acid (RNA and DNA) by real-time PCR (qPCR) and reverse-transcriptase PCR (qRT-PCR)., Results: Microscopy detected 65/195 cases of malaria infection [95% confidence interval (CI) 52-78]. HRP2 and aldolase EIA had similar sensitivity levels detecting antigen in 65/195 (95% CI, 52-78) and 57/195 (95% CI, 45-70) cases. Discordants in antigen detection vs. microscopy occurred at <470 parasites/μl and <4900 parasites/μl for HRP2 and aldolase, respectively. Detection of total nucleic acid allowed a 3 log lower limit of detection than just DNA detection by real-time PCR in vitro. In clinical specimens, 114/195 (95% CI, 100-127) were qPCR positive (DNA), and 187/195 (95% CI, 179-191) were qRT-PCR positive (DNA plus RNA)., Conclusions: The prevalence of submicroscopic malaria infection was significantly higher when detecting total nucleic acid than just DNA in this outpatient population during the high transmission season. Defining standards for submicroscopic infection will be important for control programmes, diagnostics development efforts and molecular epidemiology studies., (© 2011 Blackwell Publishing Ltd.)

Published

2011

16. Antimalarial drug sensitivity profile of western Kenya Plasmodium falciparum field isolates determined by a SYBR Green I in vitro assay and molecular analysis.

Author

Akala HM, Eyase FL, Cheruiyot AC, Omondi AA, Ogutu BR, Waters NC, Johnson JD, Polhemus ME, Schnabel DC, and Walsh DS

Subjects

Adolescent, Adult, Animals, Child, Child, Preschool, Follow-Up Studies, Humans, Infant, Kenya, Antimalarials pharmacology, Plasmodium falciparum drug effects

Abstract

In vitro drug sensitivity and molecular analyses of Plasmodium falciparum track drug resistance. DNA-binding fluorescent dyes like SYBR Green I may allow field laboratories, proximal to P. falciparum collection sites, to conduct drug assays. In 2007-2008, we assayed 121 P. falciparum field isolates from western Kenya for 50% inhibitory concentrations (IC(50)) against 6 antimalarial drugs using a SYBR Green I in vitro assay: 91 immediate ex vivo (IEV) and 30 culture-adapted, along with P. falciparum reference clones D6 (chloroquine [CQ] sensitive) and W2 (CQ resistant). We also assessed P. falciparum mdr1 (Pfmdr1) copy number and single nucleotide polymorphisms (SNPs) at four codons. The IC(50)s for IEV and culture-adapted P. falciparum isolates were similar, and approximated historical IC(50)s. For Pfmdr1, mean copy number was 1, with SNPs common at codons 86 and 184. The SYBR Green I assay adapted well to our field-based laboratory, for both IEV and culture-adapted P. falciparum, warranting continued use.

Published

2011

17. Outpatient upper respiratory tract viral infections in children with malaria symptoms in Western Kenya.

Author

Waitumbi JN, Kuypers J, Anyona SB, Koros JN, Polhemus ME, Gerlach J, Steele M, Englund JA, Neuzil KM, and Domingo GJ

Subjects

Child, Child, Preschool, Cohort Studies, Cross-Sectional Studies, Female, Humans, Kenya epidemiology, Malaria complications, Malaria epidemiology, Male, Outpatients, Respiratory Tract Infections complications, Respiratory Tract Infections epidemiology, Virus Diseases epidemiology, Virus Diseases virology, Virus Shedding, Malaria diagnosis, Respiratory Tract Infections diagnosis, Respiratory Tract Infections virology, Virus Diseases diagnosis

Abstract

A cross-sectional study was performed in children 5 through 10 years of age presenting to outpatient clinics in Nyanza Province, Kenya, in which nasal swab and blood specimens were collected during the high malaria transmission season. Patients presenting with malaria-like symptoms within 4 days of fever onset were enrolled in the study. Plasmodium parasitemia was determined by blood smear microscopy. Nasal swabs were screened for a panel of respiratory viruses by polymerase chain reaction. Influenza A, rhinoviruses, and other respiratory viruses were detected in 18%, 26%, and 12% of 197 specimens, respectively. Four of 36 patients with influenza A had a positive malaria blood slide, compared with 20 of 52 patients with rhinovirus. A significant burden of disease caused by influenza A in febrile children during the study period was observed, highlighting the need for further research into the burden of influenza disease in regions where malaria is holoendemic.

