Ahilanandan Dushianthan1,2, Andrew F Cumpstey1,2, Matteo Ferrari1,2, William Thomas1,2, Ramani S Moonesinghe3,3, Charlotte Summers4, Hugh Montgomery5, Michael Pw Grocott1,2,6. 1. Critical Care Research Group, Southampton National Institute of Health Research Biomedical Research Centre, University Hospital Southampton/University of Southampton, Southampton, UK. 2. Integrative Physiology and Critical Illness Group, Clinical and Experimental Sciences, Faculty of Medicine, University of Southampton, Southampton, UK. 3. Department of Anaesthesia and Perioperative Medicine, University College Hospital, London, UK. 4. Department of Medicine, University of Cambridge School of Clinical Medicine, Cambridge, UK. 5. Centre for Human Health and Performance, Department of Medicine, University College London, London, UK. 6. Department of Anesthesiology, Duke University School of Medicine, Durham, NC, USA.
Coronavirus disease 2019 (COVID-19), a novel disease caused by infection with severe
acute respiratory syndrome coronavirus 2 (SARS-CoV2), has since caused an extreme
burden on critical care units worldwide.[1-3] As of December 2020, an
estimated 250,000 patients have been admitted to hospitals in the UK.[4] Data obtained
from hospitals in England, Wales and Northern Ireland between the period 01/03/2020
to 18/12/2020, suggests that there were 18,612 COVID-19 related ICU admissions with
a mortality of 36%, while 8% were still receiving critical care.[5] Guidelines for
ventilatory support and ICU Covid-19 management were rapidly generated, primarily
from expert opinion based on accepted care bundles used to manage Acute Respiratory
Distress Syndrome (ARDS).[6] However, clinicians soon realised that COVID-19 was a
distinct complex multi-system clinical entity that might not behave or respond to
treatment in the same way as ‘typical’ ARDS.[7],[8]Clinicians were forced to learn and adapt quickly to deal with this new disease
during the first wave of the pandemic. For example, there is evidence that the use
of invasive ventilation reduced over time.[9] We have previously reported a
survey on intensive care physicians’ perceptions of diagnosis and management of
patients with ARDS.[10] To explore how UK critical care physicians adapted their
usual management of acute hypoxic respiratory failure (AHRF) for COVID-19 and
compare with our previous results, we modified our survey to be specific to COVID-19
and address the following areas:Diagnostic definitions for acute respiratory failure associated with
COVID-19Relative frequency of different pharmacological and ventilatory
management strategies adopted to treat COVID-19Availability of post ICU discharge follow-up and rehabilitation measures
for COVID-19 patientsParticipation in clinical trials investigating novel COVID-19
treatments
Methods
We refined a previous survey of perceptions and management of ARDS practice to
address key questions related to the care of critically ill patients with COVID-19
and to compare our findings with previously published comparative data where
available.[10] The refined survey was specific to adult (>18 yrs.) ICU
patients with AHRF, presumed or confirmed to be secondary to COVID-19.We developed an electronic survey (Survey Monkey) accessible through a hyperlink or
QR code. The survey contained 27 questions (18 questions modified from the original
survey and 9 additional questions novel for this survey) and was piloted internally
by the investigator team and subsequently with independent critical care consultants
at University Hospital Southampton (online Appendix 1). We incorporated the
following sections: (i) contextual information describing the type, size and
location of the intensive care unit being surveyed; (ii) diagnostic and phenotypic
description of COVID-19; (iii) management approaches including ventilation, fluid
balance and pharmacological strategies; (iv) follow-up including post discharge
approaches and rehabilitation programmes offered; (v) involvement of patients in
clinical trials; and (vi) availability of health informatics to enable rapid
identification of patients.Intensive care physicians across the UK were encouraged to participate by
dissemination to local intensive care teams through Critical Care Regional Network
leaders and promotion in the Intensive Care Society (ICS) newsletter. Senior
(ideally consultant level) clinicians from every intensive care unit were approached
by the Critical Care Network leads and asked to complete the survey. Because of the
urgency of acquisition of this data to help steer ongoing guideline development, the
survey only remained open online for a one month period between 16 May 2020 and 17
June 2020.Results were analysed with the help of the SurveyMonkey system and GraphPad Prism
software version 8.0.0 La Jolla California, USA. Numerical data are presented as
percentages of the total respondents to each particular question. Survey data
relevant to COVID-19 were compared to previously collected data in relation to adult
ARDS.
