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7. Antidepressants in pregnancy: applying causal epidemiological methods to understand service-use outcomes in women and long-term neurodevelopmental outcomes in exposed children

Author

Heuvelman Hein, Davies Neil M, Ben-Shlomo Yoav, Emond Alan, Evans Jonathan, Gunnell David, Liebling Rachel, Morris Richard, Payne Rupert, Storey Claire, Viner Maria, and Rai Dheeraj

Subjects
humans, child, cohort studies, female, pregnancy, united kingdom, patient admission, mothers, depression, depressive disorder, major, outpatients, pregnancy outcome, pregnant women, live birth, secondary care, inpatients, attention deficit disorder with hyperactivity, intellectual disability, propensity score, autism spectrum disorder, autistic disorder, follow-up studies, mental health, antidepressive agents, self-injurious behavior, medical records, primary health care, emergency service, hospital, hospitals, prescriptions, receptors, serotonin, socioeconomic factors, confidence intervals, regression analysis, referral and consultation, delivery of health care, cognition, decision making, Medical technology, R855-855.5
Abstract

Background Antidepressants are commonly prescribed during pregnancy, despite a lack of evidence from randomised trials on the benefits or risks. Some studies have reported associations of antidepressants during pregnancy with adverse offspring neurodevelopment, but whether or not such associations are causal is unclear. Objectives To study the associations of antidepressants for depression in pregnancy with outcomes using multiple methods to strengthen causal inference. Design This was an observational cohort design using multiple methods to strengthen causal inference, including multivariable regression, propensity score matching, instrumental variable analysis, negative control exposures, comparison across indications and exposure discordant pregnancies analysis. Setting This took place in UK general practice. Participants Participants were pregnant women with depression. Interventions The interventions were initiation of antidepressants in pregnancy compared with no initiation, and continuation of antidepressants in pregnancy compared with discontinuation. Main outcome measures The maternal outcome measures were the use of primary care and secondary mental health services during pregnancy, and during four 6-month follow-up periods up to 24 months after pregnancy, and antidepressant prescription status 24 months following pregnancy. The child outcome measures were diagnosis of autism, diagnosis of attention deficit hyperactivity disorder and intellectual disability. Data sources UK Clinical Practice Research Datalink. Results Data on 80,103 pregnancies were used to study maternal primary care outcomes and were linked to 34,274 children with at least 4-year follow-up for neurodevelopmental outcomes. Women who initiated or continued antidepressants during pregnancy were more likely to have contact with primary and secondary health-care services during and after pregnancy and more likely to be prescribed an antidepressant 2 years following the end of pregnancy than women who did not initiate or continue antidepressants during pregnancy (odds ratioinitiation 2.16, 95% confidence interval 1.95 to 2.39; odds ratiocontinuation 2.40, 95% confidence interval 2.27 to 2.53). There was little evidence for any substantial association with autism (odds ratiomultivariableregression 1.10, 95% confidence interval 0.90 to 1.35; odds ratiopropensityscore 1.06, 95% confidence interval 0.84 to 1.32), attention deficit hyperactivity disorder (odds ratiomultivariableregression 1.02, 95% confidence interval 0.80 to 1.29; odds ratiopropensityscore 0.97, 95% confidence interval 0.75 to 1.25) or intellectual disability (odds ratiomultivariableregression 0.81, 95% confidence interval 0.55 to 1.19; odds ratiopropensityscore 0.89, 95% confidence interval 0.61 to 1.31) in children of women who continued antidepressants compared with those who discontinued antidepressants. There was inconsistent evidence of an association between initiation of antidepressants in pregnancy and diagnosis of autism in offspring (odds ratiomultivariableregression 1.23, 95% confidence interval 0.85 to 1.78; odds ratiopropensityscore 1.64, 95% confidence interval 1.01 to 2.66) but not attention deficit hyperactivity disorder or intellectual disability; however, but results were imprecise owing to smaller numbers. Limitations Several causal-inference analyses lacked precision owing to limited numbers. In addition, adherence to the prescribed treatment was not measured. Conclusions Women prescribed antidepressants during pregnancy had greater service use during and after pregnancy than those not prescribed antidepressants. The evidence against any substantial association with autism, attention deficit hyperactivity disorder or intellectual disability in the children of women who continued compared with those who discontinued antidepressants in pregnancy is reassuring. Potential association of initiation of antidepressants during pregnancy with offspring autism needs further investigation. Future work Further research on larger samples could increase the robustness and precision of these findings. These methods applied could be a template for future pharmaco-epidemiological investigation of other pregnancy-related prescribing safety concerns. Funding This project was funded by the National Institute for Health and Care Research (NIHR) Health Technology Assessment programme (15/80/19) and will be published in full in Health Technology Assessment; Vol. 27, No. 15. See the NIHR Journals Library website for further project information. Plain language summary About one in seven women experience depression during pregnancy. Left untreated, this may harm them and their unborn babies. However, the decision to take antidepressants during pregnancy is difficult because women often worry about the risks to their unborn baby. Research findings have been inconsistent, so women often do not have clear information to enable them to make informed decisions. We studied women’s and children’s outcomes after starting (compared with not starting) or continuing (compared with stopping) antidepressants in pregnancy. We used a large UK primary care database and several novel methods of analysis. We tracked 80,103 pregnancies of women with depression for up to 2 years after pregnancy. We also tracked 34,274 children from these pregnancies for at least 4 years to check for developmental outcomes. Women prescribed antidepressants were more likely than women not prescribed antidepressants to use general practice and mental health services during and after pregnancy, and to be prescribed antidepressants 2 years after pregnancy. This suggests that antidepressants were being prescribed to women with greater clinical need. Women who continued antidepressants in pregnancy had no higher likelihood than those who discontinued antidepressants of autism, attention deficit hyperactivity disorder or intellectual disability in their children. This should reassure women making the decision to continue taking their medications in pregnancy. Women who started antidepressants in pregnancy may possibly have had a slightly higher likelihood of autism in their children than those who did not start them. These findings were not seen in all analyses and were based on smaller numbers; therefore, they should be viewed with caution. Importantly, over 98 in every 100 children of women who initiated or continued antidepressants in pregnancy did not receive an autism diagnosis. The findings may help women and clinicians make informed decisions on treatment with antidepressants in pregnancy. Scientific summary Background Depression is common in women of childbearing age and up to one in seven women experience depression during pregnancy. Untreated depression may have serious consequences, such as distress, self-neglect and suicidal behaviour, in affected women and birth complications in their babies. Many women with depression may, therefore, encounter a situation in which they need to decide whether to start or continue an antidepressant during their pregnancy; however, the potential for resulting harm to the neurodevelopment of their offspring is a common concern. In the absence of randomised controlled trials, the information available to guide these decisions is based on observational data, which are subject to confounding. Given that maternal depression may itself lead to adverse outcomes, isolating any effect of antidepressants from the underlying depression is particularly difficult: a problem known as confounding by indication. In the absence of randomised trials, studies designed to emulate such trials and using methods to account for confounding may help triangulate results and strengthen causal inference. Objectives This research aimed to simulate two scenarios that could be tested in pregnant women with depression in a hypothetical target randomised controlled trial asking the following research questions: Does the initiation of antidepressants for depression during pregnancy affect maternal service use outcomes and childhood neurodevelopmental outcomes? Does the continuation of antidepressant use during pregnancy for depression affect maternal service use outcomes and childhood neurodevelopmental outcomes? The data were interrogated using several methods of causal inference, and assessed in relation to dose response, timing of exposure and type of antidepressants according to class and their serotonin-receptor affinity. Methods Design: This was an observational cohort design, with use of multiple methods to strengthen causal inference. Setting and participants: This took place in UK general practice. Participants were UK primary care patients, specifically pregnant women with depression. Data sources: This study used data from the Clinical Practice Research Datalink (CPRD), a large ongoing database of anonymised primary care medical records in the UK. The CPRD’s pregnancy register was used to identify the dates and stages of pregnancy, and the CPRD mother–baby link allowed for the linkage of the records of pregnant women with their live born offspring. For consenting CPRD practices in England, the primary care records were linked to Hospital Episode Statistics, which include registers for inpatient admissions, outpatient care and accident and emergency (A&E) attendance in England, and with mortality data from the Office for National Statistics and Census small-area socioeconomic data. Eligible patients: The data extract covered dates between 1 January 1995 and 31 December 2017. Within this time frame, we identified 344,720 pregnancies in the pregnancy register for which there was evidence of depressive symptoms, or prescription of an antidepressant up to 1 year before or during pregnancy. From this sample, we constructed two cohorts: (1) the pregnant women’s cohort, which contained all pregnancies for which women could be followed up for at least 2 years beyond the pregnancy end date, regardless of the pregnancy outcome or ability to link to the child; (2) the mother and child cohort, which consisted of pregnancies followed up at least until delivery that could be linked with the patient records of the children arising from these pregnancies. The pregnant women’s cohort: The exclusion criteria were (1) records for which the general practice was not yet up to standard, as defined by CPRD (n = 61,704); (2) where the patient had not yet registered with her current general practice 1 year prior to conception (n = 93,638); (3) records suggesting that the woman had transferred out of the general practice while still pregnant (n = 15,627); (4) records with

