Your search keyword '"Eunice W. Kagucia"' showing total 14 results

1. Temporal trends of SARS-CoV-2 seroprevalence during the first wave of the COVID-19 epidemic in Kenya

Author

Ifedayo M. O. Adetifa, Sophie Uyoga, John N. Gitonga, Daisy Mugo, Mark Otiende, James Nyagwange, Henry K. Karanja, James Tuju, Perpetual Wanjiku, Rashid Aman, Mercy Mwangangi, Patrick Amoth, Kadondi Kasera, Wangari Ng’ang’a, Charles Rombo, Christine Yegon, Khamisi Kithi, Elizabeth Odhiambo, Thomas Rotich, Irene Orgut, Sammy Kihara, Christian Bottomley, Eunice W. Kagucia, Katherine E. Gallagher, Anthony Etyang, Shirine Voller, Teresa Lambe, Daniel Wright, Edwine Barasa, Benjamin Tsofa, Philip Bejon, Lynette I. Ochola-Oyier, Ambrose Agweyu, J. Anthony G. Scott, and George M. Warimwe

Subjects

Science

Abstract

The reported burden of SARS-CoV-2 has been relatively low in tropical Africa compared to Europe and the Americas, but estimating true infection rates is challenging. Here, the authors screen blood donors in Kenya for SARS-CoV-2 antibodies and describe spatiotemporal seroprevalence dynamics.

Published

2021

2. SARS-CoV-2 seroprevalence in three Kenyan health and demographic surveillance sites, December 2020-May 2021

Author

Anthony O. Etyang, Ifedayo Adetifa, Richard Omore, Thomas Misore, Abdhalah K. Ziraba, Maurine A. Ng’oda, Evelyn Gitau, John Gitonga, Daisy Mugo, Bernadette Kutima, Henry Karanja, Monica Toroitich, James Nyagwange, James Tuju, Perpetual Wanjiku, Rashid Aman, Patrick Amoth, Mercy Mwangangi, Kadondi Kasera, Wangari Ng’ang’a, Donald Akech, Antipa Sigilai, Boniface Karia, Angela Karani, Shirine Voller, Charles N. Agoti, Lynette I. Ochola-Oyier, Mark Otiende, Christian Bottomley, Amek Nyaguara, Sophie Uyoga, Katherine Gallagher, Eunice W. Kagucia, Dickens Onyango, Benjamin Tsofa, Joseph Mwangangi, Eric Maitha, Edwine Barasa, Philip Bejon, George M. Warimwe, J. Anthony G. Scott, and Ambrose Agweyu

Subjects

Public aspects of medicine, RA1-1270

Abstract

Background Most of the studies that have informed the public health response to the COVID-19 pandemic in Kenya have relied on samples that are not representative of the general population. We conducted population-based serosurveys at three Health and Demographic Surveillance Systems (HDSSs) to determine the cumulative incidence of infection with SARS-CoV-2. Methods We selected random age-stratified population-based samples at HDSSs in Kisumu, Nairobi and Kilifi, in Kenya. Blood samples were collected from participants between 01 Dec 2020 and 27 May 2021. No participant had received a COVID-19 vaccine. We tested for IgG antibodies to SARS-CoV-2 spike protein using ELISA. Locally-validated assay sensitivity and specificity were 93% (95% CI 88–96%) and 99% (95% CI 98–99.5%), respectively. We adjusted prevalence estimates using classical methods and Bayesian modelling to account for the sampling scheme and assay performance. Results We recruited 2,559 individuals from the three HDSS sites, median age (IQR) 27 (10–78) years and 52% were female. Seroprevalence at all three sites rose steadily during the study period. In Kisumu, Nairobi and Kilifi, seroprevalences (95% CI) at the beginning of the study were 36.0% (28.2–44.4%), 32.4% (23.1–42.4%), and 14.5% (9.1–21%), and respectively; at the end they were 42.0% (34.7–50.0%), 50.2% (39.7–61.1%), and 24.7% (17.5–32.6%), respectively. Seroprevalence was substantially lower among children (Conclusion By May 2021 in three broadly representative populations of unvaccinated individuals in Kenya, seroprevalence of anti-SARS-CoV-2 IgG was 25–50%. There was wide variation in cumulative incidence by location and age.

Published

2022

3. Evaluation of Dried Blood and Cerebrospinal Fluid Filter Paper Spots for Storing and Transporting Clinical Material for the Molecular Diagnosis of Invasive Meningococcal Disease

Author

Brenda A. Kwambana-Adams, Stephen A. Clark, Nicole Tay, Schadrac Agbla, Chrispin Chaguza, Eunice W. Kagucia, Ray Borrow, and Robert S. Heyderman

Subjects

Neisseria meningitidis, invasive meningococcal disease, meningitis, bacteraemia, dried filter paper spot, cerebrospinal fluid, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

