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5. Identifying merozoite targets of protective immunity against Plasmodium falciparum malaria

Author

Kamuyu, Gathoni

Subjects
616.9
Abstract

The observation that individuals living in malaria endemic regions who are repeatedly infected with P. falciparum can acquire immunity, first to severe, then to uncomplicated clinical episodes of malaria, and finally to high parasite densities, provides hope that a vaccine is achievable. Immunoglobulins have been identified as a key component of naturally acquired immunity and identifying the targets and mechanisms by which this protection is achieved is a clear research priority. To date, only a small proportion of the parasite proteome has been evaluated in the context of naturally acquired immunity. This thesis was aimed at contributing to this knowledge gap by identifying novel potential antigen targets of protective antibodies and validating these in samples from Tanzanian adults. First, to identify merozoite antigens that were immunogenic, I resolved proteins extracted from P. falciparum merozoites by two-dimensional gel electrophoresis and tested these for reactivity with immunoglobulins from malaria immune adults. Immunoreactive proteins were then identified by mass-spectrometry. In complementary studies, purified P. falciparum merozoites were treated with proteolytic enzymes to release proteins localised on the surface of merozoites, which were subsequently identified by mass-spectrometry. Using stringent criteria, where I combined the data obtained from 2D-immunoblots and surface-trypsinization experiments with bioinformatics prediction (for the presence of a signal peptide and/or transmembrane domain), I narrowed down to 222 potential merozoite vaccine targets. These included known surface and/or immunogenic proteins such as the 6-cysteine proteins (Pf12, Pf38, Pf41), MSP-1, 3, 7, 9, 10, GLURP, AMA1, GAMA, MTRAP, LSA3 and RhopH3 as well as many unstudied proteins. From the set of unstudied proteins, I prioritised 27 antigens for immunoprofiling and identified 19 antigens that are targets of naturally acquired antibodies and potential novel vaccine candidates. Next, using a cohort of adults living in a village in Tanzania that experiences hyperendemic malaria transmission throughout the year, I examined antibody responses to the novel potential vaccine candidates to test whether they were correlated with protective immunity. I began by identifying a panel of antigens that were immunogenic and elicited a stable antibody response in adults. Subsequently, I identified six antigens that were individually associated with protection from clinical episodes of malaria. Individuals who became ill during the follow-up period had significantly lower levels of these antibodies compared to those who did not. These antigens were the pantothenate transporter (PfPAT), a putative amino acid transporter (PF3D7_0629500), PF3D7_0830500, PF3D7_1025300, PF3D7_1345100 and PF3D7_1401600. In addition, the breadth of antibody responses to the tested antigens was associated with protection from clinical malaria. Finally, four of these six antigens strongly correlated with protective effector functions. Antibody responses to PfPAT were strongly correlated to both the ability to fix soluble factor C1q (C1q-fixation) to merozoites as well as with their interaction with neutrophils to release reactive species (ADRB). In addition, antibody responses to the putative amino acid transporter, PF3D7_1345100 and PF3D7_1401600 were strongly associated with C1q-fixation ability. Recruitment of the soluble factor C1q onto the surface of merozoite results in lysis via the classical complement pathway. The release of reactive oxygen species by neutrophils is thought to be toxic to the intra-erythrocytic stages of the parasites and is associated with parasite clearance. This thesis shows that 19 antigens, some of which have been studied for the first time in this work, are targets of naturally acquired antibody responses. Six of these antigens appeared to be associated with protective immunity to malaria in adults and correlated strongly with immune effector mechanisms that are thought to be important for parasite clearance. These findings provide a set of antigens that warrant further evaluation for inclusion into the vaccine pre-clinical development pipeline.

Published
2017
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8. Development and validation of a diagnostic aid for convulsive epilepsy in sub-Saharan Africa: a retrospective case-control study

Author

Jones, Gabriel Davis, primary, Kariuki, Symon M, additional, Ngugi, Anthony K, additional, Mwesige, Angelina Kakooza, additional, Masanja, Honorati, additional, Owusu-Agyei, Seth, additional, Wagner, Ryan, additional, Cross, J Helen, additional, Sander, Josemir W, additional, Newton, Charles R, additional, Sen, Arjune, additional, Abban, Hanna, additional, Adjei, Patrick, additional, Ae-Ngibise, Ken, additional, Agbokey, Francis, additional, Aissaoui, Lisa, additional, Akpalu, Albert, additional, Akpalu, Bright, additional, Asiamah, Sabina, additional, Asiki, Gershim, additional, Atieno, Mercy, additional, Bauni, Evasius, additional, Bhwana, Dan, additional, Bitta, Mary, additional, Bottomley, Christian, additional, Chabi, Martin, additional, Chengo, Eddie, additional, Chowdhary, Neerja, additional, Connor, Myles, additional, Cross, Helen, additional, Collinson, Mark, additional, Darkwa, Emmanuel, additional, Denison, Timothy, additional, Doku, Victor, additional, Dua, Tarun, additional, Egesa, Isaac, additional, Godi, Tony, additional, Gómez-Olivé, F. Xavier, additional, Grassi, Simone, additional, Iddi, Samuel, additional, Junior, Daniel Nana Yaw Abankwah, additional, Kahn, Kathleen, additional, Kakooza, Angelina, additional, Kariuki, Symon, additional, Kamuyu, Gathoni, additional, Khalayi, Clarah, additional, Kimambo, Henrika, additional, Kleinschmidt, Immo, additional, Kwasa, Thomas, additional, Mahone, Sloan, additional, Manolova, Gergana, additional, Mathew, Alexander, additional, Matuja, William, additional, McDaid, David, additional, Mmbando, Bruno, additional, Mtai Mwanga, Daniel, additional, Muli, Dorcas, additional, Mung'ala Odera, Victor, additional, Murunga Wekesah, Frederick, additional, Mushi, Vivian, additional, Ngugi, Anthony, additional, Odermatt, Peter, additional, Odhiambo, Rachael, additional, O Mageto, James, additional, Otieno, Peter, additional, Pariyo, George, additional, Peterson, Stefan, additional, Sander, Josemir, additional, Sottie, Cynthia, additional, Sylvester, Isolide, additional, Tollman, Stephen, additional, Thoya, Yvonne, additional, Twine, Rhian, additional, Vallentin, Sonia, additional, Walker, Richard, additional, and Waruingi, Stella, additional

Published
2023
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10. Strain Specific Variations in Acinetobacter baumannii Complement Sensitivity

Author

Kamuyu, Gathoni, Ercoli, Giuseppe, Ramos-Sevillano, Elisa, Willcocks, Sam, Kewcharoenwong, Chidchamai, Kiratisin, Pattarachai, Taylor, Peter W, Wren, Brendan W, Lertmemongkolchai, Ganjana, Stabler, Richard A, and Brown, Jeremy S

Subjects
Immunology, Immunology and Allergy
Abstract

The complement system is required for innate immunity against Acinetobacter baumannii, an important cause of antibiotic resistant systemic infections. A. baumannii strains differ in their susceptibility to the membrane attack complex (MAC) formed from terminal complement pathway proteins, but the reasons for this variation remain poorly understood. We have characterized in detail the complement sensitivity phenotypes of nine A. baumannii clinical strains and some of the factors that might influence differences between strains. Using A. baumannii laboratory strains and flow cytometry assays, we first reconfirmed that both opsonization with the complement proteins C3b/iC3b and MAC formation were inhibited by the capsule. There were marked differences in C3b/iC3b and MAC binding between the nine clinical A. baumannii strains, but this variation was partially independent of capsule composition or size. Opsonization with C3b/iC3b improved neutrophil phagocytosis of most strains. Importantly, although C3b/iC3b binding and MAC formation on the bacterial surface correlated closely, MAC formation did not correlate with variations between A. baumannii strains in their levels of serum resistance. Genomic analysis identified only limited differences between strains in the distribution of genes required for serum resistance, but RNAseq data identified three complement-resistance genes that were differentially regulated between a MAC resistant and two MAC intermediate resistant strains when cultured in serum. These data demonstrate that clinical A. baumannii strains vary in their sensitivity to different aspects of the complement system, and that the serum resistance phenotype was influenced by factors in addition to the amount of MAC forming on the bacterial surface.

