43 results on '"Leyland, K"'
Search Results
2. 2001P Epidemiology and treatment patterns of patients with locally advanced or metastatic urothelial cancer in France: A non-interventional database study
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Joly Lobbedez, F., Roupret, M., Culine, S., Tricotel, A., Casarotto, E., Minacori, R., Strunz-McKendry, T., Karzazi, K., Leyland, K., Vuillet, M., and Thomas, M-C.
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- 2024
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3. Differential visceral blood flow in the hyperdynamic circulation of patients with liver cirrhosis
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McAvoy, N. C., Semple, S., Richards, J. M. J., Robson, A. J., Patel, D., Jardine, A. G. M., Leyland, K., Cooper, A. S., Newby, D. E., and Hayes, P. C.
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- 2016
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4. Response to: ‘Painful knee but not hand osteoarthritis is an independent predictor of mortality over 23 years follow-up of a population-based cohort of middle-aged women’ by Gao et al
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Kluzek, S, Sanchez-Santos, M T, Leyland, K M, Judge, A, Newton, J, and Arden, N K
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- 2016
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5. Clinical and molecular associations with outcomes at two years after acute knee injury: a longitudinal study in the Knee Injury Cohort at the Kennedy (KICK)
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Garriga, C, Goff, M, Paterson, E, Hrusecka, R, Hamid, B, Alderson, J, Leyland, K, Honeyfield, L, Greenshields, L, Satchithananda, K, Lim, A, Arden, NK, Judge, A, Williams, A, Vincent, TL, and Watt, FE
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MODEL ,Science & Technology ,SYNOVIAL-FLUID ,Rheumatology ,RUPTURE ,MARKERS ,CARTILAGE ,MURINE OSTEOARTHRITIS ,ARTHRITIS ,Life Sciences & Biomedicine ,ANTERIOR CRUCIATE LIGAMENT ,GENE-EXPRESSION ,INFLAMMATORY CYTOKINES - Abstract
Background: Joint Injury is a major risk factor for osteoarthritis (OA) and an opportunity to prospectively examine its early processes. We investigated whether predefined baseline factors including demographic, clinical factors and protein analytes in knee synovial fluid (sf/SF) and in plasma/serum were associated with clinically relevant outcomes at two years after knee injury. Methods: This was a longitudinal cohort study (REC10/H0805/39;NCT02667756) with 150 individuals aged 16-50 recruited within 8 weeks of a clinically significant acute knee injury (effusion and structural injury on MRI), which was typically being treated surgically. Twelve SF and four plasma/serum biomarkers were measured by immunoassay as the exposures of interest. Primary outcome was “Knee Injury and Osteoarthritis Outcome Score” (KOOS)4. X-ray/3T-MRI knees were taken at baseline and two years. Linear and logistic regression models adjusting for predefined covariates assessed associations with 2year KOOS4 and secondary endpoints including new symptomatic (regular knee symptoms), tibio-femoral radiographic OA (TFROA, Kellgren Lawrence Grade 2 or more on an X-ray) respectively. Findings: Baseline KOOS4, medium/large knee effusion and moderate/severe SF blood staining and their interaction significantly predicted 2year KOOS4 (Coeff. -20·5 [95% confidence interval -34·8, -6·18]. Of the predefined markers, only sfMCP-1 and sfIL-6 -showed independent associations with 2year KOOS4 (-0.015[0.027,-0.004] and -0.0005[-0.0009,-0.0001] per change in 1 pg/ml units respectively), jointly with the interaction of effusion and blood staining accounting for 39% of outcome variability. New TFROA at two years was associated with baseline meniscal tear (OR5·7[1·25,25·92]). 13/22(59·1%) with new TFROA had no NHANES frequent knee symptoms. Only 3month medium/large effusion was associated with new symptomatic TFROA at two years (OR14·0[1·86,105·27]). No sf/blood markers were associated with predefined structural/symptomatic outcomes. Interpretation: Effusion-haemarthrosis was strongly associated with symptomatic outcomes after acute knee injury. The SF molecular protein response to acute knee injury (best represented by MCP-1 and IL-6) was independently associated with symptomatic but not with structural outcomes, with the biomarkers overall playing a minor role relative to clinical predictors. The relationship between symptoms and structure after acute knee injury and their apparent dissociation early in this process needs to be better understood to make clinical progress.
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- 2021
6. Longitudinal study of thyroid function in Down's syndrome in the first two decades
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Gibson, P.A., Newton, R.W., Selby, K., Price, D.A., Leyland, K., and Addison, G.M.