Published

2010

18. Evaluation of recurrent parasitemia after artemether-lumefantrine treatment for uncomplicated malaria in children in western Kenya.

Author

Woodring JV, Ogutu B, Schnabel D, Waitumbi JN, Olsen CH, Walsh DS, Heppner DG Jr, and Polhemus ME

Subjects

Animals, Antimalarials administration & dosage, Artemether, Lumefantrine Drug Combination, Child, Preschool, Drug Combinations, Humans, Infant, Kenya, Malaria blood, Malaria parasitology, Malaria Vaccines administration & dosage, Plasmodium classification, Plasmodium isolation & purification, Recurrence, Antimalarials therapeutic use, Artemisinins therapeutic use, Ethanolamines therapeutic use, Fluorenes therapeutic use, Malaria drug therapy

Abstract

From April 2005 to April 2006, a phase 2 malaria vaccine trial in Kenya enrolled 400 children aged 12-47 months. Each received mixed supervised and unsupervised artemether-lumefantrine for uncomplicated malaria, using a standard six-dose regimen, by weight. Children were followed for detection of parasitemia and clinical malaria. A median of two negative malaria blood films occurred during every recurrent parasitemia (RP) episode, suggesting reinfection over late recrudescence. Median time to RP after starting artemether-lumefantrine was 37 days (36-38). Of 2,020 evaluable artemether-lumefantrine treatments, there were no RPs in 99% by day 14, 71% by day 28, and 41% by day 42. By World Health Organization standards, 71% of treatment courses had adequate responses. Although recrudescence in some cannot be ruled out, our cohort had a shorter median time to RP compared with other artemether-lumefantrine treatment studies. This underscores patient counseling on completing all treatment doses for optimal protection from RP.

Published

2010

19. Recombinant Liver Stage Antigen-1 (LSA-1) formulated with AS01 or AS02 is safe, elicits high titer antibody and induces IFN-gamma/IL-2 CD4+ T cells but does not protect against experimental Plasmodium falciparum infection.

Author

Cummings JF, Spring MD, Schwenk RJ, Ockenhouse CF, Kester KE, Polhemus ME, Walsh DS, Yoon IK, Prosperi C, Juompan LY, Lanar DE, Krzych U, Hall BT, Ware LA, Stewart VA, Williams J, Dowler M, Nielsen RK, Hillier CJ, Giersing BK, Dubovsky F, Malkin E, Tucker K, Dubois MC, Cohen JD, Ballou WR, and Heppner DG Jr

Subjects

Adjuvants, Immunologic pharmacology, Adult, Antibodies, Protozoan blood, Antibody Formation, Female, Humans, Immunity, Cellular, Immunity, Humoral, Immunization Schedule, Immunization, Secondary, Interferon-gamma immunology, Interleukin-2 immunology, Malaria Vaccines administration & dosage, Malaria Vaccines adverse effects, Malaria, Falciparum immunology, Male, Parasitemia immunology, Plasmodium falciparum immunology, Recombinant Proteins immunology, Sporozoites immunology, Young Adult, Antigens, Protozoan immunology, CD4-Positive T-Lymphocytes immunology, Malaria Vaccines immunology, Malaria, Falciparum prevention & control