Published
2022

13. Sequential Vaccination With Heterologous Acinetobacter baumannii Strains Induces Broadly Reactive Antibody Responses

Author

Kamuyu, Gathoni, Suen Cheng, Yat, Willcocks, Sam, Kewcharoenwong, Chidchamai, Kiratisin, Pattarachai, Taylor, Peter W, Wren, Brendan W, Lertmemongkolchai, Ganjana, Stabler, Richard A, and Brown, Jeremy

Subjects
bacteria, biochemical phenomena, metabolism, and nutrition
Abstract

Antibody therapy may be an alternative treatment option for infections caused by the multi-drug resistant (MDR) bacterium Acinetobacter baumannii. As A. baumannii has multiple capsular serotypes, a universal antibody therapy would need to target conserved protein antigens rather than the capsular polysaccharides. We have immunized mice with single or multiple A. baumannii strains to induce antibody responses to protein antigens, and then assessed whether these responses provide cross-protection against a collection of genetically diverse clinical A. baumannii isolates. Immunized mice developed antibody responses to multiple protein antigens. Flow cytometry IgG binding assays and immunoblots demonstrated improved recognition of both homologous and heterologous clinical strains in sera from mice immunized with multiple strains compared to a single strain. The capsule partially inhibited bacterial recognition by IgG and the promotion of phagocytosis by human neutrophils. However, after immunization with multiple strains, serum antibodies to protein antigens promoted neutrophil phagocytosis of heterologous A. baumannii strains. In an infection model, mice immunized with multiple strains had lower bacterial counts in the spleen and liver following challenge with a heterologous strain. These data demonstrate that antibodies targeting protein antigens can improve immune recognition and protection against diverse A. baumannii strains, providing support for their use as an antibody therapy.

Published
2021

15. Distinct kinetics in antibody responses to 111 Plasmodium falciparum antigens identifies novel serological markers of recent malaria exposure

Author

Yman, Victor, primary, Tuju, James, additional, White, Michael T, additional, Kamuyu, Gathoni, additional, Mwai, Kennedy, additional, Kibinge, Nelson, additional, Asghar, Muhammad, additional, Sundling, Christopher, additional, Sonden, Klara, additional, Murungi, Linda, additional, Kiboi, Daniel, additional, Kimathi, Rinther, additional, Chege, Timothy, additional, Chepsat, Emily, additional, Kiyuka, Patience, additional, Nyamako, Lydia, additional, Osier, Faith H A, additional, and Farnert, Anna, additional

Published
2020
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16. Plasmodium falciparum Merozoite Associated Armadillo Protein (PfMAAP) Is Apically Localized in Free Merozoites and Antibodies Are Associated With Reduced Risk of Malaria

Author

Aniweh, Yaw, primary, Nyarko, Prince B., additional, Charles-Chess, Essel, additional, Ansah, Felix, additional, Osier, Faith H. A., additional, Quansah, Evelyn, additional, Thiam, Laty Gaye, additional, Kamuyu, Gathoni, additional, Marsh, Kevin, additional, Conway, David J., additional, Tetteh, Kevin K. A., additional, and Awandare, Gordon A., additional

Published
2020
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18. Electroencephalographic features of convulsive epilepsy in Africa: A multicentre study of prevalence, pattern and associated factors

Author

Kariuki, Symon M., White, Steven, Chengo, Eddie, Wagner, Ryan G., Ae-Ngibise, Kenneth A., Kakooza-Mwesige, Angelina, Ngugi, Anthony K., Sander, Josemir W., Neville, Brian G., Newton, Charles R., Wagner, Ryan, Twine, Rhian, Connor, Myles, Olivé, F. Xavier Gómez, Collinson, Mark, Kahn, Kathleen, Tollman, Stephen, Masanja, Honratio, Mathew, Alexander, Kakooza, Angelina, Pariyo, George, Peterson, Stefan, Ndyomughenyi, Donald, Odhiambo, Rachael, Chabi, Martin, Bauni, Evasius, Kamuyu, Gathoni, Odera, Victor Mung ala, Mageto, James O., Ae-Ngibise, Ken, Akpalu, Bright, Akpalu, Albert, Agbokey, Francis, Adjei, Patrick, Owusu-Agyei, Seth, Bottomley, Christian, Kleinschmidt, Immo, Doku, Victor C K, Odermatt, Peter, Neville, Brian, Nutman, Thomas, Wilkins, Patricia, and Noh, John

Subjects
Adult, Male, Pediatrics, medicine.medical_specialty, Adolescent, Clinical Neurology, Electroencephalography, Article, Temporal lobe, Young Adult, 03 medical and health sciences, symbols.namesake, Epilepsy, 0302 clinical medicine, Physiology (medical), Prevalence, medicine, Humans, Active convulsive epilepsy, 030212 general & internal medicine, Poisson regression, Young adult, Child, Seizure frequency, medicine.diagnostic_test, business.industry, Electroencephalographic features, Middle Aged, medicine.disease, Sensory Systems, Confidence interval, 3. Good health, Risk factors, Neurology, Relative risk, Africa, symbols, Female, Neurology (clinical), business, 030217 neurology & neurosurgery
Abstract

Highlights • Electroencephalographic abnormalities are common in Africans with epilepsy, with an adjusted prevalence of 2.7 (95% confidence interval, 2.5–2.9) per 1000 population. • Electroencephalographic abnormalities are associated with preventable factors such as adverse perinatal events and frequent seizures. • Electroencephalography is helpful in identifying focal epilepsy in Africa, where timing of focal aetiologies is problematic and there is a lack of neuroimaging services., Objective We investigated the prevalence and pattern of electroencephalographic (EEG) features of epilepsy and the associated factors in Africans with active convulsive epilepsy (ACE). Methods We characterized electroencephalographic features and determined associated factors in a sample of people with ACE in five African sites. Mixed-effects modified Poisson regression model was used to determine factors associated with abnormal EEGs. Results Recordings were performed on 1426 people of whom 751 (53%) had abnormal EEGs, being an adjusted prevalence of 2.7 (95% confidence interval (95% CI), 2.5–2.9) per 1000. 52% of the abnormal EEG had focal features (75% with temporal lobe involvement). The frequency and pattern of changes differed with site. Abnormal EEGs were associated with adverse perinatal events (risk ratio (RR) = 1.19 (95% CI, 1.07–1.33)), cognitive impairments (RR = 1.50 (95% CI, 1.30–1.73)), use of anti-epileptic drugs (RR = 1.25 (95% CI, 1.05–1.49)), focal seizures (RR = 1.09 (95% CI, 1.00–1.19)) and seizure frequency (RR = 1.18 (95% CI, 1.10–1.26) for daily seizures; RR = 1.22 (95% CI, 1.10–1.35) for weekly seizures and RR = 1.15 (95% CI, 1.03–1.28) for monthly seizures)). Conclusions EEG abnormalities are common in Africans with epilepsy and are associated with preventable risk factors. Significance EEG is helpful in identifying focal epilepsy in Africa, where timing of focal aetiologies is problematic and there is a lack of neuroimaging services.

Published
2016

19. KILchip v1.0: A Novel Plasmodium falciparum Merozoite Protein Microarray to Facilitate Malaria Vaccine Candidate Prioritization

Author

Kamuyu, Gathoni, primary, Tuju, James, additional, Kimathi, Rinter, additional, Mwai, Kennedy, additional, Mburu, James, additional, Kibinge, Nelson, additional, Chong Kwan, Marisa, additional, Hawkings, Sam, additional, Yaa, Reuben, additional, Chepsat, Emily, additional, Njunge, James M., additional, Chege, Timothy, additional, Guleid, Fatuma, additional, Rosenkranz, Micha, additional, Kariuki, Christopher K., additional, Frank, Roland, additional, Kinyanjui, Samson M., additional, Murungi, Linda M., additional, Bejon, Philip, additional, Färnert, Anna, additional, Tetteh, Kevin K. A., additional, Beeson, James G., additional, Conway, David J., additional, Marsh, Kevin, additional, Rayner, Julian C., additional, and Osier, Faith H. A., additional

Published
2018
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20. Plasmodium falciparum malaria parasite var gene expression is modified by host antibodies: longitudinal evidence from controlled infections of Kenyan adults with varying natural exposure