Published
2023
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8. COVID-19 trajectories among 57 million adults in England: a cohort study using electronic health records

Author

Abbasizanjani, Hoda, Ahmed, Nida, Ahmed, Badar, Akbari, Ashley, Akinoso-Imran, Abdul Qadr, Allara, Elias, Allery, Freya, Angelantonio, Emanuele Di, Ashworth, Mark, Ayyar-Gupta, Vandana, Babu-Narayan, Sonya, Bacon, Seb, Ball, Steve, Banerjee, Ami, Barber, Mark, Barrett, Jessica, Bennie, Marion, Berry, Colin, Beveridge, Jennifer, Birney, Ewan, Bojanić, Lana, Bolton, Thomas, Bone, Anna, Boyle, Jon, Braithwaite, Tasanee, Bray, Ben, Briffa, Norman, Brind, David, Brown, Katherine, Buch, Maya, Canoy, Dexter, Caputo, Massimo, Carragher, Raymond, Carson, Alan, Cezard, Genevieve, Chang, Jen-Yu Amy, Cheema, Kate, Chin, Richard, Chudasama, Yogini, Cooper, Jennifer, Copland, Emma, Crallan, Rebecca, Cripps, Rachel, Cromwell, David, Curcin, Vasa, Curry, Gwenetta, Dale, Caroline, Danesh, John, Das-Munshi, Jayati, Dashtban, Ashkan, Davies, Alun, Davies, Joanna, Davies, Gareth, Davies, Neil, Day, Joshua, Delmestri, Antonella, Denaxas, Spiros, Denholm, Rachel, Dennis, John, Denniston, Alastair, Deo, Salil, Dhillon, Baljean, Docherty, Annemarie, Dong, Tim, Douiri, Abdel, Downs, Johnny, Dregan, Alexandru, Ellins, Elizabeth A, Elwenspoek, Martha, Falck, Fabian, Falter, Florian, Fan, Yat Yi, Firth, Joseph, Fraser, Lorna, Friebel, Rocco, Gavrieli, Amir, Gerstung, Moritz, Gilbert, Ruth, Gillies, Clare, Glickman, Myer, Goldacre, Ben, Goldacre, Raph, Greaves, Felix, Green, Mark, Grieco, Luca, Griffiths, Rowena, Gurdasani, Deepti, Halcox, Julian, Hall, Nick, Hama, Tuankasfee, Handy, Alex, Hansell, Anna, Hardelid, Pia, Hardy, Flavien, Harris, Daniel, Harrison, Camille, Harron, Katie, Hassaine, Abdelaali, Hassan, Lamiece, Healey, Russell, Hemingway, Harry, Henderson, Angela, Herz, Naomi, Heyl, Johannes, Hidajat, Mira, Higginson, Irene, Hinchliffe, Rosie, Hippisley-Cox, Julia, Ho, Frederick, Hocaoglu, Mevhibe, Hollings, Sam, Horne, Elsie, Hughes, David, Humberstone, Ben, Inouye, Mike, Ip, Samantha, Islam, Nazrul, Jackson, Caroline, Jenkins, David, Jiang, Xiyun, Johnson, Shane, Kadam, Umesh, Kallis, Costas, Karim, Zainab, Kasan, Jake, Katsoulis, Michalis, Kavanagh, Kim, Kee, Frank, Keene, Spencer, Kent, Seamus, Khalid, Sara, Khawaja, Anthony, Khunti, Kamlesh, Killick, Richard, Kinnear, Deborah, Knight, Rochelle, Kolamunnage-Dona, Ruwanthi, Kontopantelis, Evan, Kurdi, Amanj, Lacey, Ben, Lai, Alvina, Lambarth, Andrew, Larzjan, Milad Nazarzadeh, Lawler, Deborah, Lawrence, Thomas, Lawson, Claire, Li, Qiuju, Li, Ken, Llinares, Miguel Bernabeu, Lorgelly, Paula, Lowe, Deborah, Lyons, Jane, Lyons, Ronan, Machado, Pedro, Macleod, Mary Joan, Macleod, John, Malgapo, Evaleen, Mamas, Mamas, Mamouei, Mohammad, Manohar, Sinduja, Mapeta, Rutendo, Martelli, Javiera Leniz, Martos, David Moreno, Mateen, Bilal, McCarthy, Aoife, Melville, Craig, Milton, Rebecca, Mizani, Mehrdad, Moncusi, Marta Pineda, Morales, Daniel, Mordi, Ify, Morrice, Lynn, Morris, Carole, Morris, Eva, Mu, Yi, Mueller, Tanja, Murdock, Lars, Nafilyan, Vahé, Nicholson, George, Nikiphorou, Elena, Nolan, John, Norris, Tom, Norris, Ruth, North, Laura, North, Teri-Louise, O'Connell, Dan, Oliver, Dominic, Oluyase, Adejoke, Olvera-Barrios, Abraham, Omigie, Efosa, Onida, Sarah, Padmanabhan, Sandosh, Palmer, Tom, Pasea, Laura, Patel, Riyaz, Payne, Rupert, Pell, Jill, Petitjean, Carmen, Pherwani, Arun, Pickrell, Owen, Pierotti, Livia, Pirmohamed, Munir, Priedon, Rouven, Prieto-Alhambra, Dani, Proudfoot, Alastair, Quinn, Terry, Quint, Jennifer, Raffetti, Elena, Rahimi, Kazem, Rao, Shishir, Razieh, Cameron, Roberts, Brian, Rogers, Caroline, Rossdale, Jennifer, Salim, Safa, Samani, Nilesh, Sattar, Naveed, Schnier, Christian, Schwartz, Roy, Selby, David, Seminog, Olena, Shabnam, Sharmin, Shah, Ajay, Shelton, Jon, Sheppard, James, Sinha, Shubhra, Skrypak, Mirek, Slapkova, Martina, Sleeman, Katherine, Smith, Craig, Sofat, Reecha, Sosenko, Filip, Sperrin, Matthew, Steeg, Sarah, Sterne, Jonathan, Stoica, Serban, Sudell, Maria, Sudlow, Cathie, Sun, Luanluan, Suseeladevi, Arun Karthikeyan, Sweeting, Michael, Sydes, Matt, Takhar, Rohan, Tang, Howard, Thygesen, Johan, Tilston, George, Tochel, Claire, Toit, Clea du, Tomlinson, Christopher, Toms, Renin, Torabi, Fatemeh, Torralbo, Ana, Townson, Julia, Tufail, Adnan, Tungamirai, Tapiwa, Varma, Susheel, Vollmer, Sebastian, Walker, Venexia, Wang, Tianxiao, Wang, Huan, Warwick, Alasdair, Watkinson, Ruth, Watson, Harry, Whiteley, William, Whittaker, Hannah, Wilde, Harry, Wilkinson, Tim, Williams, Gareth, Williams, Michelle, Williams, Richard, Withnell, Eloise, Wolfe, Charles, Wood, Angela, Wright, Lucy, Wu, Honghan, Wu, Jinge, Wu, Jianhua, Yates, Tom, Zaccardi, Francesco, Zhang, Haoting, Zhang, Huayu, Zuccolo, Luisa, Thygesen, Johan H, Mizani, Mehrdad A, Banerjee, Amitava, Lai, Alvina G, Li, Kezhi, Mateen, Bilal A, Sterne, Jonathan A C, Pagel, Christina, and Whiteley, William N