Results
Characteristics of respondents
One hundred and thirty-seven responses were received from 89 UK centres between
16 May and 17 June 2020 (Figure 1). Of these centres, 74 (84.3%) from England and the rest
were from Wales (4.5%), Scotland (5.6%) and Northern Ireland (5.6%)
respectively. This represents approximately 27% of the hospitals participating
in the Intensive Care National Audit and Research Centre (ICNARC: Wales,
England, Ireland) and Scottish Intensive Care Society Audit Group (SICSAG)
Case-Mix programmes.[11],[12] The majority of
respondents were consultants (90%), with the remainder being SpR/StRs level
(6.6%) and clinical/research fellows (2.2%). Most units were described by the
respondents as general intensive care units (91.2%), followed by specialist
cardiac (2.9%) and others (5.8%) included specialist neurology and hepatology
units. The median number of ICU beds reported by respondents was 16 (range
4–100) with additional COVID-19 surge capacity to a median of further 21 ICU
beds (range 0–170). The median number of in-patient beds per hospital was 600
(range 11–1,500).
Figure 1.
A pictorial representation of the locations of hospitals from which the
responses obtained.
A pictorial representation of the locations of hospitals from which the
responses obtained.
Disease classification
When asked about the presence of the H and L clinical phenotypes which has been
suggested as distinct clinical entities in COVID-19 pneumonia,[7] almost all
(>99%) respondents answered these questions regarding the existence of such
phenotypes and whether recognising such phenotypes altered management
approaches. The majority of responders (40.4%) reported that it was neither easy
nor difficult to differentiate H and L sub-types, and 49.6% reported that they
did not change their ventilation strategy according to these conceptual
phenotypes. In COVID-19 AHRF, ARDS was mainly diagnosed using the Berlin
Definition (57.8%). Others used no diagnostic criteria (22.2%) or a combination
of American European Consensus Criteria (AECC), Lung Injury score and Berlin
Definition of ARDS (10.4%).
Specialist imaging for diagnosis and management
This question was based on the use of specialist imaging for the diagnosis and
management of patients with AHRF in COVID-19. Lung USS was performed primarily
during clinical deterioration (44.3%) and frequent use was rare (22.1%). Similar
to the USS, a thoracic CT scan was reportedly undertaken mainly during clinical
deterioration by 70.8%. Transthoracic echocardiogram was performed on admission
and frequently by 34.8%, and during clinical deterioration in 32.6% and
admission and infrequently by 29.6%.
Pharmacological agents
The responses to these questions were categorised as “routinely”, “occasionally”,
“individualised”, “part of clinical trial” and “never”. Similar to our previous
survey, for the purpose of this report, we pooled the “occasional” and
“individualised according to patient” categories together (Figure 2).
Figure 2.
The pharmacological therapies used to treat COVID-19 patients with acute
hypoxic respiratory failure.
The pharmacological therapies used to treat COVID-19 patients with acute
hypoxic respiratory failure.
Antibiotics and antivirals
Antibiotics were given on admission routinely by 51.8% with a COVID-19 specific
protocol (29.3%) or as for standard use in community-acquired pneumonia (48.1%).
The antibiotic guidance was based on microbiology (51.9%), blood C-reactive
protein (CRP) (29.3%) or serum procalcitonin (PCT) (59.4%) concentrations.
Antivirals were mainly given in the context of a clinical trial.
Corticosteroids
Corticosteroids were used in some form by 93.4% and of which 44.5% were reported
to be part of a clinical trial. While some used corticosteroids occasionally or
in an individualised patient fashion (45.3%), routine use was rare (3.7%).
Methylprednisolone was the most commonly used steroid outside the context of a
clinical trial, and the most typical dose was 1 mg/kg/day (57.1%) with a
duration of <7 days (46.8%). The timing of the initiation of steroids outside
a clinical trial was variable: with 39.3% starting within 7–14 days of ICU
admission, and 2.3%, 6.7%, 15.7% and 19.1% at <72 hours, <7 days >14
days or ‘anytime’ respectively. The reasons for the initiation of
corticosteroids outside a clinical trial were as an anti-inflammatory (21.3%),
anti-fibrotic (26.2%) or to treat bronchiolitis obliterans organising pneumonia
(14.8%) or a combination of all of these (21.3%).