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Down syndrome -- Complications and side effects ,Thyroid gland -- Research - Published
- 2005
7. The natural history of radiographic knee osteoarthritis: A fourteen-year population-based cohort study
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Leyland, K. M., Hart, D. J., Javaid, M. K., Judge, A., Kiran, A., Soni, A., Goulston, L. M., Cooper, C., Spector, T. D., and Arden, N. K.
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- 2012
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8. Prevalence of reported knee pain over twelve years in a community-based cohort
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Soni, A., Kiran, A., Hart, D. J., Leyland, K. M., Goulston, L., Cooper, C., Javaid, M. K., Spector, T. D., and Arden, N. K.
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- 2012
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9. Predictive factors for patient reported symptoms and radiographic structural change at 2 years after acute knee injury
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Garriga, C., primary, Goff, M., additional, Leyland, K., additional, Paterson, E., additional, Hrusecka, R., additional, Hamid, B., additional, Honeyfield, L., additional, Satchithananda, K., additional, Lim, A., additional, Arden, N.K., additional, Judge, A., additional, Williams, A., additional, Vincent, T.L., additional, and Watt, F.E., additional
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- 2020
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10. The measurement of charge transfer cross-sections
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Leyland, K. S.
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539.6 - Published
- 1978
11. The prevalence of hand and wrist osteoarthritis in elite former cricket and rugby union players
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Jones, M, Davies, M, Shah, K, Kemp, S, Peirce, N, Leyland, K, Stokes, K, Judge, A, Newton, J, Furniss, D, and Arden, N
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Aging ,Athlete ,Epidemiology ,Prevalence ,Injury ,human activities - Abstract
Objectives: This study aimed to determine the prevalence of hand and wrist osteoarthritis in former elite cricket and rugby union players, by sport and playing position, and to define the prevalence of severe hand injury, and its association with hand osteoarthritis.Design: Cross-sectionalMethods: Data from cross-sectional studies of former elite male cricket and rugby players were used to determine the prevalence of hand pain, physician-diagnosed osteoarthritis, and previous severe injury. Multivariable logistic regression was used to determine the association of previous injury with pain and osteoarthritis.Results: Data from 200 cricketers and 229 rugby players were available. Complete case analysis resulted in 127 cricketers and 140 rugby players. Hand pain was more prevalent amongst cricketers (19.7%) than rugby players (10.0%). The prevalence did not differ between cricket and rugby players for hand osteoarthritis (2.4% and 3.6%), wrist osteoarthritis (1.6% and 2.1%), or previous severe hand injury (36.2% and 31.4%). No significant association between previous hand injury and pain or osteoarthritis was identified in either sport. Conclusions: Former elite cricketers reported more hand pain than rugby players. No significant association was found between self-reported severe injury and hand osteoarthritis in either cohort, potentially indicating that risk factors aside from injury may be more prominent in the development of hand osteoarthritis.
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- 2019
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12. The presence of blood in the joint and the immediate molecular response in synovial fluid are independently associated with worse clinical outcomes at 2 years after human knee injury
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Garriga, C, Goff, M, Leyland, K, Paterson, E, Hrusecka, R, Hamid, B, Honeyfield, L, Satchithananda, K, Lim, A, Arden, N, Judge, A, Williams, A, Vincent, T, and Watt, F
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- 2019
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13. Novel Approach to Estimate Osteoarthritis Progression: Use of the Reliable Change Index in the Evaluation of Joint Space Loss
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Parsons, C.M., Judge, A., Leyland, K., Bruyere, O., Dop, F. Petit, Chapurlat, R., Reginster, J.Y., Edwards, M.H., Dennison, E.M., Riel, P.L.C.M. van, Cooper, C., Inskip, H., Parsons, C.M., Judge, A., Leyland, K., Bruyere, O., Dop, F. Petit, Chapurlat, R., Reginster, J.Y., Edwards, M.H., Dennison, E.M., Riel, P.L.C.M. van, Cooper, C., and Inskip, H.