Published
2022
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9. Computationally efficient methods for fitting mixed models to electronic health records data

Author

Rhodes, Kirsty, Turner, Rebecca, Payne, Rupert, and White, Ian

Subjects
Statistics - Methodology
Abstract

Motivated by two case studies using primary care records from the Clinical Practice Research Datalink, we describe statistical methods that facilitate the analysis of tall data, with very large numbers of observations. Our focus is on investigating the association between patient characteristics and an outcome of interest, while allowing for variation among general practices. We explore ways to fit mixed effects models to tall data, including predictors of interest and confounding factors as covariates, and including random intercepts to allow for heterogeneity in outcome among practices. We introduce: (1) weighted regression and (2) meta-analysis of estimated regression coefficients from each practice. Both methods reduce the size of the dataset, thus decreasing the time required for statistical analysis. We compare the methods to an existing subsampling approach. All methods give similar point estimates, and weighted regression and meta-analysis give similar standard errors for point estimates to analysis of the entire dataset, but the subsampling method gives larger standard errors. Where all data are discrete, weighted regression is equivalent to fitting the mixed model to the entire dataset. In the presence of a continuous covariate, meta-analysis is useful. Both methods are easy to implement in standard statistical software.

Published
2017

10. Collaborative discussions between GPs and pharmacists to optimise patient medication: a qualitative study within a UK primary care clinical trial.

Author

Parslow, Roxanne M, Duncan, Lorna J, Caddick, Barbara, Chew-Graham, Carolyn A, Turner, Katrina, Payne, Rupert A, Man, Cindy, Guthrie, Bruce, Blair, Peter S, and McCahon, Deborah

Subjects
INTERPROFESSIONAL collaboration, PHARMACIST-patient relationships, MEDICATION reconciliation, GENERAL practitioners, PHARMACISTS
Abstract

Background: There has been significant investment in pharmacists working in UK general practice to improve the effective and safe use of medicines. However, evidence of how to optimise collaboration between GPs and pharmacists in the context of polypharmacy (multiple medication) is lacking. Aim: To explore GP and pharmacist views and experiences of in-person, interprofessional collaborative discussions (IPCDs) as part of a complex intervention to optimise medication use for patients with polypharmacy in general practice. Design and setting: A mixed-method process evaluation embedded within the Improving Medicines use in People with Polypharmacy in Primary Care (IMPPP) trial conducted in Bristol and the West Midlands, between February 2021 and September 2023. Method: Audio-recordings of IPCDs between GPs and pharmacists, along with individual semi-structured interviews to explore their reflections on these discussions, were used. All recordings were transcribed verbatim and analysed thematically. Results: A total of 14 practices took part in the process evaluation from February 2022 to September 2023; 17 IPCD meetings were audio-recorded, discussing 30 patients (range 1–6 patients per meeting). In all, six GPs and 13 pharmacists were interviewed. The IPCD was highly valued by GPs and pharmacists who described benefits, including: strengthening their working relationship; gaining in confidence to manage more complex patients; and learning from each other. It was often challenging, however, to find time for the IPCDs. Conclusion: The model of IPCD used in this study provided protected time for GPs and pharmacists to work together to deliver whole-patient care, with both professions finding this beneficial. Protected time for interprofessional liaison and collaboration, and structured interventions may facilitate improved patient care. [ABSTRACT FROM AUTHOR]

Published
2024
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14. EFFECT OF ANTIHYPERTENSIVE DEPRESCRIBING ON SERIOUS ADVERSE EVENTS, MORTALITY, AND CARDIOVASCULAR DISEASE: LONG-TERM FOLLOW-UP OF THE OPTIMISE RANDOMISED CONTROLLED TRIAL

Author

Sheppard, James, primary, Temple, Eleanor, additional, Wang, Ariel, additional, Smith, Anne, additional, Pollock, Stephanie, additional, Ford, Gary, additional, Hobbs, Richard, additional, Kenealy, Nicola, additional, Lown, Mark, additional, De Lusignan, Simon, additional, Mant, Jonathan, additional, Mccartney, David, additional, Payne, Rupert, additional, Williams, Marney, additional, Yu, Ly -Mee, additional, and Mcmanus, Richard, additional

Published
2024
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16. The association between antihypertensive treatment and serious adverse events by age and frailty: A cohort study

Author

Sheppard, James P., Koshiaris, Constantinos, Stevens, Richard, Lay-Flurrie, Sarah, Banerjee, Amitava, Bellows, Brandon K., Clegg, Andrew, Hobbs, F. D. Richard, Payne, Rupert A., Swain, Subhashisa, Usher-Smith, Juliet A., and McManus, Richard J.