Anticoagulation
When asked regarding the use of therapeutic anticoagulation or augmented
anticoagulation in the absence of clinical thromboembolism, all respondents
(100%) answered this question. Therapeutic (rather than prophylactic)
anticoagulation in the absence of a clinical thromboembolism was used
‘routinely’, ‘individualised or occasionally’, and ‘never’ by 7.3%, 54.0% and
24.1% respectively. 14.6% used therapeutic anticoagulation in the context of a
clinical trial. Augmented anticoagulation was used routinely more often (58.8%),
and on an individualised/occasional basis by 28.7%. We did not explore the
rationale for both full/therapeutic and augmented anticoagulation.
Other pharmacotherapies
The use of other pharmacotherapies, including any other immune-modulating agents,
neuromuscular agents, pulmonary vasodilators and convalescent plasma, are
detailed in Figure
2.
Use of high flow nasal oxygen and non-invasive ventilation
The use of HFNO, continuous positive airway pressure (CPAP) and bilevel positive
airway pressure ventilation (BiPAP) was assessed, including in the context of
prone positioning, and nearly all respondents answered (99.2%). The use of CPAP
with or without proning was the commonest method of oxygenation beyond face mask
oxygen (Figure 3). We
did not perform analysis of individual responses and as a result, not able to
report on the use of combined interventions.
Figure 3.
The use of non-invasive ventilation, CPAP and high flow nasal oxygen.
CPAP: continuous positive airway pressure; HFNO: high flow nasal
oxygen.
The use of non-invasive ventilation, CPAP and high flow nasal oxygen.CPAP: continuous positive airway pressure; HFNO: high flow nasal
oxygen.
Invasive ventilation strategies, targets and rescue therapies
The commonest indication for intubation was a combination of both work of
breathing and oxygenation indices (81.0%). The primary ventilation strategy was
partial compliance with the ARDSNet protocol with deviation from PEEP
recommendations (63.7%) with a tidal volume target of 6.1–8.0 mL/kg predicted
body weight (PBW) (60.3%) followed by 4.0-6.0 mL/kg/PBW (38.2%). The PEEP
titration was commonly guided by the degree of hypoxia (60.8%). The majority
adopted permissive targets with a hypoxic range of 7.1-9.0 kPa (87.5%). Details
of the primary ventilation strategy, variables used to guide titration of PEEP,
the permissive targets for hypercapnia, pH and hypoxia in comparison to the
previous survey are presented in Figure 4. Rescue therapies included
prone positioning (99.3%), recruitment manoeuvres (51.5%), ECMO (46.3%), and
pulmonary vasodilators (35.3%).
Figure 4.
Comparison of ARDS (2013) and COVID-19 surveys conducted for to assess
the primary ventilation strategy (a), variables used for the guidance
for positive end expiratory pressure (PEEP) titration (b), and
permissive targets for PaCO2 (c), pH (d) and PaO2
(e).
Comparison of ARDS (2013) and COVID-19 surveys conducted for to assess
the primary ventilation strategy (a), variables used for the guidance
for positive end expiratory pressure (PEEP) titration (b), and
permissive targets for PaCO2 (c), pH (d) and PaO2
(e).
Prone positioning
Prone positioning was used based on PaO2/FiO2 by 69.3%,
routinely (17.5%), and as a rescue measure (13.1%). The most frequent prone
durations were 16–18 hours (65.9%) and 12–16 hours (27.9%). An unlimited number
of prone cycles were performed by 47.4%, and 43.9% continued proning until
improvements in PaO2/FiO2 were seen. Sixty percent of
respondents reported the presence of a dedicated prone team.
Fluid balance
Most responders (86.7%) would target a euvolaemic fluid balance, and 8.9%
targeted a “dry” state. The preferred resuscitation fluids were crystalloids
(89.8%). Most (53.5%) would use a combination of diuretics, fluid restriction
and haemofiltration to achieve their fluid balance targets.
Tracheostomy
A routine tracheotomy was considered by 47.5% and occasionally by 44.5%. However,
on both occasions, the preferred timing was after 7 days (late). Tracheostomy
was performed rarely by just 7.3%.
Participation in clinical research and data collection
There was excellent participation in clinical research; the studies were
REMAP-CAP (84.6%), ISARIC (41.0%), GenOMICC (71.2%), Recovery Respiratory
Support (68.2%) and REALIST (15.5%) (Figure 5). Pre-existing COVID-19
specific data collection was available in 93.8% centres. This was research
specific in 32.6% of centres.
Figure 5.