To improve the storage and transport of clinical specimens for the diagnosis of Neisseria meningitidis (Nm) infections in resource-limited settings, we have evaluated the performance of dried blood spot (DBS) and dried cerebrospinal fluid spot (DCS) assays. DBS and DCS were prepared on filter paper from liquid specimens previously tested for Nm in the United Kingdom. Nm was detected and genogrouped by real-time PCR performed on crude genomic DNA extracted from the DBS (n = 226) and DCS (n = 226) specimens. Targeted whole-genome sequencing was performed on a subset of specimens, DBS (n = 4) and DCS (n = 6). The overall agreement between the analysis of liquid and dried specimens was (94.2%; 95% CI 90.8–96.7) for blood and (96.4%; 95% CI 93.5–98.0) for cerebrospinal fluid. Relative to liquid specimens as the reference, the DBS and DCS assays had sensitivities of (89.1%; 95% CI 82.7–93.8) and (94.2%; 95% CI 88.9–97.5), respectively, and both assays had specificities above 98%. A genogroup was identified by dried specimen analysis for 81.9% of the confirmed meningococcal infections. Near full-length Nm genome sequences (>86%) were obtained for all ten specimens tested which allowed determination of the sequence type, clonal complex, presence of antimicrobial resistance and other meningococcal genotyping. Dried blood and CSF filter spot assays offer a practical alternative to liquid specimens for the molecular and genomic characterisation of invasive meningococcal diseases in low-resource settings.

Published

2022

4. Global Landscape Review of Serotype-Specific Invasive Pneumococcal Disease Surveillance among Countries Using PCV10/13: The Pneumococcal Serotype Replacement and Distribution Estimation (PSERENADE) Project

Author

Maria Deloria Knoll, Julia C. Bennett, Maria Garcia Quesada, Eunice W. Kagucia, Meagan E. Peterson, Daniel R. Feikin, Adam L. Cohen, Marissa K. Hetrich, Yangyupei Yang, Jenna N. Sinkevitch, Krow Ampofo, Laurie Aukes, Sabrina Bacci, Godfrey Bigogo, Maria-Cristina C. Brandileone, Michael G. Bruce, Romina Camilli, Jesús Castilla, Guanhao Chan, Grettel Chanto Chacón, Pilar Ciruela, Heather Cook, Mary Corcoran, Ron Dagan, Kostas Danis, Sara de Miguel, Philippe De Wals, Stefanie Desmet, Yvonne Galloway, Theano Georgakopoulou, Laura L. Hammitt, Markus Hilty, Pak-Leung Ho, Sanjay Jayasinghe, James D. Kellner, Jackie Kleynhans, Mirjam J. Knol, Jana Kozakova, Karl Gústaf Kristinsson, Shamez N. Ladhani, Claudia S. Lara, Maria Eugenia León, Tiia Lepp, Grant A. Mackenzie, Lucia Mad’arová, Allison McGeer, Tuya Mungun, Jason M. Mwenda, J. Pekka Nuorti, Néhémie Nzoyikorera, Kazunori Oishi, Lucia Helena De Oliveira, Metka Paragi, Tamara Pilishvili, Rodrigo Puentes, Eric Rafai, Samir K. Saha, Larisa Savrasova, Camelia Savulescu, J. Anthony Scott, Kevin J. Scott, Fatima Serhan, Lena Petrova Setchanova, Nadja Sinkovec Zorko, Anna Skoczyńska, Todd D. Swarthout, Palle Valentiner-Branth, Mark van der Linden, Didrik F. Vestrheim, Anne von Gottberg, Inci Yildirim, Kyla Hayford, and the PSERENADE Team

Subjects

global, invasive pneumococcal disease, pneumococcal meningitis, surveillance, pneumococcal conjugate vaccines, Biology (General), QH301-705.5

Abstract

Serotype-specific surveillance for invasive pneumococcal disease (IPD) is essential for assessing the impact of 10- and 13-valent pneumococcal conjugate vaccines (PCV10/13). The Pneumococcal Serotype Replacement and Distribution Estimation (PSERENADE) project aimed to evaluate the global evidence to estimate the impact of PCV10/13 by age, product, schedule, and syndrome. Here we systematically characterize and summarize the global landscape of routine serotype-specific IPD surveillance in PCV10/13-using countries and describe the subset that are included in PSERENADE. Of 138 countries using PCV10/13 as of 2018, we identified 109 with IPD surveillance systems, 76 of which met PSERENADE data collection eligibility criteria. PSERENADE received data from most (n = 63, 82.9%), yielding 240,639 post-PCV10/13 introduction IPD cases. Pediatric and adult surveillance was represented from all geographic regions but was limited from lower income and high-burden countries. In PSERENADE, 18 sites evaluated PCV10, 42 PCV13, and 17 both; 17 sites used a 3 + 0 schedule, 38 used 2 + 1, 13 used 3 + 1, and 9 used mixed schedules. With such a sizeable and generally representative dataset, PSERENADE will be able to conduct robust analyses to estimate PCV impact and inform policy at national and global levels regarding adult immunization, schedule, and product choice, including for higher valency PCVs on the horizon.