Author

Abdi, Abdirahman I., primary, Hodgson, Susanne H., additional, Muthui, Michelle K., additional, Kivisi, Cheryl A., additional, Kamuyu, Gathoni, additional, Kimani, Domtila, additional, Hoffman, Stephen L., additional, Juma, Elizabeth, additional, Ogutu, Bernhards, additional, Draper, Simon J., additional, Osier, Faith, additional, Bejon, Philip, additional, Marsh, Kevin, additional, and Bull, Peter C., additional

Published
2017
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21. Prevalence and factors associated with convulsive status epilepticus in Africans with epilepsy

Author

Kariuki, Symon M, Kakooza-Mwesige, Angelina, Wagner, Ryan G, Chengo, Eddie, White, Steven, Kamuyu, Gathoni, Ngugi, Anthony K, Sander, Josemir W, Neville, Brian GR, Newton, Charles RJ, and SEEDS Writing Group

Subjects
parasitic diseases
Abstract

OBJECTIVE: We conducted a community survey to estimate the prevalence and describe the features, risk factors, and consequences of convulsive status epilepticus (CSE) among people with active convulsive epilepsy (ACE) identified in a multisite survey in Africa. METHODS: We obtained clinical histories of CSE and neurologic examination data among 1,196 people with ACE identified from a population of 379,166 people in 3 sites: Agincourt, South Africa; Iganga-Mayuge, Uganda; and Kilifi, Kenya. We performed serologic assessment for the presence of antibodies to parasitic infections and HIV and determined adherence to antiepileptic drugs. Consequences of CSE were assessed using a questionnaire. Logistic regression was used to identify risk factors. RESULTS: The adjusted prevalence of CSE in ACE among the general population across the 3 sites was 2.3 per 1,000, and differed with site (p < 0.0001). Over half (55%) of CSE occurred in febrile illnesses and focal seizures were present in 61%. Risk factors for CSE in ACE were neurologic impairments, acute encephalopathy, previous hospitalization, and presence of antibody titers to falciparum malaria and HIV; these differed across sites. Burns (15%), lack of education (49%), being single (77%), and unemployment (78%) were common in CSE; these differed across the 3 sites. Nine percent with and 10% without CSE died. CONCLUSIONS: CSE is common in people with ACE in Africa; most occurs with febrile illnesses, is untreated, and has focal features suggesting preventable risk factors. Effective prevention and the management of infections and neurologic impairments may reduce the burden of CSE in ACE.

Published
2015

22. Incidence, Remission and Mortality of Convulsive Epilepsy in Rural Northeast South Africa

Author

Wagner, Ryan G, Bottomley, Christian, Ngugi, Anthony K, Ibinda, Fredrick, Gómez-Olivé, F Xavier, Kahn, Kathleen, Tollman, Stephen, Newton, Charles R, SEEDS Writing Group, Wagner, Ryan, Twine, Rhian, Connor, Myles, Collinson, Mark, Masanja, Honratio, Mathew, Alexander, Kakooza, Angelina, Pariyo, George, Peterson, Stefan, Ndyo-mughenyi, Donald, Odhiambo, Rachael, Chengo, Eddie, Chabi, Martin, Bauni, Evasius, Kamuyu, Gathoni, Odera, Victor Mung'ala, Mageto, James O, Ae-Ngibise, Ken, Akpalu, Bright, Akpalu, Albert, Agbokey, Francis, Adjei, Patrick, Owusu-Agyei, Seth, Kleinschmidt, Immo, Doku, Victor CK, Odermatt, Peter, Neville, Brian, Sander, Josemir W, White, Steve, Nutman, Thomas, Wilkins, Patricia, and Noh, John

Subjects
Adult, Male, Rural Population, medicine.medical_specialty, Pediatrics, Adolescent, Science, Population, Context (language use), Disease, South Africa, Young Adult, 03 medical and health sciences, Epilepsy, 0302 clinical medicine, Risk Factors, Cause of Death, Environmental health, Epidemiology, Humans, Medicine, 030212 general & internal medicine, Mortality, Child, education, education.field_of_study, Multidisciplinary, business.industry, Incidence, Incidence (epidemiology), Mortality rate, 1. No poverty, Public Health, Global Health, Social Medicine and Epidemiology, medicine.disease, 3. Good health, Folkhälsovetenskap, global hälsa, socialmedicin och epidemiologi, Cross-Sectional Studies, Population Surveillance, Life expectancy, Female, business, 030217 neurology & neurosurgery, Research Article
Abstract

BackgroundEpilepsy is one of the most common neurological conditions globally, estimated to constitute 0.75% of the global burden of disease, with the majority of this burden found in low- and middle- income countries (LMICs). Few studies from LMICs, including much of sub-Saharan Africa, have described the incidence, remission or mortality rates due to epilepsy, which are needed to quantify the burden and inform policy. This study investigates the epidemiological parameters of convulsive epilepsy within a context of high HIV prevalence and an emerging burden of cardiovascular disease.MethodsA cross-sectional population survey of 82,818 individuals, in the Agincourt Health and Socio-demographic Surveillance Site (HDSS) in rural northeast South Africa was conducted in 2008, from which 296 people were identified with active convulsive epilepsy. A follow-up survey was conducted in 2012. Incidence and mortality rates were estimated, with duration and remission rates calculated using the DISMOD II software package.ResultsThe crude incidence for convulsive epilepsy was 17.4/100,000 per year (95%CI: 13.1-23.0). Remission was 4.6% and 3.9% per year for males and females, respectively. The standardized mortality ratio was 2.6 (95%CI: 1.7-3.5), with 33.3% of deaths directly related to epilepsy. Mortality was higher in men than women (adjusted rate ratio (aRR) 2.6 (95%CI: 1.2-5.4)), and was significantly associated with older ages (50+ years versus those 0-5 years old (RR 4.8 (95%CI: 0.6-36.4)).ConclusionsThe crude incidence was lower whilst mortality rates were similar to other African studies; however, this study found higher mortality amongst older males. Efforts aimed at further understanding what causes epilepsy in older people and developing interventions to reduce prolonged seizures are likely to reduce the overall burden of ACE in rural South Africa.

Published
2015

23. Evaluating controlled human malaria infection in Kenyan adults with varying degrees of prior exposure to Plasmodium falciparum using sporozoites administered by intramuscular injection

Author

Hodgson, Susanne H., Juma, Elizabeth, Salim, Amina, Magiri, Charles, Kimani, Domtila, Njenga, Daniel, Muia, Alfred, Cole, Andrew O., Ogwang, Caroline, Awuondo, Ken, Lowe, Brett, Munene, Marianne, Billingsley, Peter F., James, Eric R., Gunasekera, Anusha, Sim, B. Kim L., Njuguna, Patricia, Rampling, Thomas W., Richman, Adam, Abebe, Yonas, Kamuyu, Gathoni, Muthui, Michelle, Elias, Sean C., Molyneux, Sassy, Gerry, Stephen, Macharia, Alex, Williams, Thomas N., Bull, Peter C., Hill, Adrian V. S., Osier, Faith H., Draper, Simon J., Bejon, Philip, Hoffman, Stephen L., Ogutu, Bernhards, and Marsh, Kevin

Subjects
falciparum, parasitic diseases, malaria, challenge, Public Health, CHMI, immunity
Abstract

Background: Controlled human malaria infection (CHMI) studies are a vital tool to accelerate vaccine and drug development. As CHMI trials are performed in a controlled environment, they allow unprecedented, detailed evaluation of parasite growth dynamics (PGD) and immunological responses. However, CHMI studies have not been routinely performed in malaria-endemic countries or used to investigate mechanisms of naturally-acquired immunity (NAI) to Plasmodium falciparum. Methods: We conducted an open-label, randomized CHMI pilot-study using aseptic, cryopreserved P. falciparum sporozoites (PfSPZ Challenge) to evaluate safety, infectivity and PGD in Kenyan adults with low to moderate prior exposure to P. falciparum (Pan African Clinical Trial Registry: PACTR20121100033272). Results: All participants developed blood-stage infection confirmed by quantitative polymerase chain reaction (qPCR). However one volunteer (110) remained asymptomatic and blood-film negative until day 21 post-injection of PfSPZ Challenge. This volunteer had a reduced parasite multiplication rate (PMR) (1.3) in comparison to the other 27 volunteers (median 11.1). A significant correlation was seen between PMR and screening anti-schizont Enzyme Linked Immunosorbent Assays (ELISA) OD (p = 0.044, R = −0.384) but not when volunteer 110 was excluded from the analysis (p = 0.112, R = −0.313). Conclusions: PfSPZ Challenge is safe and infectious in malaria-endemic populations and could be used to assess the efficacy of malaria vaccines and drugs in African populations. Whilst our findings are limited by sample size, our pilot study has demonstrated for the first time that NAI may impact on PMR post-CHMI in a detectable fashion, an important finding that should be evaluated in further CHMI studies.