Clinical research participation (a) and availability of rehabilitation
facilities (b) post-ICU discharge.
Clinical research participation (a) and availability of rehabilitation
facilities (b) post-ICU discharge.
Follow-up and the availability of rehabilitation programmes
COVID-19 routine follow-up was available for this cohort of patients following
hospital discharge in 66.2%. Physical, pulmonary, nutritional, psychological and
neurocognitive rehabilitation was available at 29.6%, 14.1%, 14.8%, 19.1% and
6.7% of the respondent’s units, respectively (Figure 5). We did not differentiate if
these rehabilitation measures are specific to COVID-19 or common for all ICU
patients.
Discussion
This was a cross-sectional survey conducted among the UK intensive care physicians
describing the management of patients admitted with COVID-19 related acute hypoxemic
respiratory failure. The response rate lower than would normally be anticipated, but
in the context of the initial surge of the pandemic with demanding clinical duties,
this level of response may be understandable, and we believe still contributes
meaningful and useful results. Most of the respondents were consultants from general
ICUs across the UK. This survey demonstrates significant variations in the
management of patients with COVID-19 related AHRF across the UK. This is the first
survey of this nature to be conducted in the UK and may provide helpful insights for
clinicians and guidelines writers as the pandemic evolves.The key findings concerning clinical phenotypes and respiratory support were: (i)
most clinicians were not able to differentiate the claimed sub-types of COVID-19
pneumonia,[7] in general described a spectrum of phenotypes over the course of
the illness, and most did not base their clinical management on a distinction
between such phenotypes; (ii) Most clinicians reported using non-invasive
ventilation with the preferred choice being CPAP with self-proning; (iii) Bilevel
NIV and HFNO were used by 50 and 40–45% of respondents respectively, reflecting a
highly polarised response for the use of bilevel NIV and HFNO with a roughly 50:50
divide. (iv) a majority of respondents reported that their ventilation approach was
based on the ARDSnet protocol for tidal volumes but with deviations from the
recommended PEEP settings; (v); permissive targets were allowed for pH,
PaCO2 and PaO2 and were similar to the previous ARDS
survey responses. Overall, compared with the previous ARDS survey, full compliance
of ARDSnet ventilation protocol was less (19.3% vs 34%) with increased use of APRV
(24.4% vs 3.7%) in COVID-19 patients. Routine and late (>7 days) tracheostomy was
the preferred options in both surveys.[10]There key findings in relation to pharmacotherapy were: (i) Antibiotic use was almost
universal whereas antivirals were only prescribed in the context of clinical trials;
(ii) PCT was commonly used in preference to CRP to guide antibiotic prescription in
COVID-19 patients (iii) Rapid diagnostic PCR platforms to assess bacterial, and
other viral co-infections were available in some centres (iii) Corticosteroids were
commonly prescribed outside clinical trials, particularly methylprednisolone (23% of
respondents). Among those who gave methylprednisolone, it was given at various time
points of the disease process, early within 7 days (47%), between 7–14 days (38%),
and >14 days by the rest at a dose of 1–2 mg/kg/day; (iv) Corticosteroids were
given for mitigating inflammation, as an anti-fibrotic, and to treat bronchiolitis
obliterans organising pneumonia; (v) Augmented prophylactic anticoagulation was used
routinely by 59% of respondents with 94% adopting this approach for some patients.
Most survey responses (135 out of 137) were provided before the publication of the
Randomised Evaluation of COVID-19 Therapy (RECOVERY) study results, which
demonstrated benefit from the use of dexamethasone and all responses predated the
subsequent publication of the Randomised Embedded Multi-factorial, Adaptive platform
trial for Community-Acquired pneumonia (REMAP-CAP) results in relation to
Hydrocortisone use.[13],[14] In comparison with the previous ARDS survey, there was
increased use of corticosteroids for any reason including as part of a clinical
trial (93% vs 70%) and routine use of neuromuscular agents (44.5% vs 15%).[10]Participation in clinical trials was extraordinary, with a substantial majority
reporting enrolment into REMAP-CAP (82%).[14] This was much higher than our
previous ARDS survey. Although routine follow-up after discharge took place in
nearly two-thirds of units, less than one third offered any form of routine
rehabilitation.The limitations of the study include a low response rate which may in part be a
consequence of the high clinical workload pertaining to the COVID-19 burden at the
time that the study was conducted. Although responses were obtained from most of the
Critical Care Networks across the UK, it was not inclusive of all hospitals within
that Network. Moreover, there were multiple responses from individual hospitals.
