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Dive into the research topics where Claire Heath is active.

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Featured researches published by Claire Heath.


Open Forum Infectious Diseases | 2017

Malaria and Chikungunya Detected Using Molecular Diagnostics Among Febrile Kenyan Children

Jesse J. Waggoner; Julie Brichard; Francis M. Mutuku; Bryson Ndenga; Claire Heath; Alisha Mohamed-Hadley; Malaya K. Sahoo; John M. Vulule; Martina I. Lefterova; Niaz Banaei; Dunstan Mukoko; Benjamin A. Pinsky; A. Desiree LaBeaud

Abstract Background In sub-Saharan Africa, malaria is frequently overdiagnosed as the cause of an undifferentiated febrile illness, whereas arboviral illnesses are presumed to be underdiagnosed. Methods Sera from 385 febrile Kenyan children, who presented to 1 of 4 clinical sites, were tested using microscopy and real-time molecular assays for dengue virus (DENV), chikungunya virus (CHIKV), malaria, and Leptospira. Results Malaria was the primary clinical diagnosis for 254 patients, and an arboviral infection (DENV or CHIKV) was the primary diagnosis for 93 patients. In total, 158 patients (41.0%) had malaria and 32 patients (8.3%) had CHIKV infections. Compared with real-time polymerase chain reaction, microscopy demonstrated a percent positive agreement of 49.7%. The percentage of malaria cases detected by microscopy varied significantly between clinical sites. Arboviral infections were the clinical diagnosis for patients on the Indian Ocean coast (91 of 238, 38.2%) significantly more often than patients in the Lake Victoria region (2 of 145, 1.4%; P < .001). However, detection of CHIKV infections was significantly higher in the Lake Victoria region (19 of 145 [13.1%] vs 13 of 239 [5.4%]; P = .012). Conclusions The clinical diagnosis of patients with an acute febrile illness, even when aided by microscopy, remains inaccurate in malaria-endemic areas, contributing to inappropriate management decisions.


Open Forum Infectious Diseases | 2018

The Identification of Risk Factors for Chronic Chikungunya Arthralgia in Grenada, West Indies: A Cross-Sectional Cohort Study

Claire Heath; Jason Lowther; Tp Noël; Idis Mark-George; Derek B. Boothroyd; George Mitchell; C. N. L. Macpherson; A. Desiree LaBeaud

Abstract Background Chikungunya virus (CHIKV) is a re-emerging arboviral pathogen. In 2014, an explosive CHIKV outbreak occurred in Grenada, West Indies, infecting approximately 60% of the population. In approximately 50% of cases, CHIKV infection transitions to painful arthralgia that can persist for years. Elucidation of the risk factors for chronic disease is imperative to the development of effective risk management strategies and specific therapeutics. Methods We conducted a cross-sectional study of 240 people who were tested for CHIKV during the outbreak. We administered questionnaires to examine demographic, behavioral, psychological, social, and environmental factors to identify associations with chronic disease. Physical examinations were performed and persistent symptoms were recorded. Results Ethnicity and socioeconomic status were not associated with risk of chronic joint pain. Female sex increased risk, and age was demonstrated to be predictive of chronic CHIKV sequelae. Mosquito avoidance behaviors did not reduce risk. Patients suffering joint pains, generalized body ache, and weakness in the extremities during acute infection were more likely to develop chronic arthralgia, and an increased duration of acute disease also increased risk. Conclusions These data demonstrate that chronic CHIKV affects people across the ethnic and socioeconomic spectrum, and it is not reduced by vector avoidance activity. Increased duration of acute symptoms, in particular acute joint pain, was strongly correlated with the risk of persistent arthralgia, thus effective clinical management of acute CHIKV disease could reduce burden of chronic CHIKV.


Emerging Infectious Diseases | 2017

Unrecognized Dengue Virus Infections in Children, Western Kenya, 2014–2015

David Vu; Noah Mutai; Claire Heath; John M. Vulule; Francis M. Mutuku; Bryson Ndenga; A. Desiree LaBeaud

We detected a cluster of dengue virus infections in children in Kenya during July 2014–June 2015. Most cases were serotype 1, but we detected all 4 serotypes, including co-infections with 2 serotypes. Our findings implicate dengue as a cause of febrile illness in this population and highlight a need for robust arbovirus surveillance.


