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2. Improving the representativeness of UK’s national COVID-19 Infection Survey through spatio-temporal regression and post-stratification

Author

Pouwels, Koen B., Eyre, David W., House, Thomas, Aspey, Ben, Matthews, Philippa C., Stoesser, Nicole, Newton, John N., Diamond, Ian, Studley, Ruth, Taylor, Nick G. H., Bell, John I., Farrar, Jeremy, Kolenchery, Jaison, Marsden, Brian D., Hoosdally, Sarah, Jones, E. Yvonne, Stuart, David I., Crook, Derrick W., Peto, Tim E. A., and Walker, A. Sarah

Published
2024
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10. Excess resource use and cost of drug-resistant infections for six key pathogens in Europe: a systematic review and Bayesian meta-analysis

Author

Lorenzo Argante, Barana, Benedetta, Cappelli, Eva, De Rui, Maria Elena, Galia, Liliana, Geurtsen, Jeroen, Guedes, Mariana, Mejia, Jorly, Palladino, Andrea, Pezzani, Maria Diletta, Piljic, Alen, Kingston, Rhys, Vella, Venanzio, Pouwels, Koen B., Schmidt, Johannes E., Abdelatif El-Abasiri, Radwa A., Reyna-Villasmil, Eduardo, Hassoun-Kheir, Nasreen, Harbarth, Stephan, Rodríguez-Baño, Jesús, Tacconelli, Evelina, Arieti, Fabiana, Gladstone, Beryl Primrose, de Kraker, Marlieke E.A., Naylor, Nichola R., and Robotham, Julie V.

Published
2024
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11. A systematic review on the excess health risk of antibiotic-resistant bloodstream infections for six key pathogens in Europe

Author

Barana, Benedetta, Cappelli, Eva, De Rui, Maria Elena, El-Abasiri, Radwa A., Galia, Liliana, Geurtsen, Jeroen, Mejia, Jorly, Palladino, Andrea, Piljic, Alen, Rajendran, Nithya Babu, Reyna-Villasmil, Eduardo, Schmidt, Johannes E., Hassoun-Kheir, Nasreen, Guedes, Mariana, Ngo Nsoga, Marie-Therese, Argante, Lorenzo, Arieti, Fabiana, Gladstone, Beryl P., Kingston, Rhys, Naylor, Nichola R., Pezzani, Maria D., Pouwels, Koen B., Robotham, Julie V., Rodríguez-Baño, Jesús, Tacconelli, Evelina, Vella, Venanzio, Harbarth, Stephan, and de Kraker, Marlieke E.A.

Published
2024
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12. Inferring Risks of Coronavirus Transmission from Community Household Data

Author

House, Thomas, Riley, Heather, Pellis, Lorenzo, Pouwels, Koen B., Bacon, Sebastian, Eidukas, Arturas, Jahanshahi, Kaveh, Eggo, Rosalind M., and Walker, A. Sarah

Subjects
Statistics - Applications, Quantitative Biology - Populations and Evolution, 62P10
Abstract

The response of many governments to the COVID-19 pandemic has involved measures to control within- and between-household transmission, providing motivation to improve understanding of the absolute and relative risks in these contexts. Here, we perform exploratory, residual-based, and transmission-dynamic household analysis of the Office for National Statistics (ONS) COVID-19 Infection Survey (CIS) data from 26 April 2020 to 15 July 2021 in England. This provides evidence for: (i) temporally varying rates of introduction of infection into households broadly following the trajectory of the overall epidemic and vaccination programme; (ii) Susceptible-Infectious Transmission Probabilities (SITPs) of within-household transmission in the 15-35% range; (iii) the emergence of the Alpha and Delta variants, with the former being around 50% more infectious than wildtype and 35% less infectious than Delta within households; (iv) significantly (in the range 25-300%) more risk of bringing infection into the household for workers in patient-facing roles pre-vaccine; (v) increased risk for secondary school-age children of bringing the infection into the household when schools are open; (vi) increased risk for primary school-age children of bringing the infection into the household when schools were open since the emergence of new variants., Comment: 27 pages, 7 figures

Published
2021

15. Community prevalence of SARS-CoV-2 in England from April to November, 2020: results from the ONS Coronavirus Infection Survey

Author

Pouwels, Koen B., Walker, A. Sarah, Crook, Derrick, Matthews, Philippa C., Peto, Tim, Pritchard, Emma, Stoesser, Nicole, Vihta, Karina-Doris, Howarth, Alison, Doherty, George, Kavanagh, James, Chau, Kevin K., Hatch, Stephanie B., Ebner, Daniel, Martins Ferreira, Lucas, Christott, Thomas, Marsden, Brian D., Dejnirattisai, Wanwisa, Mongkolsapaya, Juthathip, Hoosdally, Sarah, Cornall, Richard, Stuart, David I., Screaton, Gavin, Eyre, David, Bell, John, Cox, Stuart, Paddon, Kevin, James, Tim, House, Thomas, Newton, John N., Robotham, Julie V., Birrell, Paul, Jordan, Helena, Sheppard, Tim, Athey, Graham, Moody, Dan, Curry, Leigh, Brereton, Pamela, Hay, Jodie, Vansteenhouse, Harper, Bell, Iain, Diamond, Ian, Lambert, Alex, Benton, Pete, Rourke, Emma, Hawkes, Stacey, Henry, Sarah, Scruton, James, Stokes, Peter, Thomas, Tina, Allen, John, Black, Russell, Bovill, Heather, Braunholtz, David, Brown, Dominic, Collyer, Sarah, Crees, Megan, Daglish, Colin, Davies, Byron, Donnarumma, Hannah, Douglas-Mann, Julia, Felton, Antonio, Finselbach, Hannah, Fordham, Eleanor, Ipser, Alberta, Jenkins, Joe, Jones, Joel, Kent, Katherine, Kerai, Geeta, Lloyd, Lina, Masding, Victoria, Osborn, Ellie, Patel, Alpi, Pereira, Elizabeth, Pett, Tristan, Randall, Melissa, Reeve, Donna, Shah, Palvi, Snook, Ruth, Studley, Ruth, Sutherland, Esther, Swinn, Eliza, Thomas, Heledd, Tudor, Anna, Weston, Joshua, Leib, Shayla, Tierney, James, Farkas, Gabor, Cobb, Raf, Van Galen, Folkert, Compton, Lewis, Irving, James, Clarke, John, Mullis, Rachel, Ireland, Lorraine, Airimitoaie, Diana, Nash, Charlotte, Cox, Danielle, Fisher, Sarah, Moore, Zoe, McLean, James, Kerby, Matt, Pouwels, Koen B, Robotham, Julie V, Birrell, Paul J, Gelman, Andrew, Bowers, Nikola, Boreham, Ian, Lewis, James, Bell, John I, Newton, John N, Farrar, Jeremy, and Walker, Ann Sarah

Published
2021
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16. Bleeding risk in patients prescribed dual antiplatelet therapy and triple therapy after coronary interventions: the ADAPTT retrospective population-based cohort studies

Author

Harris Jessica, Pouwels Koen B, Johnson Thomas, Sterne Jonathan, Pithara Christalla, Mahadevan Kalaivani, Reeves Barney, Benedetto Umberto, Loke Yoon, Lasserson Daniel, Doble Brett, Hopewell-Kelly Noreen, Redwood Sabi, Wordsworth Sarah, Mumford Andrew, Rogers Chris, and Pufulete Maria