Abstract

Plasmodium falciparum Liver Stage Antigen 1 (LSA-1) is a pre-erythrocytic stage antigen. Our LSA-1 vaccine candidate is a recombinant protein with full-length C- and N-terminal flanking domains and two of the 17 amino acid repeats from the central repeat region termed "LSA-NRC." We describe the first Phase I/II study of this recombinant LSA-NRC protein formulated with either the AS01 or AS02 adjuvant system. We conducted an open-label Phase I/II study. Thirty-six healthy malaria-naïve adults received one of four formulations by intra-deltoid injection on a 0 and 1 month schedule; low dose (LD) LSA-NRC/AS01:10microg LSA-NRC/0.5ml AS01 (n=5), high dose (HD) LSA-NRC/AS01: 50microg LSA-NRC/0.5ml AS01 (n=13); LD LSA-NRC/AS02: 10microg LSA-NRC/0.5ml AS02 (n=5) and HD LSA-NRC/AS02: 50microg LSA-NRC/0.5ml AS02 (n=13). Two weeks post-second immunization, the high dose vaccinees and 6 non-immunized infectivity controls underwent experimental malaria sporozoite challenge. The vaccines showed a reassuring safety profile but were moderately reactogenic. There were no serious adverse events. All subjects seroconverted after the first immunization. Following the second immunization, LSA-1-specific CD4+ T cells producing two cytokines (IL-2 and IFN-gamma) were found by intra-cellular staining in all subjects in the LD LSA-NRC/AS01B group and in 3 of 5 subjects in the LD LSA-NRC/AS02 group. In contrast, the HD LSA-NRC/AS01 and HD LSA-NRC/AS02 group subjects had fewer LSA-1-specific CD4+ T cells, and minimal to no IFN-gamma responses. There was no increase in LSA-1-specific CD8+ T cells found in any group. Per protocol, 22 high dose vaccinees, but no low dose vaccinees, underwent P. falciparum homologous malaria challenge (3D7 clone). All vaccinees became parasitemic and there was no delay in their pre-patent period versus controls (p=0.95). LSA-NRC/AS01 and LSA-NRC/AS02 elicited antigen-specific antibody and CD4+ T cell responses, but elicited no protective immunity. Although the optimal antigen dose of LSA-NRC may not have been selected for the challenge portion of the protocol, further vaccine development based upon LSA-1 should not be excluded and should include alternative vaccine platforms able to elicit additional effector mechanisms such as CD8+ T cells., (Copyright 2009. Published by Elsevier Ltd.)

Published

2010

20. A randomized controlled trial of local heat therapy versus intravenous sodium stibogluconate for the treatment of cutaneous Leishmania major infection.

Author

Aronson NE, Wortmann GW, Byrne WR, Howard RS, Bernstein WB, Marovich MA, Polhemus ME, Yoon IK, Hummer KA, Gasser RA Jr, Oster CN, and Benson PM

Subjects

Adolescent, Adult, Animals, Antimony Sodium Gluconate administration & dosage, Drug-Related Side Effects and Adverse Reactions, Female, Humans, Injections, Intravenous, Male, Middle Aged, Treatment Outcome, Young Adult, Antimony Sodium Gluconate therapeutic use, Hyperthermia, Induced, Leishmania major drug effects, Leishmania major radiation effects, Leishmaniasis, Cutaneous drug therapy, Leishmaniasis, Cutaneous therapy

Abstract

Background: Cutaneous Leishmania major has affected many travelers including military personnel in Iraq and Afghanistan. Optimal treatment for this localized infection has not been defined, but interestingly the parasite is thermosensitive., Methodology/principal Findings: Participants with parasitologically confirmed L. major infection were randomized to receive intravenous sodium stibogluconate (SSG) 20mg/kg/day for ten doses or localized ThermoMed (TM) device heat treatment (applied at 50 degrees C for 30 seconds) in one session. Those with facial lesions, infection with other species of Leishmania, or more than 20 lesions were excluded. Primary outcome was complete re-epithelialization or visual healing at two months without relapse over 12 months. Fifty-four/56 enrolled participants received intervention, 27 SSG and 27 TM. In an intent to treat analysis the per subject efficacy at two months with 12 months follow-up was 54% SSG and 48% TM (p = 0.78), and the per lesion efficacy was 59% SSG and 73% TM (p = 0.053). Reversible abdominal pain/pancreatitis, arthralgias, myalgias, headache, fatigue, mild cytopenias, and elevated transaminases were more commonly present in the SSG treated participants, whereas blistering, oozing, and erythema were more common in the TM arm., Conclusions/significance: Skin lesions due to L. major treated with heat delivered by the ThermoMed device healed at a similar rate and with less associated systemic toxicity than lesions treated with intravenous SSG., Clinical Trial Registration: ClinicalTrials.gov NCT 00884377.