American Journal of Tropical Medicine and Hygiene | 2018

Nasopharyngeal carriage of streptococcus pneumoniae in children in Coastal Kenya

Claire Heath; Monica Nayakwadi-Singer; Charles H. King; Indu Malhotra; Francis M. Mutuku; Dunstan Mukoko; A. Desiree LaBeaud

Streptococcus pneumoniae (SP) is a leading cause of child mortality globally, killing around half a million children aged 5 years and less per year. Nasopharyngeal carriage of SP is a prerequisite to disease, and the prevalence of colonization reaches 100% within the first few years of life. Serotype prevalence varies geographically, impacting the serotype coverage of pneumococcal vaccines, and serotype prevalence data are limited from large regions of the world, including sub-Saharan Africa. We enrolled 323 unvaccinated children, aged 4-7 years from coastal Kenya and obtained nasopharyngeal swab samples before and after vaccination with the 10-valent pneumococcal vaccine. Vaccination did not reduce the overall prevalence of pneumococcal carriage in our cohort, with 65 (20%) children colonized before vaccination and 63 (19.4%) colonized postvaccination. However, the prevalence of vaccine-included serotypes (vaccine strains) declined from 43% to 19% of positive swabs, whereas non-vaccine serotypes increased from 46% to 73%. This study contributes to the few data available regarding pneumococcal carriage and serotype prevalence in Kenya and is in concordance with reports of dynamic serotype replacement, driven by vaccine pressure.


Pediatrics | 2017

Pneumococcal Vaccine Response After Exposure to Parasites in Utero, in Infancy, or Mid-Childhood

Monica Nayakwadi Singer; Claire Heath; Jackson Muinde; Virginia Gildengorin; Francis M. Mutuku; David Vu; Dunstan Mukoko; Christopher L. King; Indu Malhotra; Charles H. King; A. Desiree LaBeaud

This infant cohort study in Kenya found that pneumococcal vaccine response is not affected in children exposed to or infected with parasites. BACKGROUND AND OBJECTIVE: Streptococcus pneumoniae is a leading cause of mortality before age 5, but few studies examine details of childhood response to pneumococcal vaccine in less-developed settings. Although malnutrition, HIV, and concurrent infections can impair response, evidence suggests that chronic parasitic infections can also contribute to poor vaccination results. The objective of this study was to determine whether response to pneumococcal vaccine varied among children either exposed to parasitic infections in utero, previously infected in infancy, or infected at the time of immunization. METHODS: Children from a 2006 to 2010 maternal–infant cohort were eligible for the current study. Children were screened for malaria, schistosomiasis, filariasis, intestinal helminths, and protozoa. Data on in utero exposure and early life infections were linked, and baseline antipneumococcal immunoglobulin G levels and nasopharyngeal carrier status were determined. Participants received decavalent pneumococcal vaccine, and 4 weeks later, serology was repeated to assess vaccine response. RESULTS: A total of 281 children were included. Preimmunity was associated with greater postvaccination increments in anti–pneumococcal polysaccharide immunoglobulin G, especially serotypes 4, 7, 9, 18C, and 19. Present-day growth stunting was independently associated with weaker responses to 1, 4, 6B, 7, 9V, and 19. Previous exposure to Trichuris was associated with stronger responses to 1, 5, 6B, 7, 18C, and 23, but other parasite exposures were not consistently associated with response. CONCLUSIONS: In our cohort, hyporesponsiveness to pneumococcal conjugate vaccine was associated with growth stunting but not parasite exposure. Parasite-related vaccine response deficits identified before age 3 do not persist into later childhood.


Annals of global health | 2016

Dengue virus and malaria co-infection in Kenyan children

David Vu; K. Ripp; N. Mutai; Bryson Ndenga; Claire Heath; A.D. LaBeaud


American Journal of Tropical Medicine and Hygiene | 2017

Development of a Real-Time Reverse Transcription Polymerase Chain Reaction for O’nyong-nyong Virus and Evaluation with Clinical and Mosquito Specimens from Kenya

Jesse J. Waggoner; Claire Heath; Bryson Ndenga; Francis M. Mutuku; Malaya K. Sahoo; Alisha Mohamed-Hadley; John M. Vulule; Dunstan Mukoko; A. Desiree LaBeaud; Benjamin A. Pinsky


Open Forum Infectious Diseases | 2016

Identification of factors associated with chronic chikungunya disease in patients in Grenada, West Indies.

Claire Heath; Jason Lowther; Tp Noël; Idis Mark-George; Derek B. Boothroyd; C. N. L. Macpherson; A. Desiree LaBeaud


Open Forum Infectious Diseases | 2016

Dengue Viremia in Kenyan children With Acute Febrile Illness

David Vu; Noah Mutai; Claire Heath; Bryson Ndenga; A. Desiree LaBeaud


Journal of health disparities research and practice | 2016

Detection of Dengue Virus in Acutely Febrile Children in Kenya

Raymond Thicklin; Claire Heath; Elysse Grossi-Soyster; David Vu; Angelle Desiree Lebeaud

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Bryson Ndenga

Kenya Medical Research Institute

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Francis M. Mutuku

Technical University of Mombasa

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Dunstan Mukoko

University of California

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John M. Vulule

Kenya Medical Research Institute

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Charles H. King

Case Western Reserve University

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