Subjects
Medical technology, R855-855.5
Abstract

Background Bleeding among populations undergoing percutaneous coronary intervention or coronary artery bypass grafting and among conservatively managed patients with acute coronary syndrome exposed to different dual antiplatelet therapy and triple therapy (i.e. dual antiplatelet therapy plus an anticoagulant) has not been previously quantified. Objectives The objectives were to estimate hazard ratios for bleeding for different antiplatelet and triple therapy regimens, estimate resources and the associated costs of treating bleeding events, and to extend existing economic models of the cost-effectiveness of dual antiplatelet therapy. Design The study was designed as three retrospective population-based cohort studies emulating target randomised controlled trials. Setting The study was set in primary and secondary care in England from 2010 to 2017. Participants Participants were patients aged ≥ 18 years undergoing coronary artery bypass grafting or emergency percutaneous coronary intervention (for acute coronary syndrome), or conservatively managed patients with acute coronary syndrome. Data sources Data were sourced from linked Clinical Practice Research Datalink and Hospital Episode Statistics. Interventions Coronary artery bypass grafting and conservatively managed acute coronary syndrome: aspirin (reference) compared with aspirin and clopidogrel. Percutaneous coronary intervention: aspirin and clopidogrel (reference) compared with aspirin and prasugrel (ST elevation myocardial infarction only) or aspirin and ticagrelor. Main outcome measures Primary outcome: any bleeding events up to 12 months after the index event. Secondary outcomes: major or minor bleeding, all-cause and cardiovascular mortality, mortality from bleeding, myocardial infarction, stroke, additional coronary intervention and major adverse cardiovascular events. Results The incidence of any bleeding was 5% among coronary artery bypass graft patients, 10% among conservatively managed acute coronary syndrome patients and 9% among emergency percutaneous coronary intervention patients, compared with 18% among patients prescribed triple therapy. Among coronary artery bypass grafting and conservatively managed acute coronary syndrome patients, dual antiplatelet therapy, compared with aspirin, increased the hazards of any bleeding (coronary artery bypass grafting: hazard ratio 1.43, 95% confidence interval 1.21 to 1.69; conservatively-managed acute coronary syndrome: hazard ratio 1.72, 95% confidence interval 1.15 to 2.57) and major adverse cardiovascular events (coronary artery bypass grafting: hazard ratio 2.06, 95% confidence interval 1.23 to 3.46; conservatively-managed acute coronary syndrome: hazard ratio 1.57, 95% confidence interval 1.38 to 1.78). Among emergency percutaneous coronary intervention patients, dual antiplatelet therapy with ticagrelor, compared with dual antiplatelet therapy with clopidogrel, increased the hazard of any bleeding (hazard ratio 1.47, 95% confidence interval 1.19 to 1.82), but did not reduce the incidence of major adverse cardiovascular events (hazard ratio 1.06, 95% confidence interval 0.89 to 1.27). Among ST elevation myocardial infarction percutaneous coronary intervention patients, dual antiplatelet therapy with prasugrel, compared with dual antiplatelet therapy with clopidogrel, increased the hazard of any bleeding (hazard ratio 1.48, 95% confidence interval 1.02 to 2.12), but did not reduce the incidence of major adverse cardiovascular events (hazard ratio 1.10, 95% confidence interval 0.80 to 1.51). Health-care costs in the first year did not differ between dual antiplatelet therapy with clopidogrel and aspirin monotherapy among either coronary artery bypass grafting patients (mean difference £94, 95% confidence interval –£155 to £763) or conservatively managed acute coronary syndrome patients (mean difference £610, 95% confidence interval –£626 to £1516), but among emergency percutaneous coronary intervention patients were higher for those receiving dual antiplatelet therapy with ticagrelor than for those receiving dual antiplatelet therapy with clopidogrel, although for only patients on concurrent proton pump inhibitors (mean difference £1145, 95% confidence interval £269 to £2195). Conclusions This study suggests that more potent dual antiplatelet therapy may increase the risk of bleeding without reducing the incidence of major adverse cardiovascular events. These results should be carefully considered by clinicians and decision-makers alongside randomised controlled trial evidence when making recommendations about dual antiplatelet therapy. Limitations The estimates for bleeding and major adverse cardiovascular events may be biased from unmeasured confounding and the exclusion of an eligible subgroup of patients who could not be assigned an intervention. Because of these limitations, a formal cost-effectiveness analysis could not be conducted. Future work Future work should explore the feasibility of using other UK data sets of routinely collected data, less susceptible to bias, to estimate the benefit and harm of antiplatelet interventions. Trial registration This trial is registered as ISRCTN76607611. Funding This project was funded by the National Institute for Health and Care Research (NIHR) Health Technology Assessment programme and will be published in full in Health Technology Assessment; Vol. 27, No. 8. See the NIHR Journals Library website for further project information. Plain language summary People who have a heart attack are treated with a stent to open up the blocked artery that caused the heart attack, with surgery to bypass the blocked artery or with medication only. Whatever the treatment, they are prescribed one or more antiplatelet drugs, either aspirin only or aspirin and an additional antiplatelet (clopidogrel, prasugrel or ticagrelor), for 12 months after the heart attack. Antiplatelets are given to prevent another heart attack, but increase the risk of bleeding. We used a large general practice database and a database describing patients’ attendances and admissions to hospital to determine how many people bleed with different antiplatelet combinations. We found that, overall, up to 1 in 10 people taking antiplatelets (rising to 2 in 10 if also taking an anticoagulant such as warfarin or dabigatran) reported a bleed. Among patients treated with surgery or medication only, we compared aspirin only (which is a less potent therapy) with aspirin and clopidogrel (a more potent therapy). Among patients treated with stents, we compared aspirin and clopidogrel (less potent therapy) with aspirin and prasugrel or ticagrelor (more potent therapy). In all three populations, the more potent therapy increased the risk of bleeding by about one and a half times, but this was not offset by a reduced risk of having a subsequent heart attack. This may be explained by low adherence to the medication: between one-third and almost half of all patients did not adhere to their regimen, and non-adherence was generally higher among patients taking a more potent therapy. It may also be explained by bias inherent in the study, for example if the groups prescribed different antiplatelet regimens had different risks of having another heart attack. Nevertheless, the results show that doctors should be cautious about prescribing more potent antiplatelet therapy because it may increase serious bleeds without necessarily reducing the number of heart attacks. Scientific summary Background Dual antiplatelet therapy (DAPT), a combination of aspirin and clopidogrel, prasugrel or ticagrelor, is recommended for up to 12 months for secondary prevention of ischaemic events (heart attack and stroke) among people undergoing coronary interventions [coronary artery bypass grafting (CABG) and percutaneous coronary intervention (PCI)] and people with acute coronary syndrome (ACS) who are medically managed. Randomised controlled trials (RCTs) in these populations suggest that DAPT increases the risk of bleeding compared with aspirin monotherapy, and that more potent DAPT (with prasugrel and ticagrelor) increases the risk of bleeding compared with less potent DAPT (with clopidogrel). Adding an anticoagulant to DAPT (e.g. for the management of atrial fibrillation), known as triple therapy (TT), increases risk further. ‘Real-world’ bleeding among populations exposed to different DAPT and TT regimens has not been previously quantified. The economic impact of bleeding events is poorly characterised, in particular for minor bleeding, as is their impact on health-related quality of life (HRQoL). Objectives 1.Estimate rates of major and minor bleeding events with different DAPT (and TT) exposures among CABG, PCI and conservatively treated ACS patients. 2.Estimate hazard ratios (HRs) for bleeding for different antiplatelet regimens: for the PCI cohort, we compared aspirin and clopidogrel (AC) with aspirin and prasugrel (AP) or aspirin and ticagrelor (AT); for the CABG and ACS no-procedure cohorts, we compared aspirin with AC. 3.Review the literature to estimate the deterioration in utility (quality-adjusted life-years) of patients who have minor or major bleeding events. 4.Revise/extend existing economic models of the cost-effectiveness of different DAPT regimens to include estimates of the incidence of minor and major bleeding events and associated impacts on utility in the general population. 5.Estimate the resources required and associated costs incurred of treating major and minor events of the alternative DAPT (TT) exposures in the three specified patient populations. 6.Understand patients’ perspectives of DAPT, and the factors that influence responses to nuisance bleeding focusing on adherence and information-seeking (this objective was identified through the patient and public involvement work after the start of the ADAPTT study). Methods Objectives 1 and 2 We conducted a study to identify confounders systematically by performing a systematic review of RCTs and cohort studies; conducting semistructured interviews with six cardiac surgeons, six cardiologists and five general practitioners (GPs); and conducting a survey of 79 cardiologists and 31 cardiac surgeons. We used linked Clinical Practice Research Datalink (CPRD) and Hospital Episode Statistics (HES) data to assemble populations (CABG, PCI and conservatively managed ACS patients) eligible for three ‘target trials’. Inclusion criteria for the target trial were as follows: ≥ 18 years of age, ≥ 1 year of data in CPRD before the index event, no prescription for DAPT or anticoagulants in the preceding 3 months and a prescription for aspirin or DAPT within 2 months of discharge after the index event. The primary outcome was any bleeding event (CPRD or HES data) up to 12 months after the index event. We described rates of bleeding among patients prescribed different DAPT regimens and TT. We estimated adjusted HRs for time to first bleed comparing DAPT with AC (reference) versus aspirin monotherapy for CABG and conservatively managed ACS patient, and, in the emergency PCI population, DAPT with prasugrel versus DAPT with clopidogrel for ST-elevation myocardial infarction (STEMI) patients only and DAPT with ticagrelor versus DAPT with clopidogrel for all the emergency PCI population. We prespecified five sensitivity analyses and conducted three: sensitivity analysis 1 – multiple imputation for eligible patients for whom we had no data to assign an intervention; sensitivity analysis 3 – restricted to patients at low risk of bleeding; and sensitivity analysis 4 – repeating primary outcome analysis without censoring of any CPRD or HES bleed events at transfer-out or last collection date. The transfer-out or last collection date reflect the date that a patient leaves the general practice or the date that the last capture from CPRD was made. Objective 3 A systematic review was conducted of primary research and decision-analytic modelling studies reporting utility decrements for bleeds related to DAPT through a search of MEDLINE, PubMed and references of included studies. A health elicitation study was undertaken, comprising 21 participants (PCI, CABG and conservatively managed ACS) who completed an elicitation exercise involving vignettes describing minor and major bleeds and the EuroQol-5 Dimensions, three-level