Published

2010

21. Impact of RTS,S/AS02(A) and RTS,S/AS01(B) on genotypes of P. falciparum in adults participating in a malaria vaccine clinical trial.

Author

Waitumbi JN, Anyona SB, Hunja CW, Kifude CM, Polhemus ME, Walsh DS, Ockenhouse CF, Heppner DG, Leach A, Lievens M, Ballou WR, Cohen JD, and Sutherland CJ

Subjects

Adolescent, Adult, Alleles, Epitopes, T-Lymphocyte chemistry, Female, Genotype, Haplotypes, Humans, Male, Polymorphism, Genetic, Sequence Analysis, DNA, Malaria parasitology, Malaria prevention & control, Malaria Vaccines therapeutic use, Plasmodium falciparum genetics, Plasmodium falciparum metabolism

Abstract

Objective: RTS,S, a candidate vaccine for malaria, is a recombinant protein expressed in yeast containing part of the circumsporozoite protein (CSP) sequence of 3D7 strain of Plasmodium falciparum linked to the hepatitis B surface antigen in a hybrid protein. The RTS,S antigen is formulated with GSK Biologicals' proprietary Adjuvant Systems AS02(A) or AS01(B). A recent trial of the RTS,S/AS02(A) and RTS,S/AS01(B) vaccines evaluated safety, immunogenicity and impact on the development of parasitemia of the two formulations. Parasite isolates from this study were used to determine the molecular impact of RTS,S/AS02(A) and RTS,S/AS01(B) on the multiplicity of infection (MOI) and the csp allelic characteristics of subsequent parasitemias., Design: The distribution of csp sequences and the MOI of the infecting strains were examined at baseline and in break-through infections from vaccinated individuals and from those receiving a non-malarial vaccine., Setting: The study was conducted in Kombewa District, western Kenya., Participants: Semi-immune adults from the three study arms provided isolates at baseline and during break-through infections., Outcome: Parasite isolates used for determining MOI and divergence of csp T cell-epitopes were 191 at baseline and 87 from break-through infections., Results: Grouping recipients of RTS,S/AS01(A) and RTS,S/AS02(B) together, vaccine recipients identified as parasite-positive by microscopy contained significantly fewer parasite genotypes than recipients of the rabies vaccine comparator (median in pooled RTS,S groups: 3 versus 4 in controls, P = 0.0313). When analyzed separately, parasitaemic individuals in the RTS,S/AS01(B) group, but not the RTS,S/AS02(A) group, were found to have significantly fewer genotypes than the comparator group. Two individual amino acids found in the vaccine construct (Q339 in Th2R and D371 in Th3R) were observed to differ in incidence between vaccine and comparator groups but in different directions; parasites harboring Q339 were less common among pooled RTS,S/AS vaccine recipients than among recipients of rabies vaccine, whereas parasites with D371 were more common among the RTS,S/AS groups., Conclusions: It is concluded that both RTS,S/AS vaccines reduce multiplicity of infection. Our results do not support the hypothesis that RTS,S/AS vaccines elicit preferential effects against pfcsp alleles with sequence similarity to the 3D7 pfcsp sequence employed in the vaccine construct.

Published

2009

22. Evaluation of RTS,S/AS02A and RTS,S/AS01B in adults in a high malaria transmission area.

Author

Polhemus ME, Remich SA, Ogutu BR, Waitumbi JN, Otieno L, Apollo S, Cummings JF, Kester KE, Ockenhouse CF, Stewart A, Ofori-Anyinam O, Ramboer I, Cahill CP, Lievens M, Dubois MC, Demoitie MA, Leach A, Cohen J, Ballou WR, and Heppner DG Jr

Subjects

Adult, Double-Blind Method, Follow-Up Studies, Humans, Kenya epidemiology, Malaria epidemiology, Malaria Vaccines adverse effects, Single-Blind Method, Treatment Outcome, Malaria prevention & control, Malaria Vaccines therapeutic use