Consequently, we may have introduced non-responder and multiple responder bias
affecting the integrity of the results and the generalisability and validity.
Additional selection bias may have been introduced due to the electronic design of
the survey. The questions regarding pharmacotherapies and the non-invasive
ventilation, the answer domains were classified as “routinely”, “occasionally”,
“individualised according to patient”, part of a clinical trial or “never”. To
mitigate any confusions between the terms “occasionally” and “individualised
according to patient”, we presented the data combining these two domains.This manuscript summarises the experience of UK intensive care physician’s clinical
management during the first wave of the COVID-19 pandemic based on the responses to
a structured survey. Despite the rapid and substantial accumulation of knowledge
from randomised controlled trials and large observational cohort studies around the
world, unanswered research questions remain regarding many aspects of COVID-19
management in intensive care setting including: effectiveness of early use of
CPAP/NIV in hypoxic patients, the timing of the transition from CPAP/NIV to invasive
mechanical ventilation, the use of pharmacotherapies such as routine admission
antibiotics, high dose corticosteroids, pulmonary vasodilators, augmented or
therapeutic anticoagulation, antiplatelets, the utility of PCT to guide antibiotic
prescription, as well as the most beneficial oxygen and fluid balance targets.
Although it may not be feasible to answer all of these questions through clinical
trials, this list emphasises the importance of recruiting patients into the
established platform trials as well as the value of clear guidelines synthesising
clinical experience and existing evidence to improve outcomes during this
challenging and uncertain time.Click here for additional data file.Supplemental material, sj-pdf-1-inc-10.1177_17511437211002352 for Intensive care
physicians’ perceptions of the diagnosis & management of patients with acute
hypoxic respiratory failure associated with COVID-19: A UK based survey by A
Dushianthan, AF Cumpstey, M Ferrari, W Thomas, SR Moonesinghe, C Summers, H
Montgomery and MPW Grocott in Journal of the Intensive Care Society
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Franck Pourcine; Mehran Monchi; David Luis; Romain Mercier; Anne Sagnier; Nathalie Verrier; Cecile Caplin; Shidasp Siami; Christelle Aparicio; Sarah Vautier; Asma Jeblaoui; Muriel Fartoukh; Laura Courtin; Vincent Labbe; Cécile Leparco; Grégoire Muller; Mai-Anh Nay; Toufik Kamel; Dalila Benzekri; Sophie Jacquier; Emmanuelle Mercier; Delphine Chartier; Charlotte Salmon; PierreFrançois Dequin; Francis Schneider; Guillaume Morel; Sylvie L’Hotellier; Julio Badie; Fernando Daniel Berdaguer; Sylvain Malfroy; Chaouki Mezher; Charlotte Bourgoin; Bruno Megarbane; Nicolas Deye; Isabelle Malissin; Laetitia Sutterlin; Christophe Guitton; Cédric Darreau; Mickaël Landais; Nicolas Chudeau; Alain Robert; Pierre Moine; Nicholas Heming; Virginie Maxime; Isabelle Bossard; Tiphaine Barbarin Nicholier; Gwenhael Colin; Vanessa Zinzoni; Natacham Maquigneau; André Finn; Gabriele Kreß; Uwe Hoff; Carl Friedrich Hinrichs; Jens Nee; Mathias Pletz; Stefan Hagel; Juliane