version (EQ-5D-3L), and the EuroQol-5 Dimensions, five-level version (EQ-5D-5L). Utility decrements were derived using linear regression, and were compared with existing estimates. Objective 4 No formal cost-effectiveness evaluation was undertaken. Objective 5 Data on health-care use were derived from the linked CPRD–HES data set. The total health-care costs associated with the different antiplatelet regimens in the three target trials were measured at 1, 2 and 3 years after the start of follow-up. We used inverse probability of treatment weighting to adjust for the same confounders identified for the main ADAPTT analysis. The total health-care costs at 1, 2 and 3 years of follow-up were estimated by fitting weighted generalised linear models with gamma distribution and log-link. Objective 6 Two focus groups were conducted with patients at the early stages of treatment (0–3 months, nine participants), and two with patients coming to the end of treatment (9–12 months, 12 participants), to explore their experiences with DAPT. Recordings were transcribed verbatim, anonymised and analysed using framework analysis. Research findings Objectives 1 and 2 Confounders study A total of 70 potential confounders were identified by systematic review, clinician interviews and surveys; of these, 34 (49%) were classified as true confounders (factors that influence both the assigned intervention and the outcome), of which 31 (91%) were identified by systematic review and three (9%) by clinician interview, and 31 (91%) were confirmed by the survey. The clinician interviews identified hard-to-measure factors not identified in the review (drug potency, resistance to antiplatelet medication and clinician concerns about adherence). Data that would enable the characterisation of risk, including presentation risk and procedural risk factors, were unavailable for 17 of the 34 confounders (50%). The ADAPTT study A proportion of eligible participants were excluded from each target trial because they could not be assigned an intervention at baseline (17%, 40% and 9% of the CABG, conservatively managed ACS and emergency PCI patients, respectively). The incidence of any bleeding was 5%, 10% and 9% in CABG patients, conservatively managed ACS patients and emergency PCI patients, respectively; the corresponding rates of minor bleeding were 4%, 7% and 7%, respectively. Compared with aspirin monotherapy, DAPT was associated with an increase in the hazards of any bleeding and of major adverse cardiovascular events (MACEs) among CABG [HR 1.72, 95% confidence interval (CI) 1.15 to 2.57, and HR 2.06, 95% CI 1.23 to 3.46, respectively] and conservatively managed ACS patients (HR 1.43, 95% CI 1.21 to 1.69, and HR 1.57, 95% CI 1.38 to 1.78, respectively). Among emergency PCI patients, compared with less potent DAPT (with clopidogrel), more potent DAPT with ticagrelor (ACS and STEMI patients only) or prasugrel (STEMI patients only) increased the hazard of bleeding (HR 1.47, 95% CI 1.19 to 1.82; HR 1.47, 95% CI 1.08 to 2.00; and HR 1.77, 95% CI 1.21 to 2.58, respectively), but there was no association with MACEs (HR 1.06, 95% CI 0.89 to 1.27; HR 1.21, 95% CI 0.94 to 1.56; and HR 1.10, 95% CI 0.80 to 1.51, respectively). Sensitivity analyses using multiple imputation to impute for the intervention assigned at baseline did not materially change these results. Non-adherence to the treatment assigned at baseline was generally higher in the CABG and conservatively-managed ACS target trials (affecting up to 46% and 44% of patients, respectively) than in the in emergency PCI (affecting up to 33% of patients). Triple therapy The median duration of TT was 3.5 months. The incidence of any bleeding among patients prescribed TT was 18%. There was no difference in the incidence of any bleeding, or of major bleeding or minor bleeding, between patients on TT with warfarin and patients on TT with a non-vitamin K oral anticoagulant (NOAC). However, mortality from bleeding was higher among patients on TT with a NOAC than among patients on TT with warfarin (2% vs. 0%), as was the incidence of stroke (4% vs. 0%). Objective 3 Twelve eligible studies were included for review. Reported utility decrements ranged from –0.002 to –0.03 for minor bleeds and –0.007 to –0.05 for major bleeds. Data sources used to estimate the decrements lacked relevance to our population group, and few studies adequately reported details of their measurement and valuation approaches. Our patient health elicitation study elicited utility decrements that overlapped existing estimates, ranging from –0.000848 to –0.00828 for minor bleeds and from –0.0187 to –0.0621 for major bleeds. However, the magnitude of difference depended on the instrument (EQ-5D-5L or EQ-5D-3L), estimation method and valuation approach applied. Objective 5 The mean total health-care cost in the year prior to the index event was much higher for CABG patients (£13,601) than for conservatively managed ACS (£3528) or emergency PCI patients (£3625). For CABG patients, mean costs were similar between different antiplatelet regimens (£13,623 for aspirin monotherapy and £13,537 for DAPT with clopidogrel). For conservatively managed ACS, patients on DAPT with clopidogrel had a lower mean total health-care cost in the year prior to the index date than patients on aspirin monotherapy (£3317 vs. £3857, respectively). Among emergency PCI patients, those initiated on DAPT with clopidogrel had a higher mean total health-care cost in the year prior to the index event (£4492) than those initiated on DAPT with prasugrel (STEMI patients only) (£1660) or ticagrelor (£2829). Among the CABG population, there was no difference in mean cumulative health-care costs between initiation of DAPT with clopidogrel and initiation of aspirin monotherapy; the mean difference at 1, 2 and 3 years was £94 (95% CI –£555 to £763), £236 (95% CI –£831 to £1223) and £113 (95% CI –£1318 to £1102), respectively. Among the conservatively managed ACS population, the mean cumulative health-care costs were estimated to be slightly higher if all patients were treated with DAPT with clopidogrel than if all were treated with aspirin monotherapy; the mean difference at 1, 2 and 3 years was £610 (95% CI –£626 to £1516), £1118 (95% CI –£226 to £2206) and £1225 (95% CI –£426 to £2423), respectively, although there was considerable overlap between CIs. For emergency PCI patients, the estimated cumulative health-care costs were comparable under the different antiplatelet regimens among patients not receiving concurrent proton pump inhibitor (PPI) prescriptions, but were higher for patients receiving DAPT with ticagrelor than for patients receiving DAPT with clopidogrel. At 1 year, for example, the predicted mean difference in health-care costs if all patients received DAPT with ticagrelor rather than DAPT with clopidogrel was £72 (95% CI –£532 to £762) among those not receiving concurrent PPI therapy and £1145 (95% CI £269 to £2195) among those receiving concurrent PPI therapy. Among STEMI patients receiving concurrent PPI therapy, DAPT with prasugrel was associated with higher costs than DAPT with clopidogrel or DAPT with ticagrelor. Objective 6 Participants would adhere to DAPT when they believed that DAPT was important to ACS outcomes. Those who had experienced nuisance bleeding reported symptoms to be mild and manageable and did not report the bleed to their GP. Adherence was influenced by participants’ and their families’ understanding of the risks and benefits of DAPT, and their ability to manage symptoms. Factors influencing knowledge about DAPT included access to medication counselling; processing of and engaging with information communicated during medication counselling; and access to timely, relevant and expert information and advice after discharge from hospital. Conclusions There is underascertainment of minor/nuisance bleeding in the CPRD, probably as a result of under-reporting of nuisance bleeding by patients to their GPs. In three retrospective population-based cohort studies emulating target trials, there was an increased risk of bleeding among patients receiving DAPT compared with those receiving aspirin monotherapy (CABG and conservatively managed ACS patients) and among patients receiving more potent DAPT than among those receiving less potent DAPT (emergency PCI patients), but not the expected decrease in MACEs. We identified several potential biases that may have influenced the results of the ADAPTT study as a result of imperfect emulation of the defined target trials: (1) selection bias – we excluded a subgroup of the eligible population because they could not be assigned an intervention; (2) confounding – we had no data for half of the confounders identified, including procedure-related characteristics and disease complexity, and evidence from clinician interviews and surveys that clinicians balance bleeding and ischaemic risk when prescribing DAPT to their patients; and (3) non-adherence to DAPT, which was substantial, and generally higher in the stronger antiplatelet treatment groups. Medication knowledge and understanding, and confidence in dealing with symptoms facilitate positive attitudes towards adherence to DAPT, but may be hindered by opportunities to access relevant, timely and appropriate medication counselling. Although we derived relevant utility decrements for the included population using a patient elicitation exercise, based on standardised definitions of minor and major bleeding events, using a validated HRQoL instrument and valued using general population tariffs, we could not conduct a formal cost-effectiveness analysis given the uncertainty around the estimates for bleeding. Nevertheless, the results using routinely collected data need to be carefully considered by clinicians and decision-makers, given that the increased risk of bleeding we observed with more potent DAPT was not offset by a reduced risk of cardiovascular events and that several recent large meta-analyses of RCTs have also failed to show a conclusive benefit of more potent antiplatelet therapy on cardiovascular events. Future work Future research should explore the feasibility of using other UK data sets of routinely collected data, less susceptible to bias, to estimate the benefit and harm of antiplatelet interventions. Research is needed to develop guidance for identifying confounders and how confounders should be organised into confounding domains to facilitate consistent implementation of the Risk Of Bias In Non-randomized Studies – of Interventions (ROBINS-I) tool. The principle of designing an observational study to emulate a RCT by first defining a target trial appears to be a robust approach, highlighting where the emulation succeeds or fails. Nevertheless, further research is required to validate instances in which an emulation is considered to have been successful, ideally prospectively (i.e. using observational data to emulate ongoing RCTs before their data are analysed and the results are known).We recommend that our utility decrements are used in future cost-effectiveness analyses of DAPT in a UK setting, particularly for minor bleeding events for which existing evidence is limited. In addition, we recommend that future research focuses on quantifying the value of information from reducing the uncertainty of our estimated utility decrements. This research would demonstrate whether or not conducting a larger, more robust study to collect additional information on the HRQoL impact of minor and major bleeds for patients taking DAPT would be an efficient use of resources. The qualitative study with patients highlighted that medication knowledge and understanding, and confidence in dealing with symptoms, facilitate positive attitudes towards adherence to DAPT, but that, currently, there are limited opportunities for patients to access relevant, timely and appropriate DAPT medication counselling. Future qualitative research should focus on developing an intervention to support service users taking DAPT. Trial registration This trial is registered as ISRCTN76607611. Funding This project was funded by the National Institute for Health and Care Research (NIHR) Health Technology Assessment programme and will be published in full in Health Technology Assessment; Vol. 27, No. 8. See the NIHR Journals Library website for further project information.