Abstract

Background: This study advances the clinical development of the RTS,S/AS01B candidate malaria vaccine to malaria endemic populations. As a primary objective it compares the safety and reactogenicity of RTS,S/AS01B to the more extensively evaluated RTS,S/AS02A vaccine., Methodology: A Phase IIb, single centre, double-blind, controlled trial of 6 months duration with a subsequent 6 month single-blind follow-up conducted in Kisumu West District, Kenya between August 2005 and August 2006. 255 healthy adults aged 18 to 35 years were randomized (1ratio1ratio1) to receive 3 doses of RTS,S/AS02A, RTS,S/AS01B or rabies vaccine (Rabipur; Chiron Behring GmbH) at months 0, 1, 2. The primary objective was the occurrence of severe (grade 3) solicited or unsolicited general (i.e. systemic) adverse events (AEs) during 7 days follow up after each vaccination., Principal Findings: Both candidate vaccines had a good safety profile and were well tolerated. One grade 3 systemic AE occurred within 7 days of vaccination (RTS,S/AS01B group). No unsolicited AEs or SAEs were related to vaccine. A marked increase in anti-CS antibody GMTs was observed post Dose 2 of both RTS,S/AS01B (31.6 EU/mL [95% CI: 23.9 to 41.6]) and RTS,S/AS02A (16.7 EU/mL [95% CI: 12.9 to 21.7]). A further increase was observed post Dose 3 in both the RTS,S/AS01B (41.4 EU/mL [95% CI: 31.7 to 54.2]) and RTS,S/AS02A (21.4 EU/mL [95% CI: 16.0 to 28.7]) groups. Anti-CS antibody GMTs were significantly greater with RTS,S/AS01B compared to RTS,S/AS02A at all time points post Dose 2 and Dose 3. Both candidate vaccines produced strong anti-HBs responses. Vaccine efficacy in the RTS,S/AS01B group was 29.5% (95% CI: -15.4 to 56.9, p = 0.164) and in the RTS,S/AS02A group 31.7% (95% CI: -11.6 to 58.2, p = 0.128)., Conclusions: Both candidate malaria vaccines were well tolerated over a 12 month surveillance period. A more favorable immunogenicity profile was observed with RTS,S/AS01B than with RTS,S/AS02A., Trial Registration: Clinicaltrials.gov NCT00197054.

Published

2009

23. Bullous erythema multiforme after treatment with Malarone, a combination antimalarial composed of atovaquone and proguanil hydrochloride.

Author

Remich SA, Otieno W, Polhemus ME, Ogutu B, and Walsh DS

Subjects

Antimalarials administration & dosage, Atovaquone administration & dosage, Drug Combinations, Female, Humans, Kenya, Malaria, Falciparum parasitology, Middle Aged, Proguanil administration & dosage, Antimalarials adverse effects, Atovaquone adverse effects, Erythema Multiforme etiology, Malaria, Falciparum drug therapy, Proguanil adverse effects

Abstract

We report on a Kenyan woman who developed bullous erythema multiforme, in association with Malarone treatment.

Published

2008

24. Malaria treatment with atovaquone-proguanil in malaria-immune adults: implications for malaria intervention trials and for pre-exposure prophylaxis of malaria.

Author

Polhemus ME, Remich S, Ogutu B, Waitumbi J, Lievens M, Ballou WR, and Heppner DG Jr

Subjects

Adolescent, Adult, Animals, Chemoprevention, Humans, Kaplan-Meier Estimate, Kenya, Malaria Vaccines administration & dosage, Plasmodium falciparum drug effects, Plasmodium falciparum immunology, Time Factors, Antimalarials therapeutic use, Atovaquone therapeutic use, Malaria, Falciparum drug therapy, Malaria, Falciparum immunology, Malaria, Falciparum parasitology, Malaria, Falciparum prevention & control, Parasitemia drug therapy, Parasitemia immunology, Parasitemia parasitology, Proguanil therapeutic use

Abstract

Eighty adults in areas of Kenya where malaria is holoendemic received presumptive treatment with atovaquone-proguanil and were followed closely. The time to the first Plasmodium falciparum parasitemia was 32 days. This prolonged prophylaxis period has implications for study design when used in malaria intervention trials and cautiously suggests clinical investigation of potential preexposure prophylaxis of malaria.

