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Effect of childhood vaccination and antibiotic use on pneumococcal populations and genome-wide associations with disease among children in Nepal: an observational study

BACKGROUND: Pneumococcal disease is a leading cause of bacterial pneumonia and invasive bacterial disease among children globally. The reason some strains of pneumococci are more likely to cause disease, and how interventions such as vaccines and antibiotics affect pneumococcal strains is poorly und...

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Autores principales: Kandasamy, Rama, Lo, Stephanie, Gurung, Meeru, Carter, Michael J, Gladstone, Rebecca, Lees, John, Shrestha, Sonu, Thorson, Stephen, Bijukchhe, Sanjeev, Gautam, Madhav C, Shrestha, Reetu, Gurung, Sunaina, Khadka, Bibek, McGee, Lesley, Breiman, Robert F, Murdoch, David R, Kelly, Dominic F, Shrestha, Shrijana, Bentley, Stephen D, Pollard, Andrew J
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier Ltd 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9242864/
https://www.ncbi.nlm.nih.gov/pubmed/35779566
http://dx.doi.org/10.1016/S2666-5247(22)00066-0
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author Kandasamy, Rama
Lo, Stephanie
Gurung, Meeru
Carter, Michael J
Gladstone, Rebecca
Lees, John
Shrestha, Sonu
Thorson, Stephen
Bijukchhe, Sanjeev
Gautam, Madhav C
Shrestha, Reetu
Gurung, Sunaina
Khadka, Bibek
McGee, Lesley
Breiman, Robert F
Murdoch, David R
Kelly, Dominic F
Shrestha, Shrijana
Bentley, Stephen D
Pollard, Andrew J
author_facet Kandasamy, Rama
Lo, Stephanie
Gurung, Meeru
Carter, Michael J
Gladstone, Rebecca
Lees, John
Shrestha, Sonu
Thorson, Stephen
Bijukchhe, Sanjeev
Gautam, Madhav C
Shrestha, Reetu
Gurung, Sunaina
Khadka, Bibek
McGee, Lesley
Breiman, Robert F
Murdoch, David R
Kelly, Dominic F
Shrestha, Shrijana
Bentley, Stephen D
Pollard, Andrew J
author_sort Kandasamy, Rama
collection PubMed
description BACKGROUND: Pneumococcal disease is a leading cause of bacterial pneumonia and invasive bacterial disease among children globally. The reason some strains of pneumococci are more likely to cause disease, and how interventions such as vaccines and antibiotics affect pneumococcal strains is poorly understood. We aimed to identify genetic regions under selective pressure and those associated with disease through the analysis of pneumococcal whole-genome sequences. METHODS: Whole-genome sequencing was performed on pneumococcal isolates collected between January, 2005, and May, 2018, in Kathmandu, Nepal, which included programmatic ten-valent pneumococcal conjugate vaccine (PCV10) introduction in 2015. Isolates were from three distinct cohorts: nasopharyngeal swabs of healthy community-based children, nasopharyngeal swabs of children admitted to hospital with pneumonia, and sterile-site cultures from children admitted to hospital. Across these cohorts we examined serotype distribution, antibiotic resistance, strain distribution, and regions of recombination to determine genes that were undergoing diversifying selection. Genome-wide association studies comparing pneumonia and sterile-site isolates with healthy carriage were used to determine novel variants associated with disease. FINDINGS: After programmatic introduction of PCV10, there was a decline in vaccine covered serotypes; however, strains that had expressed these serotypes continued to exist in the post-PCV population. We identified GPSC9 to be a strain of concern due to its high prevalence in disease, multidrug resistance, and ability to switch to an unencapsulated phenotype via insertion of virulence factor pspC into the cps locus. Antibiotic resistance loci to co-trimoxazole were found to be prevalent (pre-PCV10 78% vs post-PCV10 81%; p=0·27) and increasingly prevalent to penicillin (pre-PCV10 15% vs post-PCV10 32%; p<0·0001). Regions with multiple recombinations were identified spanning the surface protein virulence factors pspA and pspC and antibiotic targets pbpX, folA, folC, folE, and folP. Furthermore, we identified variants in lacE2 to be strongly associated with isolates from children with pneumonia and PRIP to be strongly associated with isolates from sterile sites. INTERPRETATION: Our work highlights the effect of pneumococcal conjugate vaccines, antibiotics, and host–pathogen interaction in pneumococcal variation, and the pathogen's capability of adapting to these factors at both population-wide and strain-specific levels. Ongoing surveillance of disease-associated strains and further investigation of lacE2 and PRIP as serotype-independent targets for therapeutic interventions is required. FUNDING: Gavi, The Vaccine Alliance; WHO; Bill & Melinda Gates Foundation; Wellcome Sanger Institute; and US Centers for Disease Control and Prevention.