Subjects
Biological sciences
Abstract

Background Antihypertensives are effective at reducing the risk of cardiovascular disease, but limited data exist quantifying their association with serious adverse events, particularly in older people with frailty. This study aimed to examine this association using nationally representative electronic health record data. Methods and findings This was a retrospective cohort study utilising linked data from 1,256 general practices across England held within the Clinical Practice Research Datalink between 1998 and 2018. Included patients were aged 40+ years, with a systolic blood pressure reading between 130 and 179 mm Hg, and not previously prescribed antihypertensive treatment. The main exposure was defined as a first prescription of antihypertensive treatment. The primary outcome was hospitalisation or death within 10 years from falls. Secondary outcomes were hypotension, syncope, fractures, acute kidney injury, electrolyte abnormalities, and primary care attendance with gout. The association between treatment and these serious adverse events was examined by Cox regression adjusted for propensity score. This propensity score was generated from a multivariable logistic regression model with patient characteristics, medical history and medication prescriptions as covariates, and new antihypertensive treatment as the outcome. Subgroup analyses were undertaken by age and frailty. Of 3,834,056 patients followed for a median of 7.1 years, 484,187 (12.6%) were prescribed new antihypertensive treatment in the 12 months before the index date (baseline). Antihypertensives were associated with an increased risk of hospitalisation or death from falls (adjusted hazard ratio [aHR] 1.23, 95% confidence interval (CI) 1.21 to 1.26), hypotension (aHR 1.32, 95% CI 1.29 to 1.35), syncope (aHR 1.20, 95% CI 1.17 to 1.22), acute kidney injury (aHR 1.44, 95% CI 1.41 to 1.47), electrolyte abnormalities (aHR 1.45, 95% CI 1.43 to 1.48), and primary care attendance with gout (aHR 1.35, 95% CI 1.32 to 1.37). The absolute risk of serious adverse events with treatment was very low, with 6 fall events per 10,000 patients treated per year. In older patients (80 to 89 years) and those with severe frailty, this absolute risk was increased, with 61 and 84 fall events per 10,000 patients treated per year (respectively). Findings were consistent in sensitivity analyses using different approaches to address confounding and taking into account the competing risk of death. A strength of this analysis is that it provides evidence regarding the association between antihypertensive treatment and serious adverse events, in a population of patients more representative than those enrolled in previous randomised controlled trials. Although treatment effect estimates fell within the 95% CIs of those from such trials, these analyses were observational in nature and so bias from unmeasured confounding cannot be ruled out. Conclusions Antihypertensive treatment was associated with serious adverse events. Overall, the absolute risk of this harm was low, with the exception of older patients and those with moderate to severe frailty, where the risks were similar to the likelihood of benefit from treatment. In these populations, physicians may want to consider alternative approaches to management of blood pressure and refrain from prescribing new treatment., Author(s): James P. Sheppard 1,*, Constantinos Koshiaris 1, Richard Stevens 1, Sarah Lay-Flurrie 1, Amitava Banerjee 2, Brandon K. Bellows 3, Andrew Clegg 4, F. D. Richard Hobbs 1, Rupert [...]

Published
2023
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17. The Use of Primary Care Big Data in Understanding the Pharmacoepidemiology of COVID-19: A Consensus Statement From the COVID-19 Primary Care Database Consortium

Author

Dambha-Miller, Hajira, Griffin, Simon J., Young, Duncan, Watkinson, Peter, Tan, Pui San, Clift, Ashley K., Payne, Rupert A., Coupland, Carol, Hopewell, Jemma C., Mant, Jonathan, Martin, Richard M., and Hippisley-Cox, Julia

Subjects
Medical research -- Methods, Medicine, Experimental -- Methods, Big data -- Usage -- Health aspects, Medical records -- Usage, Primary health care, Health, Science and technology
Abstract

The use of big data containing millions of primary care medical records provides an opportunity for rapid research to help inform patient care and policy decisions during the first and subsequent waves of the coronavirus disease 2019 (COVID-19) pandemic. Routinely collected primary care data have previously been used for national pandemic surveillance, quantifying associations between exposures and outcomes, identifying high risk populations, and examining the effects of interventions at scale, but there is no consensus on how to effectively conduct or report these data for COVID-19 research. A COVID-19 primary care database consortium was established in April 2020 and its researchers have ongoing COVID-19 projects in overlapping data sets with over 40 million primary care records in the United Kingdom that are variously linked to public health, secondary care, and vital status records. This consensus agreement is aimed at facilitating transparency and rigor in methodological approaches, and consistency in defining and reporting cases, exposures, confounders, stratification variables, and outcomes in relation to the pharmacoepidemiology of COVID-19. This will facilitate comparison, validation, and meta-analyses of research during and after the pandemic. Key words: big data; coronavirus; epidemiology; primary health care, INTRODUCTION Primary care big data refers to routinely collected anonymized general practitioner (GP) electronic health records that form large and complex longitudinal databases, often with hundreds of variables at an [...]

Published
2021
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20. Politicians, experts, and patient representatives call for the UK government to reverse the rate of antidepressant prescribing

Author

Davies, James, primary, Read, John, additional, Kruger, Danny, additional, Crisp, Nigel, additional, Lamb, Norman, additional, Dixon, Michael, additional, Everington, Sam, additional, Hollins, Sheila, additional, Moncrieff, Joanna, additional, Giurca, Bogdan Chiva, additional, van Tulleken, Chris, additional, Chouinard, Guy, additional, Dooley, Michael, additional, Guy, Anne, additional, Horowitz, Mark, additional, Kinderman, Peter, additional, Johnstone, Lucy, additional, Montagu, Luke, additional, Nardi, Antonio E, additional, Stacey, Sarah, additional, Bell, Martin, additional, Tresidder, Andrew, additional, Watson, Jo, additional, Lewis, Stevie, additional, Spada, Marcantonio, additional, Payne, Rupert, additional, Akhtar, Naveed, additional, Buckland, Christian, additional, Levett, Jon, additional, Whitcombe, Sue, additional, and Marshall-Andrews, Laura, additional

Published
2023
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22. Development and validation of the Cambridge Multimorbidity Score

Author

Payne, Rupert A., Mendonca, Silvia C., Elliott, Marc N., Saunders, Catherine L., Edwards, Duncan A., Marshall, Martin, and Roland, Martin

Subjects
Mortality -- United Kingdom -- Comparative analysis, Comorbidity -- Research -- Comparative analysis, Health care reform -- Comparative analysis, Death, Hospital admission and discharge, Resource allocation, Health, General practitioners, Health
Abstract

BACKGROUND: Health services have failed to respond to the pressures of multimorbidity. Improved measures of multimorbidity are needed for conducting research, planning services and allocating resources. METHODS: We modelled the association between 37 morbidities and 3 key outcomes (primary care consultations, unplanned hospital admission, death) at 1 and 5 years. We extracted development (n = 300000) and validation (n = 150000) samples from the UK Clinical Practice Research Datalink. We constructed a general-outcome multimorbidity score by averaging the standardized weights of the separate outcome scores. We compared performance with the Charlson Comorbidity Index. RESULTS: Models that included all 37 conditions were acceptable predictors of general practitioner consultations (C-index 0.732, 95% confidence interval [CI] 0.731-0.734), unplanned hospital admission (C-index 0.742, 95% CI 0.7370.747) and death at 1 year (C-index 0.912, 95% CI 0.905-0.918). Models reduced to the 20 conditions with the greatest combined prevalence/weight showed similar predictive ability (C-indices 0.727, 95% CI 0.725-0.728; 0.738, 95% CI 0.732-0.743; and 0.910, 95% CI 0.904-0.917, respectively). They also predicted 5-year outcomes similarly for consultations and death (C-indices 0.735, 95% CI 0.7340.736, and 0.889, 95% CI 0.885-0.892, respectively) but performed less well for admissions (C-index 0.708, 95% CI 0.705- 0.712). The performance of the general-outcome score was similar to that of the outcome-specific models. These models performed significantly better than those based on the Charlson Comorbidity Index for consultations (C-index 0.691, 95% CI 0.690-0.693) and admissions (C-index 0.703, 95% CI 0.697-0.709) and similarly for mortality (C-index 0.907, 95% CI 0.900-0.914). INTERPRETATION: The Cambridge Multimorbidity Score is robust and can be either tailored or not tailored to specific health outcomes. It will be valuable to those planning clinical services, policymakers allocating resources and researchers seeking to account for the effect of multimorbidity., Patients with multiple long-term health conditions are commonly seen by clinicians in generalist and specialist settings. (1,2) Services and policies have failed to respond to the pressures that multimorbidity places [...]