- Abstract
Contains fulltext : 202254.pdf (publisher's version ) (Closed access), OBJECTIVE: Osteoarthritis-related changes in joint space measurements over time are small and sensitive to measurement error. The Reliable Change Index (RCI) determines whether the magnitude of change observed in an individual can be attributed to true change. This study aimed to examine the RCI as a novel approach to estimating osteoarthritis progression. METHODS: Data were from 167 men and 392 women with knee osteoarthritis (diagnosed using the American College of Rheumatology criteria) randomized to the placebo arm of the 3-year Strontium Ranelate Efficacy in Knee Osteoarthritis trial (SEKOIA) and assessed annually. The RCI was used to determine whether the magnitude of change in joint space width (JSW) on radiographs between study years was likely to be true or due to measurement error. RESULTS: Between consecutive years, 57-69% of participants had an apparent decrease (change <0) in JSW, while 31-43% of participants had annual changes indicating improvement in JSW. The RCI identified JSW decreases in only 6.0% of patients between baseline and year 1, and in 4.5% of patients between the remaining study years. The apparent increases in JSW were almost eliminated between baseline and year 1, and between years 1 and 2 only 1.3% of patients had a significant increase, dropping to 0.9% between years 2 and 3. CONCLUSION: The RCI provides a method to identify change in JSW, removing many apparent changes that are likely to be due to measurement error. This method appears to be useful for assessing change in JSW from radiographs in clinical and research settings.
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- 2019
14. School based screening for hypothyroidism in Down's syndrome by dried blood spot TSH measurement
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Noble, S E, Leyland, K, Findlay, C A, Clark, C E, Redfern, J, Mackenzie, J M, Girdwood, R W A, and Donaldson, M D C
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- 2000
15. The association of knee osteoarthritis and premature mortality in the community: an international individual patient level meta-analysis in six prospective cohorts
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Leyland, K, Gates, L, Sanchez-Santos, M, Prieto-Alhambra, D, Judge, A, Collins, G, Cleveland, R, Felson, D, Jordan, J, Callahan, L, Nevitt, M, Hosnijeh, F, Van Meurs, J, Jones, G, Newton, J, Batt, M, Altman, D, Cooper, C, and Arden, N
- Abstract
To combine individual participant data (IPD) from major international population-based cohorts, using harmonised OA data, to assess whether subjects with knee OA have an increased association with premature mortality.
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- 2018
16. Reply; in response to Yang, Tuo et al. 'Was the effect of obesity on the relative risk of replacement surgery in knee osteoarthritis patients overestimated?'
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Leyland, K, Arden, N, and Prieto-Alhambra, D
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- 2016
17. The association between radiographic knee osteoarthritis and pain: an epidemiological analysis of a twenty-year community-based cohort
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Leyland, K, Arden, N, Javaid, M, Judge, A, Arden, N, Javaid, M, and Judge, A
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Musculoskeletal system--Diseases--Epidemiology - Abstract
Background: Knee osteoarthritis (OA) is one of the leading musculoskeletal burdens in the world, causing both structural damage and pain to the joint. Radiographs are the most common imaging method for diagnosing OA, however the relationship between radiographic changes (ROA) and symptoms is not well understood. This thesis will establish the natural history of twenty-year ROA, compare diagnostic methods of ROA assessment, evaluate the cross-sectional relationship between ROA and pain, and will determine the long-term predictive validity of features of ROA with future knee replacements (TKRs). Methods: Data from the Chingford women's study, a twenty-year prospective UK-based cohort was used for the analysis. Risk factors included atlas-based ROA scoring methods and quantitative joint space width (JSW), which were analysed against pain and TKR outcome measures. A novel method for assessing joint space on low-contrast x-rays was developed which had high reproducibility and validity. Results: The twenty-year natural history of ROA showed relatively low levels of annual incidence (3.8%), progression (3.6%), and worsening (4.5%), and emphasised the involvement of both medial and lateral osteophytes. Severe joint space narrowing (JSN) had the best construct validity with pain, while any size of lateral tibial osteophyte had good construct validity. Medial quantitative JSW had good construct validity, but no predictive validity with future TKRs. Lateral JSN and osteophytes had the best predictive validity for future TKR. Conclusion: This research demonstrates that radiographic scoring methods have strong construct and predictive validity with symptomatic knee OA. These results support the use of x-rays to identify early disease changes which indicate future joint failure.