Published
2023
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17. Antibody responses and correlates of protection in the general population after two doses of the ChAdOx1 or BNT162b2 vaccines

Author

Wei, Jia, Pouwels, Koen B., Stoesser, Nicole, Matthews, Philippa C., Diamond, Ian, Studley, Ruth, Rourke, Emma, Cook, Duncan, Bell, John I., Newton, John N., Farrar, Jeremy, Howarth, Alison, Marsden, Brian D., Hoosdally, Sarah, Jones, E. Yvonne, Stuart, David I., Crook, Derrick W., Peto, Tim E. A., Walker, A. Sarah, and Eyre, David W.

Published
2022
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20. Expert consensus on antimicrobial resistance research priorities to focus development and implementation of antibacterial vaccines and monoclonal antibodies.

Author

Hassoun-Kheir, Nasreen, Guedes, Mariana, Arieti, Fabiana, Pezzani, Maria Diletta, Gladstone, Beryl Primrose, Robotham, Julie V., Pouwels, Koen B., Kingston, Rhys, Carmeli, Yehuda, Cassini, Alessandro, Cecchini, Michele, Drobniewski, Francis, Frost, Isabel, Geurtsen, Jeroen, Kronenberg, Andreas, Nu Htay, Mila Nu, Paul, Mical, Rocha-Pereira, Nuno, Rodríguez-Baño, Jesús, and Scudeller, Luigia

Published
2024
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21. Effect of Delta variant on viral burden and vaccine effectiveness against new SARS-CoV-2 infections in the UK

Author

Pouwels, Koen B., Pritchard, Emma, Matthews, Philippa C., Stoesser, Nicole, Eyre, David W., Vihta, Karina-Doris, and House, Thomas

Subjects
Infection control -- Methods, Viremia -- Measurement, Biological sciences, Health
Abstract

The effectiveness of the BNT162b2 and ChAdOx1 vaccines against new severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infections requires continuous re-evaluation, given the increasingly dominant B.1.617.2 (Delta) variant. In this study, we investigated the effectiveness of these vaccines in a large, community-based survey of randomly selected households across the United Kingdom. We found that the effectiveness of BNT162b2 and ChAdOx1 against infections (new polymerase chain reaction (PCR)-positive cases) with symptoms or high viral burden is reduced with the B.1.617.2 variant (absolute difference of 10-13% for BNT162b2 and 16% for ChAdOx1) compared to the B.1.1.7 (Alpha) variant. The effectiveness of two doses remains at least as great as protection afforded by prior natural infection. The dynamics of immunity after second doses differed significantly between BNT162b2 and ChAdOx1, with greater initial effectiveness against new PCR-positive cases but faster declines in protection against high viral burden and symptomatic infection with BNT162b2. There was no evidence that effectiveness varied by dosing interval, but protection was higher in vaccinated individuals after a prior infection and in younger adults. With B.1.617.2, infections occurring after two vaccinations had similar peak viral burden as those in unvaccinated individuals. SARS-CoV-2 vaccination still reduces new infections, but effectiveness and attenuation of peak viral burden are reduced with B.1.617.2. A large, community-based study in the United Kingdom indicates that the effectiveness of BNT162b2 and ChAdOx1 vaccines against SARS-CoV-2 infections with symptoms or high viral burden is reduced with the Delta variant compared to the Alpha variant., Author(s): Koen B. Pouwels [sup.1] [sup.2] , Emma Pritchard [sup.1] [sup.3] , Philippa C. Matthews [sup.3] [sup.4] [sup.5] , Nicole Stoesser [sup.1] [sup.3] [sup.4] [sup.5] , David W. Eyre [sup.1] [...]