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spelling pubmed-92428642022-07-01 Effect of childhood vaccination and antibiotic use on pneumococcal populations and genome-wide associations with disease among children in Nepal: an observational study Kandasamy, Rama Lo, Stephanie Gurung, Meeru Carter, Michael J Gladstone, Rebecca Lees, John Shrestha, Sonu Thorson, Stephen Bijukchhe, Sanjeev Gautam, Madhav C Shrestha, Reetu Gurung, Sunaina Khadka, Bibek McGee, Lesley Breiman, Robert F Murdoch, David R Kelly, Dominic F Shrestha, Shrijana Bentley, Stephen D Pollard, Andrew J Lancet Microbe Articles BACKGROUND: Pneumococcal disease is a leading cause of bacterial pneumonia and invasive bacterial disease among children globally. The reason some strains of pneumococci are more likely to cause disease, and how interventions such as vaccines and antibiotics affect pneumococcal strains is poorly understood. We aimed to identify genetic regions under selective pressure and those associated with disease through the analysis of pneumococcal whole-genome sequences. METHODS: Whole-genome sequencing was performed on pneumococcal isolates collected between January, 2005, and May, 2018, in Kathmandu, Nepal, which included programmatic ten-valent pneumococcal conjugate vaccine (PCV10) introduction in 2015. Isolates were from three distinct cohorts: nasopharyngeal swabs of healthy community-based children, nasopharyngeal swabs of children admitted to hospital with pneumonia, and sterile-site cultures from children admitted to hospital. Across these cohorts we examined serotype distribution, antibiotic resistance, strain distribution, and regions of recombination to determine genes that were undergoing diversifying selection. Genome-wide association studies comparing pneumonia and sterile-site isolates with healthy carriage were used to determine novel variants associated with disease. FINDINGS: After programmatic introduction of PCV10, there was a decline in vaccine covered serotypes; however, strains that had expressed these serotypes continued to exist in the post-PCV population. We identified GPSC9 to be a strain of concern due to its high prevalence in disease, multidrug resistance, and ability to switch to an unencapsulated phenotype via insertion of virulence factor pspC into the cps locus. Antibiotic resistance loci to co-trimoxazole were found to be prevalent (pre-PCV10 78% vs post-PCV10 81%; p=0·27) and increasingly prevalent to penicillin (pre-PCV10 15% vs post-PCV10 32%; p<0·0001). Regions with multiple recombinations were identified spanning the surface protein virulence factors pspA and pspC and antibiotic targets pbpX, folA, folC, folE, and folP. Furthermore, we identified variants in lacE2 to be strongly associated with isolates from children with pneumonia and PRIP to be strongly associated with isolates from sterile sites. INTERPRETATION: Our work highlights the effect of pneumococcal conjugate vaccines, antibiotics, and host–pathogen interaction in pneumococcal variation, and the pathogen's capability of adapting to these factors at both population-wide and strain-specific levels. Ongoing surveillance of disease-associated strains and further investigation of lacE2 and PRIP as serotype-independent targets for therapeutic interventions is required. FUNDING: Gavi, The Vaccine Alliance; WHO; Bill & Melinda Gates Foundation; Wellcome Sanger Institute; and US Centers for Disease Control and Prevention. Elsevier Ltd 2022-07 /pmc/articles/PMC9242864/ /pubmed/35779566 http://dx.doi.org/10.1016/S2666-5247(22)00066-0 Text en © 2022 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license https://creativecommons.org/licenses/by/4.0/This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Articles
Kandasamy, Rama
Lo, Stephanie
Gurung, Meeru
Carter, Michael J
Gladstone, Rebecca
Lees, John
Shrestha, Sonu
Thorson, Stephen
Bijukchhe, Sanjeev
Gautam, Madhav C
Shrestha, Reetu
Gurung, Sunaina
Khadka, Bibek
McGee, Lesley
Breiman, Robert F
Murdoch, David R
Kelly, Dominic F
Shrestha, Shrijana
Bentley, Stephen D
Pollard, Andrew J
Effect of childhood vaccination and antibiotic use on pneumococcal populations and genome-wide associations with disease among children in Nepal: an observational study
title Effect of childhood vaccination and antibiotic use on pneumococcal populations and genome-wide associations with disease among children in Nepal: an observational study
title_full Effect of childhood vaccination and antibiotic use on pneumococcal populations and genome-wide associations with disease among children in Nepal: an observational study
title_fullStr Effect of childhood vaccination and antibiotic use on pneumococcal populations and genome-wide associations with disease among children in Nepal: an observational study
title_full_unstemmed Effect of childhood vaccination and antibiotic use on pneumococcal populations and genome-wide associations with disease among children in Nepal: an observational study
title_short Effect of childhood vaccination and antibiotic use on pneumococcal populations and genome-wide associations with disease among children in Nepal: an observational study
title_sort effect of childhood vaccination and antibiotic use on pneumococcal populations and genome-wide associations with disease among children in nepal: an observational study
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9242864/
https://www.ncbi.nlm.nih.gov/pubmed/35779566
http://dx.doi.org/10.1016/S2666-5247(22)00066-0
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