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41 research outputs found

Kinematics and Ground Reaction Force Determination: A Demonstration Quantifying Locomotor Abilities of Young Adult, Middle-aged, and Geriatric Rats

Author: Assem Hisham
Kerr Brendan
Neville Tanya
Ngan Sybil
Webb Aubrey A.
Publication venue: MyJove Corporation
Publication date
Field of study

Behavior, in its broadest definition, can be defined as the motor manifestation of physiologic processes. As such, all behaviors manifest through the motor system. In the fields of neuroscience and orthopedics, locomotion is a commonly evaluated behavior for a variety of disease models. For example, locomotor recovery after traumatic injury to the nervous system is one of the most commonly evaluated behaviors 1-3. Though locomotion can be evaluated using a variety of endpoint measurements (e.g. time taken to complete a locomotor task, etc), semiquantitative kinematic measures (e.g. ordinal rating scales (e.g. Basso Beattie and Bresnahan locomotor (BBB) rating scale, etc)) and surrogate measures of behaviour (e.g. muscle force, nerve conduction velocity, etc), only kinetics (force measurements) and kinematics (measurements of body segments in space) provide a detailed description of the strategy by which an animal is able to locomote 1. Though not new, kinematic and kinetic measurements of locomoting rodents is now more readily accessible due to the availability of commercially available equipment designed for this purpose. Importantly, however, experimenters need to be very familiar with theory of biomechanical analyses and understand the benefits and limitations of these forms of analyses prior to embarking on what will become a relatively labor-intensive study. The present paper aims to describe a method for collecting kinematic and ground reaction force data using commercially available equipment. Details of equipment and apparatus set-up, pre-training of animals, inclusion and exclusion criteria of acceptable runs, and methods for collecting the data are described. We illustrate the utility of this behavioral analysis technique by describing the kinematics and kinetics of strain-matched young adult, middle-aged, and geriatric rats

Crossref

PubMed Central

Variation in Genes Related to Cochlear Biology Is Strongly Associated with Adult-Onset Deafness in Border Collies

Author: Chang Melanie L.
Erdman Carolyn A.
Hamilton Steven P.
Hytönen Marjo Kristiina
Lam Ernest T.
Lohi Hannes
Neff Mark W.
Robertson Kathryn R.
Ruhe Alison L.
Webb Aubrey A.
Williams D. Colette
Yokoyama Jennifer S.
Publication venue
Publication date: 01/09/2012
Field of study

WOS:000309817900003Peer reviewe

Crossref

Directory of Open Access Journals

PubMed Central

PDXScholar (Portland State University)

eScholarship - University of California

Helsingin yliopiston digitaalinen arkisto

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Prognostic model to predict postoperative acute kidney injury in patients undergoing major gastrointestinal surgery based on a national prospective observational cohort study.

Author: Aamir A
Abbas J
Abbas N
Abbott TEF
Abdalla M
Abdikadir H
Abuhussein N
Acquaah F
Adamson R
Adeleye O
Adeogun A
Adlan A
Aftab R
Afzal Z
Agarwal M
Aglan H
Agnew CJF
Agrawal R
Ahern D
Ahluwalia J
Ahluwalia V
Ahmad A
Ahmad K
Ahmed H
Ahmed I
Ahmed L
Ahmed N
Ahmed P
Ainger E
Ainsworth P
Aishwarya G
Ajibola-Taylor O
Akhbari M
Akhtar A
Akhtar R
Akpenyi O
Al-Ausi M
Al-Huneidi R
Al-Khudairi R
Al-Masri S
Al-Mousawi A
Al-Saadi N
Alagappan A
Alberts J
Alfa-Wali M
Ali A
Ali B
Ali I
Ali M
Ali Q
Ali S
Alturki N
Alwandi A
Amani L
Amarnath T
Amer M
Amin H
Amin MN
Amoah R
Amoah-Arko A
Anandarajah C
Ananthavarathan P
Andah EJE
Andrew K
Andrews H
Ang A
Ang HL
Ang JJ
Ani C
Anilkumar A
Anto N
Anwar S
Apperley H
Appleton S
Aquilina T
Archer M
Arif T
Arneill M
Arnell S
Arnold TJ
Arshad A
Arthur J
Arulkumaran N
Arya J
Asad M
Asemota N
Ashaye T
Ashdown T
Ashour R
Ashraf MR
Ashwood J
Asif U
Atkin G
Atkins B
Attalla M
Aubrey-Jones D
Auckburally S
Auld F
Auluck I
Azam S
Aziz R
Azizi A
Azmi F
Babatunde F
Babu VS
Bachi A
Bagga R
Bains H
Bajwa DS
Baker A
Baker C
Balai E
Balian V
Ball M
Bamford M
Bana R
Banfield DA
Bannard-Smith J
Barai I
Barclay J
Barfi L
Barker C
Barker M
Barmayehvar B
Barnfield J
Barnor-Ahiaku E
Baron C
Barr CJ
Barraclough J
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Beasley W
Beattie G
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Springford LR
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STARSurg Collaborative Writing Committee, Data analysis, Steering committee, Advisory group, Regional leads, Collaborators and validators
STARSurg Collaborative Writing Committee, Data analysis, Steering committee, Advisory group, Regional leads, Collaborators and validators, Nepogodiev, D
Stechman M
Stewart D
Stewart E
Stewart H
Stewart R
Stickler E
Stoddart MT
Stokes E
Stott G
Strang S
Stringer H
Stringfellow TD
Stubbing-Moore A
Sturrock S
Subar D
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Sukirthan N
Sukumar S
Sulaiman SK
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Suresh R
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Suri A
Svolkinas D
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Tariq A
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Tayeh S
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Taylor Z
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Thachettu A
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Thoms BL
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Yasin IH
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Ye W
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Yin ZD
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Yogeswara T
York J
Yousaf A
Youssef H
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Zanichelli D
Zaver V
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Zheleniakova T
Zhu Y
Zornoza A
Zubikarai G
Zulkifli A
Zuzarte L
Publication venue: 'Wiley'
Publication date: 18/05/2018
Field of study