Published
2021
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23. Detecting changes in population trends in infection surveillance using community SARS-CoV-2 prevalence as an exemplar

Author

Pritchard, Emma, primary, Vihta, Karina-Doris, additional, Eyre, David W, additional, Hopkins, Susan, additional, Peto, Tim E A, additional, Matthews, Philippa C, additional, Stoesser, Nicole, additional, Studley, Ruth, additional, Rourke, Emma, additional, Diamond, Ian, additional, Pouwels, Koen B, additional, Walker, Ann Sarah, additional, and Infection Survey Team, the COVID-19, additional

Published
2024
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24. A systematic review on the excess health risk of antibiotic-resistant bloodstream infections for six key pathogens in Europe

Author

Hassoun-Kheir, Nasreen, primary, Guedes, Mariana, additional, Ngo Nsoga, Marie-Therese, additional, Argante, Lorenzo, additional, Arieti, Fabiana, additional, Gladstone, Beryl P., additional, Kingston, Rhys, additional, Naylor, Nichola R., additional, Pezzani, Maria D., additional, Pouwels, Koen B., additional, Robotham, Julie V., additional, Rodríguez-Baño, Jesús, additional, Tacconelli, Evelina, additional, Vella, Venanzio, additional, Harbarth, Stephan, additional, de Kraker, Marlieke E.A., additional, Barana, Benedetta, additional, Cappelli, Eva, additional, De Rui, Maria Elena, additional, El-Abasiri, Radwa A., additional, Galia, Liliana, additional, Geurtsen, Jeroen, additional, Mejia, Jorly, additional, Palladino, Andrea, additional, Piljic, Alen, additional, Rajendran, Nithya Babu, additional, Reyna-Villasmil, Eduardo, additional, and Schmidt, Johannes E., additional

Published
2024
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26. Impact of vaccination on new SARS-CoV-2 infections in the United Kingdom

Author

Pritchard, Emma, Matthews, Philippa C., Stoesser, Nicole, Eyre, David W., Gethings, Owen, Vihta, Karina-Doris, Jones, Joel, House, Thomas, VanSteenHouse, Harper, Bell, Iain, Bell, John I., Newton, John N., Farrar, Jeremy, Diamond, Ian, Rourke, Emma, Studley, Ruth, Crook, Derrick, Peto, Tim E. A., Walker, A. Sarah, and Pouwels, Koen B.

Published
2021
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28. A systematic review on the excess health risk of antibiotic-resistant bloodstream infections for six key pathogens in Europe

Author

Rodríguez-Baño, Jesús [0000-0001-6732-9001], Hassoun-Kheir, Nasreen, Guedes, Mariana, Ngo Nsoga, Marie Therese, Argante, Lorenzo, Arieti, Fabiana, Gladstone, Beryl Primrose, Kingston, Rhys, Naylor, Nichola R., Pezzani, Maria Diletta, Pouwels, Koen B., Robotham, Julie V., Rodríguez-Baño, Jesús, Tacconelli, Evelina, Vella, Venanzio, Harbarth, Stephan, Kraker, Marlieke de, PrIMAVeRa Work Package, Barana, Benedetta, Cappelli, Eva, De Rui, Maria Elena, El-Abasiri, Radwa A., Galia, Liliana, Geurtsen, Jeroen, Mejia, Jorly, Palladino, Andrea, Piljic, Alen, Rajendran, N. B., Reyna-Villasmil, Eduardo, Schmidt, Johannes, Rodríguez-Baño, Jesús [0000-0001-6732-9001], Hassoun-Kheir, Nasreen, Guedes, Mariana, Ngo Nsoga, Marie Therese, Argante, Lorenzo, Arieti, Fabiana, Gladstone, Beryl Primrose, Kingston, Rhys, Naylor, Nichola R., Pezzani, Maria Diletta, Pouwels, Koen B., Robotham, Julie V., Rodríguez-Baño, Jesús, Tacconelli, Evelina, Vella, Venanzio, Harbarth, Stephan, Kraker, Marlieke de, PrIMAVeRa Work Package, Barana, Benedetta, Cappelli, Eva, De Rui, Maria Elena, El-Abasiri, Radwa A., Galia, Liliana, Geurtsen, Jeroen, Mejia, Jorly, Palladino, Andrea, Piljic, Alen, Rajendran, N. B., Reyna-Villasmil, Eduardo, and Schmidt, Johannes

Abstract

[Background] Antimicrobial resistance is a global threat, which requires novel intervention strategies, for which priority pathogens and settings need to be determined., [Objectives] We evaluated pathogen-specific excess health burden of drug-resistant bloodstream infections (BSIs) in Europe., [Methods] A systematic review and meta-analysis., [Data sources] MEDLINE, Embase, and grey literature for the period January 1990 to May 2022., [Study eligibility criteria] Studies that reported burden data for six key drug-resistant pathogens: carbapenem-resistant (CR) Pseudomonas aeruginosa and Acinetobacter baumannii, third-generation cephalosporin or CR Escherichia coli and Klebsiella pneumoniae, methicillin-resistant Staphylococcus aureus (MRSA) and vancomycin-resistant Enterococcus faecium. Excess health outcomes compared with drug-susceptible BSIs or uninfected patients. For MRSA and third-generation cephalosporin E. coli and K. pneumoniae BSIs, five or more European studies were identified. For all others, the search was extended to high-income countries., [Participants] Paediatric and adult patients diagnosed with drug-resistant BSI., [Interventions] Not applicable., [Assessment of risk of bias] An adapted version of the Joanna-Briggs Institute assessment tool., [Methods of data synthesis] Random-effect models were used to pool pathogen-specific burden estimates., [Results] We screened 7154 titles, 1078 full-texts and found 56 studies on BSIs. Most studies compared outcomes of drug-resistant to drug-susceptible BSIs (46/56, 82.1%), and reported mortality (55/56 studies, 98.6%). The pooled crude estimate for excess all-cause mortality of drug-resistant versus drug-susceptible BSIs ranged from OR 1.31 (95% CI 1.03–1.68) for CR P. aeruginosa to OR 3.44 (95% CI 1.62–7.32) for CR K. pneumoniae. Pooled crude estimates comparing mortality to uninfected patients were available for vancomycin-resistant Enterococcus and MRSA BSIs (OR of 11.19 [95% CI 6.92–18.09] and OR 6.18 [95% CI 2.10–18.17], respectively)., [Conclusions] Drug-resistant BSIs are associated with increased mortality, with the magnitude of the effect influenced by pathogen type and comparator. Future research should address crucial knowledge gaps in pathogen- and infection-specific burdens to guide development of novel interventions.