Published
2020
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24. Pulse transit time and the pulse wave contour as measured by photoplethysmography : the effect of drugs and exercise

Author

Payne, Rupert Alistair, Maxwell, Simon., and Webb, David

Subjects
612.1, blood pressure, arterial stiffness, cardiovascular physiology
Abstract

Photoplethysmography (PPG) is a simple means of measuring the pulse wave in humans, exploitable for the purposes of timing the arrival of the pulse at a particular point in the arterial tree, and for pulse contour analysis. This thesis describes a methodology for measuring arterial pulse transit time (PTT) from cardiac ejection to pulse arrival at the finger. It describes the effect on PTT of drug and exercise induced changes in BP. The nature of the relationship between the PPG and arterial pressure is also examined, and the PTT technique extended to assessment of conduit vessel pulse wave velocity (PWV) during exercise. PTT measured from ECG R-wave to PPG finger wave (rPTT) had a negative correlation (R2=0.39) with systolic BP (SBP), unaffected by vasoactive drugs in some but not all persons. rPTT showed similar beat-to-beat variability to SBP, unaffected by drugs. rPTT correlated weakly with diastolic (DBP) and mean (MAP) pressure. Cardiac pre-ejection period (PEP) formed a substantial and variable part of rPTT (12% to 35%). Transit time adjusted for PEP (pPTT) correlated better with DBP (R2=0.41) and MAP (R2=0.45), than with SBP. The PPG wave tracked changes in the peripheral pressure wave. Drugs had little effect on the generalised transfer function (GTF) describing the association between arterial and PPG waves. Strenuous exercise induced a large decrease in rPTT, mainly accounted for by decreases in PEP (53% of the total change in rPTT) and in transit time from aorta to distal brachial artery (33%). In contrast, minimal change in transit time from wrist to finger tip occurred with exercise. Simultaneous ear-finger PPG signals were used to measure conduit artery PWV during exercise. Ear-finger PWV (PWVef) overestimated carotid-radial PWV throughout exertion (overall bias 0.81±1.05ms-1, p<0.001), but the degree of difference remained constant. The increase in PWVef with exercise, was greater (1.18±0.54ms-1, p=0.035) in healthy subjects with a positive cardiovascular family history compared to those without. PPG enables analysis of the pulse contour during exercise, but estimation of the radial pressure wave from finger PPG by use of a GTF derived at rest, resulted in inaccuracy following exertion. These effects were variable and relatively short-lived. Furthermore, a resting GTF used to determine central pressure from the peripheral wave, resulted in underestimation of SBP (-5.9±2.1mmHg) and central pressure augmentation index (-8.3±2.9%), which persisted for 10 minutes post-exercise. rPTT had a negative linear association with SBP (R2=0.94) during strenuous exercise, slightly stronger than during recovery (R2=0.85). Differences existed in area-undercurve of the rPTT/SBP relationship between exercise and recovery, due to discrepancies in rate and degree of recovery of SBP and PEP. The linear relationship between the rPTT/SBP during exercise was affected by aerobic capacity, and the regression slope was less in the anaerobic compared to aerobic phase of exercise due to minimal change in PEP during anaerobic exertion. The correlation between rPTT/SBP did not change with prolonged aerobic exercise. Finally, measures of baroreflex sensitivity during exercise, were not significantly different between actual beat-to-beat SBP and SBP estimated using rPTT. In conclusion, absolute BP cannot be reliably estimated by measurement of rPTT following administration of drugs and during exercise. However, rPTT may have a role in measuring BP variability and in the assessing exercise capacity. PPG may also be useful in determining the effects of exercise on arterial stiffness, and for estimating the pressure wave contour, although its use during exercise for the latter purpose must be treated with caution.

Published
2009

25. Using the Primary care Academic CollaboraTive to explore the characteristics and healthcare use of older housebound patients in England: protocol for a retrospective observational study and clinician survey (the CHiP study)

Author

Winn, Elizabeth, primary, Kissane, Madeleine, additional, Merriel, Samuel WD, additional, Brain, Thomas, additional, Silverwood, Victoria A, additional, Whitehead, Ishbel Orla, additional, Howe, Laura D, additional, Payne, Rupert A, additional, and Duncan, Polly, additional

Published
2023
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26. Understanding Measurement of postural hypotension: a nationwide survey of primary care practice in England

Author

Clark, Chris, primary, McDonagh, Sinéad, additional, Cross, Rosina, additional, Masoli, Jane, additional, Konya, Judit, additional, Abel, Gary, additional, Sheppard, James, additional, Jakubowski, Beth, additional, Bhanu, Cini, additional, Fordham, Jayne, additional, Turner, Katrina, additional, Lamb, Sallie, additional, Payne, Rupert, additional, McManus, Richard, additional, and Campbell, John, additional

Published
2023
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30. THE ASSOCIATION BETWEEN ANTIHYPERTENSIVE TREATMENT AND SERIOUS ADVERSE EVENTS BY PREVIOUS HISTORY OF ADVERSE EVENTS: AN OBSERVATIONAL COHORT STUDY

Author

Sheppard, James, primary, Koshiaris, Constantinos, additional, Stevens, Richard, additional, Lay-Flurrie, Sarah, additional, Banerjee, Amitava, additional, Bellows, Brandon, additional, Clegg, Andrew, additional, Hobbs, Richard, additional, Payne, Rupert, additional, Swain, Subhashsia, additional, Usher-Smith, Juliet, additional, and McManus, Richard, additional

Published
2023
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31. Development and external validation of a risk prediction model for falls in patients with an indication for antihypertensive treatment: retrospective cohort study

Author

Archer, Lucinda, Koshiaris, Constantinos, Lay-Flurrie, Sarah, Snell, Kym IE, Riley, Richard D, Stevens, Richard, Banerjee, Amitava, Usher-Smith, Juliet A, Clegg, Andrew, Payne, Rupert A, Hobbs, FD Richard, McManus, Richard J, Sheppard, James P, STRAtifying Treatments In The Multi-Morbid Frail ElderlY (STRATIFY) Investigators, Archer, Lucinda [0000-0003-2504-2613], Snell, Kym IE [0000-0001-9373-6591], Banerjee, Amitava [0000-0001-8741-3411], Usher-Smith, Juliet A [0000-0002-8501-2531], Payne, Rupert A [0000-0002-5842-4645], McManus, Richard J [0000-0003-3638-028X], Sheppard, James P [0000-0002-4461-8756], and Apollo - University of Cambridge Repository

Subjects
Cohort Studies, Models, Statistical, Humans, Prognosis, Antihypertensive Agents, Aged, Retrospective Studies
Abstract