Background: Acute illness, existing co-morbidities and surgical stress response can all contribute to postoperative acute kidney injury (AKI) in patients undergoing major gastrointestinal surgery. The aim of this study was prospectively to develop a pragmatic prognostic model to stratify patients according to risk of developing AKI after major gastrointestinal surgery. Methods: This prospective multicentre cohort study included consecutive adults undergoing elective or emergency gastrointestinal resection, liver resection or stoma reversal in 2-week blocks over a continuous 3-month period. The primary outcome was the rate of AKI within 7 days of surgery. Bootstrap stability was used to select clinically plausible risk factors into the model. Internal model validation was carried out by bootstrap validation. Results: A total of 4544 patients were included across 173 centres in the UK and Ireland. The overall rate of AKI was 14·2 per cent (646 of 4544) and the 30-day mortality rate was 1·8 per cent (84 of 4544). Stage 1 AKI was significantly associated with 30-day mortality (unadjusted odds ratio 7·61, 95 per cent c.i. 4·49 to 12·90; P < 0·001), with increasing odds of death with each AKI stage. Six variables were selected for inclusion in the prognostic model: age, sex, ASA grade, preoperative estimated glomerular filtration rate, planned open surgery and preoperative use of either an angiotensin-converting enzyme inhibitor or an angiotensin receptor blocker. Internal validation demonstrated good model discrimination (c-statistic 0·65). Discussion: Following major gastrointestinal surgery, AKI occurred in one in seven patients. This preoperative prognostic model identified patients at high risk of postoperative AKI. Validation in an independent data set is required to ensure generalizability

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Convalescent plasma in patients admitted to hospital with COVID-19 (RECOVERY): a randomised controlled, open-label, platform trial

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Abbas A.
Abbas F.
Abbas M.
Abbasi S.
Abbass H.
Abbott A.
Abdallah N.
Abdelaziz A.
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Abeer Ul Amna A.U.A.
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Abrams J.
Abu H.-J.
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Abung A.
Aceampong Y.
Achara A.
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Acton C.
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Zulfikar S.
Zullo C.
Zuriaga-Alvaro A.
Zuurbier W.
Zyengi S.
Publication venue: 'Elsevier BV'
Publication date: 29/05/2021
Field of study

Background: Many patients with COVID-19 have been treated with plasma containing anti-SARS-CoV-2 antibodies. We aimed to evaluate the safety and efficacy of convalescent plasma therapy in patients admitted to hospital with COVID-19. Methods: This randomised, controlled, open-label, platform trial (Randomised Evaluation of COVID-19 Therapy [RECOVERY]) is assessing several possible treatments in patients hospitalised with COVID-19 in the UK. The trial is underway at 177 NHS hospitals from across the UK. Eligible and consenting patients were randomly assigned (1:1) to receive either usual care alone (usual care group) or usual care plus high-titre convalescent plasma (convalescent plasma group). The primary outcome was 28-day mortality, analysed on an intention-to-treat basis. The trial is registered with ISRCTN, 50189673, and ClinicalTrials.gov, NCT04381936. Findings: Between May 28, 2020, and Jan 15, 2021, 11558 (71%) of 16287 patients enrolled in RECOVERY were eligible to receive convalescent plasma and were assigned to either the convalescent plasma group or the usual care group. There was no significant difference in 28-day mortality between the two groups: 1399 (24%) of 5795 patients in the convalescent plasma group and 1408 (24%) of 5763 patients in the usual care group died within 28 days (rate ratio 1·00, 95% CI 0·93–1·07; p=0·95). The 28-day mortality rate ratio was similar in all prespecified subgroups of patients, including in those patients without detectable SARS-CoV-2 antibodies at randomisation. Allocation to convalescent plasma had no significant effect on the proportion of patients discharged from hospital within 28 days (3832 [66%] patients in the convalescent plasma group vs 3822 [66%] patients in the usual care group; rate ratio 0·99, 95% CI 0·94–1·03; p=0·57). Among those not on invasive mechanical ventilation at randomisation, there was no significant difference in the proportion of patients meeting the composite endpoint of progression to invasive mechanical ventilation or death (1568 [29%] of 5493 patients in the convalescent plasma group vs 1568 [29%] of 5448 patients in the usual care group; rate ratio 0·99, 95% CI 0·93–1·05; p=0·79). Interpretation: In patients hospitalised with COVID-19, high-titre convalescent plasma did not improve survival or other prespecified clinical outcomes. Funding: UK Research and Innovation (Medical Research Council) and National Institute of Health Research

Enlighten

Tocilizumab in patients admitted to hospital with COVID-19 (RECOVERY): a randomised, controlled, open-label, platform trial

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Abbas A.
Abbas F.
Abbas M.
Abbasi S.
Abbass H.
Abbott A.
Abdallah N.
Abdelaziz A.
Abdelfattah M.
Abdelqader B.
Abdul Rasheed A.
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Abdul-Kadir R.
Abdul-Raheem R.
Abdulakeem A.
Abdulmumeen A.
Abdulshukkoor N.
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Abed El Khaleq Y.
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Abeer Ul Amna A.
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Abo-Leyah H.
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Abraham M.
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Abraheem A.
Abrams J.
Abu H.-J.
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Abubacker S.M.
Abung A.
Aceampong Y.
Achara A.
Acharya D.
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Zuriaga-Alvaro A.
Publication venue: 'Elsevier BV'
Publication date: 01/05/2021
Field of study

Background: In this study, we aimed to evaluate the effects of tocilizumab in adult patients admitted to hospital with COVID-19 with both hypoxia and systemic inflammation. Methods: This randomised, controlled, open-label, platform trial (Randomised Evaluation of COVID-19 Therapy [RECOVERY]), is assessing several possible treatments in patients hospitalised with COVID-19 in the UK. Those trial participants with hypoxia (oxygen saturation <92% on air or requiring oxygen therapy) and evidence of systemic inflammation (C-reactive protein ≥75 mg/L) were eligible for random assignment in a 1:1 ratio to usual standard of care alone versus usual standard of care plus tocilizumab at a dose of 400 mg–800 mg (depending on weight) given intravenously. A second dose could be given 12–24 h later if the patient's condition had not improved. The primary outcome was 28-day mortality, assessed in the intention-to-treat population. The trial is registered with ISRCTN (50189673) and ClinicalTrials.gov (NCT04381936). Findings: Between April 23, 2020, and Jan 24, 2021, 4116 adults of 21 550 patients enrolled into the RECOVERY trial were included in the assessment of tocilizumab, including 3385 (82%) patients receiving systemic corticosteroids. Overall, 621 (31%) of the 2022 patients allocated tocilizumab and 729 (35%) of the 2094 patients allocated to usual care died within 28 days (rate ratio 0·85; 95% CI 0·76–0·94; p=0·0028). Consistent results were seen in all prespecified subgroups of patients, including those receiving systemic corticosteroids. Patients allocated to tocilizumab were more likely to be discharged from hospital within 28 days (57% vs 50%; rate ratio 1·22; 1·12–1·33; p<0·0001). Among those not receiving invasive mechanical ventilation at baseline, patients allocated tocilizumab were less likely to reach the composite endpoint of invasive mechanical ventilation or death (35% vs 42%; risk ratio 0·84; 95% CI 0·77–0·92; p<0·0001). Interpretation: In hospitalised COVID-19 patients with hypoxia and systemic inflammation, tocilizumab improved survival and other clinical outcomes. These benefits were seen regardless of the amount of respiratory support and were additional to the benefits of systemic corticosteroids. Funding: UK Research and Innovation (Medical Research Council) and National Institute of Health Research