Ankert; Steffi Kolanos; Frank Bloos; Sirak Petros; Bastian Pasieka; Kevin Kunz; Peter Appelt; Bianka Schütze; Stefan Kluge; Axel Nierhaus; Dominik Jarczak; Kevin Roedl; Dirk Weismann; Anna Frey; Vivantes Klinikum Neukölln; Lorenz Reill; Michael Distler; Astrid Maselli; János Bélteczki; István Magyar; Ágnes Fazekas; Sándor Kovács; Viktória Szőke; Gábor Szigligeti; János Leszkoven; Daniel Collins; Patrick Breen; Stephen Frohlich; Ruth Whelan; Bairbre McNicholas; Michael Scully; Siobhan Casey; Maeve Kernan; Peter Doran; Michael O’Dywer; Michelle Smyth; Leanne Hayes; Oscar Hoiting; Marco Peters; Els Rengers; Mirjam Evers; Anton Prinssen; Jeroen Bosch Ziekenhuis; Koen Simons; Wim Rozendaal; F Polderman; P de Jager; M Moviat; A Paling; A Salet; Emma Rademaker; Anna Linda Peters; E de Jonge; J Wigbers; E Guilder; M Butler; Keri-Anne Cowdrey; Lynette Newby; Yan Chen; Catherine Simmonds; Rachael McConnochie; Jay Ritzema Carter; Seton Henderson; Kym Van Der Heyden; Jan Mehrtens; Tony Williams; Alex Kazemi; Rima Song; Vivian Lai; Dinu Girijadevi; Robert Everitt; Robert Russell; Danielle Hacking; Ulrike Buehner; Erin Williams; Troy Browne; Kate Grimwade; Jennifer Goodson; Owen Keet; Owen Callender; Robert Martynoga; Kara Trask; Amelia Butler; Livia Schischka; Chelsea Young; Eden Lesona; Shaanti Olatunji; Yvonne Robertson; Nuno José; Teodoro Amaro dos Santos Catorze; Tiago Nuno Alfaro de Lima Pereira; Lucilia Maria Neves Pessoa; Ricardo Manuel Castro Ferreira; Joana Margarida Pereira Sousa Bastos; Simin Aysel Florescu; Delia Stanciu; Miahela Florentina Zaharia; Alma Gabriela Kosa; Daniel Codreanu; Yaseen Marabi; Eman Al Qasim; Mohamned Moneer Hagazy; Lolowa Al Swaidan; Hatim Arishi; Rosana Muñoz-Bermúdez; Judith Marin-Corral; Anna Salazar Degracia; Francisco Parrilla Gómez; Maria Isabel Mateo López; Jorge Rodriguez Fernandez; Sheila Cárcel Fernández; Rosario Carmona Flores; Rafael León López; Carmen de la Fuente Martos; Angela Allan; Petra Polgarova; Neda Farahi; Stephen McWilliam; Daniel Hawcutt; Laura Rad; Laura O’Malley; Jennifer Whitbread; Olivia Kelsall; Laura Wild; Jessica Thrush; Hannah Wood; Karen Austin; Adrian Donnelly; Martin Kelly; Sinéad O’Kane; Declan McClintock; Majella Warnock; Paul Johnston; Linda Jude Gallagher; Clare Mc Goldrick; Moyra Mc Master; Anna Strzelecka; Rajeev Jha; Michael Kalogirou; Christine Ellis; Vinodh Krishnamurthy; Vashish Deelchand; Jon Silversides; Peter McGuigan; Kathryn Ward; Aisling O’Neill; Stephanie Finn; Barbara Phillips; Dee Mullan; Laura Oritz-Ruiz de Gordoa; Matthew Thomas; Katie Sweet; Lisa Grimmer; Rebekah Johnson; Jez Pinnell; Matt Robinson; Lisa Gledhill; Tracy Wood; Matt Morgan; Jade Cole; Helen Hill; Michelle Davies; David Antcliffe; Maie Templeton; Roceld Rojo; Phoebe Coghlan; Joanna Smee; Euan Mackay; Jon Cort; Amanda Whileman; Thomas Spencer; Nick Spittle; Vidya Kasipandian; Amit Patel; Suzanne Allibone; Roman Mary Genetu; Mohamed Ramali; Alison Ghosh; Peter Bamford; Emily London; Kathryn Cawley; Maria Faulkner; Helen Jeffrey; Tim Smith; Chris Brewer; Jane Gregory; James Limb; Amanda Cowton; Julie O’Brien; Nikitas Nikitas; Colin Wells; Liana Lankester; Mark Pulletz; Patricia Williams; Jenny Birch; Sophie Wiseman; Sarah Horton; Ana Alegria; Salah Turki; Tarek Elsefi; Nikki Crisp; Louise