Published
2014
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24. New antigens for multi-component blood-stage vaccines against Plasmodium falciparum malaria

Author

Osier, Faith H, Mackinnon, Margaret J, Crosnier, Cécile, Fegan, Gregory, Kamuyu, Gathoni, Wanaguru, Madushi, Ogada, Edna, McDade, Brian, Rayner, Julian C, Wright, Gavin J, and Marsh, Kevin

Subjects
Time Factors, Merozoites, Plasmodium falciparum, Age Factors, Infant, Newborn, Protozoan Proteins, Antibodies, Protozoan, Infant, Antigens, Protozoan, Kenya, Article, Peptide Fragments, Seroepidemiologic Studies, Child, Preschool, parasitic diseases, Malaria Vaccines, Humans, Prospective Studies, Malaria, Falciparum, Child, Biomarkers
Abstract

An effective blood stage vaccine against Plasmodium falciparum remains a research priority but the number of antigens that have been translated to candidates for testing in clinical trials remains limited. Investigations of the large number of potential targets found in the parasite proteome have been constrained by an inability to produce natively folded recombinant antigens for immunological studies. We overcame these constraints by generating a large library of demonstrably biochemically active merozoite surface and secreted full-length ectodomain proteins. We then systematically examined the antibody reactivity against these proteins in a cohort of Kenyan children (n=286) who were sampled at the start of a malaria transmission season and prospectively monitored for clinical episodes of malaria over the ensuing six months. We found that antibodies to previously untested or little-studied proteins had superior or equivalent potential protective efficacy to the handful of current leading malaria vaccine candidates. Moreover, cumulative responses to combinations comprising five of the ten top ranked antigens, including PF3D7_1136200, MSP2, RhopH3, P41, MSP11, MSP3, PF3D7_0606800, AMA1, Pf113 and MSRP1 were associated with 100% protection against clinical episodes of malaria. These data suggest that not only are there many more potential vaccine candidates for the vaccine development pipeline, but also that highly effective vaccination may be achieved through combining a selection of these antigens as observed in nature.

Published
2014

25. Exposure to multiple parasites is associated with the prevalence of active convulsive epilepsy in sub-Saharan Africa

Author

Kamuyu, Gathoni, Bottomley, Christian, Mageto, James, Lowe, Brett, Wilkins, Patricia P., Noh, John C., Nutman, Thomas B., Ngugi, Anthony K., Odhiambo, Rachael, Wagner, Ryan G., Kakooza-Mwesige, Angelina, Owusu-Agyei, Seth, Ae-Ngibise, Kenneth, Masanja, Honorati, Osier, Faith H. A., Odermatt, Peter, Newton, Charles R., and Study of Epidemiology of Epilepsy in Demographic Sites group

Subjects
lcsh:Arctic medicine. Tropical medicine, lcsh:RC955-962, lcsh:Public aspects of medicine, parasitic diseases, lcsh:RA1-1270
Abstract

BACKGROUND: Epilepsy is common in developing countries, and it is often associated with parasitic infections. We investigated the relationship between exposure to parasitic infections, particularly multiple infections and active convulsive epilepsy (ACE), in five sites across sub-Saharan Africa. METHODS AND FINDINGS: A case-control design that matched on age and location was used. Blood samples were collected from 986 prevalent cases and 1,313 age-matched community controls and tested for presence of antibodies to Onchocerca volvulus, Toxocara canis, Toxoplasma gondii, Plasmodium falciparum, Taenia solium and HIV. Exposure (seropositivity) to Onchocerca volvulus (OR = 1.98; 95%CI: 1.52-2.58, p

Published
2014

26. Changes in Serological Immunology Measures in UK and Kenyan Adults Post-controlled Human Malaria Infection

Author

Hodgson, Susanne H., primary, Llewellyn, David, additional, Silk, Sarah E., additional, Milne, Kathryn H., additional, Elias, Sean C., additional, Miura, Kazutoyo, additional, Kamuyu, Gathoni, additional, Juma, Elizabeth A., additional, Magiri, Charles, additional, Muia, Alfred, additional, Jin, Jing, additional, Spencer, Alexandra J., additional, Longley, Rhea J., additional, Mercier, Thomas, additional, Decosterd, Laurent, additional, Long, Carole A., additional, Osier, Faith H., additional, Hoffman, Stephen L., additional, Ogutu, Bernhards, additional, Hill, Adrian V. S., additional, Marsh, Kevin, additional, and Draper, Simon J., additional

Published
2016
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27. Binding of Plasmodium falciparum Merozoite Surface Proteins DBLMSP and DBLMSP2 to Human Immunoglobulin M Is Conserved among Broadly Diverged Sequence Variants

Author

Crosnier, Cécile, primary, Iqbal, Zamin, additional, Knuepfer, Ellen, additional, Maciuca, Sorina, additional, Perrin, Abigail J., additional, Kamuyu, Gathoni, additional, Goulding, David, additional, Bustamante, Leyla Y., additional, Miles, Alistair, additional, Moore, Shona C., additional, Dougan, Gordon, additional, Holder, Anthony A., additional, Kwiatkowski, Dominic P., additional, Rayner, Julian C., additional, Pleass, Richard J., additional, and Wright, Gavin J., additional

Published
2016
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28. Prevalence and factors associated with convulsive status epilepticus in Africans with epilepsy

Author

Kariuki, Symon M., Kakooza-Mwesige, Angelina, Wagner, Ryan G., Chengo, Eddie, White, Steven, Kamuyu, Gathoni, Ngugi, Anthony K., Sander, Josemir W., Neville, Brian G. R., Newton, Charles R. J., Kariuki, Symon M., Kakooza-Mwesige, Angelina, Wagner, Ryan G., Chengo, Eddie, White, Steven, Kamuyu, Gathoni, Ngugi, Anthony K., Sander, Josemir W., Neville, Brian G. R., and Newton, Charles R. J.

Abstract

Objective:We conducted a community survey to estimate the prevalence and describe the features, risk factors, and consequences of convulsive status epilepticus (CSE) among people with active convulsive epilepsy (ACE) identified in a multisite survey in Africa.Methods:We obtained clinical histories of CSE and neurologic examination data among 1,196 people with ACE identified from a population of 379,166 people in 3 sites: Agincourt, South Africa; Iganga-Mayuge, Uganda; and Kilifi, Kenya. We performed serologic assessment for the presence of antibodies to parasitic infections and HIV and determined adherence to antiepileptic drugs. Consequences of CSE were assessed using a questionnaire. Logistic regression was used to identify risk factors.Results:The adjusted prevalence of CSE in ACE among the general population across the 3 sites was 2.3 per 1,000, and differed with site (p < 0.0001). Over half (55%) of CSE occurred in febrile illnesses and focal seizures were present in 61%. Risk factors for CSE in ACE were neurologic impairments, acute encephalopathy, previous hospitalization, and presence of antibody titers to falciparum malaria and HIV; these differed across sites. Burns (15%), lack of education (49%), being single (77%), and unemployment (78%) were common in CSE; these differed across the 3 sites. Nine percent with and 10% without CSE died.Conclusions:CSE is common in people with ACE in Africa; most occurs with febrile illnesses, is untreated, and has focal features suggesting preventable risk factors. Effective prevention and the management of infections and neurologic impairments may reduce the burden of CSE in ACE.