Enlighten

Dimethyl fumarate in patients admitted to hospital with COVID-19 (RECOVERY): a randomised, controlled, open-label, platform trial

Author: Abbas M.
Abdul Rasheed A.
Abdul A.
Abdul-Kadir R.
Abdusamad K.
Abernethy K.
Aboelela H.
Abouzaid M.
Abraham M.
Abraham T.
Abrams J.
Abu H.
Abu-Arafeh A.
Acton C.
Adam F.
Adam M.
Adams C.
Adams C.
Adams D.
Adams L.
Addo A.
Adedeji O.
Adegoke K.
Adewunmi E.
Adeyemo T.
Agbeko R.
Aggarwal S.
Ahmad S.
Ahmed A.
Ahmed I.
Ahmed M.
Ahmed R.
Ahmed R.
Ainsworth M.
Ajmi A.
Akili S.
Al Aaraj A.
Al Balushi A.
Al-Asadi A.
Al-Khalil M.
Al-Ramadhani B.
Al-Saadi Z.
Al-Shahi Salman R.
Al-Sheklly B.
Albert P.
Alegria A.
Alexander A.
Alexander P.
Alhabsha O.
Ali M.
Ali M.
Aliberti E.
Alin J.
Aliyuda F.
Alkhudhayri A.
Allan N.
Allanson A.
Allen E.
Allen L.
Alshaer I.
Altaf S.
Amezaga M.
Amin A.
Amit B.
Anand A.
Anantapatnaikuni S.
Anderson L.
Anderson M.
Anderson M.
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Aniruddhan K.
Antonina Z.
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Publication venue: Springer Science and Business Media LLC
Publication date: 31/01/2024
Field of study

Dimethyl fumarate (DMF) inhibits inflammasome-mediated inflammation and has been proposed as a treatment for patients hospitalised with COVID-19. This randomised, controlled, open-label platform trial (Randomised Evaluation of COVID-19 Therapy [RECOVERY]), is assessing multiple treatments in patients hospitalised for COVID-19 (NCT04381936, ISRCTN50189673). In this assessment of DMF performed at 27 UK hospitals, adults were randomly allocated (1:1) to either usual standard of care alone or usual standard of care plus DMF. The primary outcome was clinical status on day 5 measured on a seven-point ordinal scale. Secondary outcomes were time to sustained improvement in clinical status, time to discharge, day 5 peripheral blood oxygenation, day 5 C-reactive protein, and improvement in day 10 clinical status. Between 2 March 2021 and 18 November 2021, 713 patients were enroled in the DMF evaluation, of whom 356 were randomly allocated to receive usual care plus DMF, and 357 to usual care alone. 95% of patients received corticosteroids as part of routine care. There was no evidence of a beneficial effect of DMF on clinical status at day 5 (common odds ratio of unfavourable outcome 1.12; 95% CI 0.86-1.47; p = 0.40). There was no significant effect of DMF on any secondary outcome

White Rose Research Online

Effects of fluoxetine on functional outcomes after acute stroke (FOCUS): a pragmatic, double-blind, randomised, controlled trial

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Abbott L
Abbott W
Abdul-Hamid A
Abdul-Saheb M
Abousleiman Y
Abubakar S
Adedoyin T
Adie K
Affley B
Ahlquist K
Ahmad N
Ahmed A
Ahmed S
Ahmed Z
Al Hussayni S
Al-Samarrai N
Alam I
Alam S
Ali A
Ali K
Allen C
Allen J
Allison J
Allsop H
Allsop L
Almadenboyle C
Alvares W
Alwis L
Alwis L
Amero J
Amis E
Amlani S
Amor K
Anazodo C
Anderson R
Andrews J
Anjum T
Annamalai A
Annison F
Anthony A
Appiatse G
Archer J
Argandona L
Arif S
Armer C
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Aruldoss P
Arundell L-L
Ashcroft P
Asokanathan A
Aubrey B
Augustin M
Auld G
Austin D
Awolesi J
Ayer J
Azim A
Badiani B
Bahk A
Bailey D
Bailey L
Bakawala R
Baker J
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Balami J
Balasubramanian V
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Ball J
Ball L
Balogun I
Bamford E
Bamford J
Banaras A
Barber M
Barbon E
Barcroft H
Barker J
Barron C
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Barry A
Barugh A
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Bateman G
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Beardmore C
Bedford C
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Bell J
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Besley S
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Bharaj K
Bhargava M
Bhattad M
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Board J
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Zachariah G
Zhang L
Publication venue: 'Elsevier BV'
Publication date: 01/01/2019
Field of study