Published

2008

25. Persistence of vaccinia at the site of smallpox vaccination.

Author

Cummings JF, Polhemus ME, Hawkes C, Klote M, Ludwig GV, and Wortmann G

Subjects

Humans, Prospective Studies, Smallpox virology, Smallpox Vaccine administration & dosage, Smallpox Vaccine adverse effects, Vaccinia virus immunology, Vaccinia virus metabolism, Smallpox prevention & control, Smallpox Vaccine pharmacokinetics, Vaccinia virus isolation & purification

Abstract

Persistence of vaccinia at vaccination sites may help determine the risk associated with secondary transmission. Culture, PCR, and antigen detection were performed on serial vaccination site swab specimens. On day 21 after vaccination, 37% of volunteers were culture positive, most of whom had received vaccine for the first time. Vaccinia is detectable at least through day 21 after vaccination.

Published

2008

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

Author

Waitumbi JN, Kifude CM, Withers MR, Polhemus ME, Heppner DG Jr, and Ogutu BR

Subjects

Base Sequence, Chromatography, High Pressure Liquid, Genotype, Globins genetics, Humans, Molecular Sequence Data, Phenotype, Hemoglobins, Abnormal genetics, Hemoglobins, Abnormal metabolism

Published

2007

27. 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 ME, Magill AJ, Cummings JF, Kester KE, Ockenhouse CF, Lanar DE, Dutta S, Barbosa A, Soisson L, Diggs CL, Robinson SA, Haynes JD, Stewart VA, Ware LA, Brando C, Krzych U, Bowden RA, Cohen JD, Dubois MC, Ofori-Anyinam O, De-Kock E, Ballou WR, and Heppner DG Jr

Subjects

Adjuvants, Immunologic, Adolescent, Adult, Animals, Antibodies, Protozoan blood, Cell Line, Cell Proliferation, Cells, Cultured, Cricetinae, Drug Combinations, Enzyme-Linked Immunosorbent Assay, Escherichia coli genetics, Female, Fluorescent Antibody Technique, Indirect, Headache, Humans, Immunization, Secondary, Interferon-gamma biosynthesis, Interleukin-5 biosynthesis, Leukocytes, Mononuclear immunology, Lipid A immunology, Malaria Vaccines administration & dosage, Male, Merozoites immunology, Mesocricetus, Middle Aged, Pain, Plasmodium falciparum growth & development, Sporozoites immunology, Vaccines, Synthetic immunology, Antigens, Protozoan immunology, Lipid A analogs & derivatives, Malaria Vaccines adverse effects, Malaria Vaccines immunology, Membrane Proteins immunology, Plasmodium falciparum immunology, Protozoan Proteins immunology, Saponins immunology

Abstract

We report the first safety and immunogenicity trial of the Plasmodium falciparum vaccine candidate FMP2.1/AS02A, a recombinant E. coli-expressed protein based upon the apical membrane antigen-1 (AMA-1) of the 3D7 clone formulated with the AS02A adjuvant. We conducted an open-label, staggered-start, dose-escalating Phase I trial in 23 malaria-naïve volunteers who received 8, 20 or 40microg of FMP2.1 in a fixed volume of 0.5mL of AS02A on a 0, 1, and 2 month schedule. Nineteen of 23 volunteers received all three scheduled immunizations. The most frequent solicited local and systemic adverse events associated with immunization were injection site pain (68%) and headache (29%). There were no significant laboratory abnormalities or vaccine-related serious adverse events. All volunteers seroconverted after second immunization as determined by ELISA. Immune sera recognized sporozoites and merozoites by immunofluorescence assay (IFA), and exhibited both growth inhibition and processing inhibition activity against homologous (3D7) asexual stage parasites. Post-immunization, peripheral blood mononuculear cells exhibited FMP2.1-specific lymphoproliferation and IFN-gamma and IL-5 ELISPOT assay responses. This is the first PfAMA-1-based vaccine shown to elicit both potent humoral and cellular immunity in humans. Encouraged by the potential of FMP1/AS02A to target host immunity against PfAMA-1 that is known to be expressed by sporozoite, hepatic and erythrocytic stages, we have initiated field trials of FMP2.1/AS02A in an endemic population in the Republic of Mali.