OBJECTIVE: To develop and externally validate the STRAtifying Treatments In the multi-morbid Frail elderlY (STRATIFY)-Falls clinical prediction model to identify the risk of hospital admission or death from a fall in patients with an indication for antihypertensive treatment. DESIGN: Retrospective cohort study. SETTING: Primary care data from electronic health records contained within the UK Clinical Practice Research Datalink (CPRD). PARTICIPANTS: Patients aged 40 years or older with at least one blood pressure measurement between 130 mm Hg and 179 mm Hg. MAIN OUTCOME MEASURE: First serious fall, defined as hospital admission or death with a primary diagnosis of a fall within 10 years of the index date (12 months after cohort entry). Model development was conducted using a Fine-Gray approach in data from CPRD GOLD, accounting for the competing risk of death from other causes, with subsequent recalibration at one, five, and 10 years using pseudo values. External validation was conducted using data from CPRD Aurum, with performance assessed through calibration curves and the observed to expected ratio, C statistic, and D statistic, pooled across general practices, and clinical utility using decision curve analysis at thresholds around 10%. RESULTS: Analysis included 1 772 600 patients (experiencing 62 691 serious falls) from CPRD GOLD used in model development, and 3 805 366 (experiencing 206 956 serious falls) from CPRD Aurum in the external validation. The final model consisted of 24 predictors, including age, sex, ethnicity, alcohol consumption, living in an area of high social deprivation, a history of falls, multiple sclerosis, and prescriptions of antihypertensives, antidepressants, hypnotics, and anxiolytics. Upon external validation, the recalibrated model showed good discrimination, with pooled C statistics of 0.833 (95% confidence interval 0.831 to 0.835) and 0.843 (0.841 to 0.844) at five and 10 years, respectively. Original model calibration was poor on visual inspection and although this was improved with recalibration, under-prediction of risk remained (observed to expected ratio at 10 years 1.839, 95% confidence interval 1.811 to 1.865). Nevertheless, decision curve analysis suggests potential clinical utility, with net benefit larger than other strategies. CONCLUSIONS: This prediction model uses commonly recorded clinical characteristics and distinguishes well between patients at high and low risk of falls in the next 1-10 years. Although miscalibration was evident on external validation, the model still had potential clinical utility around risk thresholds of 10% and so could be useful in routine clinical practice to help identify those at high risk of falls who might benefit from closer monitoring or early intervention to prevent future falls. Further studies are needed to explore the appropriate thresholds that maximise the model's clinical utility and cost effectiveness.

Published
2022

32. Association of strong opioids and antibiotics prescribing with GP burnout: a retrospective cross-sectional study

Author

Hodkinson, Alexander, primary, Zghebi, Salwa S, additional, Kontopantelis, Evangelos, additional, Grigoroglou, Christos, additional, Ashcroft, Darren M, additional, Hann, Mark, additional, Chew-Graham, Carolyn A, additional, Payne, Rupert A, additional, Little, Paul, additional, de Lusignan, Simon, additional, Zhou, Anli, additional, Esmail, Aneez, additional, and Panagioti, Maria, additional

Published
2023
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34. Predicting the risk of acute kidney injury in primary care: derivation and validation of STRATIFY-AKI

Author

Koshiaris, Constantinos, primary, Archer, Lucinda, additional, Lay-Flurrie, Sarah, additional, Snell, Kym IE, additional, Riley, Richard D, additional, Stevens, Richard, additional, Banerjee, Amitava, additional, Usher-Smith, Juliet A, additional, Clegg, Andrew, additional, Payne, Rupert A, additional, Ogden, Margaret, additional, Hobbs, FD Richard, additional, McManus, Richard J, additional, and Sheppard, James P, additional

Published
2023
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37. Novel oral iron therapy for iron deficiency anaemia: How to value safety in a new drug?

Author

Culeddu, Giovanna, Su, Li, Cheng, Yafeng, Pereira, Dora IA, Payne, Rupert A, Powell, Jonathan J, Hughes, Dyfrig A, Culeddu, Giovanna [0000-0001-5032-4255], Su, Li [0000-0003-0919-3462], Pereira, Dora IA [0000-0001-5688-4448], Payne, Rupert A [0000-0002-5842-4645], Powell, Jonathan J [0000-0003-2738-1715], Hughes, Dyfrig A [0000-0001-8247-7459], Apollo - University of Cambridge Repository, Pereira, Dora I. A. [0000-0001-5688-4448], Payne, Rupert A. [0000-0002-5842-4645], Powell, Jonathan J. [0000-0003-2738-1715], and Hughes, Dyfrig A. [0000-0001-8247-7459]

Subjects
iron‐deficiency anaemia, Anemia, Iron-Deficiency, Drug-Related Side Effects and Adverse Reactions, Cost-Benefit Analysis, Iron Deficiencies, cost‐effectiveness, iron-deficiency anaemia, cost and cost analysis, iron, Humans, Female, Salts, ORIGINAL ARTICLES, cost-effectiveness, health care economics and organizations, ORIGINAL ARTICLE
Abstract

Aims: Novel oral iron supplements may be associated with a reduced incidence of adverse drug reactions compared to standard treatments of iron deficiency anaemia. The aim was to establish their value‐based price under conditions of uncertainty surrounding their tolerability. Methods: A discrete‐time Markov model was developed to assess the value‐based price of oral iron preparations based on their incremental cost per quality‐adjusted life year (QALY) gained from the perspective of the NHS in the UK. Primary and secondary care resource use and health state occupancy probabilities were estimated from routine electronic health records; and unit costs and health state utilities were derived from published sources. Patients were pre‐menopausal women with iron deficiency anaemia who were prescribed oral iron supplementation between 2000 and 2014. Results: The model reflecting current use of iron salts yielded a mean total cost to the NHS of £779, and 0.84 QALYs over 12 months. If a new iron preparation were to reduce the risk of adverse drug reactions by 30–40%, then its value‐based price, based on a threshold of £20 000 per QALY, would be in the region of £10–£13 per month, or about 7–9 times the average price of basic iron salts. Conclusions: There are no adequate, direct comparisons of new oral iron supplements to ferrous iron salts, and therefore other approaches are needed to assess their value. Our modelling shows that they are potentially cost‐effective at prices that are an order of magnitude higher than existing iron salts.

Published
2021
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38. Cost-Effectiveness of Antihypertensive Deprescribing in Primary Care: a Markov Modelling Study Using Data From the OPTiMISE Trial

Author

Jowett, Sue, Kodabuckus, Shahela, Ford, Gary A, Hobbs, FD Richard, Lown, Mark, Mant, Jonathan, Payne, Rupert, McManus, Richard J, Sheppard, James P, OPTiMISE Investigators, Jowett, Sue [0000-0001-8936-3745], Ford, Gary A [0000-0001-8719-4968], Hobbs, FD Richard [0000-0001-7976-7172], Payne, Rupert [0000-0002-5842-4645], McManus, Richard J [0000-0003-3638-028X], Sheppard, James P [0000-0002-4461-8756], and Apollo - University of Cambridge Repository

Subjects
aged, Deprescriptions, hypertension, quality of life, Primary Health Care, drug-related side effects and adverse reactions, Cost-Benefit Analysis, Humans, blood pressure, Quality-Adjusted Life Years, Antihypertensive Agents, cardiovascular diseases
Abstract

