19 results on '"Smith-Palmer A"'
Search Results
2. Systematic Literature Review of Studies Reporting Measures of Functional Outcome or Quality of Life in People with Negative Symptoms of Schizophrenia
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Hadzi Boskovic D, Smith-Palmer J, Pöhlmann J, Pollock RF, Hwang S, and Bruhn D
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schizophrenia ,quality of life ,functional outcomes ,negative symptoms ,Medicine (General) ,R5-920 - Abstract
Dusica Hadzi Boskovic,1 Jayne Smith-Palmer,2 Johannes Pöhlmann,2 Richard F Pollock,2 Steve Hwang,1 David Bruhn1 1Global Value and Real World Evidence, Otsuka Pharmaceutical Development & Commercialization Inc, Princeton, NJ, USA; 2Covalence Research Ltd, Harpenden, Hertfordshire, UKCorrespondence: Jayne Smith-Palmer, Email smith-palmer@covalence-research.comAim: Negative symptoms of schizophrenia (NSS) have been linked with poor functional outcomes. A literature review was performed to identify instruments used to assess functional outcomes and quality of life in clinical trials and observational studies conducted in groups of people with NSS.Methods: Literature search strings were designed using Medical Subject Headings combined with free-text terms and searches were performed using the PubMed, Embase and the Cochrane Library databases. For inclusion, articles were required to be published as full-text articles, in English, over the period 2011– 2021, include at least one group or treatment arm of people with NSS and report either functional outcomes or quality of life (QoL).Results: Literature searches identified a total of 3,268 unique hits. After two rounds of screening, 37 publications (covering 35 individual studies) were included in the review. A total of fourteen different instruments were used to assess functional outcomes and eleven different instruments were used to assess QoL. In studies in people with NSS, the most frequently used functional outcome measures were the Personal and Social Performance scale and the Global Assessment of Functioning. The most frequently used QoL instruments included the Manchester Short Assessment of Quality of Life, the Heinrich Carpenter Quality of Life Scale, the Schizophrenia Quality of Life Scale and the EQ-5D.Conclusion: A large number of measures have been used to assess functional outcomes and QoL in people with NSS, these include both generic and condition-specific as well as both interviewer-administered and self-reported instruments.Keywords: schizophrenia, quality of life, functional outcomes, negative symptoms
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- 2024
3. Genomic epidemiology of SARS-CoV-2 in a university outbreak setting and implications for public health planning
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Sema Nickbakhsh, Joseph Hughes, Nicolaos Christofidis, Emily Griffiths, Sharif Shaaban, Jessica Enright, Katherine Smollett, Kyriaki Nomikou, Natasha Palmalux, Lily Tong, Stephen Carmichael, Vattipally B. Sreenu, Richard Orton, Emily J. Goldstein, Rachael M. Tomb, The COVID-19 Genomics UK (COG-UK) Consortium, Kate Templeton, Rory N. Gunson, Ana da Silva Filipe, Catriona Milosevic, Emma Thomson, David L. Robertson, Matthew T. G. Holden, Christopher J. R. Illingworth, and Alison Smith-Palmer
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Medicine ,Science - Abstract
Abstract Whole genome sequencing of SARS-CoV-2 has occurred at an unprecedented scale, and can be exploited for characterising outbreak risks at the fine-scale needed to inform control strategies. One setting at continued risk of COVID-19 outbreaks are higher education institutions, associated with student movements at the start of term, close living conditions within residential halls, and high social contact rates. Here we analysed SARS-CoV-2 whole genome sequences in combination with epidemiological data to investigate a large cluster of student cases associated with University of Glasgow accommodation in autumn 2020, Scotland. We identified 519 student cases of SARS-CoV-2 infection associated with this large cluster through contact tracing data, with 30% sequencing coverage for further analysis. We estimated at least 11 independent introductions of SARS-CoV-2 into the student population, with four comprising the majority of detected cases and consistent with separate outbreaks. These four outbreaks were curtailed within a week following implementation of control measures. The impact of student infections on the local community was short-term despite an underlying increase in community infections. Our study highlights the need for context-specific information in the formation of public health policy for higher educational settings.