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- 2016
18. Obesity and the relative risk of replacement surgery in knee osteoarthritis patients: A prospective cohort study
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Leyland, K, Judge, A, Diez-Perez, A, Carr, A, Cooper, C, Arden, N, Prieto-Alhambra, D, and Javaid, M
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Objective: It is unclear what the impact of obesity has on the progression of knee osteoarthritis (KOA), from diagnosis to knee replacement (KR) surgery. This research examines the relative risk of KR surgery in overweight/obese patients with newly diagnosed knee osteoarthritis in a community population. Methods: Subjects were selected from the SIDIAP database, which compiles comprehensive clinical information collected by healthcare professionals for 80% of the population of Catalonia, Spain (>5.5 million people). Patients newly diagnosed with KOA in primary care between 2006 and 2011 were included. KR was ascertained using ICD-9-CM codes from linked hospital admissions data. Multivariable Cox regression models were fitted for KR according to BMI, and were adjusted for relevant confounders. Population proportional attributable risk was calculated. Results: 105,189 participants were followed up for a median (inter-quartile range) of 2.6 (1.3-4.2) years. 7,512 (7.1%) patients underwent KR. Adjusted HRs for KR were: 1.41 (95% CI 1.27 to 1.57) for overweight, 1.97 (1.78 to 2.18) for obese I, 2.39 (2.15 to 2.67) for obese II, and 2.67 (2.34 to 3.04) for obese III compared to normal-weight. The effect of BMI on risk of KR was stronger amongst younger participants. The population attributable risk of obesity for KOA-related KR is 31.0%. Conclusion: Overweight and obese patients are at over 40% and 100% increased risk of KR surgery compared to normal-weight respectively. This association is even stronger in younger patients. Weight reduction strategies could potentially reduce the need for KR surgery by 31% amongst KOA patients. This article is protected by copyright. All rights reserved.
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- 2015
19. THE INFLUENCE OF OVERWEIGHT/OBESITY ON THE RISK OF TOTAL KNEE ARTHROPLASTY AMONGST PATIENTS WITH NEWLY DIAGNOSED KNEE OSTEOARTHRITIS: A POPULATION-BASED COHORT STUDY
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Prieto-Alhambra, D, Leyland, K, Judge, A, Javaid, M, Cooper, C, and Arden, N
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- 2013
20. A COMPARISON OF FOUR RADIOGRAPHIC SCORING METHODS FOR KNEE OSTEOARTHRITIS - SHORT AND MEDIUM TERM REPRODUCIBILITY
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Leyland, K, Bottomley, N, Judge, A, Spector, T, Hart, D, Javaid, M, and Arden, K
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- 2011
21. Painful knee but not hand osteoarthritis is an independent predictor of mortality over 23 years follow-up of a population-based cohort of middle-aged women
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Kluzek, S, primary, Sanchez-Santos, M T, additional, Leyland, K M, additional, Judge, A, additional, Spector, T D, additional, Hart, D, additional, Cooper, C, additional, Newton, J, additional, and Arden, N K, additional
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- 2015
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22. Higher serum levels of cartilage oligomeric matrix protein (comp) are associated with self-reported knee pain
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Kluzek, S., primary, Bay-Jensen, A-C., additional, Spector, T., additional, Hart, D., additional, Leyland, K., additional, Sanchez-Santos, M., additional, Arden, N., additional, and Newton, J., additional
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- 2014
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23. Pragmatic approach to quantitative sensory testing in knee osteoarthritis: measures of mechanical pain sensitivity predict concordant pain and structural status
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Soni, A., primary, Batra, R., additional, Leyland, K., additional, Gwylim, S., additional, Spector, T., additional, Hart, D., additional, Arden, N., additional, Cooper, C., additional, Tracey, I., additional, and Javaid, M., additional
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- 2014
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24. THU0520 The Influence of Overweight/Obesity on the Risk of Total Knee Arthroplasty amongst Patients with Newly Diagnosed Knee Osteoarthritis: A Population-Based Cohort Study
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Prieto-Alhambra, D., primary, Leyland, K., additional, Judge, A., additional, Javaid, M. K., additional, Cooper, C., additional, and Arden, N. K., additional
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- 2013
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25. Basic Science * 208. Stem Cell Factor Expression is Increased in the Skin of Patients with Systemic Sclerosis and Promotes Proliferation and Migration of Fibroblasts in vitro