BACKGROUND: Deprescribing of antihypertensive medications for older patients with normal blood pressure is recommended by some clinical guidelines, where the potential harms of treatment may outweigh the benefits. This study aimed to assess the cost-effectiveness of this approach. METHODS: A Markov patient-level simulation was undertaken to model the effect of withdrawing one antihypertensive compared with usual care, over a life-time horizon. Model population characteristics were estimated using data from the OPTiMISE antihypertensive deprescribing trial, and the effects of blood pressure changes on outcomes were derived from the literature. Health-related quality of life was modeled in Quality-Adjusted Life Years (QALYs) and presented as costs per QALY gained. RESULTS: In the base-case analysis, medication reduction resulted in lower costs than usual care (mean difference £185), but also lower QALYs (mean difference 0.062) per patient over a life-time horizon. Usual care was cost-effective at £2975 per QALY gained (more costly, but more effective). Medication reduction resulted more heart failure and stroke/TIA events but fewer adverse events. Medication reduction may be the preferred strategy at a willingness-to-pay of £20 000/QALY, where the baseline absolute risk of serious drug-related adverse events was ≥7.7% a year (compared with 1.7% in the base-case). CONCLUSIONS: Although there was uncertainty around many of the assumptions underpinning this model, these findings suggest that antihypertensive medication reduction should not be attempted in many older patients with controlled systolic blood pressure. For populations at high risk of adverse effects, deprescribing may be beneficial, but a targeted approach would be required in routine practice.

Published
2022
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39. Can't prescribe, can't dispense: the challenge of medicine shortages.

Author

Kallis, Tomazo J and Payne, Rupert A

Subjects
HORMONE therapy, NON-medical prescribing, ATTENTION-deficit hyperactivity disorder, EUROPE-Great Britain relations, IMPORT quotas, CLINICAL governance, DRUG prices
Abstract

The article discusses the increasing problem of medicine shortages in the UK primary care system, with various factors contributing to the issue. Medicine shortages can be caused by demand surge, capacity reduction, and coordination failure within the complex medicine supply network. Current solutions include Serious Shortage Protocols and regulatory actions by the Medicines and Healthcare products Regulatory Agency, while future solutions may involve encouraging generic prescribing and empowering community pharmacists with limited prescribing rights. The article emphasizes the need for additional solutions and interprofessional collaboration to address the impact of medicine shortages on patients and healthcare professionals. [Extracted from the article]

Published
2024
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40. Improving Medicines use in People with Polypharmacy in Primary Care (IMPPP): Protocol for a multicentre cluster randomised trial comparing a complex intervention for medication optimization against usual care

Author

Payne, Rupert A., primary, Blair, Peter S., additional, Caddick, Barbara, additional, Chew-Graham, Carolyn A., additional, Dreischulte, Tobias, additional, Duncan, Lorna J., additional, Guthrie, Bruce, additional, Mann, Cindy, additional, Parslow, Roxanne M., additional, Round, Jeff, additional, Salisbury, Chris, additional, Turner, Katrina M., additional, Turner, Nicholas L., additional, and McCahon, Deborah, additional

Published
2022
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41. Development and external validation of a risk prediction model for falls in patients with an indication for antihypertensive treatment: retrospective cohort study

Author

Archer, Lucinda, primary, Koshiaris, Constantinos, additional, Lay-Flurrie, Sarah, additional, Snell, Kym I E, additional, Riley, Richard D, additional, Stevens, Richard, additional, Banerjee, Amitava, additional, Usher-Smith, Juliet A, additional, Clegg, Andrew, additional, Payne, Rupert A, additional, Hobbs, F D Richard, additional, McManus, Richard J, additional, and Sheppard, James P, additional

Published
2022
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45. Improving Medicines use in People with Polypharmacy in Primary Care (IMPPP)

Author

Payne, Rupert, Blair, Peter, Caddick, Barbara, Chew-Graham, Carolyn, Dreischulte, Tobias, Duncan, Lorna, Guthrie, Bruce, Mann, Cindy, Parslow, Roxanne, Round, Jeff, Salisbury, Chris, turner, katrina, Turner, Nicholas, and mccahon, deborah

Subjects
general practice, primary care, medicines optimisation, Medicine and Health Sciences, clinical trial, polypharmacy
Abstract

Polypharmacy is increasingly common, and is associated with undesirable consequences. Polypharmacy management necessitates balancing therapeutic benefits and risks, and varying clinical and patient priorities. Current guidance for managing polypharmacy is not supported by high quality evidence. The aim of the Improving Medicines use in People with Polypharmacy in Primary Care (IMPPP) trial is to evaluate the effectiveness of an intervention to optimise medication use for patients with polypharmacy in a general practice setting.

Published
2022
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48. Investigating the links between diagnostic uncertainty, emotional exhaustion, and turnover intention in General Practitioners working in the United Kingdom

Author

Zhou, Anli Yue, primary, Zghebi, Salwa S., additional, Hodkinson, Alexander, additional, Hann, Mark, additional, Grigoroglou, Christos, additional, Ashcroft, Darren M., additional, Esmail, Aneez, additional, Chew-Graham, Carolyn A., additional, Payne, Rupert, additional, Little, Paul, additional, Lusignan, Simon de, additional, Cherachi-Sohi, Sudeh, additional, Spooner, Sharon, additional, Zhou, Andrew K., additional, Kontopantelis, Evangelos, additional, and Panagioti, Maria, additional

Published
2022
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49. COVID-19 trajectories among 57 million adults in England: a cohort study using electronic health records