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- 2022
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4. Genomic epidemiology of SARS-CoV-2 in a university outbreak setting and implications for public health planning
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Nickbakhsh, Sema, Hughes, Joseph, Christofidis, Nicolaos, Griffiths, Emily, Shaaban, Sharif, Enright, Jessica, Smollett, Katherine, Nomikou, Kyriaki, Palmalux, Natasha, Tong, Lily, Carmichael, Stephen, Sreenu, Vattipally B., Orton, Richard, Goldstein, Emily J., Tomb, Rachael M., Templeton, Kate, Gunson, Rory N., da Silva Filipe, Ana, Milosevic, Catriona, Thomson, Emma, Robertson, David L., Holden, Matthew T. G., Illingworth, Christopher J. R., and Smith-Palmer, Alison
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- 2022
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5. A scoping review of risk factors and transmission routes associated with human giardiasis outbreaks in high-income settings
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Krumrie, Sarah, Capewell, Paul, Smith-Palmer, Alison, Mellor, Dominic, Weir, Willie, and Alexander, Claire L.
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- 2022
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6. A European Cost–Utility Analysis of the MiniMed™ 780G Advanced Hybrid Closed-Loop System Versus Intermittently Scanned Continuous Glucose Monitoring with Multiple Daily Insulin Injections in People Living with Type 1 Diabetes
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Jendle, Johan, primary, Buompensiere, Maria Ida, additional, Ozdemir Saltik, Asli Zeynep, additional, de Portu, Simona, additional, Smith-Palmer, Jayne, additional, Pollock, Richard F., additional, and Cohen, Ohad, additional
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- 2023
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7. Lutetium oxodotreotide (177Lu-Dotatate) for the treatment of unresectable or metastatic progressive gastroenteropancreatic neuroendocrine tumors: a cost-effectiveness analysis for Scotland
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Smith-Palmer, J., Leeuwenkamp, O. R., Virk, J., and Reed, N.
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- 2021
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8. Analysis of Escherichia coli O157 strains in cattle and humans between Scotland and England & Wales: implications for human health
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Chase-Topping, Margo, primary, Dallman, Timothy J., additional, Allison, Lesley, additional, Lupolova, Nadejda, additional, Matthews, Louise, additional, Mitchell, Sonia, additional, Banks, Christopher J., additional, Prentice, Jamie, additional, Brown, Helen, additional, Tongue, Sue, additional, Henry, Madeleine, additional, Evans, Judith, additional, Gunn, George, additional, Hoyle, Deborah, additional, McNeilly, Tom N., additional, Fitzgerald, Stephen, additional, Smith-Palmer, Alison, additional, Shaaban, Sharif, additional, Holmes, Anne, additional, Hanson, Mary, additional, Woolhouse, Mark, additional, Didelot, Xavier, additional, Jenkins, Claire, additional, and Gally, David L., additional
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- 2023
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9. Evaluating public health effects of risk-based travel policy for the COVID-19 epidemic in Scotland
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McLachlan, Isobel, primary, Huntley, Selene, additional, Leslie, Kirstin, additional, Bishop, Jennifer, additional, Redman, Christopher, additional, Yebra, Gonzalo, additional, Shaaban, Sharif, additional, Christofidis, Nicolaos, additional, Lycett, Samantha, additional, Holden, Matthew T.G., additional, Robertson, David L, additional, Smith-Palmer, Alison, additional, Hughes, Joseph, additional, and Nickbakhsh, Sema, additional
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- 2023
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10. A European Cost-Utility Analysis of the MiniMedTM 780G Advanced Hybrid Closed-Loop System versus Intermittently Scanned Continuous Glucose Monitoring with Multiple Daily Insulin Injections in People Living with Type 1 Diabetes
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Jendle, Johan, Buompensiere, Maria Ida, Ozdemir Saltik, Asli Zeynep, de Portu, Simona, Smith-Palmer, Jayne, Pollock, Richard, Cohen, Ohad, Jendle, Johan, Buompensiere, Maria Ida, Ozdemir Saltik, Asli Zeynep, de Portu, Simona, Smith-Palmer, Jayne, Pollock, Richard, and Cohen, Ohad
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Background: Advanced hybrid closed-loop (AHCL) automated insulin delivery systems are the most effective therapy in terms of assisting people with type 1 diabetes (T1D) to achieve glycemic targets; however, the cost can represent a barrier to uptake. Here, a cost-utility analysis of the MiniMedTM 780G AHCL system (MM780G) versus intermittently-scanned continuous glucose monitoring (is-CGM) plus multiple daily insulin injections (MDI) in people with T1D not achieving glycemic goals was performed across six European countries. Methods: Clinical input data were sourced from the ADAPT trial. Assuming a baseline HbA1c of 9.04%, HbA1c reductions of 1.54% for AHCL and 0.2% for is-CGM+MDI were assumed. The analyses were performed from a payer perspective over a time horizon of 40 years and an annual discount rate of 3% was applied. Results: Across all countries, the use of AHCL was projected to result in an incremental gain in quality-adjusted life expectancy of >2 quality-adjusted life years (QALYs) versus is-CGM+MDI. Lifetime direct costs were higher with AHCL resulting in incremental cost-utility ratios for AHCL versus is-CGM+MDI ranging from EUR 11,765 per QALY gained in Austria to EUR 43,963 per QALY gained in Italy. Conclusions: For people with T1D managed with is-CGM+MDI not achieving glycemic targets, initiation of the MM780G system was projected to improve long-term clinical outcomes; however, due to differences in healthcare costs between countries, the health economic outcomes differ. In the countries included here, AHCL is likely to be cost-effective relative to is-CGM+MDI for people not achieving glycemic goals with is-CGM+MDI. The ADAPT trial is registered with ClinicalTrials.gov, NCT04235504.