Published

2021

5. Changes in Invasive Pneumococcal Disease Caused by Streptococcus pneumoniae Serotype 1 following Introduction of PCV10 and PCV13: Findings from the PSERENADE Project

Author

Julia C. Bennett, Marissa K. Hetrich, Maria Garcia Quesada, Jenna N. Sinkevitch, Maria Deloria Knoll, Daniel R. Feikin, Scott L. Zeger, Eunice W. Kagucia, Adam L. Cohen, Krow Ampofo, Maria-Cristina C. Brandileone, Dana Bruden, Romina Camilli, Jesús Castilla, Guanhao Chan, Heather Cook, Jennifer E. Cornick, Ron Dagan, Tine Dalby, Kostas Danis, Sara de Miguel, Philippe De Wals, Stefanie Desmet, Theano Georgakopoulou, Charlotte Gilkison, Marta Grgic-Vitek, Laura L. Hammitt, Markus Hilty, Pak-Leung Ho, Sanjay Jayasinghe, James D. Kellner, Jackie Kleynhans, Mirjam J. Knol, Jana Kozakova, Karl G. Kristinsson, Shamez N. Ladhani, Laura MacDonald, Grant A. Mackenzie, Lucia Mad’arová, Allison McGeer, Jolita Mereckiene, Eva Morfeldt, Tuya Mungun, Carmen Muñoz-Almagro, J. Pekka Nuorti, Metka Paragi, Tamara Pilishvili, Rodrigo Puentes, Samir K. Saha, Aalisha Sahu Khan, Larisa Savrasova, J. Anthony Scott, Anna Skoczyńska, Shigeru Suga, Mark van der Linden, Jennifer R. Verani, Anne von Gottberg, Brita A. Winje, Inci Yildirim, Khalid Zerouali, Kyla Hayford, and the PSERENADE Team

Subjects

invasive pneumococcal disease, pneumococcal conjugate vaccines, serotypes, vaccine impact, Biology (General), QH301-705.5

Abstract

Streptococcus pneumoniae serotype 1 (ST1) was an important cause of invasive pneumococcal disease (IPD) globally before the introduction of pneumococcal conjugate vaccines (PCVs) containing ST1 antigen. The Pneumococcal Serotype Replacement and Distribution Estimation (PSERENADE) project gathered ST1 IPD surveillance data from sites globally and aimed to estimate PCV10/13 impact on ST1 IPD incidence. We estimated ST1 IPD incidence rate ratios (IRRs) comparing the pre-PCV10/13 period to each post-PCV10/13 year by site using a Bayesian multi-level, mixed-effects Poisson regression and all-site IRRs using a linear mixed-effects regression (N = 45 sites). Following PCV10/13 introduction, the incidence rate (IR) of ST1 IPD declined among all ages. After six years of PCV10/13 use, the all-site IRR was 0.05 (95% credibility interval 0.04–0.06) for all ages, 0.05 (0.04–0.05) for

Published

2021

6. Quantifying previous SARS-CoV-2 infection through mixture modelling of antibody levels

Author

Anthony Etyang, James Nyagwange, Ambrose Agweyu, Ifedayo M. O. Adetifa, John N. Gitonga, Christian Bottomley, George M. Warimwe, Eunice W. Kagucia, David James Nokes, Sophie Uyoga, Daisy Mugo, Henry K. Karanja, Jacob G. Scott, Katherine E. Gallagher, and M. Otiende

Subjects

Statistical methods, Coronavirus disease 2019 (COVID-19), Epidemiology, Science, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Population, General Physics and Astronomy, Antibody level, Antibodies, Viral, Sensitivity and Specificity, Article, General Biochemistry, Genetics and Molecular Biology, COVID-19 Serological Testing, 03 medical and health sciences, External data, 0302 clinical medicine, Bias, Seroepidemiologic Studies, Statistics, Humans, Mixture modelling, 030212 general & internal medicine, Sensitivity (control systems), education, 030304 developmental biology, Mathematics, 0303 health sciences, education.field_of_study, Models, Statistical, Multidisciplinary, SARS-CoV-2, Infectious-disease diagnostics, COVID-19, General Chemistry, Mixture model, Kenya, QR, 3. Good health, RA

Abstract

As countries decide on vaccination strategies and how to ease movement restrictions, estimating the proportion of the population previously infected with SARS-CoV-2 is important for predicting the future burden of COVID-19. This proportion is usually estimated from serosurvey data in two steps: first the proportion above a threshold antibody level is calculated, then the crude estimate is adjusted using external estimates of sensitivity and specificity. A drawback of this approach is that the PCR-confirmed cases used to estimate the sensitivity of the threshold may not be representative of cases in the wider population—e.g., they may be more recently infected and more severely symptomatic. Mixture modelling offers an alternative approach that does not require external data from PCR-confirmed cases. Here we illustrate the bias in the standard threshold-based approach by comparing both approaches using data from several Kenyan serosurveys. We show that the mixture model analysis produces estimates of previous infection that are often substantially higher than the standard threshold analysis., The proportion of a population that has previously been infected by a pathogen is typically estimated using antibody thresholds adjusted for sensitivity and specificity. Here, the authors present a model-based alternative to threshold methods which accounts for antibody waning and other sources of spectrum bias.