Allen; Iain McCullagh; Philip Robinson; Carole Hays; Maite Babio-Galan; Hannah Stevenson; Divya Khare; Meredith Pinder; Selvin Selvamoni; Amitha Gopinath; Richard Pugh; Daniel Menzies; Callum Mackay; Elizabeth Allan; Gwyneth Davies; Kathryn Puxty; Claire McCue; Susanne Cathcart; Naomi Hickey; Jane Ireland; Hakeem Yusuff; Graziella Isgro; Chris Brightling; Michelle Bourne; Michelle Craner; Malcolm Watters; Rachel Prout; Louisa Davies; Suzannah Pegler; Lynsey Kyeremeh; Gill Arbane; Karen Wilson; Linda Gomm; Federica Francia; Stephen Brett; Sonia Sousa Arias; Rebecca Elin Hall; Joanna Budd; Charlotte Small; Janine Birch; Emma Collins; Jeremy Henning; Stephen Bonner; Keith Hugill; Emanuel Cirstea; Dean Wilkinson; Michal Karlikowski; Helen Sutherland; Elva Wilhelmsen; Jane Woods; Julie North; Dhinesh Sundaran; Laszlo Hollos; Susan Coburn; Joanne Walsh; Margaret Turns; Phil Hopkins; John Smith; Harriet Noble; Maria Theresa Depante; Emma Clarey; Shondipon Laha; Mark Verlander; Alexandra Williams; Abby Huckle; Andrew Hall; Jill Cooke; Caroline Gardiner-Hill; Carolyn Maloney; Hafiz Qureshi; Neil Flint; Sarah Nicholson; Sara Southin; Andrew Nicholson; Barbara Borgatta; Ian Turner-Bone; Amie Reddy; Laura Wilding; Loku Chamara Warnapura; Ronan Agno Sathianathan; David Golden; Ciaran Hart; Jo Jones; Jonathan Bannard-Smith; Joanne Henry; Katie Birchall; Fiona Pomeroy; Rachael Quayle; Arystarch Makowski; Beata Misztal; Iram Ahmed; Thyra KyereDiabour; Kevin Naiker; Richard Stewart; Esther Mwaura; Louise Mew; Lynn Wren; Felicity Willams; Richard Innes; Patricia Doble; Joanne Hutter; Charmaine Shovelton; Benjamin Plumb; Tamas Szakmany; Vincent Hamlyn; Nancy Hawkins; Sarah Lewis; Amanda Dell; Shameer Gopal; Saibal Ganguly; Andrew Smallwood; Nichola Harris; Stella Metherell; Juan Martin Lazaro; Tabitha Newman; Simon Fletcher; Jurgens Nortje; Deirdre Fottrell-Gould; Georgina Randell; Mohsin Zaman; Einas Elmahi; Andrea Jones; Kathryn Hall; Gary Mills; Kim Ryalls; Helen Bowler; Jas Sall; Richard Bourne; Zoe Borrill; Tracey Duncan; Thomas Lamb; Joanne Shaw; Claire Fox; Jeronimo Moreno Cuesta; Kugan Xavier; Dharam Purohit; Munzir Elhassan; Dhanalakshmi Bakthavatsalam; Matthew Rowland; Paula Hutton; Archana Bashyal; Neil Davidson; Clare Hird; Manish Chhablani; Gunjan Phalod; Amy Kirkby; Simon Archer; Kimberley Netherton; Henrik Reschreiter; Julie Camsooksai; Sarah Patch; Sarah Jenkins; David Pogson; Steve Rose; Zoe Daly; Lutece Brimfield; Helen Claridge; Dhruv Parekh; Colin Bergin; Michelle Bates; Joanne Dasgin; Christopher McGhee; Malcolm Sim; Sophie Kennedy Hay; Steven Henderson; Mandeep-Kaur Phull; Abbas Zaidi; Tatiana Pogreban; Lace Paulyn Rosaroso; Daniel Harvey; Benjamin Lowe; Megan Meredith; Lucy Ryan; Anil Hormis; Rachel Walker; Dawn Collier; Sarah Kimpton; Susan Oakley; Kevin Rooney; Natalie Rodden; Emma Hughes; Nicola Thomson; Deborah McGlynn; Andrew Walden; Nicola Jacques; Holly Coles; Emma Tilney; Emma Vowell; Martin Schuster-Bruce; Sally Pitts; Rebecca Miln; Laura Purandare; Luke Vamplew; Michael Spivey; Sarah Bean; Karen Burt; Lorraine Moore; Christopher Day; Charly Gibson; Elizabeth Gordon; Letizia Zitter; Samantha Keenan; Evelyn Baker; Shiney Cherian; Sean Cutler; Anna Roynon-Reed; Kate Harrington; Ajay Raithatha; Kris Bauchmuller; Norfaizan