Published
2015
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29. Clinical features, proximate causes, and consequences of active convulsive epilepsy in Africa

Author

Kariuki, Symon M, Matuja, William, Akpalu, Albert, Kakooza-Mwesige, Angelina, Chabi, Martin, Wagner, Ryan G, Connor, Myles, Chengo, Eddie, Ngugi, Anthony K, Odhiambo, Rachael, Bottomley, Christian, White, Steven, Sander, Josemir W, Neville, Brian GR, Newton, Charles RJC, SEEDS writing group, Twine, Rhian, Gómez Olivé, F Xavier, Collinson, Mark, Kahn, Kathleen, Tollman, Stephen, Masanja, Honratio, Mathew, Alexander, Pariyo, George, Peterson, Stefan, Ndyomughenyi, Donald, Bauni, Evasius, Kamuyu, Gathoni, Odera, Victor Mung'ala, Mageto, James O, Ae-Ngibise, Ken, Akpalu, Bright, Agbokey, Francis, Adjei, Patrick, Owusu-Agyei, Seth, Kleinschmidt, Immo, Doku, Victor CK, Odermatt, Peter, Nutman, Thomas, Wilkins, Patricia, and Noh, John

Abstract

PURPOSE: Epilepsy is common in sub-Saharan Africa (SSA), but the clinical features and consequences are poorly characterized. Most studies are hospital-based, and few studies have compared different ecological sites in SSA. We described active convulsive epilepsy (ACE) identified in cross-sectional community-based surveys in SSA, to understand the proximate causes, features, and consequences. METHODS: We performed a detailed clinical and neurophysiologic description of ACE cases identified from a community survey of 584,586 people using medical history, neurologic examination, and electroencephalography (EEG) data from five sites in Africa: South Africa; Tanzania; Uganda; Kenya; and Ghana. The cases were examined by clinicians to discover risk factors, clinical features, and consequences of epilepsy. We used logistic regression to determine the epilepsy factors associated with medical comorbidities. KEY FINDINGS: Half (51%) of the 2,170 people with ACE were children and 69% of seizures began in childhood. Focal features (EEG, seizure types, and neurologic deficits) were present in 58% of ACE cases, and these varied significantly with site. Status epilepticus occurred in 25% of people with ACE. Only 36% received antiepileptic drugs (phenobarbital was the most common drug [95%]), and the proportion varied significantly with the site. Proximate causes of ACE were adverse perinatal events (11%) for onset of seizures before 18 years; and acute encephalopathy (10%) and head injury prior to seizure onset (3%). Important comorbidities were malnutrition (15%), cognitive impairment (23%), and neurologic deficits (15%). The consequences of ACE were burns (16%), head injuries (postseizure) (1%), lack of education (43%), and being unmarried (67%) or unemployed (57%) in adults, all significantly more common than in those without epilepsy. SIGNIFICANCE: There were significant differences in the comorbidities across sites. Focal features are common in ACE, suggesting identifiable and preventable causes. Malnutrition and cognitive and neurologic deficits are common in people with ACE and should be integrated into the management of epilepsy in this region. Consequences of epilepsy such as burns, lack of education, poor marriage prospects, and unemployment need to be addressed.

Published
2013

30. Multiple clinical episodes of Plasmodium falciparum malaria in a low transmission intensity setting: exposure versus immunity

Author

Rono, Josea, primary, Färnert, Anna, additional, Murungi, Linda, additional, Ojal, John, additional, Kamuyu, Gathoni, additional, Guleid, Fatuma, additional, Nyangweso, George, additional, Wambua, Juliana, additional, Kitsao, Barnes, additional, Olotu, Ally, additional, Marsh, Kevin, additional, and Osier, Faith HA, additional

Published
2015
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31. New antigens for a multicomponent blood-stage malaria vaccine

Author

Osier, Faith H., primary, Mackinnon, Margaret J., additional, Crosnier, Cécile, additional, Fegan, Gregory, additional, Kamuyu, Gathoni, additional, Wanaguru, Madushi, additional, Ogada, Edna, additional, McDade, Brian, additional, Rayner, Julian C., additional, Wright, Gavin J., additional, and Marsh, Kevin, additional

Published
2014
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32. Prevalence of active convulsive epilepsy in sub-Saharan Africa and associated risk factors : cross-sectional and case-control studies

Author

Ngugi, Anthony K., Bottomley, Christian, Kleinschmidt, Immo, Wagner, Ryan G., Kakooza-Mwesige, Angelina, Ae-Ngibise, Kenneth, Owusu-Agyei, Seth, Masanja, Honorati, Kamuyu, Gathoni, Odhiambo, Rachael, Chengo, Eddie, Sander, Josemir W., Newton, Charles R., Ngugi, Anthony K., Bottomley, Christian, Kleinschmidt, Immo, Wagner, Ryan G., Kakooza-Mwesige, Angelina, Ae-Ngibise, Kenneth, Owusu-Agyei, Seth, Masanja, Honorati, Kamuyu, Gathoni, Odhiambo, Rachael, Chengo, Eddie, Sander, Josemir W., and Newton, Charles R.

Abstract

Background The prevalence of epilepsy in sub-Saharan Africa seems to be higher than in other parts of the world, but estimates vary substantially for unknown reasons. We assessed the prevalence and risk factors of active convulsive epilepsy across five centres in this region. Methods We did large population-based cross-sectional and case-control studies in five Health and Demographic Surveillance System centres: Kilifi, Kenya (Dec 3, 2007-July 31, 2008); Agincourt, South Africa (Aug 4, 2008-Feb 27, 2009); Iganga-Mayuge, Uganda (Feb 2, 2009-Oct 30, 2009); Ifakara, Tanzania (May 4, 2009-Dec 31, 2009); and Kintampo, Ghana (Aug 2, 2010-April 29, 2011). We used a three-stage screening process to identify people with active convulsive epilepsy. Prevalence was estimated as the ratio of confirmed cases to the population screened and was adjusted for sensitivity and attrition between stages. For each case, an age-matched control individual was randomly selected from the relevant centre's census database. Fieldworkers masked to the status of the person they were interviewing administered questionnaires to individuals with active convulsive epilepsy and control individuals to assess sociodemographic variables and historical risk factors (perinatal events, head injuries, and diet). Blood samples were taken from a randomly selected subgroup of 300 participants with epilepsy and 300 control individuals from each centre and were screened for antibodies to Toxocara canis, Toxoplasma gondii, Onchocerca volvulus, Plasmodium falciparum, Taenia solium, and HIV. We estimated odds ratios (ORs) with logistic regression, adjusted for age, sex, education, employment, and marital status. Results 586 607 residents in the study areas were screened in stage one, of whom 1711 were diagnosed as having active convulsive epilepsy. Prevalence adjusted for attrition and sensitivity varied between sites: 7.8 per 1000 people (95% CI 7.5-8.2) in Kilifi, 7.0 (6.2-7.4) in Agincourt, 10.3 (9.5-11.1) in Iga

Published
2013
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33. A threshold concentration of anti-merozoite antibodies is required for protection from clinical episodes of malaria

Author

Murungi, Linda M, Kamuyu, Gathoni, Lowe, Brett, Bejon, Philip, Theisen, Michael, Kinyanjui, Samson M, Marsh, Kevin, Osier, Faith H A, Murungi, Linda M, Kamuyu, Gathoni, Lowe, Brett, Bejon, Philip, Theisen, Michael, Kinyanjui, Samson M, Marsh, Kevin, and Osier, Faith H A

Abstract

Antibodies to selected Plasmodium falciparum merozoite antigens are often reported to be associated with protection from malaria in one epidemiological cohort, but not in another. Here, we sought to understand this paradox by exploring the hypothesis that a threshold concentration of antibodies is necessary for protection. We analyzed data from two independent cohorts along the Kenyan coast, one in which antibodies to AMA1, MSP-2 and MSP-3 were associated with protection from malaria (Chonyi) and another in which this association was not observed (Junju). We used a malaria reference reagent to standardize antibody measurements across both cohorts, and applied statistical methods to derive the threshold concentration of antibodies against each antigen that best correlated with a reduced risk of malaria (the protective threshold), in the Chonyi cohort. We then tested whether antibodies in Junju reached the protective threshold concentrations observed in the Chonyi cohort. Except for children under 3 years, the age-matched proportions of children achieving protective threshold concentrations of antibodies against AMA1 and MSP-2 were significantly lower in Junju compared to Chonyi (Fishers exact test, P

Published
2013

34. Analysis of antibodies to newly described Plasmodium falciparum merozoite antigens supports MSPDBL2 as a predicted target of naturally acquired immunity