Author

Thygesen, Johan H, primary, Tomlinson, Christopher, additional, Hollings, Sam, additional, Mizani, Mehrdad A, additional, Handy, Alex, additional, Akbari, Ashley, additional, Banerjee, Amitava, additional, Cooper, Jennifer, additional, Lai, Alvina G, additional, Li, Kezhi, additional, Mateen, Bilal A, additional, Sattar, Naveed, additional, Sofat, Reecha, additional, Torralbo, Ana, additional, Wu, Honghan, additional, Wood, Angela, additional, Sterne, Jonathan A C, additional, Pagel, Christina, additional, Whiteley, William N, additional, Sudlow, Cathie, additional, Hemingway, Harry, additional, Denaxas, Spiros, additional, Abbasizanjani, Hoda, additional, Ahmed, Nida, additional, Ahmed, Badar, additional, Akinoso-Imran, Abdul Qadr, additional, Allara, Elias, additional, Allery, Freya, additional, Angelantonio, Emanuele Di, additional, Ashworth, Mark, additional, Ayyar-Gupta, Vandana, additional, Babu-Narayan, Sonya, additional, Bacon, Seb, additional, Ball, Steve, additional, Banerjee, Ami, additional, Barber, Mark, additional, Barrett, Jessica, additional, Bennie, Marion, additional, Berry, Colin, additional, Beveridge, Jennifer, additional, Birney, Ewan, additional, Bojanić, Lana, additional, Bolton, Thomas, additional, Bone, Anna, additional, Boyle, Jon, additional, Braithwaite, Tasanee, additional, Bray, Ben, additional, Briffa, Norman, additional, Brind, David, additional, Brown, Katherine, additional, Buch, Maya, additional, Canoy, Dexter, additional, Caputo, Massimo, additional, Carragher, Raymond, additional, Carson, Alan, additional, Cezard, Genevieve, additional, Chang, Jen-Yu Amy, additional, Cheema, Kate, additional, Chin, Richard, additional, Chudasama, Yogini, additional, Copland, Emma, additional, Crallan, Rebecca, additional, Cripps, Rachel, additional, Cromwell, David, additional, Curcin, Vasa, additional, Curry, Gwenetta, additional, Dale, Caroline, additional, Danesh, John, additional, Das-Munshi, Jayati, additional, Dashtban, Ashkan, additional, Davies, Alun, additional, Davies, Joanna, additional, Davies, Gareth, additional, Davies, Neil, additional, Day, Joshua, additional, Delmestri, Antonella, additional, Denholm, Rachel, additional, Dennis, John, additional, Denniston, Alastair, additional, Deo, Salil, additional, Dhillon, Baljean, additional, Docherty, Annemarie, additional, Dong, Tim, additional, Douiri, Abdel, additional, Downs, Johnny, additional, Dregan, Alexandru, additional, Ellins, Elizabeth A, additional, Elwenspoek, Martha, additional, Falck, Fabian, additional, Falter, Florian, additional, Fan, Yat Yi, additional, Firth, Joseph, additional, Fraser, Lorna, additional, Friebel, Rocco, additional, Gavrieli, Amir, additional, Gerstung, Moritz, additional, Gilbert, Ruth, additional, Gillies, Clare, additional, Glickman, Myer, additional, Goldacre, Ben, additional, Goldacre, Raph, additional, Greaves, Felix, additional, Green, Mark, additional, Grieco, Luca, additional, Griffiths, Rowena, additional, Gurdasani, Deepti, additional, Halcox, Julian, additional, Hall, Nick, additional, Hama, Tuankasfee, additional, Hansell, Anna, additional, Hardelid, Pia, additional, Hardy, Flavien, additional, Harris, Daniel, additional, Harrison, Camille, additional, Harron, Katie, additional, Hassaine, Abdelaali, additional, Hassan, Lamiece, additional, Healey, Russell, additional, Henderson, Angela, additional, Herz, Naomi, additional, Heyl, Johannes, additional, Hidajat, Mira, additional, Higginson, Irene, additional, Hinchliffe, Rosie, additional, Hippisley-Cox, Julia, additional, Ho, Frederick, additional, Hocaoglu, Mevhibe, additional, Horne, Elsie, additional, Hughes, David, additional, Humberstone, Ben, additional, Inouye, Mike, additional, Ip, Samantha, additional, Islam, Nazrul, additional, Jackson, Caroline, additional, Jenkins, David, additional, Jiang, Xiyun, additional, Johnson, Shane, additional, Kadam, Umesh, additional, Kallis, Costas, additional, Karim, Zainab, additional, Kasan, Jake, additional, Katsoulis, Michalis, additional, Kavanagh, Kim, additional, Kee, Frank, additional, Keene, Spencer, additional, Kent, Seamus, additional, Khalid, Sara, additional, Khawaja, Anthony, additional, Khunti, Kamlesh, additional, Killick, Richard, additional, Kinnear, Deborah, additional, Knight, Rochelle, additional, Kolamunnage-Dona, Ruwanthi, additional, Kontopantelis, Evan, additional, Kurdi, Amanj, additional, Lacey, Ben, additional, Lai, Alvina, additional, Lambarth, Andrew, additional, Larzjan, Milad Nazarzadeh, additional, Lawler, Deborah, additional, Lawrence, Thomas, additional, Lawson, Claire, additional, Li, Qiuju, additional, Li, Ken, additional, Llinares, Miguel Bernabeu, additional, Lorgelly, Paula, additional, Lowe, Deborah, additional, Lyons, Jane, additional, Lyons, Ronan, additional, Machado, Pedro, additional, Macleod, Mary Joan, additional, Macleod, John, additional, Malgapo, Evaleen, additional, Mamas, Mamas, additional, Mamouei, Mohammad, additional, Manohar, Sinduja, additional, Mapeta, Rutendo, additional, Martelli, Javiera Leniz, additional, Martos, David Moreno, additional, Mateen, Bilal, additional, McCarthy, Aoife, additional, Melville, Craig, additional, Milton, Rebecca, additional, Mizani, Mehrdad, additional, Moncusi, Marta Pineda, additional, Morales, Daniel, additional, Mordi, Ify, additional, Morrice, Lynn, additional, Morris, Carole, additional, Morris, Eva, additional, Mu, Yi, additional, Mueller, Tanja, additional, Murdock, Lars, additional, Nafilyan, Vahé, additional, Nicholson, George, additional, Nikiphorou, Elena, additional, Nolan, John, additional, Norris, Tom, additional, Norris, Ruth, additional, North, Laura, additional, North, Teri-Louise, additional, O'Connell, Dan, additional, Oliver, Dominic, additional, Oluyase, Adejoke, additional, Olvera-Barrios, Abraham, additional, Omigie, Efosa, additional, Onida, Sarah, additional, Padmanabhan, Sandosh, additional, Palmer, Tom, additional, Pasea, Laura, additional, Patel, Riyaz, additional, Payne, Rupert, additional, Pell, Jill, additional, Petitjean, Carmen, additional, Pherwani, Arun, additional, Pickrell, Owen, additional, Pierotti, Livia, additional, Pirmohamed, Munir, additional, Priedon, Rouven, additional, Prieto-Alhambra, Dani, additional, Proudfoot, Alastair, additional, Quinn, Terry, additional, Quint, Jennifer, additional, Raffetti, Elena, additional, Rahimi, Kazem, additional, Rao, Shishir, additional, Razieh, Cameron, additional, Roberts, Brian, additional, Rogers, Caroline, additional, Rossdale, Jennifer, additional, Salim, Safa, additional, Samani, Nilesh, additional, Schnier, Christian, additional, Schwartz, Roy, additional, Selby, David, additional, Seminog, Olena, additional, Shabnam, Sharmin, additional, Shah, Ajay, additional, Shelton, Jon, additional, Sheppard, James, additional, Sinha, Shubhra, additional, Skrypak, Mirek, additional, Slapkova, Martina, additional, Sleeman, Katherine, additional, Smith, Craig, additional, Sosenko, Filip, additional, Sperrin, Matthew, additional, Steeg, Sarah, additional, Sterne, Jonathan, additional, Stoica, Serban, additional, Sudell, Maria, additional, Sun, Luanluan, additional, Suseeladevi, Arun Karthikeyan, additional, Sweeting, Michael, additional, Sydes, Matt, additional, Takhar, Rohan, additional, Tang, Howard, additional, Thygesen, Johan, additional, Tilston, George, additional, Tochel, Claire, additional, Toit, Clea du, additional, Toms, Renin, additional, Torabi, Fatemeh, additional, Townson, Julia, additional, Tufail, Adnan, additional, Tungamirai, Tapiwa, additional, Varma, Susheel, additional, Vollmer, Sebastian, additional, Walker, Venexia, additional, Wang, Tianxiao, additional, Wang, Huan, additional, Warwick, Alasdair, additional, Watkinson, Ruth, additional, Watson, Harry, additional, Whiteley, William, additional, Whittaker, Hannah, additional, Wilde, Harry, additional, Wilkinson, Tim, additional, Williams, Gareth, additional, Williams, Michelle, additional, Williams, Richard, additional, Withnell, Eloise, additional, Wolfe, Charles, additional, Wright, Lucy, additional, Wu, Jinge, additional, Wu, Jianhua, additional, Yates, Tom, additional, Zaccardi, Francesco, additional, Zhang, Haoting, additional, Zhang, Huayu, additional, and Zuccolo, Luisa, additional

Published
2022
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