Ahmad; Irina Grecu; Dawn Trodd; Jane Martin; Caroline Wrey Brown; Ana-Marie Arias; Thomas Craven; David Hope; Jo Singleton; Sarah Clark; Nicola Rae; Ingeborg Welters; David Oliver Hamilton; Karen Williams; Victoria Waugh; David Shaw; Zudin Puthucheary; Timothy Martin; Filipa Santos; Ruzena Uddin; Alastair Somerville; Kate Colette Tatham; Shaman Jhanji; Ethel Black; Arnold Dela Rosa; Ryan Howle; Redmond Tully; Andrew Drummond; Joy Dearden; Jennifer Philbin; Sheila Munt; Alain Vuylsteke; Charles Chan; Saji Victor; Ramprasad Matsa; Minerva Gellamucho; Ben Creagh-Brown; Joe Tooley; Laura Montague; Fiona De Beaux; Laetitia Bullman; Ian Kersiake; Carrie Demetriou; Sarah Mitchard; Lidia Ramos; Katie White; Phil Donnison; Maggie Johns; Ruth Casey; Lehentha Mattocks; Sarah Salisbury; Paul Dark; Andrew Claxton; Danielle McLachlan; Kathryn Slevin; Stephanie Lee; Jonathan Hulme; Sibet Joseph; Fiona Kinney; Ho Jan Senya; Aneta Oborska; Abdul Kayani; Bernard Hadebe; Rajalakshmi Orath Prabakaran; Lesley Nichols; Matt Thomas; Ruth Worner; Beverley Faulkner; Emma Gendall; Kati Hayes; Colin Hamilton-Davies; Carmen Chan; Celina Mfuko; Hakam Abbass; Vineela Mandadapu; Susannah Leaver; Daniel Forton; Kamal Patel; Elankumaran Paramasivam; Matthew Powell; Richard Gould; Elizabeth Wilby; Clare Howcroft; Dorota Banach; Ziortza Fernández de Pinedo Artaraz; Leilani Cabreros; Ian White; Maria Croft; Nicky Holland; Rita Pereira; Ahmed Zaki; David Johnson; Matthew Jackson; Hywel Garrard; Vera Juhaz; Alistair Roy; Anthony Rostron; Lindsey Woods; Sarah Cornell; Suresh Pillai; Rachel Harford; Tabitha Rees; Helen Ivatt; Ajay Sundara Raman; Miriam Davey; Kelvin Lee; Russell Barber; Manish Chablani; Farooq Brohi; Vijay Jagannathan; Michele Clark; Sarah Purvis; Bill Wetherill; Ahilanandan Dushianthan; Rebecca Cusack; Kim de Courcy-Golder; Simon Smith; Susan Jackson; Ben Attwood; Penny Parsons; Valerie Page; Xiao Bei Zhao; Deepali Oza; Jonathan Rhodes; Tom Anderson; Sheila Morris; Charlotte Xia Le Tai; Amy Thomas; Alexandra Keen; Stephen Digby; Nicholas Cowley; Laura Wild; David Southern; Harsha Reddy; Andy Campbell; Claire Watkins; Sara Smuts; Omar Touma; Nicky Barnes; Peter Alexander; Tim Felton; Susan Ferguson; Katharine Sellers; Joanne Bradley-Potts; David Yates; Isobel Birkinshaw; Kay Kell; Nicola Marshall; Lisa Carr-Knott; Charlotte Summers Journal: JAMA Date: 2020-10-06 Impact factor: 56.272
Authors: James C Doidge; Doug W Gould; Paloma Ferrando-Vivas; Paul R Mouncey; Karen Thomas; Manu Shankar-Hari; David A Harrison; Kathryn M Rowan Journal: Am J Respir Crit Care Med Date: 2021-03-01 Impact factor: 21.405
Authors: C Michael Roberts; Marcel Levi; Martin McKee; Richard Schilling; Wei Shen Lim; Michael P W Grocott Journal: Br J Anaesth Date: 2020-06-20 Impact factor: 9.166
Authors: Peter Horby; Wei Shen Lim; Jonathan R Emberson; Marion Mafham; Jennifer L Bell; Louise Linsell; Natalie Staplin; Christopher Brightling; Andrew Ustianowski; Einas Elmahi; Benjamin Prudon; Christopher Green; Timothy Felton; David Chadwick; Kanchan Rege; Christopher Fegan; Lucy C Chappell; Saul N Faust; Thomas Jaki; Katie Jeffery; Alan Montgomery; Kathryn Rowan; Edmund Juszczak; J Kenneth Baillie; Richard Haynes; Martin J Landray Journal: N Engl J Med Date: 2020-07-17 Impact factor: 91.245