Background Results of small trials indicate that fluoxetine might improve functional outcomes after stroke. The FOCUS trial aimed to provide a precise estimate of these effects. Methods FOCUS was a pragmatic, multicentre, parallel group, double-blind, randomised, placebo-controlled trial done at 103 hospitals in the UK. Patients were eligible if they were aged 18 years or older, had a clinical stroke diagnosis, were enrolled and randomly assigned between 2 days and 15 days after onset, and had focal neurological deficits. Patients were randomly allocated fluoxetine 20 mg or matching placebo orally once daily for 6 months via a web-based system by use of a minimisation algorithm. The primary outcome was functional status, measured with the modified Rankin Scale (mRS), at 6 months. Patients, carers, health-care staff, and the trial team were masked to treatment allocation. Functional status was assessed at 6 months and 12 months after randomisation. Patients were analysed according to their treatment allocation. This trial is registered with the ISRCTN registry, number ISRCTN83290762. Findings Between Sept 10, 2012, and March 31, 2017, 3127 patients were recruited. 1564 patients were allocated fluoxetine and 1563 allocated placebo. mRS data at 6 months were available for 1553 (99·3%) patients in each treatment group. The distribution across mRS categories at 6 months was similar in the fluoxetine and placebo groups (common odds ratio adjusted for minimisation variables 0·951 [95% CI 0·839–1·079]; p=0·439). Patients allocated fluoxetine were less likely than those allocated placebo to develop new depression by 6 months (210 [13·43%] patients vs 269 [17·21%]; difference 3·78% [95% CI 1·26–6·30]; p=0·0033), but they had more bone fractures (45 [2·88%] vs 23 [1·47%]; difference 1·41% [95% CI 0·38–2·43]; p=0·0070). There were no significant differences in any other event at 6 or 12 months. Interpretation Fluoxetine 20 mg given daily for 6 months after acute stroke does not seem to improve functional outcomes. Although the treatment reduced the occurrence of depression, it increased the frequency of bone fractures. These results do not support the routine use of fluoxetine either for the prevention of post-stroke depression or to promote recovery of function. Funding UK Stroke Association and NIHR Health Technology Assessment Programme

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Dimethyl fumarate in patients admitted to hospital with COVID-19 (RECOVERY): a randomised, controlled, open-label, platform trial