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- 2023
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11. Analysis of Escherichia coli O157 strains in cattle and humans between Scotland and England & Wales: implications for human health.
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IRAS OH Epidemiology Microbial Agents, IRAS – One Health Microbial, Chase-Topping, Margo, Dallman, Timothy J, Allison, Lesley, Lupolova, Nadejda, Matthews, Louise, Mitchell, Sonia, Banks, Christopher J, Prentice, Jamie, Brown, Helen, Tongue, Sue, Henry, Madeleine, Evans, Judith, Gunn, George, Hoyle, Deborah, McNeilly, Tom N, Fitzgerald, Stephen, Smith-Palmer, Alison, Shaaban, Sharif, Holmes, Anne, Hanson, Mary, Woolhouse, Mark, Didelot, Xavier, Jenkins, Claire, Gally, David L, IRAS OH Epidemiology Microbial Agents, IRAS – One Health Microbial, Chase-Topping, Margo, Dallman, Timothy J, Allison, Lesley, Lupolova, Nadejda, Matthews, Louise, Mitchell, Sonia, Banks, Christopher J, Prentice, Jamie, Brown, Helen, Tongue, Sue, Henry, Madeleine, Evans, Judith, Gunn, George, Hoyle, Deborah, McNeilly, Tom N, Fitzgerald, Stephen, Smith-Palmer, Alison, Shaaban, Sharif, Holmes, Anne, Hanson, Mary, Woolhouse, Mark, Didelot, Xavier, Jenkins, Claire, and Gally, David L
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- 2023
12. Benefits and Implications of the Breakthrough Device Designation Program
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Smith, Palmer
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United States. Food and Drug Administration ,Medical equipment ,Physiological apparatus ,Science and technology - Abstract
The U.S. Food and Drug Administration (FDA) introduced the Breakthrough Device Designation (BDD) Program in 2018 as a replacement for the Expedited Access Pathway and Priority Review for medical devices [...]