Author

Tetteh, Kevin K A, Osier, Faith H A, Salanti, Ali, Kamuyu, Gathoni, Drought, Laura, Failly, Marilyne, Martin, Christophe, Marsh, Kevin, Conway, David J, Tetteh, Kevin K A, Osier, Faith H A, Salanti, Ali, Kamuyu, Gathoni, Drought, Laura, Failly, Marilyne, Martin, Christophe, Marsh, Kevin, and Conway, David J

Abstract

Prospective studies continue to identify malaria parasite genes with particular patterns of polymorphism which indicate they may be under immune selection, and the encoded proteins require investigation. Sixteen new recombinant protein reagents were designed to characterize three such polymorphic proteins expressed in Plasmodium falciparum schizonts and merozoites: MSPDBL1 (also termed MSP3.4) and MSPDBL2 (MSP3.8), which possess Duffy binding-like (DBL) domains, and SURFIN4.2, encoded by a member of the surface-associated interspersed (surf) multigene family. After testing the antigenicities of these reagents by murine immunization and parasite immunofluorescence, we analyzed naturally acquired antibody responses to the antigens in two cohorts in coastal Kenya in which the parasite was endemic (Chonyi [n = 497] and Ngerenya [n = 461]). As expected, the prevalence and levels of serum antibodies increased with age. We then investigated correlations with subsequent risk of clinical malaria among children

Published
2013

36. Correction: Corrigendum: The blood-stage malaria antigen PfRH5 is susceptible to vaccine-inducible cross-strain neutralizing antibody

Author

Douglas, Alexander D., primary, Williams, Andrew R., additional, Illingworth, Joseph J., additional, Kamuyu, Gathoni, additional, Biswas, Sumi, additional, Goodman, Anna L., additional, Wyllie, David H., additional, Crosnier, Cécile, additional, Miura, Kazutoyo, additional, Wright, Gavin J., additional, Long, Carole A., additional, Osier, Faith H., additional, Marsh, Kevin, additional, Turner, Alison V., additional, Hill, Adrian V. S., additional, and Draper, Simon J., additional

Published
2013
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38. The Ratio of Monocytes to Lymphocytes in Peripheral Blood Correlates with Increased Susceptibility to Clinical Malaria in Kenyan Children

Author

Warimwe, George M., primary, Murungi, Linda M., additional, Kamuyu, Gathoni, additional, Nyangweso, George M., additional, Wambua, Juliana, additional, Naranbhai, Vivek, additional, Fletcher, Helen A., additional, Hill, Adrian V. S., additional, Bejon, Philip, additional, Osier, Faith H. A., additional, and Marsh, Kevin, additional

Published
2013
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39. Anti-merozoite antibodies induce natural killer cell effector function and are associated with immunity against malaria

Author

Odera, Dennis O., Tuju, James, Mwai, Kennedy, Nkumama, Irene N., Fürle, Kristin, Chege, Timothy, Kimathi, Rinter, Diehl, Stefan, Musasia, Fauzia K., Rosenkranz, Micha, Njuguna, Patricia, Hamaluba, Mainga, Kapulu, Melissa C., Frank, Roland, Osier, Faith H. A., Abdi, Abdirahman I., Chi, Primus Che, de Laurent, Zaydah, Jao, Irene, Kamuya, Dorcas, Kamuyu, Gathoni, Makale, Johnstone, Murungi, Linda, Musyoki, Jennifer, Muthui, Michelle, Mwacharo, Jedidah, Kariuki, Silvia, Mwanga, Daniel, Mwongeli, Joyce, Ndungu, Francis, Njue, Maureen, Nyangweso, George, Kimani, Domitila, Ngoi, Joyce M., Musembi, Janet, Ngoto, Omar, Otieno, Edward, Ooko, Michael, Shangala, Jimmy, Wambua, Juliana, Mohammed, Khadija Said, Omuoyo, Donwilliams, Mosobo, Moses, Kibinge, Nelson, Kinyanjui, Sam, Bejon, Philip, Lowe, Brett, Marsh, Kevin, Marsh, Vicki, Abebe, Yonas, Billingsley, Peter F., Sim, Betty Kim Lee, Hoffman, Stephen L., James, Eric R., Richie, Thomas L., Audi, Agnes, Olewe, Fredrick, Oloo, James, Ongecha, John, Ongas, Martin O., Koskei, Nelly, Bull, Peter C., Hodgson, Susanne H., Kivisi, Cheryl, Imwong, Mallika, Murphy, Sean C., Ogutu, Bernhards, Tarning, Joel, Winterberg, Markus, and Williams, Thomas N.

Abstract

Natural killer (NK) cells are potent immune effectors that can be activated via antibody-mediated Fc receptor engagement. Using multiparameter flow cytometry, we found that NK cells degranulate and release IFN-γ upon stimulation with antibody-opsonized Plasmodium falciparummerozoites. Antibody-dependent NK (Ab-NK) activity was largely strain transcending and enhanced invasion inhibition into erythrocytes. Ab-NK was associated with the successful control of parasitemia after experimental malaria challenge in African adults. In an independent cohort study in children, Ab-NK increased with age, was boosted by concurrent P. falciparuminfections, and was associated with a lower risk of clinical episodes of malaria. Nine of the 14 vaccine candidates tested induced Ab-NK, including some less well-characterized antigens: P41, P113, MSP11, RHOPH3, and Pf_11363200. These data highlight an important role of Ab-NK activity in immunity against malaria and provide a potential mechanism for evaluating vaccine candidates.

Published
2023
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40. Analysis of Antibodies to Newly Described Plasmodium falciparumMerozoite Antigens Supports MSPDBL2 as a Predicted Target of Naturally Acquired Immunity

Author

Tetteh, Kevin K. A., Osier, Faith H. A., Salanti, Ali, Kamuyu, Gathoni, Drought, Laura, Failly, Marilyne, Martin, Christophe, Marsh, Kevin, and Conway, David J.

Abstract

ABSTRACTProspective studies continue to identify malaria parasite genes with particular patterns of polymorphism which indicate they may be under immune selection, and the encoded proteins require investigation. Sixteen new recombinant protein reagents were designed to characterize three such polymorphic proteins expressed in Plasmodium falciparumschizonts and merozoites: MSPDBL1 (also termed MSP3.4) and MSPDBL2 (MSP3.8), which possess Duffy binding-like (DBL) domains, and SURFIN4.2, encoded by a member of the surface-associated interspersed (surf) multigene family. After testing the antigenicities of these reagents by murine immunization and parasite immunofluorescence, we analyzed naturally acquired antibody responses to the antigens in two cohorts in coastal Kenya in which the parasite was endemic (Chonyi [n= 497] and Ngerenya [n= 461]). As expected, the prevalence and levels of serum antibodies increased with age. We then investigated correlations with subsequent risk of clinical malaria among children <11 years of age during 6 months follow-up surveillance. Antibodies to the polymorphic central region of MSPDBL2 were associated with reduced risk of malaria in both cohorts, with statistical significance remaining for the 3D7 allelic type after adjustment for individuals' ages in years and antibody reactivity to whole-schizont extract (Chonyi, risk ratio, 0.51, and 95% confidence interval [CI], 0.28 to 0.93; Ngerenya, risk ratio, 0.38, and 95% CI, 0.18 to 0.82). For the MSPDBL1 Palo Alto allelic-type antigen, there was a protective association in one cohort (Ngerenya, risk ratio, 0.53, and 95% CI, 0.32 to 0.89), whereas the other antigens showed no protective associations after adjustment. These findings support the prediction that antibodies to the polymorphic region of MSPDBL2 contribute to protective immunity.