Published

2021

7. Changes in Invasive Pneumococcal Disease Caused by Streptococcus pneumoniae Serotype 1 following Introduction of PCV10 and PCV13: Findings from the PSERENADE Project

Author

Laura MacDonald, Dana Bruden, Scott L. Zeger, Guanhao Chan, Jenna N. Sinkevitch, Karl Gústaf Kristinsson, Khalid Zerouali, Adam L. Cohen, Anne von Gottberg, Eva Morfeldt, Eunice W. Kagucia, Mark van der Linden, Markus Hilty, Stefanie Desmet, Sanjay Jayasinghe, Jolita Mereckiene, Maria Garcia Quesada, Krow Ampofo, Shigeru Suga, Rodrigo Puentes, Grant A. Mackenzie, Sara de Miguel, Daniel R. Feikin, Metka Paragi, J. Anthony G. Scott, Jesus Castilla, Jennifer E. Cornick, Heather Cook, Samir K. Saha, Larisa Savrasova, Kyla Hayford, Kostas Danis, Romina Camilli, Charlotte Gilkison, Jana Kozakova, Julia C. Bennett, Ron Dagan, Shamez N Ladhani, Tuya Mungun, Philippe De Wals, Aalisha Sahu Khan, Theano Georgakopoulou, Maria Deloria Knoll, Inci Yildirim, Laura L. Hammitt, Marta Grgic-Vitek, Marissa K. Hetrich, Jennifer R. Verani, Carmen Muñoz-Almagro, Anna Skoczynska, Lucia Mad'arova, Mirjam J Knol, Brita Askeland Winje, Tamara Pilishvili, Pak-Leung Ho, Maria-Cristina C. Brandileone, J. Pekka Nuorti, Tine Dalby, Jackie Kleynhans, Allison McGeer, James D. Kellner, Team, PSERENADE, Tampere University, and Health Sciences

Subjects

Vacunas, 0301 basic medicine, Serotype, Pediatrics, MENINGITIS, Antígens, Vacunes, 0302 clinical medicine, invasive pneumococcal disease, Credible interval, Immunologia, 030212 general & internal medicine, PROTECTION, lcsh:QH301-705.5, Vaccines, Pneumococs, Incidence (epidemiology), pneumococcal conjugate vaccines, Antígenos, Pneumococcus, Data availability, 3142 Public health care science, environmental and occupational health, Streptococcus pneumoniae, symbols, Life Sciences & Biomedicine, CONJUGATE VACCINE, Microbiology (medical), medicine.medical_specialty, serotypes, Pneumococcal disease, Streptococcus pneumoniae serotype, Immunology, 030106 microbiology, vaccine impact, Inmunología, Microbiology, 03 medical and health sciences, symbols.namesake, Virology, medicine, Poisson regression, Antigens, Disease burden, BURKINA-FASO, Science & Technology, business.industry, 500 Science, bacterial infections and mycoses, EARLY IMPACT, n/a, lcsh:Biology (General), 570 Life sciences, biology, business

Abstract

Streptococcus pneumoniae serotype 1 (ST1) was an important cause of invasive pneumococcaldisease (IPD) globally before the introduction of pneumococcal conjugate vaccines (PCVs) containingST1 antigen. The Pneumococcal Serotype Replacement and Distribution Estimation (PSERENADE)project gathered ST1 IPD surveillance data from sites globally and aimed to estimatePCV10/13 impact on ST1 IPD incidence. We estimated ST1 IPD incidence rate ratios (IRRs) comparingthe pre‐PCV10/13 period to each post‐PCV10/13 year by site using a Bayesian multi‐level, mixedeffectsPoisson regression and all‐site IRRs using a linear mixed‐effects regression (N = 45 sites).Following PCV10/13 introduction, the incidence rate (IR) of ST1 IPD declined among all ages. Aftersix years of PCV10/13 use, the all‐site IRR was 0.05 (95% credibility interval 0.04–0.06) for all ages,0.05 (0.04–0.05) for &lt, 5 years of age, 0.08 (0.06–0.09) for 5–17 years, 0.06 (0.05–0.08) for 18–49 years,0.06 (0.05–0.07) for 50–64 years, and 0.05 (0.04–0.06) for ≥65 years. PCV10/13 use in infant immunizationprograms was followed by a 95% reduction in ST1 IPD in all ages after approximately 6years. Limited data availability from the highest ST1 disease burden countries using a 3+0 scheduleconstrains generalizability and data from these settings are needed.