Published

2007

28. Hb Kenya among Luo adults and young children in malaria holoendemic Western Kenya: screened by high performance liquid chromatography and confirmed by polymerase chain reaction.

Author

Kifude CM, Polhemus ME, Heppner DG Jr, Withers MR, Ogutu BR, and Waitumbi JN

Subjects

Adolescent, Adult, Child, Preschool, Chromatography, High Pressure Liquid, Cohort Studies, Endemic Diseases, Female, Humans, Infant, Kenya epidemiology, Male, Polymerase Chain Reaction, Fetal Hemoglobin analysis, Hemoglobin A2 analysis, Hemoglobinopathies diagnosis, Hemoglobins, Abnormal analysis, Malaria epidemiology

Abstract

Hb Kenya, a fusion hemoglobin (Hb) resulting from a crossover between the (A)gamma- and beta-globin genes, is accompanied by an increased level of fetal Hb (Hb F) in adult life. This study describes the use of cation exchange high performance liquid chromatography (HPLC) in the identification of Hb Kenya and of a polymerase chain reaction (PCR) method for confirmatory diagnosis. Data came from 584 children and 406 adults who were screened for eligibility for malaria vaccine trials at Kombewa, Western Kenya. Sixteen subjects (13 children and three adults) had elevated Hb F (5.0-28.4%; normal <5.0%). Of these, 11 had an apparent markedly elevated Hb A(2) (9.2-22.9%) and were confirmed by gap-PCR as having the 22.7 kb deletion characteristic of Hb Kenya. Of the five cases with elevated Hb F but normal A(2), none had Hb Kenya. We propose that in this population, the finding by cation exchange HPLC of an elevated Hb F (>9.0%) and of an apparently increased Hb A(2) (>9.2%), may suggest the presence of Hb Kenya. However, given the inability of differentiating Hb Kenya from a truly elevated Hb A(2) by routine cation exchange HPLC, it is imperative to confirm the Hb Kenya mutation by gap-PCR.

Published

2007

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

Author

Heppner DG Jr, Kester KE, Ockenhouse CF, Tornieporth N, Ofori O, Lyon JA, Stewart VA, Dubois P, Lanar DE, Krzych U, Moris P, Angov E, Cummings JF, Leach A, Hall BT, Dutta S, Schwenk R, Hillier C, Barbosa A, Ware LA, Nair L, Darko CA, Withers MR, Ogutu B, Polhemus ME, Fukuda M, Pichyangkul S, Gettyacamin M, Diggs C, Soisson L, Milman J, Dubois MC, Garçon N, Tucker K, Wittes J, Plowe CV, Thera MA, Duombo OK, Pau MG, Goudsmit J, Ballou WR, and Cohen J

Subjects

Academies and Institutes, Adenoviridae genetics, Animals, Antigens, Protozoan genetics, Antigens, Protozoan immunology, Antigens, Protozoan isolation & purification, Clinical Trials as Topic, Genetic Vectors, Humans, Malaria Vaccines genetics, Malaria Vaccines immunology, Malaria Vaccines pharmacology, Malaria, Falciparum prevention & control, Membrane Proteins genetics, Membrane Proteins immunology, Merozoite Surface Protein 1 genetics, Merozoite Surface Protein 1 immunology, Plasmodium falciparum genetics, Protozoan Proteins genetics, Protozoan Proteins immunology, United States, Malaria Vaccines isolation & purification, Plasmodium falciparum immunology