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- 2022
13. Spatial Analysis of Phylogenetic, Population and Deprivation Data from Scottish Sars-Cov-2 Outbreak Reveals Patterns of the Community Transmission
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Gamża, Anna, primary, Lycett, Samantha, additional, Harvey, Will, additional, Hughes, Joseph Hughes, additional, Nickbakhsh, Sema, additional, Robertson, David, additional, Smith Palmer, Alison, additional, Wood, Anthony, additional, and Kao, Rowland, additional
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- 2023
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14. A scoping review of risk factors and transmission routes associated with human giardiasis outbreaks in high-income settings
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Sarah Krumrie, Paul Capewell, Alison Smith-Palmer, Dominic Mellor, Willie Weir, and Claire L. Alexander
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Ocean Engineering - Abstract
The flagellated pathogen Giardia duodenalis is one of the leading causes of parasitic gastrointestinal illness worldwide. In many higher income countries, such as the United Kingdom, the disease is often perceived as being travel-related, likely leading to the under-reporting of sporadic cases and outbreaks. A summary of the literature describing outbreaks and risk factors in higher income countries is necessary to improve our understanding of this pathogen and identify existing knowledge gaps. Initial literature searches were carried out in September 2016 and updated at regular intervals until November 2021, using appropriate search terms in Medline, Embase and PubMed databases. A total of 75 papers met the inclusion criteria, revealing that the consumption of contaminated water and contact with young children of diaper-wearing age were the most common transmission routes leading to outbreaks of giardiasis. Of the ten studies where food was primarily associated with outbreaks, food handlers accounted for eight of these. Another reported transmission route was direct contact with fecal material, which was reported in six studies as the primary transmission route. Travel-associated giardiasis was considered the sole transmission route in two studies, whereas multiple transmission routes contributed to giardiasis outbreaks in eleven studies. The evidence around zoonotic transmission was less clear and hampered by the lack of robust and regularly applied parasite molecular typing techniques. This literature review summarizes the findings of Giardia outbreak investigations and epidemiological studies in high-income countries. Transmission routes are identified and discussed to highlight the associated risk factors. These data also indicate gaps in our current knowledge that include the need for robust, in-depth molecular studies and have underscored the importance of water as a transmission route for Giardia cysts. These future molecular studies will improve our understanding of Giardia epidemiology and transmission pathways in higher income countries to prevent spread of this significantly under-reported pathogen.
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- 2022
15. Epidemiology and genomic analysis of Shiga toxin-producing
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Ella V, Rodwell, Bhavita, Vishram, Robert, Smith, Lynda, Browning, Alison, Smith-Palmer, Lesley, Allison, Anne, Holmes, Gauri, Godbole, Noel, McCarthy, Timothy J, Dallman, and Claire, Jenkins
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renal failure ,Shiga-Toxigenic Escherichia coli ,Virulence ,Virulence Factors ,Genomics ,United Kingdom ,Enteropathogenic Escherichia coli ,Clinical Microbiology ,whole-genome sequencing ,haemolytic uraemic syndrome ,Drug Resistance, Bacterial ,Humans ,complex STEC infection ,Escherichia coli Infections - Abstract
Introduction Shiga toxin-producing Escherichia coli (STEC) is a zoonotic, foodborne gastrointestinal pathogen that has the potential to cause severe clinical outcomes, including haemolytic uraemic syndrome (HUS). STEC-HUS is the leading cause of renal failure in children and can be fatal. Over the last decade, STEC clonal complex 165 (CC165) has emerged as a cause of STEC-HUS. Gap statement There is a need to understand the pathogenicity and prevalence of this emerging STEC clonal complex in the UK, to facilitate early diagnosis, improve clinical management, and prevent and control outbreaks. Aim The aim of this study was to characterize CC165 through identification of virulence factors (VFs) and antimicrobial resistance (AMR) determinants in the genome and to integrate the genome data with the available epidemiological data to better understand the incidence and pathogenicity of this clonal complex in the UK. Methodology All isolates belonging to CC165 in the archives at the UK public health agencies were sequenced and serotyped, and the virulence gene and AMR profiles were derived from the genome using PHE bioinformatics pipelines and the Centre for Genomic Epidemiology virulence database. Results There were 48 CC165 isolates, of which 43 were STEC, four were enteropathogenic E. coli (EPEC) and one E. coli . STEC serotypes were predominately O80:H2 (n=28), and other serotypes included O45:H2 (n=9), O55:H9 (n=4), O132:H2 (n=1) and O180:H2 (n=1). All but one STEC isolate had Shiga toxin (stx) subtype stx2a or stx2d and 47/48 isolates had the eae gene encoding intimin involved in the intimate attachment of the bacteria to the human gut mucosa. We detected extra-intestinal virulence genes including those associated with iron acquisition (iro) and serum resistance (iss), indicating that this pathogen has the potential to translocate to extra-intestinal sites. Unlike other STEC clonal complexes, a high proportion of isolates (93%, 40/43) were multidrug-resistant, including resistance to aminoglycosides, beta-lactams, chloramphenicol, sulphonamides, tetracyclines and trimethoprim. Conclusion The clinical significance of this clonal complex should not be underestimated. Exhibiting high levels of AMR and a combination of STEC and extra-intestinal pathogenic E. coli (ExPEC) virulence profiles, this clonal complex is an emerging threat to public health.