Published

2021

8. Global Landscape Review of Serotype-Specific Invasive Pneumococcal Disease Surveillance among Countries Using PCV10/13: The Pneumococcal Serotype Replacement and Distribution Estimation (PSERENADE) Project

Author

Jason M. Mwenda, Grant A. Mackenzie, Marissa K. Hetrich, Michael G. Bruce, Maria-Cristina C. Brandileone, Sabrina Bacci, J. Anthony G. Scott, Fatima Serhan, Karl Gústaf Kristinsson, Stefanie Desmet, Camelia Savulescu, Sanjay Jayasinghe, Kyla Hayford, Laurie Aukes, Jana Kozakova, Laura L. Hammitt, Lúcia Helena de Oliveira, Philippe De Wals, Yangyupei Yang, Lucia Mad'arova, Julia C. Bennett, Grettel Chanto Chacón, Heather Cook, Sara de Miguel, Shamez N Ladhani, Markus Hilty, Maria Deloria Knoll, Adam L. Cohen, Kostas Danis, Romina Camilli, Maria Garcia Quesada, James D. Kellner, Guanhao Chan, Nadja Sinkovec Zorko, Mark van der Linden, Todd D. Swarthout, Eric Rafai, Jenna N. Sinkevitch, Claudia S. Lara, Anne von Gottberg, Inci Yildirim, Krow Ampofo, Rodrigo Puentes, J. Pekka Nuorti, Jesus Castilla, Tuya Mungun, Samir K. Saha, Pilar Ciruela, Jackie Kleynhans, Allison McGeer, Tamara Pilishvili, Theano Georgakopoulou, Kazunori Oishi, Anna Skoczynska, Eunice W. Kagucia, Pak-Leung Ho, Didrik F. Vestrheim, Néhémie Nzoyikorera, Daniel R. Feikin, Godfrey Bigogo, Larisa Savrasova, Ron Dagan, Tiia Lepp, Meagan E. Peterson, Mary Corcoran, Mirjam J Knol, Maria Eugenia Leon, Palle Valentiner-Branth, Yvonne Galloway, Lena Setchanova, Metka Paragi, Kevin J. Scott, Tampere University, Health Sciences, Medical Microbiology and Infection Prevention, and AII - Infectious diseases

Subjects

BACTERIAL-MENINGITIS, PNEUMONIA, AFRICA, 0301 basic medicine, Microbiology (medical), Serotype, Schedule, Pneumococcal disease, IMPACT, 030106 microbiology, Distribution (economics), CHILDREN, Microbiology, invasive pneumococcal disease, Article, 03 medical and health sciences, 0302 clinical medicine, Virology, Environmental health, EPIDEMIOLOGY, Medicine, 030212 general & internal medicine, qw_571, lcsh:QH301-705.5, Lower income, pneumococcal meningitis, Estimation, Science & Technology, Data collection, business.industry, pneumococcal conjugate vaccines, wc_217, MENINGITIS BELT, global, 3142 Public health care science, environmental and occupational health, Product choice, lcsh:Biology (General), CARRIAGE, surveillance, 570 Life sciences, biology, business, Life Sciences & Biomedicine, CONJUGATE VACCINE

Abstract

Serotype-specific surveillance for invasive pneumococcal disease (IPD) is essential for assessing the impact of 10- and 13-valent pneumococcal conjugate vaccines (PCV10/13). The Pneumococcal Serotype Replacement and Distribution Estimation (PSERENADE) project aimed to evaluate the global evidence to estimate the impact of PCV10/13 by age, product, schedule, and syndrome. Here we systematically characterize and summarize the global landscape of routine serotype-specific IPD surveillance in PCV10/13-using countries and describe the subset that are included in PSERENADE. Of 138 countries using PCV10/13 as of 2018, we identified 109 with IPD surveillance systems, 76 of which met PSERENADE data collection eligibility criteria. PSERENADE received data from most (n = 63, 82.9%), yielding 240,639 post-PCV10/13 introduction IPD cases. Pediatric and adult surveillance was represented from all geographic regions but was limited from lower income and high-burden countries. In PSERENADE, 18 sites evaluated PCV10, 42 PCV13, and 17 both, 17 sites used a 3 + 0 schedule, 38 used 2 + 1, 13 used 3 + 1, and 9 used mixed schedules. With such a sizeable and generally representative dataset, PSERENADE will be able to conduct robust analyses to estimate PCV impact and inform policy at national and global levels regarding adult immunization, schedule, and product choice, including for higher valency PCVs on the horizon.

Published

2021

9. Temporal trends of SARS-CoV-2 seroprevalence during the first wave of the COVID-19 epidemic in Kenya

Author

Henry K. Karanja, Lynette Isabella Ochola-Oyier, Sammy Kihara, Patrick Amoth, Anthony Etyang, Edwine Barasa, Christine Yegon, James Nyagwange, James Tuju, Shirine Voller, Kadondi Kasera, Wangari Ng’ang’a, Thomas Rotich, Charles Rombo, Teresa Lambe, Mark Otiende, Christian Bottomley, George M. Warimwe, Sophie Uyoga, J. Anthony G. Scott, Katherine E. Gallagher, Elizabeth Odhiambo, Khamisi Kithi, Rashid Aman, Philip Bejon, John N. Gitonga, Mercy Mwangangi, Irene Orgut, Ifedayo M. O. Adetifa, Ambrose Agweyu, Perpetual Wanjiku, Daniel B. Wright, Eunice W. Kagucia, Daisy Mugo, and Benjamin Tsofa