Published
2024

29. Excess resource use and cost of drug-resistant infections for six key pathogens in Europe: a systematic review and Bayesian meta-analysis

Author

Innovative Medicines Initiative, European Commission, Rodríguez-Baño, Jesús [0000-0001-6732-9001], Kingston, Rhys, Vella, Venanzio, Pouwels, Koen B., Schmidt, Johannes, Abdelatif El-Abasiri, Radwa A., Reyna-Villasmil, Eduardo, Hassoun-Kheir, Nasreen, Harbarth, Stephan, Rodríguez-Baño, Jesús, Tacconelli, Evelina, Arieti, Fabiana, Gladstone, Beryl Primrose, Kraker, Marlieke de, Naylor, Nichola R., Robotham, Julie V., PrIMAVeRa Work Package, Argante, Lorenzo, Barana, Benedetta, Cappelli, Eva, De Rui, Maria Elena, Galia, Liliana, Geurtsen, Jeroen, Guedes, Mariana, Mejia, Jorly, Palladino, Andrea, Pezzani, Maria Diletta, Piljic, Alen, Innovative Medicines Initiative, European Commission, Rodríguez-Baño, Jesús [0000-0001-6732-9001], Kingston, Rhys, Vella, Venanzio, Pouwels, Koen B., Schmidt, Johannes, Abdelatif El-Abasiri, Radwa A., Reyna-Villasmil, Eduardo, Hassoun-Kheir, Nasreen, Harbarth, Stephan, Rodríguez-Baño, Jesús, Tacconelli, Evelina, Arieti, Fabiana, Gladstone, Beryl Primrose, Kraker, Marlieke de, Naylor, Nichola R., Robotham, Julie V., PrIMAVeRa Work Package, Argante, Lorenzo, Barana, Benedetta, Cappelli, Eva, De Rui, Maria Elena, Galia, Liliana, Geurtsen, Jeroen, Guedes, Mariana, Mejia, Jorly, Palladino, Andrea, Pezzani, Maria Diletta, and Piljic, Alen

Abstract

[Background] Quantifying the resource use and cost of antimicrobial resistance establishes the magnitude of the problem and drives action., [Objectives] Assessment of resource use and cost associated with infections with six key drug-resistant pathogens in Europe., [Methods] A systematic review and Bayesian meta-analysis., [Data sources] MEDLINE (Ovid), Embase (Ovid), Econlit databases, and grey literature for the period 1 January 1990, to 21 June 2022., [Study eligibility criteria] Resource use and cost outcomes (including excess length of stay, overall costs, and other excess in or outpatient costs) were compared between patients with defined antibiotic-resistant infections caused by carbapenem-resistant (CR) Pseudomonas aeruginosa and Acinetobacter baumannii, CR or third-generation cephalosporin Escherichia coli (3GCREC) and Klebsiella pneumoniae, methicillin-resistant Staphylococcus aureus, and vancomycin-resistant Enterococcus faecium, and patients with drug-susceptible or no infection., [Participants] All patients diagnosed with drug-resistant bloodstream infections (BSIs)., [Interventions] NA., [Assessment of risk of bias] An adapted version of the Joanna Briggs Institute assessment tool, incorporating case-control, cohort, and economic assessment frameworks., [Methods of data synthesis] Hierarchical Bayesian meta-analyses were used to assess pathogen-specific resource use estimates., [Results] Of 5969 screened publications, 37 were included in the review. Data were sparse and heterogeneous. Most studies estimated the attributable burden by, comparing resistant and susceptible pathogens (32/37). Four studies analysed the excess cost of hospitalization attributable to 3GCREC BSIs, ranging from -€ 2465.50 to € 6402.81. Eight studies presented adjusted excess length of hospital stay estimates for methicillin-resistant S. aureus and 3GCREC BSIs (4 each) allowing for Bayesian hierarchical analysis, estimating means of 1.26 (95% credible interval [CrI], −0.72 to 4.17) and 1.78 (95% CrI, −0.02 to 3.38) days, respectively., [Conclusions] Evidence on most cost and resource use outcomes and across most pathogen-resistance combinations was severely lacking. Given the importance of this evidence for rational policymaking, further research is urgently needed.

Published
2024

30. Employment outcomes of people with Long Covid symptoms: community-based cohort study.

Author

Ayoubkhani, Daniel, Zaccardi, Francesco, Pouwels, Koen B, Walker, A Sarah, Houston, Donald, Alwan, Nisreen A, Martin, Josh, Khunti, Kamlesh, and Nafilyan, Vahé

Subjects
STATISTICAL models, JOB absenteeism, RESEARCH funding, POST-acute COVID-19 syndrome, SCIENTIFIC observation, DESCRIPTIVE statistics, DISEASE prevalence, LONGITUDINAL method, PRE-tests & post-tests, LABOR market, ODDS ratio, COMPARATIVE studies, CONFIDENCE intervals, EMPLOYMENT, COVID-19
Abstract

Background Evidence on the long-term employment consequences of SARS-CoV-2 infection is lacking. We used data from a large, community-based sample in the UK to estimate associations between Long Covid and employment outcomes. Methods This was an observational, longitudinal study using a pre–post design. We included survey participants from 3 February 2021 to 30 September 2022 when they were aged 16–64 years and not in education. Using conditional logit modelling, we explored the time-varying relationship between Long Covid status ≥12 weeks after a first test-confirmed SARS-CoV-2 infection (reference: pre-infection) and labour market inactivity (neither working nor looking for work) or workplace absence lasting ≥4 weeks. Results Of 206 299 participants (mean age 45 years, 54% female, 92% white), 15% were ever labour market inactive and 10% were ever long-term absent during follow-up. Compared with pre-infection, inactivity was higher in participants reporting Long Covid 30 to <40 weeks [adjusted odds ratio (aOR): 1.45; 95% CI: 1.17–1.81] or 40 to <52 weeks (aOR: 1.34; 95% CI: 1.05–1.72) post-infection. Combining with official statistics on Long Covid prevalence, and assuming a correct statistical model, our estimates translate to 27 000 (95% CI: 6000–47 000) working-age adults in the UK being inactive because of Long Covid in July 2022. Conclusions Long Covid is likely to have contributed to reduced participation in the UK labour market, though it is unlikely to be the sole driver. Further research is required to quantify the contribution of other factors, such as indirect health effects of the pandemic. [ABSTRACT FROM AUTHOR]

Published
2024
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31. Projecting health and economic impacts of Lassa vaccination campaigns in West Africa

Author

Smith, David R M, primary, Turner, Joanne, additional, Fahr, Patrick, additional, Attfield, Lauren A, additional, Bessell, Paul R, additional, Donnelly, Christl A, additional, Gibb, Rory, additional, Jones, Kate E, additional, Redding, David W, additional, Asogun, Danny, additional, Ayodeji, Oladele Oluwafemi, additional, Azuogu, Benedict N, additional, Fischer, William A, additional, Jan, Kamji, additional, Olayinka, Adebola T, additional, Wohl, David A, additional, Torkelson, Andrew A, additional, Dinkel, Katelyn A, additional, Nixon, Emily J, additional, Pouwels, Koen B, additional, and Hollingsworth, T Déirdre, additional

Published
2024
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32. Costs-effectiveness and cost components of pharmaceutical and non-pharmaceutical interventions affecting antibiotic resistance outcomes in hospital patients: a systematic literature review

Author

Allel, Kasim, primary, Hernández-Leal, María José, additional, Naylor, Nichola R, additional, Undurraga, Eduardo A., additional, Abou Jaoude, Gerard Joseph, additional, Bhandari, Priyanka, additional, Flanagan, Ellen, additional, Haghparast-Bidgoli, Hassan, additional, Pouwels, Koen B, additional, and Yakob, Laith, additional

Published
2024
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36. Reducing the Antigen Prevalence Target Threshold for Stopping and Restarting Mass Drug Administration for Lymphatic Filariasis Elimination: A Model-Based Cost-effectiveness Simulation in Tanzania, India and Haiti.