Published
2013
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41. Plasmodium falciparum malaria parasite var gene expression is modified by host antibodies: longitudinal evidence from controlled infections of Kenyan adults with varying natural exposure

Author

Abdi, Abdirahman I, Hodgson, Susanne H, Muthui, Michelle K, Kivisi, Cheryl A, Kamuyu, Gathoni, Kimani, Domtila, Hoffman, Stephen L, Juma, Elizabeth, Ogutu, Bernhards, Draper, Simon J, Osier, Faith, Bejon, Philip, Marsh, Kevin, and Bull, Peter

Subjects
Adult, Erythrocytes, Plasmodium falciparum, Protozoan Proteins, Antibodies, Protozoan, Gene Expression, Antigens, Protozoan, Real-Time Polymerase Chain Reaction, Kenya, 3. Good health, Host-Pathogen Interactions, Animals, Humans, Longitudinal Studies, Malaria, Falciparum

42. Exposure to multiple parasites is associated with the prevalence of active convulsive epilepsy in sub-saharan Africa

Author

Kamuyu, Gathoni, Bottomley, Christian, Mageto, James, Lowe, Brett, Wilkins, Patricia P., Noh, John C., Nutman, Thomas B., Ngugi, Anthony K., Odhiambo, Rachael, Wagner, Ryan G., Kakooza-Mwesige, Angelina, Owusu-Agyei, Seth, Ae-Ngibise, Kenneth, Masanja, Honorati, Osier, Faith H. A., Odermatt, Peter, Newton, Charles R., and Study of Epidemiology of Epilepsy in Demographic Sites group

Subjects
3. Good health

43. Plasmodium falciparum malaria parasite var gene expression is modified by host antibodies: longitudinal evidence from controlled infections of Kenyan adults with varying natural exposure

Author

Abdi, Abdirahman I, Hodgson, Susanne H, Muthui, Michelle K, Kivisi, Cheryl A, Kamuyu, Gathoni, Kimani, Domtila, Hoffman, Stephen L, Juma, Elizabeth, Ogutu, Bernhards, Draper, Simon J, Osier, Faith, Bejon, Philip, Marsh, Kevin, and Bull, Peter C

Subjects
Adult, Erythrocytes, Sporozoite, Plasmodium falciparum, Immunity, Protozoan Proteins, Antibodies, Protozoan, Gene Expression, Antigens, Protozoan, P. falciparum, Real-Time Polymerase Chain Reaction, Kenya, Antibodies, 3. Good health, PfEMP1, parasitic diseases, Host-Pathogen Interactions, Animals, Humans, Longitudinal Studies, Malaria, Falciparum, Controlled human malaria infection (CHMI)
Abstract

BACKGROUND: The PfEMP1 family of Plasmodium falciparum antigens play a key role in pathogenesis of severe malaria through their insertion into the surface of parasite infected erythrocytes, and adhesion to host cells. Previous studies have suggested that parasites expressing PfEMP1 subclasses group A and DC8, associated with severe malaria, may have a growth advantage in immunologically naïve individuals. However, this idea has not been tested in longitudinal studies. METHODS: Here we assessed expression of the var genes encoding PfEMP1, in parasites sampled from volunteers with varying prior exposure to malaria, following experimental infection by sporozoites (PfSPZ). Using qPCR, we tested for associations between the expression of various var subgroups in surviving parasite populations from each volunteer and 1) the levels of participants' antibodies to infected erythrocytes before challenge infection and 2) the apparent in vivo parasite multiplication rate. RESULTS: We show that 1) expression of var genes encoding for group A and DC8-like PfEMP1 were associated with low levels of antibodies to infected erythrocytes (αIE) before challenge, and 2) expression of a DC8-like CIDRα1.1 domain was associated with higher apparent parasite multiplication rate in a manner that was independent of levels of prior antibodies to infected erythrocytes. CONCLUSIONS: This study provides insight into the role of antibodies to infected erythrocytes surface antigens in the development of naturally acquired immunity and may help explain why specific PfEMP1 variants may be associated with severe malaria. TRIAL REGISTRATION: Pan African Clinical Trial Registry: PACTR201211000433272 . Date of registration: 10th October 2012.

44. Identifying Merozoite Targets of Protective Immunity Against Plasmodium falciparum Malaria

Author

Kamuyu, Gathoni and Kamuyu, Gathoni

Abstract

The observation that individuals living in malaria endemic regions who are repeatedly infected with P. falciparum can acquire immunity, first to severe, then to uncomplicated clinical episodes of malaria, and finally to high parasite densities, provides hope that a vaccine is achievable. Immunoglobulins have been identified as a key component of naturally acquired immunity and identifying the targets and mechanisms by which this protection is achieved is a clear research priority. To date, only a small proportion of the parasite proteome has been evaluated in the context of naturally acquired immunity. This thesis was aimed at contributing to this knowledge gap by identifying novel potential antigen targets of protective antibodies and validating these in samples from Tanzanian adults. First, to identify merozoite antigens that were immunogenic, I resolved proteins extracted from P. falciparum merozoites by two-dimensional gel electrophoresis and tested these for reactivity with immunoglobulins from malaria immune adults. Immunoreactive proteins were then identified by mass-spectrometry. In complementary studies, purified P. falciparum merozoites were treated with proteolytic enzymes to release proteins localised on the surface of merozoites, which were subsequently identified by mass-spectrometry. Using stringent criteria, where I combined the data obtained from 2D-immunoblots and surface-trypsinization experiments with bioinformatics prediction (for the presence of a signal peptide and/or transmembrane domain), I narrowed down to 222 potential merozoite vaccine targets. These included known surface and/or immunogenic proteins such as the 6-cysteine proteins (Pf12, Pf38, Pf41), MSP-1, 3, 7, 9, 10, GLURP, AMA1, GAMA, MTRAP, LSA3 and RhopH3 as well as many unstudied proteins. From the set of unstudied proteins, I prioritised 27 antigens for immunoprofiling and identified 19 antigens that are targets of naturally acquired antibo

45. Development and validation of a diagnostic aid for convulsive epilepsy in sub-Saharan Africa: a retrospective case-control study

Author

Jones, Gabriel Davis, Kariuki, Symon M., Ngugi, Anthony K., Mwesige, Angelina Kakooza, Masanja, Honorati, Owusu-Agyei, Seth, Wagner, Ryan, Cross, J. Helen, Sander, Josemir W., Newton, Charles R., Sen, Arjune, Abban, Hanna, Adjei, Patrick, Ae-Ngibise, Ken, Agbokey, Francis, Aissaoui, Lisa, Akpalu, Albert, Akpalu, Bright, Asiamah, Sabina, Asiki, Gershim, Atieno, Mercy, Bauni, Evasius, Bhwana, Dan, Bitta, Mary, Bottomley, Christian, Chabi, Martin, Chengo, Eddie, Chowdhary, Neerja, Connor, Myles, Cross, Helen, Collinson, Mark, Darkwa, Emmanuel, Denison, Timothy, Doku, Victor, Dua, Tarun, Egesa, Isaac, Godi, Tony, Gómez-Olivé, F. Xavier, Grassi, Simone, Iddi, Samuel, Junior, Daniel Nana Yaw Abankwah, Kahn, Kathleen, Kakooza, Angelina, Kariuki, Symon, Kamuyu, Gathoni, Khalayi, Clarah, Kimambo, Henrika, Kleinschmidt, Immo, Kwasa, Thomas, McDaid, David, Jones, Gabriel Davis, Kariuki, Symon M., Ngugi, Anthony K., Mwesige, Angelina Kakooza, Masanja, Honorati, Owusu-Agyei, Seth, Wagner, Ryan, Cross, J. Helen, Sander, Josemir W., Newton, Charles R., Sen, Arjune, Abban, Hanna, Adjei, Patrick, Ae-Ngibise, Ken, Agbokey, Francis, Aissaoui, Lisa, Akpalu, Albert, Akpalu, Bright, Asiamah, Sabina, Asiki, Gershim, Atieno, Mercy, Bauni, Evasius, Bhwana, Dan, Bitta, Mary, Bottomley, Christian, Chabi, Martin, Chengo, Eddie, Chowdhary, Neerja, Connor, Myles, Cross, Helen, Collinson, Mark, Darkwa, Emmanuel, Denison, Timothy, Doku, Victor, Dua, Tarun, Egesa, Isaac, Godi, Tony, Gómez-Olivé, F. Xavier, Grassi, Simone, Iddi, Samuel, Junior, Daniel Nana Yaw Abankwah, Kahn, Kathleen, Kakooza, Angelina, Kariuki, Symon, Kamuyu, Gathoni, Khalayi, Clarah, Kimambo, Henrika, Kleinschmidt, Immo, Kwasa, Thomas, and McDaid, David