Subjects

Male, Epidemiology, viruses, General Physics and Astronomy, Antibodies, Viral, law.invention, 0302 clinical medicine, law, Seroepidemiologic Studies, Prevalence, 030212 general & internal medicine, skin and connective tissue diseases, Multidisciplinary, virus diseases, Middle Aged, 3. Good health, Transmission (mechanics), Geography, Spike Glycoprotein, Coronavirus, Test performance, Female, Adult, 2019-20 coronavirus outbreak, Coronavirus disease 2019 (COVID-19), Adolescent, Science, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), 030231 tropical medicine, Enzyme-Linked Immunosorbent Assay, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Young Adult, Population screening, Seroprevalence, Humans, Epidemics, Viral immunology, SARS-CoV-2, fungi, COVID-19, Bayes Theorem, General Chemistry, biochemical phenomena, metabolism, and nutrition, Kenya, body regions, Viral infection, Immunoglobulin G, Demography

Abstract

Observed SARS-CoV-2 infections and deaths are low in tropical Africa raising questions about the extent of transmission. We measured SARS-CoV-2 IgG by ELISA in 9,922 blood donors across Kenya and adjusted for sampling bias and test performance. By 1st September 2020, 577 COVID-19 deaths were observed nationwide and seroprevalence was 9.1% (95%CI 7.6-10.8%). Seroprevalence in Nairobi was 22.7% (18.0-27.7%). Although most people remained susceptible, SARS-CoV-2 had spread widely in Kenya with apparently low associated mortality., The reported burden of SARS-CoV-2 has been relatively low in tropical Africa compared to Europe and the Americas, but estimating true infection rates is challenging. Here, the authors screen blood donors in Kenya for SARS-CoV-2 antibodies and describe spatiotemporal seroprevalence dynamics.

Published

2021

10. Temporal trends of SARS-CoV-2 seroprevalence in transfusion blood donors during the first wave of the COVID-19 epidemic in Kenya

Author

Kadondi Kasera, Mercy Mwangangi, Anthony Etyang, Sammy Kihara, Shirine Voller, Ambrose Agweyu, Christian Bottomley, Perpetual Wanjiku, Irene Orgut, John N. Gitonga, J. Anthony G. Scott, Henry K. Karanja, Sophie Uyoga, Lynette Isabella Ochola-Oyier, Daniel B. Wright, Edwine Barasa, Elizabeth Odhiambo, James Nyagwange, Ifedayo M. O. Adetifa, Rashid Aman, George M. Warimwe, James Tuju, Benjamin Tsofa, Katherine E. Gallagher, Khamisi Kithi, Thomas Rotich, Eunice W. Kagucia, Wangari Ng’ang’a, Patrick Amoth, Philip Bejon, Daisy Mugo, Mark Otiende, Christine Yegon, Charles Rombo, and Teresa Lambe

Subjects

Transmission (mechanics), Coronavirus disease 2019 (COVID-19), business.industry, law, Environmental health, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), virus diseases, Medicine, Seroprevalence, Test performance, business, law.invention, Sampling bias

Abstract

Observed SARS-CoV-2 infections and deaths are low in tropical Africa raising questions about the extent of transmission. We measured SARS-CoV-2 IgG by ELISA in 9,922 blood donors across Kenya and adjusted for sampling bias and test performance. By 1st September 2020, 577 COVID-19 deaths were observed nationwide and seroprevalence was 9.1% (95%CI 7.6-10.8%). Seroprevalence in Nairobi was 22.7% (18.0-27.7%). Although most people remained susceptible, SARS-CoV-2 had spread widely in Kenya with apparently low associated mortality.

Published

2021

11. Sero-surveillance for IgG to SARS-CoV-2 at antenatal care clinics in two Kenyan referral hospitals

Author

Kadondi Kasera, Eunice W. Kagucia, Edwine Barasa, Christian Bottomley, John N. Gitonga, Adetifa Imo., Rabia Aziza, Leonard Ndwiga, Amek Nyaguara, Wangari Ng’ang’a, Scott Jag., Henry K. Karanja, James Tuju, Patrick Amoth, Lynette Isabella Ochola-Oyier, Lucy B. Ochola, Daisy Mugo, Sophie Uyoga, Edward Otieno, Charles N. Agoti, Benjamin Tsofa, Eddy Nzomo, Gideon Nyutu, Rashid Aman, Ruth Lucinde, S Agunda, Mercy Mwangangi, Anthony Etyang, George M. Warimwe, James Nyagwange, Katherine E. Gallagher, Philip Bejon, Evanson Kamuri, Mark Otiende, K Thuranira, Ambrose Agweyu, and Perpetual Wanjiku

Subjects

medicine.medical_specialty, Kenya, Referral, Obstetrics, business.industry, Transmission (medicine), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Pandemic, medicine, Seroprevalence, Igg elisa, business, Sero surveillance

Abstract

The high proportion of SARS-CoV-2 infections that remain undetected presents a challenge to tracking the progress of the pandemic and implementing control measures in Kenya. We determined the prevalence of IgG to SARS-CoV-2 in residual blood samples from mothers attending antenatal care services at 2 referral hospitals in Kenya. We used a validated IgG ELISA for SARS-Cov-2 spike protein and adjusted the results for assay sensitivity and specificity. In Kenyatta National Hospital, Nairobi, seroprevalence in August 2020 was 49.9% (95% CI 42.7-58.0). In Kilifi County Hospital seroprevalence increased from 1.3% (95% CI 0.04-4.7) in September to 11.0% (95% CI 6.2-16.7) in November 2020. There has been substantial, unobserved transmission of SARS-CoV-2 in parts of Nairobi and Kilifi Counties.