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- 2021
16. Epidemiology and genomic analysis of Shiga toxin-producing Escherichia coli clonal complex 165 in the UK
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Rodwell, Ella V, Vishram, Bhavita, Smith, Robert, Browning, Lynda, Smith-Palmer, Alison, Allison, Lesley, Holmes, Anne, Godbole, Gauri, McCarthy, Noel, Dallman, Timothy J, Jenkins, Claire, IRAS OH Epidemiology Microbial Agents, and IRAS OH Epidemiology Microbial Agents
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Microbiology (medical) ,renal failure ,whole-genome sequencing ,haemolytic uraemic syndrome ,complex STEC infection ,General Medicine ,Microbiology ,QR - Abstract
Introduction. Shiga toxin-producing Escherichia coli (STEC) is a zoonotic, foodborne gastrointestinal pathogen that has the potential to cause severe clinical outcomes, including haemolytic uraemic syndrome (HUS). STEC-HUS is the leading cause of renal failure in children and can be fatal. Over the last decade, STEC clonal complex 165 (CC165) has emerged as a cause of STEC-HUS. Gap Statement. There is a need to understand the pathogenicity and prevalence of this emerging STEC clonal complex in the UK, to facilitate early diagnosis, improve clinical management, and prevent and control outbreaks. Aim. The aim of this study was to characterize CC165 through identification of virulence factors (VFs) and antimicrobial resistance (AMR) determinants in the genome and to integrate the genome data with the available epidemiological data to better understand the incidence and pathogenicity of this clonal complex in the UK. Methodology. All isolates belonging to CC165 in the archives at the UK public health agencies were sequenced and serotyped, and the virulence gene and AMR profiles were derived from the genome using PHE bioinformatics pipelines and the Centre for Genomic Epidemiology virulence database. Results. There were 48 CC165 isolates, of which 43 were STEC, four were enteropathogenic E. coli (EPEC) and one E. coli . STEC serotypes were predominately O80:H2 (n=28), and other serotypes included O45:H2 (n=9), O55:H9 (n=4), O132:H2 (n=1) and O180:H2 (n=1). All but one STEC isolate had Shiga toxin (stx) subtype stx2a or stx2d and 47/48 isolates had the eae gene encoding intimin involved in the intimate attachment of the bacteria to the human gut mucosa. We detected extra-intestinal virulence genes including those associated with iron acquisition (iro) and serum resistance (iss), indicating that this pathogen has the potential to translocate to extra-intestinal sites. Unlike other STEC clonal complexes, a high proportion of isolates (93%, 40/43) were multidrug-resistant, including resistance to aminoglycosides, beta-lactams, chloramphenicol, sulphonamides, tetracyclines and trimethoprim. Conclusion. The clinical significance of this clonal complex should not be underestimated. Exhibiting high levels of AMR and a combination of STEC and extra-intestinal pathogenic E. coli (ExPEC) virulence profiles, this clonal complex is an emerging threat to public health.
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- 2021
17. Listeria infection in young infants: results from a national surveillance study in the UK and Ireland
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Vergnano, S, Godbole, G, Simbo, A, Smith-Palmer, A, Cormican, M, Mark, A, and Heath, PT
- Abstract
OBJECTIVES: To describe the epidemiology, age at infection, clinical characteristics and outcome of listeria infection in young infants to inform management and empiric antibiotic choice in young infants. DESIGN: Prospective 2-year surveillance of Listeria monocytogenes infection in young infants detected through the British Paediatric Surveillance Unit 'orange card' system and triangulated with the public health laboratories. SETTING: National population study (England, Wales, Scotland and the Ireland) PATIENTS: All infants under 90 days with proven or probable invasive listeriosis MAIN OUTCOME MEASURES: Incidence, mortality, age of infection, clinical characteristics and outcome RESULTS: During a 2-year period (2017-2019), 27 cases of listeriosis in infants
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- 2021
18. Listeria infection in young infants: results from a national surveillance study in the UK and Ireland.
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Vergnano, Stefania, Godbole, Gauri, Simbo, Ameze, Smith-Palmer, Alison, Cormican, Martin, Anthony, Mark, and Heath, Paul T.