Author

Oliver, Mary Chriselda Antony, Graham, Matthew, Gass, Katherine M, Medley, Graham F, Clark, Jessica, Davis, Emma L, Reimer, Lisa J, King, Jonathan D, Pouwels, Koen B, and Hollingsworth, T Déirdre

Subjects
COST effectiveness, INFECTION control, RESEARCH funding, DRUG administration, EVALUATION of medical care, DESCRIPTIVE statistics, WORLD health, ANTIGENS, VACCINATION coverage, ELEPHANTIASIS, MATHEMATICAL models, PUBLIC health, THEORY, MOSQUITO-borne diseases, DRUG tolerance, MEDICAL care costs, DISEASE complications
Abstract

Background The Global Programme to Eliminate Lymphatic Filariasis (GPELF) aims to reduce and maintain infection levels through mass drug administration (MDA), but there is evidence of ongoing transmission after MDA in areas where Culex mosquitoes are the main transmission vector, suggesting that a more stringent criterion is required for MDA decision making in these settings. Methods We use a transmission model to investigate how a lower prevalence threshold (<1% antigenemia [Ag] prevalence compared with <2% Ag prevalence) for MDA decision making would affect the probability of local elimination, health outcomes, the number of MDA rounds, including restarts, and program costs associated with MDA and surveys across different scenarios. To determine the cost-effectiveness of switching to a lower threshold, we simulated 65% and 80% MDA coverage of the total population for different willingness to pay per disability-adjusted life-year averted for India ($446.07), Tanzania ($389.83), and Haiti ($219.84). Results Our results suggest that with a lower Ag threshold, there is a small proportion of simulations where extra rounds are required to reach the target, but this also reduces the need to restart MDA later in the program. For 80% coverage, the lower threshold is cost-effective across all baseline prevalences for India, Tanzania, and Haiti. For 65% MDA coverage, the lower threshold is not cost-effective due to additional MDA rounds, although it increases the probability of local elimination. Valuing the benefits of elimination to align with the GPELF goals, we find that a willingness to pay per capita government expenditure of approximately $1000–$4000 for 1% increase in the probability of local elimination would be required to make a lower threshold cost-effective. Conclusions Lower Ag thresholds for stopping MDAs generally mean a higher probability of local elimination, reducing long-term costs and health impacts. However, they may also lead to an increased number of MDA rounds required to reach the lower threshold and, therefore, increased short-term costs. Collectively, our analyses highlight that lower target Ag thresholds have the potential to assist programs in achieving lymphatic filariasis goals. [ABSTRACT FROM AUTHOR]

Published
2024
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40. Quantitative SARS-CoV-2 anti-spike responses to Pfizer–BioNTech and Oxford–AstraZeneca vaccines by previous infection status

Author

Eyre, David W., Lumley, Sheila F., Wei, Jia, Cox, Stuart, James, Tim, Justice, Anita, Jesuthasan, Gerald, O'Donnell, Denise, Howarth, Alison, Hatch, Stephanie B., Marsden, Brian D., Jones, E. Yvonne, Stuart, David I., Ebner, Daniel, Hoosdally, Sarah, Crook, Derrick W., Peto, Tim E.A., Walker, Timothy M., Stoesser, Nicole E., Matthews, Philippa C., Pouwels, Koen B., Walker, A. Sarah, and Jeffery, Katie

Published
2021
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41. Public preferences for delayed or immediate antibiotic prescriptions in UK primary care: A choice experiment

Author

Morrell, Liz, Buchanan, James, Roope, Laurence S. J., Pouwels, Koen B., Butler, Christopher C., Hayhoe, Benedict, Tonkin-Crine, Sarah, McLeod, Monsey, Robotham, Julie V., Holmes, Alison, Walker, A. Sarah, and Wordsworth, Sarah

Subjects
Consumer preferences -- Surveys, Drugs -- Prescribing, Respiratory tract infections -- Surveys -- Drug therapy, Primary health care -- Surveys, Antibiotics -- Dosage and administration -- Surveys, Biological sciences
Abstract

Background Delayed (or 'backup') antibiotic prescription, where the patient is given a prescription but advised to delay initiating antibiotics, has been shown to be effective in reducing antibiotic use in primary care. However, this strategy is not widely used in the United Kingdom. This study aimed to identify factors influencing preferences among the UK public for delayed prescription, and understand their relative importance, to help increase appropriate use of this prescribing option. Methods and findings We conducted an online choice experiment in 2 UK general population samples: adults and parents of children under 18 years. Respondents were presented with 12 scenarios in which they, or their child, might need antibiotics for a respiratory tract infection (RTI) and asked to choose either an immediate or a delayed prescription. Scenarios were described by 7 attributes. Data were collected between November 2018 and February 2019. Respondent preferences were modelled using mixed-effects logistic regression. The survey was completed by 802 adults and 801 parents (75% of those who opened the survey). The samples reflected the UK population in age, sex, ethnicity, and country of residence. The most important determinant of respondent choice was symptom severity, especially for cough-related symptoms. In the adult sample, the probability of choosing delayed prescription was 0.53 (95% confidence interval (CI) 0.50 to 0.56, p < 0.001) for a chesty cough and runny nose compared to 0.30 (0.28 to 0.33, p < 0.001) for a chesty cough with fever, 0.47 (0.44 to 0.50, p < 0.001) for sore throat with swollen glands, and 0.37 (0.34 to 0.39, p < 0.001) for sore throat, swollen glands, and fever. Respondents were less likely to choose delayed prescription with increasing duration of illness (odds ratio (OR) 0.94 (0.92 to 0.96, p < 0.001)). Probabilities of choosing delayed prescription were similar for parents considering treatment for a child (44% of choices versus 42% for adults, p = 0.04). However, parents differed from the adult sample in showing a more marked reduction in choice of the delayed prescription with increasing duration of illness (OR 0.83 (0.80 to 0.87) versus 0.94 (0.92 to 0.96) for adults, p for heterogeneity p < 0.001) and a smaller effect of disruption of usual activities (OR 0.96 (0.95 to 0.97) versus 0.93 (0.92 to 0.94) for adults, p for heterogeneity p < 0.001). Females were more likely to choose a delayed prescription than males for minor symptoms, particularly minor cough (probability 0.62 (0.58 to 0.66, p < 0.001) for females and 0.45 (0.41 to 0.48, p < 0.001) for males). Older people, those with a good understanding of antibiotics, and those who had not used antibiotics recently showed similar patterns of preferences. Study limitations include its hypothetical nature, which may not reflect real-life behaviour; the absence of a 'no prescription' option; and the possibility that study respondents may not represent the views of population groups who are typically underrepresented in online surveys. Conclusions This study found that delayed prescription appears to be an acceptable approach to reducing antibiotic consumption. Certain groups appear to be more amenable to delayed prescription, suggesting particular opportunities for increased use of this strategy. Prescribing choices for sore throat may need additional explanation to ensure patient acceptance, and parents in particular may benefit from reassurance about the usual duration of these illnesses., Author(s): Liz Morrell 1,*, James Buchanan 1,2,3, Laurence S. J. Roope 1,2,3, Koen B. Pouwels 1,2, Christopher C. Butler 2,4, Benedict Hayhoe 5, Sarah Tonkin-Crine 2,4, Monsey McLeod 6,7,8, Julie [...]