Published

2021

12. Seroprevalence of anti–SARS-CoV-2 IgG antibodies in Kenyan blood donors

Author

Elizabeth Odhiambo, Irene Orgut, Kadondi Kasera, George M. Warimwe, Ifedayo M. O. Adetifa, Shirine Voller, Christine Yegon, Wangari Ng’ang’a, Leonard Ndwiga, Christian Bottomley, Eunice W. Kagucia, Mark Otiende, Edwine Barasa, James Nyagwange, Charles Rombo, Teresa Lambe, Anthony Etyang, Ambrose Agweyu, Perpetual Wanjiku, J. Anthony G. Scott, Sophie Uyoga, Khamisi Kithi, James Tuju, Thomas Rotich, Daisy Mugo, Edward Otieno, Sammy Kihara, Daniel B. Wright, Zonia N. Mupe, Katherine E. Gallagher, Patrick Amoth, Charles N. Agoti, John N. Gitonga, Philip Bejon, Rashid Aman, Mercy Mwangangi, Henry K. Karanja, Lynette Isabella Ochola-Oyier, and Benjamin Tsofa

Subjects

Adult, 0301 basic medicine, Complete data, Kenya, medicine.medical_specialty, Adolescent, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Population, Blood Donors, Antibodies, Viral, Immunoglobulin G, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Medical microbiology, Seroepidemiologic Studies, Environmental health, Pandemic, Epidemiology, Global health, medicine, Humans, Seroprevalence, 030212 general & internal medicine, education, Aged, education.field_of_study, Multidisciplinary, biology, SARS-CoV-2, business.industry, Outbreak, virus diseases, COVID-19, Middle Aged, Multilevel regression, Confidence interval, 030104 developmental biology, Communicable Disease Control, biology.protein, Antibody, business, Demography

Abstract

BackgroundThere are no data on SARS-CoV-2 seroprevalence in Africa though the COVID-19 epidemic curve and reported mortality differ from patterns seen elsewhere. We estimated the anti-SARS-CoV-2 antibody prevalence among blood donors in Kenya.MethodsWe measured anti-SARS-CoV-2 spike IgG prevalence by ELISA on residual blood donor samples obtained between April 30 and June 16, 2020. Assay sensitivity and specificity were 83% (95% CI 59-96%) and 99.0% (95% CI 98.1-99.5%), respectively. National seroprevalence was estimated using Bayesian multilevel regression and post-stratification to account for non-random sampling with respect to age, sex and region, adjusted for assay performance.ResultsComplete data were available for 3098 of 3174 donors, aged 15-64 years. By comparison with the Kenyan population, the sample over- represented males (82% versus 49%), adults aged 25-34 years (40% versus 27%) and residents of coastal Counties (49% versus 9%). Crude overall seroprevalence was 5.6% (174/3098). Population-weighted, test- adjusted national seroprevalence was 5.2% (95% CI 3.7– 7.1%). Seroprevalence was highest in the 3 largest urban Counties - Mombasa (9.3% [95% CI 6.4-13.2%)], Nairobi (8.5% [95% CI 4.9-13.5%]) and Kisumu (6.5% [95% CI 3.3-11.2%]).ConclusionsWe estimate that 1 in 20 adults in Kenya had SARS-CoV-2 antibodies during the study period. By the median date of our survey, only 2093 COVID-19 cases and 71 deaths had been reported through the national screening system. This contrasts, by several orders of magnitude, with the numbers of cases and deaths reported in parts of Europe and America when seroprevalence was similar.

Published

2020

13. Individual level determinants for not receiving immunization, receiving immunization with delay, and being severely underimmunized among rural western Kenyan children

Author

David Obor, Katherine L. O'Brien, Benard Ochieng, Daniel R. Feikin, Dustin G. Gibson, Frank Odhiambo, and Eunice W. Kagucia

Subjects

Adult, Male, Rural Population, Pediatrics, medicine.medical_specialty, Adolescent, Cross-sectional study, Measles, Medication Adherence, Young Adult, Immunology and Microbiology(all), medicine, Humans, Young adult, Risk factor, General Veterinary, General Immunology and Microbiology, business.industry, Public Health, Environmental and Occupational Health, Infant, medicine.disease, veterinary(all), Kenya, Poliomyelitis, Vaccination, Infectious Diseases, Cross-Sectional Studies, Immunization, Molecular Medicine, Female, Measles vaccine, business