Abstract

Background: Identification of convulsive epilepsy in sub-Saharan Africa relies on access to resources that are often unavailable. Infrastructure and resource requirements can further complicate case verification. Using machine-learning techniques, we have developed and tested a region-specific questionnaire panel and predictive model to identify people who have had a convulsive seizure. These findings have been implemented into a free app for health-care workers in Kenya, Uganda, Ghana, Tanzania, and South Africa. Methods: In this retrospective case-control study, we used data from the Studies of the Epidemiology of Epilepsy in Demographic Sites in Kenya, Uganda, Ghana, Tanzania, and South Africa. We randomly split these individuals using a 7:3 ratio into a training dataset and a validation dataset. We used information gain and correlation-based feature selection to identify eight binary features to predict convulsive seizures. We then assessed several machine-learning algorithms to create a multivariate prediction model. We validated the best-performing model with the internal dataset and a prospectively collected external-validation dataset. We additionally evaluated a leave-one-site-out model (LOSO), in which the model was trained on data from all sites except one that, in turn, formed the validation dataset. We used these features to develop a questionnaire-based predictive panel that we implemented into a multilingual app (the Epilepsy Diagnostic Companion) for health-care workers in each geographical region. Findings: We analysed epilepsy-specific data from 4097 people, of whom 1985 (48·5%) had convulsive epilepsy, and 2112 were controls. From 170 clinical variables, we initially identified 20 candidate predictor features. Eight features were removed, six because of negligible information gain and two following review by a panel of qualified neurologists. Correlation-based feature selection identified eight variables that demonstrated predictive value; all wer

46. Identifying Merozoite Targets of Protective Immunity Against Plasmodium falciparum Malaria

Author

Kamuyu, Gathoni and Kamuyu, Gathoni

Abstract

The observation that individuals living in malaria endemic regions who are repeatedly infected with P. falciparum can acquire immunity, first to severe, then to uncomplicated clinical episodes of malaria, and finally to high parasite densities, provides hope that a vaccine is achievable. Immunoglobulins have been identified as a key component of naturally acquired immunity and identifying the targets and mechanisms by which this protection is achieved is a clear research priority. To date, only a small proportion of the parasite proteome has been evaluated in the context of naturally acquired immunity. This thesis was aimed at contributing to this knowledge gap by identifying novel potential antigen targets of protective antibodies and validating these in samples from Tanzanian adults. First, to identify merozoite antigens that were immunogenic, I resolved proteins extracted from P. falciparum merozoites by two-dimensional gel electrophoresis and tested these for reactivity with immunoglobulins from malaria immune adults. Immunoreactive proteins were then identified by mass-spectrometry. In complementary studies, purified P. falciparum merozoites were treated with proteolytic enzymes to release proteins localised on the surface of merozoites, which were subsequently identified by mass-spectrometry. Using stringent criteria, where I combined the data obtained from 2D-immunoblots and surface-trypsinization experiments with bioinformatics prediction (for the presence of a signal peptide and/or transmembrane domain), I narrowed down to 222 potential merozoite vaccine targets. These included known surface and/or immunogenic proteins such as the 6-cysteine proteins (Pf12, Pf38, Pf41), MSP-1, 3, 7, 9, 10, GLURP, AMA1, GAMA, MTRAP, LSA3 and RhopH3 as well as many unstudied proteins. From the set of unstudied proteins, I prioritised 27 antigens for immunoprofiling and identified 19 antigens that are targets of naturally acquired antibo

48. Binding of Plasmodium falciparum Merozoite Surface Proteins DBLMSP and DBLMSP2 to Human Immunoglobulin MIs Conserved among Broadly Diverged Sequence Variants.

Author

Crosnier, Cécile, Iqbal, Zamin, Knuepfer, Ellen, Maciuca, Sorina, Perrin, Abigail J., Kamuyu, Gathoni, Goulding, David, Bustamante, Leyla Y., Miles, Alistair, Moore, Shona C., Dougan, Gordon, Holder, Anthony A., Kwiatkowski, Dominic P., Rayner, Julian C., Pleass, Richard J., and Wright, Gavin J.

Subjects
*PLASMODIUM falciparum, *MEROZOITES, *PROTEIN binding, *IMMUNOGLOBULINS, *NUCLEOTIDE sequencing, *MALARIA, *GENETICS
Abstract

Diversity at pathogen genetic loci can be driven by host adaptive immune selection pressure and may reveal proteins important for parasite biology. Population-based genome sequencing of Plasmodium falciparum, the parasite responsible for the most severe form of malaria, has highlighted two related polymorphic genes called dblmsp and dblmsp2, which encode Duffy binding-like (DBL) domain-containing proteins located on the merozoite surface but whose function remains unknown. Using recombinant proteins and transgenic parasites, we show that DBLMSP and DBLMSP2 directly and avidly bind human IgM via their DBL domains. We used whole genome sequence data from over 400 African and Asian P. falciparum isolates to show that dblmsp and dblmsp2 exhibit extreme protein polymorphism in their DBL domain, with multiple variants of two major allelic classes present in every population tested. Despite this variability, the IgM binding function was retained across diverse sequence representatives. Although this interaction did not seem to have an effect on the ability of the parasite to invade red blood cells, binding ofDBLMSPandDBLMSP2to IgM inhibited the overall immunoreactivity of these proteins to IgG from patients who had been exposed to the parasite. This suggests that IgM binding might mask these proteins from the host humoral immune system. [ABSTRACT FROM AUTHOR]

Published
2016
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49. Driving consistency: CEPI-Centralized Laboratory Network's conversion factor initiative for SARS-CoV-2 clinical assays used for efficacy assessment of COVID vaccines.

Author

Azizi A, Kamuyu G, Ogbeni D, Levesque-Damphousse P, Knott D, Gagnon L, Phay-Tran S, Hussey B, Proud P, Charlton S, Clark C, and Bernasconi V

Subjects
Humans, Reproducibility of Results, Vaccine Efficacy, World Health Organization, Clinical Laboratory Techniques methods, Clinical Laboratory Techniques standards, COVID-19 Vaccines immunology, COVID-19 prevention & control, SARS-CoV-2 immunology
Abstract

To date, thousands of SARS-CoV-2 samples from many vaccine developers have been tested within the CEPI-Centralized Laboratory Network. To convert data from each clinical assay to international standard units, the WHO international standard and the CEPI standard generated by the Medicines and Healthcare products Regulatory Agency were run in multiple facilities to determine the conversion factor for each assay. Reporting results in international units advances global understanding of SARS-CoV-2 immunity and vaccine efficacy, enhancing the quality, reliability, and utility of clinical assay data.

Published
2024
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50. Sequential Vaccination With Heterologous Acinetobacter baumannii Strains Induces Broadly Reactive Antibody Responses.

Author

Kamuyu G, Suen Cheng Y, Willcocks S, Kewcharoenwong C, Kiratisin P, Taylor PW, Wren BW, Lertmemongkolchai G, Stabler RA, and Brown J

Subjects
Animals, Female, Humans, Mice, Acinetobacter baumannii immunology, Antibodies, Bacterial immunology, Antibody Formation, Bacterial Vaccines immunology, Vaccination
Abstract

Antibody therapy may be an alternative treatment option for infections caused by the multi-drug resistant (MDR) bacterium Acinetobacter baumannii. As A. baumannii has multiple capsular serotypes, a universal antibody therapy would need to target conserved protein antigens rather than the capsular polysaccharides. We have immunized mice with single or multiple A. baumannii strains to induce antibody responses to protein antigens, and then assessed whether these responses provide cross-protection against a collection of genetically diverse clinical A. baumannii isolates. Immunized mice developed antibody responses to multiple protein antigens. Flow cytometry IgG binding assays and immunoblots demonstrated improved recognition of both homologous and heterologous clinical strains in sera from mice immunized with multiple strains compared to a single strain. The capsule partially inhibited bacterial recognition by IgG and the promotion of phagocytosis by human neutrophils. However, after immunization with multiple strains, serum antibodies to protein antigens promoted neutrophil phagocytosis of heterologous A. baumannii strains. In an infection model, mice immunized with multiple strains had lower bacterial counts in the spleen and liver following challenge with a heterologous strain. These data demonstrate that antibodies targeting protein antigens can improve immune recognition and protection against diverse A. baumannii strains, providing support for their use as an antibody therapy., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Kamuyu, Suen Cheng, Willcocks, Kewcharoenwong, Kiratisin, Taylor, Wren, Lertmemongkolchai, Stabler and Brown.)

Published
2021
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