Published
2021
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43. Incidence of Respiratory Syncytial Virus Infection in Older Adults: Limitations of Current Data

Author

CTI Bont, Infectieziekten onderzoek1 (Bont), Child Health, Infection & Immunity, Rozenbaum, Mark H., Begier, Elizabeth, Kurosky, Samantha K., Whelan, Jo, Bem, Danai, Pouwels, Koen B., Postma, Maarten, Bont, Louis, CTI Bont, Infectieziekten onderzoek1 (Bont), Child Health, Infection & Immunity, Rozenbaum, Mark H., Begier, Elizabeth, Kurosky, Samantha K., Whelan, Jo, Bem, Danai, Pouwels, Koen B., Postma, Maarten, and Bont, Louis

Published
2023

45. Health and economic impacts of Lassa vaccination campaigns in West Africa

Author

Smith, David R. M., Turner, Joanne, Fahr, Patrick, Attfield, Lauren A., Bessell, Paul R., Donnelly, Christl A., Gibb, Rory, Jones, Kate E., Redding, David W., Asogun, Danny, Ayodeji, Oladele Oluwafemi, Azuogu, Benedict N., Fischer, William A., Jan, Kamji, Olayinka, Adebola T., Wohl, David A., Torkelson, Andrew A., Dinkel, Katelyn A., Nixon, Emily J., Pouwels, Koen B., and Hollingsworth, T. Déirdre

Abstract

Lassa fever is a zoonotic disease identified by the World Health Organization (WHO) as having pandemic potential. This study estimates the health-economic burden of Lassa fever throughout West Africa and projects impacts of a series of vaccination campaigns. We also model the emergence of ‘Lassa-X’—a hypothetical pandemic Lassa virus variant—and project impacts of achieving 100 Days Mission vaccination targets. Our model predicted 2.7 million (95% uncertainty interval: 2.1–3.4 million) Lassa virus infections annually, resulting over 10 years in 2.0 million (793,800–3.9 million) disability-adjusted life years (DALYs). The most effective vaccination strategy was a population-wide preventive campaign primarily targeting WHO-classified ‘endemic’ districts. Under conservative vaccine efficacy assumptions, this campaign averted $20.1 million ($8.2–$39.0 million) in lost DALY value and $128.2 million ($67.2–$231.9 million) in societal costs (2021 international dollars ($)). Reactive vaccination in response to local outbreaks averted just one-tenth the health-economic burden of preventive campaigns. In the event of Lassa-X emerging, spreading throughout West Africa and causing approximately 1.2 million DALYs within 2 years, 100 Days Mission vaccination averted 22% of DALYs given a vaccine 70% effective against disease and 74% of DALYs given a vaccine 70% effective against both infection and disease. These findings suggest how vaccination could alleviate Lassa fever’s burden and assist in pandemic preparedness.

Published
2024
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47. Impact of the COVID-19 pandemic on antimicrobial stewardship support for general practices in England: a qualitative interview study.

Author

Campbell, Anne, Borek, Aleksandra J., McLeod, Monsey, Tonkin-Crine, Sarah, Pouwels, Koen B., Roope, Laurence S. J., Hayhoe, Benedict W. J., Majeed, Azeem, Walker, A Sarah, and Holmes, Alison

Subjects
HEALTH self-care, QUALITATIVE research, RESEARCH funding, PRIMARY health care, ANTIMICROBIAL stewardship, INTERVIEWING, MEDICAL care, COVID-19 vaccines, DESCRIPTIVE statistics, SOUND recordings, THEMATIC analysis, ATTITUDES of medical personnel, RESEARCH methodology, SOCIAL support, DATA analysis software, COVID-19 pandemic, SOCIAL distancing
Abstract

Background: In England, clinical commissioning group (CCG; now replaced by Integrated Care Systems [ICSs]) and primary care network (PCN) professionals support primary care prescribers to optimise antimicrobial stewardship (AMS). Aim: To explore views and experiences of CCG and PCN staff in supporting AMS, and the impact of COVID-19 on this support. Design & setting: Qualitative interview study in primary care in England. Method: Semi-structured interviews with staff from CCG and PCNs responsible for AMS were conducted at two timepoints via telephone. These were audio-recorded, transcribed, and analysed thematically. Results: Twenty-seven interviews were conducted with 14 participants (nine CCG, five PCN) in December 2020–January 2021 and February–May 2021. The study found that AMS support was (1) deprioritised in order to keep general practice operational and deliver COVID-19 vaccines; (2) disrupted as social distancing made it harder to build relationships, conduct routine AMS activities, and challenge prescribing decisions; and (3) adapted, with opportunities identified for greater use of technology and changing patient and public perceptions of viruses and self-care. It was also found that resources to support AMS were valued if they were both novel, to counter AMS ‘fatigue’, and sufficiently familiar to fit with existing and/or future AMS. Conclusion: AMS needs to be reprioritised in general practice in the post-pandemic era and within the new ICSs in England. This should include interventions and strategies that combine novel elements with already familiar strategies to refresh prescribers’ motivation and opportunities for AMS. Behaviour change interventions should be aimed at improving the culture and processes for how PCN pharmacists voice concerns about AMS to prescribers in general practice and take advantage of the changed patient and public perceptions of viruses and self-care. [ABSTRACT FROM AUTHOR]

Published
2023
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48. Implementing antibiotic stewardship in high-prescribing English general practices: a mixed-methods study

Author

Tonkin-Crine, Sarah, primary, McLeod, Monsey, additional, Borek, Aleksandra J, additional, Campbell, Anne, additional, Anyanwu, Philip, additional, Costelloe, Céire, additional, Moore, Michael, additional, Hayhoe, Benedict, additional, Pouwels, Koen B, additional, Roope, Laurence SJ, additional, Morrell, Liz, additional, Hopkins, Susan, additional, Butler, Christopher C, additional, and Walker, Ann Sarah, additional

Published
2022
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49. Omicron-associated changes in severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) symptoms in the United Kingdom

Author

Vihta, Karina-Doris, Pouwels, Koen B, Peto, Tim EA, Pritchard, Emma, House, Thomas, Studley, Ruth, Rourke, Emma, Cook, Duncan, Diamond, Ian, Crook, Derrick, Clifton, David A, Matthews, Philippa C, Stoesser, Nicole, Eyre, David W, Walkerand, Ann Sarah, and team, COVID-19 Infection Survey

Subjects
FOS: Clinical medicine, Immunology, Infectious Disease, Genetics & Genomics
Abstract

BACKGROUND: The SARS-CoV-2 Delta variant has been replaced by the highly transmissible Omicron BA.1 variant, and subsequently by Omicron BA.2. It is important to understand how these changes in dominant variants affect reported symptoms, while also accounting for symptoms arising from other co-circulating respiratory viruses. METHODS: In a nationally representative UK community study, the COVID-19 Infection Survey, we investigated symptoms in PCR-positive infection episodes vs. PCR-negative study visits over calendar time, by age and vaccination status, comparing periods when the Delta, Omicron BA.1 and BA.2 variants were dominant. RESULTS: Between October-2020 and April-2022, 120,995 SARS-CoV-2 PCR-positive episodes occurred in 115,886 participants, with 70,683 (58%) reporting symptoms. The comparator comprised 4,766,366 PCR-negative study visits (483,894 participants); 203,422 (4%) reporting symptoms. Symptom reporting in PCR-positives varied over time, with a marked reduction in loss of taste/smell as Omicron BA.1 dominated, maintained with BA.2 (44%/45% 17 October 2021, 16%/13% 2 January 2022, 15%/12% 27 March 2022). Cough, fever, shortness of breath, myalgia, fatigue/weakness and headache also decreased after Omicron BA.1 dominated, but sore throat increased, the latter to a greater degree than concurrent increases in PCR-negatives. Fatigue/weakness increased again after BA.2 dominated, although to a similar degree to concurrent increases in PCR-negatives. Symptoms were consistently more common in adults aged 18-65 years than in children or older adults. CONCLUSIONS: Increases in sore throat (also common in the general community), and a marked reduction in loss of taste/smell, make Omicron harder to detect with symptom-based testing algorithms, with implications for institutional and national testing policies.

Published
2023
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50. Risk of Long COVID in People Infected With Severe Acute Respiratory Syndrome Coronavirus 2 After 2 Doses of a Coronavirus Disease 2019 Vaccine: Community-Based, Matched Cohort Study

Author

Ayoubkhani, Daniel, primary, Bosworth, Matthew L, additional, King, Sasha, additional, Pouwels, Koen B, additional, Glickman, Myer, additional, Nafilyan, Vahé, additional, Zaccardi, Francesco, additional, Khunti, Kamlesh, additional, Alwan, Nisreen A, additional, and Walker, A Sarah, additional

Published
2022
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