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Abdul Rasheed A.
Abdul A.
Abdul-Kadir R.
Abdusamad K.
Abernethy K.
Aboelela H.
Abouzaid M.
Abraham M.
Abraham T.
Abrams J.
Abu H.
Abu-Arafeh A.
Acton C.
Adam F.
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Adams C.
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Addo A.
Adedeji O.
Adegoke K.
Adewunmi E.
Adeyemo T.
Agbeko R.
Aggarwal S.
Ahmad S.
Ahmed A.
Ahmed I.
Ahmed M.
Ahmed R.
Ainsworth M.
Ajmi A.
Akili S.
Al Aaraj A.
Al Balushi A.
Al-Asadi A.
Al-Khalil M.
Al-Ramadhani B.
Al-Saadi Z.
Al-Shahi Salman R.
Al-Sheklly B.
Albert P.
Alegria A.
Alexander A.
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Alhabsha O.
Ali M.
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Alin J.
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Amin A.
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Anand A.
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Campbell Hewson Q.
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Campbell Mark
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Caplin B.
Capp A.
Carey C.
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Carmody M.
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Carrington Z.
Carroll A.
Carson R.
Carter J.
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Carty C.
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Casey S.
Cate H.
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Central Coordinating Office (for the RECOVERY Collaborative Group)
Century H.
Chadwick J.
Chakkarapani E.
Chakraborty A.
Chamberlain S.
Chambers E.
Chambers L.
Chan E.
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Chaplin J.
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Charles B.
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Chen F.
Cheng F.
Cherrie M.
Cheung E.
Cheyne C.
Chilcott S.
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Chin K.
Chineka R.
Chinonso E.
Chisnall B.
Chiswick C.
Chivima B.
Chmiel C.
Chrisopoulou A.
Christian P.
Christides A.
Christmas D.
Church E.
Cianci N.
Cicconi P.
Clare E.
Clark E.
Clark G.
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Clarke A.
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Clarke S.
Clay K.
Clayton-Smith J.
Cleaver C.
Clemente de la Torre C.
Clifford S.
Coakley M.
Cobain K.
Cochrane P.
Cocks S.
Coe A.
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Cohen D.
Coker O.
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Coles H.
Collier D.
Collini Paul
Collins J.
Collins V.
Colton H.
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Conteh V.
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Cook E.
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Cornwell J.
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Crawford A.
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Cremona J.
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Daglish J.
Dalgleish H.
Dalton M.
Damm E.
Darbyshire Janet
Darnell S.
Darton T.
Das S.
Dasgin J.
Data Monitoring Committee of the RECOVERY Collaborative Group
Daunt A.
Dave V.
Davey M.
Davidson N.
Davies B.
Davies C.
Davies J.
Davies K.
Davies N.
Davies P.
Davies R.
Davis A.
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Dawe C.
Dawson A.
Day Jeremy
de Fonseka D.
de Silva T.
De Soyza A.
de Vos J.
Dean K.
Deane J.
Dear J.
Deelchand V.
Deery J.
DeMets David
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Dent M.
Denton E.
Denwood T.
Dermody S.
Desai A.
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Dey P.
Dhaliwal K.
Dhani S.
Dhasmana Devesh J.
Dhillon R.
Dicks P.
Digby J.
Dimitri P.
Dismore L.
Ditchfield L.
Dixon C.
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Dobbie L.
Dobson C.
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Docherty M.
Dockrell D.
Dodds R.
Dodds S.
Dolan D.
Dolman M.
Donald L.
Donaldson D.
Donaldson K.
Donlon S.
Donohoe A.
Donohoe G.
Dosani M.
Dosanjh D.
Dowden L.
Dowling S.
Downey R.
Downs L.
Dowson S.
Drake C.
Drewett O.
Drogan H.
Drummond G.
Druryk K.
Du Thinh A.
Duckles-Leech H.
Duffield E.
Duffy H.
Duggan A.
Dummer S.
Duncan C.
Duncan F.
Duncan G.
Duncan R.
Dunleavy J.
Dunn A.
Duran B.
Durrans L.
Durrington H.
Duru I.
Dymond H.
D’Costa J.
D’Mello A.
Eades C.
Early J.
Eatough R.
Eddleston M.
Edgerley K.
Edmond N.
Edwards C.
Edwards J.
Ehiorobo L.
Ekoi M.
Elbeshy M.
Elenwa U.
Elgohary A.
Ellis C.
Ellwood A.
Elokl M.
Elsefi T.
Elyoussfi S.
Emberson Jonathan R.
Emms M.
Emond F.
Emonts M.
Essa F.
Evans B.
Evans G.
Evans M.
Evans R.
Everden C.
Everden S.
Evison L.
Ezenduka C.
Fairbairn I.
Fairclough A.
Falconer E.
Faluyi D.
Fancois V.
Farmery T.
Farooq H.
Farrell B.
Farzana S.
Fatemi A.
Fatemi M.
Faust S. N.
Faust Saul N.
Fearby S.
Felton T.
Fenlon K.
Fenn A.
Fenner I.
Fenton C.
Ferenando G.
Ferguson C.
Ferguson S.
Ferguson V.
Fernandez Lopez S.
Ferriman E.
Ferron S.
Fethers N.
Fielding J.
Finch S.
Fineman N.
Finn A.
Fiouni S.
Fisher J.
Fitzgerald F.
Flaherty J.
Fleming L.
Fletcher L.
Fogarty G.
Foot H.
Fordham I.
Forrest A.
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Foster E.
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Fowler Robert
Fowler S.
Fox A.
Fox C.
Fox S.
Frake R.
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Frankland H.
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Fullerton D.
G N.
Gabbitas E.
Gabriel C.
Gabriel Z.
Gale C.