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NEONATAL sepsis ,LISTERIOSIS ,INFANTS ,CENTRAL nervous system infections ,PROGNOSIS ,WHOLE genome sequencing ,PUBLIC health surveillance ,LISTERIA ,DISEASE incidence ,POLYMERASE chain reaction ,LONGITUDINAL method ,LEUCOCYTE disorders - Abstract
Objectives: To describe the epidemiology, age at infection, clinical characteristics and outcome of listeria infection in young infants to inform management and empiric antibiotic choice in young infants.Design: Prospective 2-year surveillance of Listeria monocytogenes infection in young infants detected through the British Paediatric Surveillance Unit 'orange card' system and triangulated with the public health laboratories.Setting: National population study (England, Wales, Scotland and the Ireland) PATIENTS: All infants under 90 days with proven or probable invasive listeriosis MAIN OUTCOME MEASURES: Incidence, mortality, age of infection, clinical characteristics and outcome RESULTS: During a 2-year period (2017-2019), 27 cases of listeriosis in infants <90 days of age were reported. The incidence of listeriosis in this study was 1.8 per 100 000 live births with 7% mortality (2/27). Nearly all cases presented within the first 24 hours of life (26/27). The majority (20/27, 74%) were born preterm and 16/24 (67%) were born to women from ethnic minority backgrounds.Conclusions: Invasive listeriosis in young infants in the UK and Ireland is rare and presents early in the neonatal period. National guidelines that recommend the use of amoxicillin as part of empiric regimes for sepsis and meningitis in infants over 1 month of age should be modified. [ABSTRACT FROM AUTHOR]- Published
- 2021
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19. Epidemiology and genomic analysis of Shiga toxin-producing Escherichia coli clonal complex 165 in the UK.
- Author
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Rodwell EV, Vishram B, Smith R, Browning L, Smith-Palmer A, Allison L, Holmes A, Godbole G, McCarthy N, Dallman TJ, and Jenkins C
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- Drug Resistance, Bacterial genetics, Enteropathogenic Escherichia coli, Escherichia coli Infections microbiology, Genomics, Humans, United Kingdom epidemiology, Virulence genetics, Virulence Factors genetics, Escherichia coli Infections epidemiology, Shiga-Toxigenic Escherichia coli genetics
- Abstract
Introduction. Shiga toxin-producing Escherichia coli (STEC) is a zoonotic, foodborne gastrointestinal pathogen that has the potential to cause severe clinical outcomes, including haemolytic uraemic syndrome (HUS). STEC-HUS is the leading cause of renal failure in children and can be fatal. Over the last decade, STEC clonal complex 165 (CC165) has emerged as a cause of STEC-HUS. Gap Statement. There is a need to understand the pathogenicity and prevalence of this emerging STEC clonal complex in the UK, to facilitate early diagnosis, improve clinical management, and prevent and control outbreaks. Aim. The aim of this study was to characterize CC165 through identification of virulence factors (VFs) and antimicrobial resistance (AMR) determinants in the genome and to integrate the genome data with the available epidemiological data to better understand the incidence and pathogenicity of this clonal complex in the UK. Methodology. All isolates belonging to CC165 in the archives at the UK public health agencies were sequenced and serotyped, and the virulence gene and AMR profiles were derived from the genome using PHE bioinformatics pipelines and the Centre for Genomic Epidemiology virulence database. Results. There were 48 CC165 isolates, of which 43 were STEC, four were enteropathogenic E. coli (EPEC) and one E. coli . STEC serotypes were predominately O80:H2 ( n =28), and other serotypes included O45:H2 ( n =9), O55:H9 ( n =4), O132:H2 ( n =1) and O180:H2 ( n =1). All but one STEC isolate had Shiga toxin ( stx ) subtype stx2a or stx2d and 47/48 isolates had the eae gene encoding intimin involved in the intimate attachment of the bacteria to the human gut mucosa. We detected extra-intestinal virulence genes including those associated with iron acquisition ( iro ) and serum resistance ( iss ), indicating that this pathogen has the potential to translocate to extra-intestinal sites. Unlike other STEC clonal complexes, a high proportion of isolates (93%, 40/43) were multidrug-resistant, including resistance to aminoglycosides, beta-lactams, chloramphenicol, sulphonamides, tetracyclines and trimethoprim. Conclusion. The clinical significance of this clonal complex should not be underestimated. Exhibiting high levels of AMR and a combination of STEC and extra-intestinal pathogenic E. coli (ExPEC) virulence profiles, this clonal complex is an emerging threat to public health.
- Published
- 2021
- Full Text
- View/download PDF
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