Abstract

Background Estimating vaccination coverage and delays are important because these measures can identify at risk sub-populations who can be targeted with interventions and public health policies. This paper sought to determine estimates and risk factors for children in rural western Kenya who did not receive immunization, received immunization with delay, or were severely underimmunized. Methods Caregivers of children aged 12–23 months old were surveyed for immunization history using written records from the immunization booklet. Risk factors for not receiving immunization, delayed immunization, and severe underimmunization were calculated using log-binomial regression. Children were categorized as delayed if a given immunization was received greater than four weeks from the age-appropriate scheduled date. Severely underimmunized children were those who were fully unvaccinated for more than 90 days and had three or more vaccines delayed or not given. Results Immunization coverage for pentavalent1, pentavalent3, measles, and fully immunized child (FIC; BCG, three doses of polio, three doses of pentavalent, and measles vaccines) were 99%, 94%, 83%, and 80%, respectively. Approximately, 10%, 24%, and 29%, of children were delayed for pentavalent1, pentavalent3, and measles, respectively. Each model produced a unique combination of risk factors with only advanced maternal age as a risk factor common to all models. Children with delayed receipt of pentavalent1 were at risk for not receiving pentavalent3 (RR: 5.20; 95%CI 3.48, 7.77), measles vaccine (RR: 1.48; 95%CI 1.12, 1.95), and not achieving FIC (RR: 1.88; 95%CI 1.51, 2.34) compared with children who received pentavalent1 on time. Conclusions Immunization coverage among 12–23 month old children was high, yet a substantial proportion of children were vaccinated with delay. Although vaccine coverage and timeliness are often conceptualized as separate measures, the finding that delayed pentavalent1 receipt was a strong risk factor for not receiving future immunizations indicates the two measures are intertwined.

Published

2015

14. Association between delayed pentavalent vaccination and immunisation drop-out in rural western Kenya: findings from a cross-sectional survey

Author

Daniel R. Feikin, Dustin G. Gibson, B Omondi, Eunice W. Kagucia, and Katherine L. O'Brien

Subjects

Pediatrics, medicine.medical_specialty, education.field_of_study, business.industry, Tetanus, lcsh:Public aspects of medicine, Diphtheria, Population, lcsh:RA1-1270, General Medicine, medicine.disease, Measles, Poliomyelitis, Vaccination, Pentavalent vaccine, Immunology, medicine, Measles vaccine, business, education

Abstract

Background The identification of determinants of vaccination coverage and delays is important because these predictors identify subsets of the population that can be targeted with public health interventions. This study's aims were to determine vaccination coverage and timeliness estimates and to identify risk factors for not being vaccinated or receiving late vaccinations in rural western Kenya. Methods The study was set in 120 villages within the Kenya Medical Research Institute and Centers for Disease Control and Prevention (KEMRI/CDC) surveillance system in rural western Kenya. In March, 2013, we did a cross-sectional survey of women in the study district who had infants aged 12–23 months. We excluded data from women who did not have their child's immunisation booklet and could provide only a verbal report of their child's immunisation history. We calculated risk factors for delayed and non-receipt of immunisation using binomial regression with log link. Infants were categorised as "delayed" if immunisation was received more than 28 days from schedule. Analyses were restricted to first and third dose of pentavalent vaccine (diphtheria, tetanus, and pertussis [DTP], hepatitis B, and Haemophilus influenzae type b), measles vaccine, and full immunisation (BCG, three doses of polio, three doses of pentavalent, and measles vaccines). Findings We surveyed 2495 women and included data from 1748 women (70%). We excluded data from 747 women (30%) who did not have their child's immunisation booklet card present. Immunisation coverage for pentavalent 1, pentavalent 3, measles, and full immunisation were 99%, 95%, 83%, and 80%, respectively. The proportions of infants with delayed pentavalent 1, pentavalent 3, and measles immunisations were 10%, 24%, and 29%, respectively. Risk factors for not receiving vaccination and delayed vaccination were, overall, similar when estimate trends and confidence intervals were taken in to account. Specifically, infants who received pentavalent 1 late were more likely than children who had the first pentavalent vaccine within schedule to not receive pentavalent 3 (adjusted RR 5·60 [95%CI 3·75–8·37]), measles vaccine (1·47 [1·11–1·94]), and full immunisation (1·87 [1·51–2·32]). Adjusted analyses for predictors of immunisation booklet present at time of survey versus verbal report found that women living closer to the health facility, women with younger infants, and those with male infants were more likely to have an immunisation booklet present at time of survey. Interpretation Immunisation coverage for pentavalent 1, pentavalent 3, and measles vaccines was high, but many children receive their vaccinations more than 28 days after the recommended scheduled date. Since late pentavalent 1 vaccination was associated with pentavalent series drop-out, not being immunised against measles, and not being fully immunised, interventions that target infants with delayed pentavalent 1 vaccination may improve overall immunisation coverage. A potential limitation of this study was that almost a third of mothers were excluded because they could provide only a verbal report of immunisation history instead of their child's immunisation booklet. If there were substantial differences in characteristics between those with an immunisation booklet and those without, and these characteristics were associated with vaccination coverage and delay, the reported estimates may be susceptible to bias. Funding The Bill and Melinda Gates Foundation.

Published

2015