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Gallagher B.
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Garden E.
Gardiner P.
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Garg I.
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Gaughan E.
Geele F.
George B.
George S.
George V.
Georgiou D.
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Giannopoulou S.
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Gibb C.
Gibbison B.
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Gibson A.
Gill L.
Gillesen A.
Gillian A.
Gilliland D.
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Gipson A.
Glasgow S.
Glover Bengtsson J.
Glynn S.
Gnanalingam C.
Godden E.
Godson E.
Goldacre R.
Goodall J.
Goodenough B.
Goodwin E.
Goodwin J.
Goonasekara M.
Gorsuch T.
Gosai J.
Gotham D.
Gould N.
Gould S.
Gourbault L.
Gowans S.
Gower H.
Graham J.
Grahamslaw J.
Grana G.
Grant A.
Grant D.
Gray A.
Gray G.
Gray J.
Gray K.
Grayson A.
Green A.
Green C.
Green Christopher A.
Green N.
Greene D.
Greenhalgh A.
Gregory K.
Greig J.
Gresty J.
Grey G.
Griffin B.
Griffin M.
Grobovaite E.
Groome R.
Grover H.
Grubb N.
Grundy J.
Guerin J.
Gureviciute A.
Gurung Rai S.
Gurung L.
Hackney P.
Hadfield D.
Hadfield S.
Haider N.
Haigh K.
Haile V.
Hainey S.
Hall A.
Hall C.
Hall E.
Hall J.
Hallas J.
Halls H.
Hamdollah-Zadeh M.
Hameed B.
Hamid I.
Hamilton G.
Hamilton M.
Hamilton S.
Hammans B.
Hammersley S.
Hammond S.
Hamoodi I.
Hampshire K.
Hampson L.
Hanci O.
Handrean S.
Handzewniak N.
Haney S.
Hanison E.
Hannington A.
Hanrath A.
Hanson A.
Hanson H.
Hanson J.
Hanson S.
Harden L.
Harding Z.
Hardman S.
Hargreaves C.
Harin A.
Harman T.
Harper C.
Harper H.
Harris J.
Harris M.
Harrison D.
Harrison M.
Harrison R.
Harrison S.
Harrod E.
Hartrey W.
Harvey A.
Harvey M.
Haslam J.
Hastings B.
Havinden-Williams M.
Hawker L.
Hayat A.
Haynes Richard
Hays C.
Haysom S.
Hazelton T.
Hazenberg P.
Headon E.
Health records (for the RECOVERY Collaborative Group)
Hector G.
Heddon S.
Henry J.
Henshall D.
Hernandez F.
Herrington W.
Heslop P.
Hester S.
Hey S.
Heywood J.
Hicks J.
Hicks S.
Higgins L.
Hill P.
Hilton J.
Hindle A.
Hindmarsh A.
Hine P.
Hird C.
Hobson S.
Hodgen L.
Hodgkinson S.
Hodgson H.
Hodgson S.
Hogg L.
Hoggett L.
Holden C.
Holdhof N.
Holland L.
Hollands M.
Holling N.
Holmes R.
Holt L.
Hope S.
Hopkins B.
Horby Peter W.
Horrobin C.
Horsley A.
Hough M.
Houghton C.
Houghton K.
Houlihan R.
Housely K.
How L.
Howard L.
Howard M.
Howard S.
Howard-Sandy L.
Howell A.
Howie L.
Hrycaiczuk J.
Htwe S.
Hudak A.
Hudson H.
Hughes G.
Hughes H.
Hughes S.
Hulbert R.
Hull D.
Hull R.
Hulme A.
Hulme P.
Hum R.
Hunt L.
Hunter E.
Hunter K.
Hunter N.
Hunter S.
Hurditch E.
Hurley K.
Hussain A.
Hussain S.
Hussain Y.
Hutchinson C.
Hutton P.
Hyslop M.
Ibrahim A.
Ibrahim M.
Ijaz M.
Ilyas F.
Ingham J.
Ingram T.
Ionita A.
Iqbal J.
Iqbal M.
Irons R.
Irving R.
Islam S.
Islim A.
Ismail O.
Iwanikiw S.
Jack C.
Jackman S.
Jackson B.
Jackson S.
Jacob J.
Jacob P.
Jacques N.
Jafar A.
Jagannathan V.
Jaime F.
Jaki Thomas
Jaly Y.
Jama R.
Jamal A.
Jamal S.
James L.
Jameson J.
Janes K.
Japp D.
Jarman C.
Jarvis C.
Jarvis R.
Jastrzebska P.
Jeebun V.
Jeffery Katie
Jeffreys N.
Jeffs B.
Jenkins P.
Jennings F.
Jennings V.
Jerry D.
Jimenez Gil A.
Johal S.
John A.
John M.
Johnson G.
Johnston B.
Johnston S.
Johnstone D.
Johnstone E.
Jones A.
Jones B.
Jones E.
Jones G.
Jones J.
Jones P.
Jones R.
Jones S.
Jones T.
Jordache R.
Jose S.
Joseph G.
Joseph R.
Josiah B.
Ju Wen Kwek A.
Judge P.
Juszczak Edmund
Kailey A.
Kalayi R.
Kamath P.
Kamfose M.
Kanabar D.
Kapoor R.
Karunaratne N.
Kaur J.
Kausar Z.
Kavanagh S.
Kay S.
Kayappurathu J.
Ke M.
Keating L.
Keddie-Gray E.
Kelly E.
Kelly R.
Kelly S.
Kendall E.
Kennedy A.
Kennedy M.
Keogan L.
Khan A.
Khan M.
Khan W.
Khatun T.
Khin H.
Khurana C.
Kibutu F.
Kidd M.
Kidney S.
Kim M.
Kimber A.
King A.
King J.
King S.
King-Oakley E.
Kirk J.
Kirkham E.
Kirkpatrick L.
Kitching T.
Kitto L.
Knight A.
Knight F.
Knight Marian
Knight S.
Knowles C.
Knowles L.
Koch O.
Koe Y.
Koirata A.
Kolakaluri E.
Kononen M.
Koo H.
Kosmidis C.
Kothandaraman E.
Koukou K.
Kountourgioti A.
Krasauskas K.
Krishnamurthy V.
Krizak S.
Krupej S.
Kudsk-Iversen S.
Kudzinskas A.
Kumar R.
Kurani A.
Kurdy M.
Kuriakose K.
Kyere-Diabour T.
Kyi N.
Labao J.
Lacson M.
Ladan Z.
Lagnado A.
Lalloo David
Lalloo F.
Lamb L.
Lamb T.
Landray Martin J.
Lane N.
Lang A.
Lang S.
Langley M.
Langoya C.
Lassa S.
Latham S.
Latham V.
Laurenson M.
Law H.
Lawless L.
Lawrence G.
Lawrence H.
Lawrie R.
Lay M.
Lazo M.
Le V.
Leach L.
Leandro L.
Lee S.
Lees D.
Legge H.
Leitch D.
Lemoine N.
Lennon K.
Levett C.
Levynska A.
Lewis H.
Lewis J.
Lewis K.
Lewis L.
Lewis N.
Liao A.
Lim Wei Shen
Linares C.
Lindergard G.
Lindsay M.
Lipscomb G.
Lipscomb K.
Little J.
Liu P.
Liu S.
Lloyd A.
Lloyd O.
Lo S.
Loader D.
Local Clinical Centre staff (for the RECOVERY Collaborative Group)
Lock S.
Locke T.
Lockett T.
Lodhia K.
Lofthouse M.
Logan M.
Logue C. A.
Lokanathan S.
Lomme K.
Looby L.
Lopez P.
Lord R.
Loro F.
Lovell M.
Low A.
Low S.
Lowe C.
Lowsby R.
Luintel A.
Luke H.
Luke J.
Lunn M.
Luo J.
Lye A.
Lyell B.
Lynch D.
Mabb H.
Macfarlane J.
Macfarlane L.
MacInnes L.
MacIntyre I.
Mackay L.
MacKenzie J.
Mackey A.
Mackintosh C.
Macmahon M.
MacRaild A.
Madden A.
Madeja N.
Mafham Marion
Magnaye L.
Maharajh A.
Mahaveer A.
Mahdi H.
Maheswaran A.
Mahmood W.
Mahmood Z.
Mahony E.
Mahungu T.
Mair L.
Majekdunmi T.