Abstract

The goal of the Malaria Vaccine Program at the Walter Reed Army Institute of Research (WRAIR) is to develop a licensed multi-antigen, multi-stage vaccine against Plasmodium falciparum able to prevent all symptomatic manifestations of malaria by preventing parasitemia. A secondary goal is to limit disease in vaccinees that do develop malaria. Malaria prevention will be achieved by inducing humoral and cellular immunity against the pre-erythrocytic circumsporozoite protein (CSP) and the liver stage antigen-1 (LSA-1). The strategy to limit disease will target immune responses against one or more blood stage antigens, merozoite surface protein-1 (MSP-1) and apical merozoite antigen-1 (AMA-1). The induction of T- and B-cell memory to achieve a sustained vaccine response may additionally require immunization with an adenovirus vector such as adenovirus serotype 35. RTS,S, a CSP-derived antigen developed by GlaxoSmithKline Biologicals in collaboration with the Walter Reed Army Institute of Research over the past 17 years, is the cornerstone of our program. RTS,S formulated in AS02A (a GSK proprietary formulation) is the only vaccine candidate shown in field trials to prevent malaria and, in one instance, to limit disease severity. Our vaccine development plan requires proof of an individual antigen's efficacy in a Phase 2 laboratory challenge or field trial prior to its integration into an RTS,S-based, multi-antigen vaccine. Progress has been accelerated through extensive partnerships with industrial, academic, governmental, and non-governmental organizations. Recent safety, immunogenicity, and efficacy trials in the US and Africa are presented, as well as plans for the development of a multi-antigen vaccine.

Published

2005

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

Author

Polhemus ME, Aronson N, Weina P, McEvoy P, Neafi R, and Wortmann G

Subjects

Adult, Animals, Antimony Sodium Gluconate therapeutic use, Antiprotozoal Agents therapeutic use, Humans, Iraq, Leishmaniasis, Cutaneous drug therapy, Male, United States, Leishmania major, Leishmaniasis, Cutaneous diagnosis, Leishmaniasis, Cutaneous pathology, Military Personnel, Neck pathology

Published

2004

31. Effects of adjuvant radiotherapy for testicular cancer on CD4+ cell count in HIV-positive patients: a case report.

Author

Harshany ML and Polhemus ME

Subjects

Adult, CD4 Lymphocyte Count, HIV Infections immunology, Humans, Male, Radiotherapy, Adjuvant adverse effects, Seminoma complications, Testicular Neoplasms complications, CD4-Positive T-Lymphocytes radiation effects, HIV Infections complications, Seminoma radiotherapy, Testicular Neoplasms radiotherapy

Abstract

The occurrence of testicular seminoma is more frequent in HIV-positive than in HIV-negative men. Management involves orchiectomy and radiotherapy for early-stage seminoma. Radiotherapy is typically well tolerated, with minimal side effects. This Case Report presents an HIV-positive patient who experienced a decrease in CD4+ cell count and an alteration of his clinical HIV disease course following radiotherapy for seminoma.

Published

2004

32. Lack of vaccinia viremia after smallpox vaccination.

Author

Cummings JF, Polhemus ME, Hawkes C, Klote M, Ludwig GV, and Wortmann G

Subjects

Antigens, Viral analysis, Humans, Immunization Programs, Polymerase Chain Reaction, Vaccinia virus genetics, Viremia chemically induced, Smallpox Vaccine adverse effects, Vaccinia chemically induced, Vaccinia virus isolation & purification

Abstract

Although the transmission of certain viral infections (human immunodeficiency virus, hepatitis B and C viruses, and West Nile virus) through donated blood products is well described, the risk of transmitting vaccinia virus after smallpox vaccination is unknown. Blood samples from patients receiving the smallpox vaccine were obtained before vaccination; then from one-half of the study group on alternate days for each of the first 10 days after vaccination; then from all patients on days 14 and 21 after vaccination. Samples were analyzed by culture, polymerase chain reaction, and antigen detection (electrochemiluminescence) assay for the presence of vaccinia virus. Two hundred and twenty samples from 28 volunteers were processed by all 3 laboratory detection methods and all were negative for the presence of vaccinia virus (confidence interval, 0%-12.3%). Viremia with vaccinia virus after smallpox vaccination appears to be an uncommon occurrence.

Published

2004

33. Persistent nephrolithiasis after discontinuation of indinavir therapy.

Author

Polhemus ME and Aronson NE

Subjects

Adult, Anti-HIV Agents therapeutic use, HIV Infections drug therapy, Humans, Indinavir therapeutic use, Kidney Calculi chemically induced, Male, Protease Inhibitors therapeutic use, Anti-HIV Agents adverse effects, Indinavir adverse effects, Kidney Diseases chemically induced, Protease Inhibitors adverse effects

Published

1998