Majumdar Jaydip
Malein Flora
Mancinelli R.
Mandal S.
Manderson L.
Mandeville J.
Mane T.
Manso K.
Mansour M.
Marecka M.
Maren D.
Margabanthu G.
Margaritopoulos G.
Maria del Rocio F.
Mariano V.
Marks B.
Marks P.
Marriott C.
Marriott N.
Marsden P.
Marshall A.
Martin H.
Martin K.
Martin M.
Martinez Garrido J.
Maseda D.
Mashate S.
Masih S.
Masoli M.
Mathen S.
Mather N.
Mathew B.
Mathews J.
Mathioudakis A.
Matila D.
Matisa E.
Matkins E.
Matovu E.
Matthews C.
May P.
Mayanagao I.
Mayer J.
Mayo T.
Mazhani T.
McAlinden P.
McAndrew J.
McBrearty C.
McBride E.
McCafferty G.
McCann C.
McCarthy E.
McCorkindale A.
McCrae J.
McCullagh I.
McCullagh L.
McCullough K.
McCullough S.
McCurrach F.
McDermott J.
McDonald S.
McDonnell N.
McEleavy I.
McEvoy E.
McGhee C.
McGrath B.
McIntyre K.
Mckie H.
Mckie L.
McLachlan H.
McLarty N.
McLeish M.
McLure S.
McMahon G.
McMaster P.
McMillan N.
McMullen H.
McNeill C.
McNeill J.
McNelis U.
McNulty M.
McSorland D.
Mead J.
Meakin O.
Mears K.
Mediana A.
Medine R.
Meghani N.
Megson S.
Mehar A.
Mehra R.
Meiring J.
Melander S.
Mellor F.
Mellor Z.
Melville A.
Melville J.
Membrey H.
Mendonca C.
Mentzer A.
Meredith M.
Merron P.
Metcalfe B.
Metryka A.
Mew L.
Mguni N.
Miah N.
Micallef D.
Michalak N.
Michalec O.
Middle J.
Middleton J.
Middleton M.
Millard J.
Miller J.
Millett L.
Milligan H.
Millington K.
Millington S.
Millward H.
Minton J.
Mishra A.
Mishra B.
Mistry H.
Mital D.
Mitchell B.
Mitchelmore P.
Mitra S.
Moatt E.
Mohamed O.
Mohammed O.
Mok J.
Molina M.
Molloy A.
Monaghan H.
Monsell K.
Montasser M.
Montgomery Alan
Moon A.
Moon J.
Moonan M.
Moore F.
Moores R.
Morales J.
Moran L.
Moray G.
Morgan A.
Morgan L.
Morgan-Smith E.
Morilla J.
Morley W.
Morris L.
Morris P.
Morris S.
Morrison S.
Morrissey M.
Morrow A.
Moss S.
Moth G.
Motherwell N.
Moulton H.
Mounce G.
Mtuwa S.
Muazzam A.
Mudawi D.
Mulcahy M.
Mulligan S.
Mumford Andrew
Munavvar Mohammed
Munt S.
Murphy S.
Murray C.
Murray D.
Murray I.
Murray K.
Murray L.
Murthy M.
Mutch C.
Muzengi N.
Mwaura E.
Nafei M.
Nagarajan T.
Naglik L.
Naguib M.
Naicker K.
Naisbitt J.
Nandani A.
Nandwani T.
Nasa S.
Natarajan N.
Nathvani M.
Navarra H.
Naveed S.
Naz M.
Neal A.
Nelson B.
Nelson S.
Nethercott D.
Newby D.
Newman T.
Newport R.
Ng S.
Ngumo A.
Nicholas N.
Nicholas P.
Nickson I.
Nicol R.
Nightingale T.
Nilsson A.
Ninan P.
Nirmalan M.
Nixon J.
Nizam Ud Din K.
Noe H.
Norton R.
Nourein K.
Nunn K.
Nunn M.
Nunnick J.
Nurgat Z.
Nuttall A.
Nwajiugo P.
Oboh C.
Obukofe R.
Odam M.
Odedra K.
Odell N.
Offord P.
Ohia U.
Okeke T.
OKell E.
Oliver A.
Oliver J.
Oliver Z.
Oomatia A.
Oram R.
Oreilly C.
Osadcow A.
Osanlou R.
Osborne N.
Osborne R.
Osborne W.
Osei-Bobie J.
Oxlade R.
O’Brien R.
O’Callaghan C.
O’Connor G.
O’Donovan C.
O’Farrell S.
O’Riordan D.
O’Sullivan E.
Padden G.
Page I.
Page S.
Pagett K.
Pajak S.
Pakou G.
Palacios A.
Palfrey H.
Pandya T.
Panes A.
Pantin C.
Parambil V.
Parashar S.
Parekh A.
Parekh D.
Parker B.
Parker J.
Parker S.
Parkinson A.
Passby L.
Passey S.
Patachako J.
Patel M.
Patel P.
Patel S.
Patience A.
Patten S.
Patterson C.
Patterson L.
Pauls L.
Paulus S.
Payne B.
Payne E.
Payne R.
Peacock L.
Pearce J.
Pearson K.
Peasley A.
Peggie H.
Pelham C.
Penman C.
Penman J.
Penman R.
Percival R.
Perez E.
Periyasamy L.
Perry A.
Perry M.
Pessoa-Amorim Guilherme
Peters C.
Peterson A.
Peto Leon
Petrova B.
Pezard-Snell M.
Phelan P.
Philbin J.
Phillips N.
PI M.
Pick S.
Pickard J.
Pickering G.
Piercy C.
Pinches H.
Pine K.
Pinjala M.
Pitchford M.
Pleass R.
Plowright M.
Plumptre C.
Pomery F.
Poole L.
Porter D.
Porter L.
Potter A.
Potts J.
Poustie V.
Power N.
Poyner E.
Pradhan V.
Prady H.
Prasath S.
Pratt A.
Pratt S.
Preiss D.
Prest C.
Price A.
Price C.
Price D.
Price K.
Price L.
Price V.
Price-Eland R.
Priest A.
Prince C.
Pringle S.
Pristopan V.
Priyash V.
Prudon Benjamin
Pugh L.
Purdue C.
Purdy R.
Pursell M.
Purvis S.
Putensen D.
Pyart E.
Quek E.
Quigley J.
Quindoyos J.
Quinn T.
Rabinowicz S.
Rafique J.
Rahman M.
Rai S.
Raithatha A.
Rajasri A.
Ramanan A.
Ramasamy M.
Ramchandani A.
Ramirez J.
Rampling T.
Ramsay J.
Ramshaw A.
Rana G.
Rand J.
Rank H.
Rankhelawon R.
Rasheed A.
Ratcliffe S.
Raw J.
Razvi Z.
RECOVERY Collaborative Group
Redknap I.
Redman N.
Rees A.
Rees M.
Rees S.
Rehman Z.
Reilly M.
Reith C.
Renshaw S.
Rey S.
Reynard C.
Reynolds H.
Rhodes J.
Rice E.
Rice M.
Rice N.
Richardson E.
Richardson N.
Rigby L.
Riley M.
Riley P.
Ripley D.
Rishton C.
Riste M.
Ritchings A.
Rivera Ortega P.
Robbins E.
Roberts V.
Robertson C.
Robertson J.
Robertson N.
Robinson J.
Robinson L.
Robinson S.
Robson S.
Roderick M.
Rodger A.
Rodgers A.
Rodgers N.
Rodgers P.
Roehr C.
Rogers J.
Rogers S.
Rogers T.
Rook C.
Rooney L.
Rosby E.
Rose A.
Rose Z.
Ross I.
Rothman A.
Rothwell J.
Roughley L.
Rowan Kathryn
Rowan N.
Rowe A.
Rowe N.
Rowley M.
Rudenko A.
Rule R.
Rushmer J.
Ryan A.
Ryan L.
Ryan P.
Rybka E.
Ryder S.
Salberg A.
Saleh M.
Salih H.
Salman R.
Salmon R.
Sam M.
Sam S.
Saminathan S.
Sammons E.
Sammut D.
Sampson J.
Samuel M.
Samuel Y.
Sanchez Gonzalez A.
Sanchez V.
Sandercock Peter
Sangombe M.
Sanju M.
Santosh R.
Sarfatti A.
Sarkar R.
Sarwar Z.
Sathyanarayanan L.
Saunderson A.
Scaletta D.
Scanlon D.
Scarratt L.
Scattergood S.
Schadenberg A.
Schafers J.
Schneblen W.
Schofield E.
Schumacher N.
Schunke N.
Scobie A.
Scoones T.
Scott A.
Scott C.
Scullion A.
Seaton I.
Sedano J.
Segovia M.
Selby F.
Sellers K.
Sen N.
Sengupta A.
Sewdin T.
Seymour J.
Shah H.
Shah R.
Shah S.
Shaibu A.
Shanahan T.
Sharaf H.
Sharma B.
Sharma O.
Sharma S.
Sharp L.
Sharratt P.
Shaw D.
Shaw J.
Shawcross A.
Shea D. O.
Sheffield J.
Shehata Z.
Shenton J.
Shepherd A.
Shepherd K.
Shepherd L.
Sheppeard R.
Sheridan H.
Sheridan R.
Sherwin S.
Shibly S.
Shiham F.
Shilladay C.
Shillitoe B.
Shioi C.
Shirley K.
Shurlock J.
Shurmer Jack
Siamia L.
Siddle E.
Sime R.
Simpson A.
Simpson D.
Simpson J.
Simpson M.
Simpson P.
Sinclair S.
Singh C.
Singh S.
Singhal P.
Sithiravel S.
Sivanadarajah S.
Skaria A.
Skehan N.
Skinner T.
Skinner V.
Skorko A.
Slack A.
Slade H.
Small E.
Smallridge A.
Smart B.
Smith C.
Smith E.
Smith H.
Smith J.
Smith L.
Smith M.
Smith N.
Smith P.
Smith R.
Smith S.
Smith T.
Smith V.
Snell D.
Sobande T.
Sobrino Diaz A.
Solly R.
Soni G.
Soor P.
Soothill G.
Soren J.
Spiller W.
Spring O.
Squires G.
Squires J.
Squires R.
Srinivasan R.
Stagg W.
Stanton A.
Staplin Natalie
Starnes D.
Steer J.
Stefania V.
Stefanowska P.
Stephens A.
Stephensen D.
Stephenson E.
Sterrenburg M.
Stevens W.
Stevenson A.
Stevenson S.
Steward M.
Stewart C.
Stewart K.
Stewart Richard
Stickley J.
Stirrup S.
Stock S.
Stockdale A.
Stone B.
Stone S.
Storey I.
Stratton E.
Stratton J.
Stubbs A.
Stuttard M.
Subudhi C.
Sugden P.
Sukumaran A.
Sundar S.
Surtees M.
Sutherland R.
Sutherland S.
Sutu M.
Swanson-Low C.
Swart T.
Swift E.
Swist-Szulik K.
Sykes D.
Sykes E.
Symon D.
Syndercombe A.
T-Michael H.
Tadros M.
Tague L.
Tahir H.
Tait J.
Talbot P.
Tallent R.
Tallon B.
Tanney C.
Tanton E.
Taribagil P.
Tarr E.
Tasiou A.
Tate A.
Taylor C.
Taylor J.
Taylor K.
Taylor L.
Taylor R.
Taylor-Siddons M.
Teasdale F.
Teasdale J.
Teasdale K.
Tebbutt J.
Telfer A.
Tempany J.
Tereszkowski-Kaminski R.
Tewkesbury D.
Thake M.
Thakker M.
Thamu B.
Thet P.
Thomas A.
Thomas E.
Thomas K.
Thomas R.
Thomas S.
Thompson E.
Thompson J.
Thompson K.
Thompson R.
Thornton D.
Thornton J.
Thornton S.
Thorpe S.
Thrasyvoulou L.
Thraves H.
Thu-Ta P.
Thwaites Guy
Tilbey S.
Timerick J.
Timmins A.
Tinkler H.
Tipper J.
Tivenan H.
Todd S.
Tohfa M.
Toohey C.
Topham K.
Topping M.
Tousis R.
Trevelyan M.
Trewick N.
Truell R.
Tsakiridou K.
Tsang C.
Tucker S.
Tufail A.
Tuff J.
Tully R.
Turbitt K.
Turgut T.
Turner G.
Turner K.
Turner S.
Turner-Bone I.
Turney S.
Tyer A.
UK National Institute for Health Research Clinical Research Network (for the RECOVERY Collaborative Group)
Ul Haq M.
Ul Hassan W.
Underwood C.
Unsworth A.
Uriel Alison
Usher R.
Ustianowski A.
Vankayalapati P.
Van’t Hoff W.
Varghese M.
Varnier G.
Vasu V.
Vatish M.
Veerasamy S.
Velankar S.
Vella N.
Velugupati A.
Venables I.
Venditti M.
Veres M.
Vergnano S.
Vernall R.
Verula J.
Vethanayagam N.
Vettikumaran S.
Victoria S.
Vinay S.
Vincent O.
Vincent R.
Vyras E.
Wade P.
Waite A.
Walden A.
Walker I.
Walker K.
Walker S.
Wallace G.
Wallendszus K.
Wallis G.
Walsh D.
Walters J.
Walton E.
Walton O.
Wang N.
Wang R.
Wang S.
Warburton S.
Ward J.
Ward L.
Ward R.
Wardle S.
Warmington J.
Warner C.
Warran S.
Warren R.
Warren Y.
Warris Adilia
Wasson E.
Waterfall H.
Waters D.
Watson A.
Watson E.
Watson J. G. R.
Watson L.
Watson R.
Watterson D.
Watts M.
Waugh V.
Wayman E.
Weatherhead M.
Webb C.
Webster I.
Weerakoon R.
Weetman M.
Wei S.
Welch J.
Welch S.
Wels R.
Welters I.
Welton R.
Wentworth L.
West R.
West S.
Western L.
Westhead R.
Weston H.
Wetherill B.
White A.
Whitehead C.
Whitehouse A.
Whitehouse T.
Whiteley J.
Whiteley S.
Whittaker E.
Whittle H.
Whittle R.
Wignall C.
Wilcock D.
Wilcock E.
Wild S.
Wilding L.
Wilding P.
Wildsmith T.
Wiles J.
Wilkins S.
Wilkinson S.
Wilkinson T.
Williams A.
Williams E.
Williams J.
Williams K.
Williams M.
Williams P.
Williams S.
Williams T.
Williamson D.
Williamson J.
Willis E.
Willis H.
Willis J.
Wilson B.
Wilson K.
Wilson L.
Win K.
Winder L.
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Publication venue: Nature Publishing Group
Publication date
Field of study

Repository@Nottingham

Potential sources of neck and back pain in clinical conditions of dogs and cats: a review

Author: Webb Aubrey A
Publication venue: http://www.elsevier.com/wps/find/homepage.cws_home
Publication date: 01/05/2003
Field of study

Pathological neck and back pain occurs in many medical conditions of dogs and cats. Pain may arise from a variety of structures including the intervertebral disks, facet joint capsules, dorsal root ganglia, vertebral ligaments, the vertebral periosteum, and the meninges. The source of this pain is dependent upon the type of disease process and its location within or surrounding the spinal column. Diseases can directly or indirectly stimulate pain sensors (nociceptors). Inflammatory diseases may hypersensitize these receptors or nociceptive pathways with inflammatory mediating substances such as serotonin, histamine and potassium. Diseases resulting in mechanical compression of nociceptors or nociceptive pathways may also result in neck and back pain. A thorough understanding of spinal pain occurring in dogs and cats will lead to more accurate diagnoses and treatment and may provide information regarding prognoses for various diseases. Evidence pointing to sources of spinal pain taken fron scientific and clinical studies of a variety of species including humans is provided. Suspected or known sources of neck and back pain occurring in several clinical conditions of dogs and cats are discussed.Ye

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