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Karrar, S., primary, Shiwen, X., additional, Nikotorowicz-Buniak, J., additional, Abraham, D. J., additional, Denton, C., additional, Stratton, R., additional, Bayley, R., additional, Kite, K. A., additional, Clay, E., additional, Smith, J. P., additional, Kitas, G. D., additional, Buckley, C., additional, Young, S. P., additional, Ye, L., additional, Zhang, L., additional, Goodall, J., additional, Gaston, H., additional, Xu, H., additional, Lutalo, P. M., additional, Zhao, Y., additional, Meng Choong, L., additional, Sangle, S., additional, Spencer, J., additional, D'Cruz, D., additional, Rysnik, O. J., additional, McHugh, K., additional, Bowness, P., additional, Rump-Goodrich, L., additional, Mattey, D., additional, Kehoe, O., additional, Middleton, J., additional, Cartwright, A., additional, Schmutz, C., additional, Askari, A., additional, Gardner, D. H., additional, Jeffery, L. E., additional, Raza, K., additional, Sansom, D. M., additional, Fitzpatrick, M., additional, Wallace, G., additional, Young, S., additional, Shaw, J., additional, Hatano, H., additional, Cauli, A., additional, Giles, J. L., additional, Mathieu, A., additional, Kollnberger, S., additional, Webster, S., additional, Ellis, L., additional, O'Brien, L. M., additional, Fitzmaurice, T. J., additional, Nazeer Moideen, A., additional, Evans, L., additional, Osgood, L., additional, Williams, A., additional, Jones, S., additional, Thomas, C., additional, O'Donnell, V., additional, Nowell, M., additional, Ouboussad, L., additional, Savic, S., additional, Dickie, L. J., additional, Hintze, J., additional, Wong, C. H., additional, Cook, G. P., additional, Buch, M., additional, Emery, P., additional, McDermott, M. F., additional, Hardcastle, S. A., additional, Gregson, C. L., additional, Deere, K., additional, Davey Smith, G., additional, Dieppe, P., additional, Tobias, J. H., additional, Dennison, E., additional, Edwards, M., additional, Bennett, J., additional, Coggon, D., additional, Palmer, K., additional, Cooper, C., additional, McWilliams, D., additional, Young, A., additional, Kiely, P. D., additional, Walsh, D., additional, Taylor, H. J., additional, Harding, I., additional, Hutchinson, J., additional, Nelson, I., additional, Blom, A., additional, Tobias, J., additional, Clark, E., additional, Parker, J., additional, Bukhari, M., additional, Jayakumar, K., additional, Kiely, P., additional, Diffin, J., additional, Lunt, M., additional, Marshall, T., additional, Chipping, J., additional, Symmons, D., additional, Verstappen, S., additional, Bluett, J., additional, Bowes, J., additional, Ho, P., additional, McHugh, N., additional, Buden, D., additional, Fitzgerald, O., additional, Barton, A., additional, Glossop, J. R., additional, Nixon, N. B., additional, Emes, R. D., additional, Dawes, P. T., additional, Farrell, W. E., additional, Mattey, D. L., additional, Scott, I. C., additional, Steer, S., additional, Seegobin, S., additional, Hinks, A. M., additional, Eyre, S., additional, Morgan, A., additional, Wilson, A. G., additional, Hocking, L., additional, Wordsworth, P., additional, Worthington, J., additional, Cope, A., additional, Lewis, C. M., additional, Guerra, S., additional, Ahmed, B. A., additional, Abraham, D., additional, Fonseca, C., additional, Robinson, J., additional, Taylor, J., additional, Haroon Rashid, L., additional, Flynn, E., additional, Isaacs, J., additional, Barrett, J. H., additional, Kingston, B., additional, Ahmed, M., additional, Kirwan, J. R., additional, Marshall, R., additional, Chapman, K., additional, Pearson, R., additional, Heycock, C., additional, Kelly, C., additional, Rynne, M., additional, Saravanan, V., additional, Hamilton, J., additional, Saeed, A., additional, Coughlan, R., additional, Carey, J. J., additional, Farah, Z., additional, Matthews, W., additional, Bell, C., additional, Petford, S., additional, Tibbetts, L.-M., additional, Douglas, K. M. J., additional, Holden, W., additional, Ledingham, J., additional, Fletcher, M., additional, Winfield, R., additional, Price, Z., additional, Mackay, K., additional, Dixon, C., additional, Oppong, R., additional, Jowett, S., additional, Nicholls, E., additional, Whitehurst, D., additional, Hill, S., additional, Hammond, A., additional, Hay, E., additional, Dziedzic, K., additional, Righetti, C., additional, Lebmeier, M., additional, Manning, V. L., additional, Hurley, M., additional, Scott, D. L., additional, Choy, E., additional, Bearne, L., additional, Nikiphorou, E., additional, Morris, S., additional, James, D., additional, Wong, E. C., additional, Long, J., additional, Fletcher, A., additional, Holmes, S., additional, Hockey, P., additional, Abbas, M., additional, Chattopadhyay, C., additional, Flint, J., additional, Gayed, M., additional, Schreiber, K., additional, Arthanari, S., additional, Nisar, M., additional, Khamashta, M., additional, Gordon, C., additional, Giles, I., additional, Robson, J., additional, Kiran, A., additional, Maskell, J., additional, Arden, N., additional, Hutchings, A., additional, Emin, A., additional, Culliford, D., additional, Dasgupta, B., additional, Hamilton, W., additional, Luqmani, R., additional, Jethwa, H., additional, Rowczenio, D., additional, Trojer, H., additional, Russell, T., additional, Loeffler, J., additional, Hawkins, P., additional, Lachmann, H., additional, Verma, I., additional, Syngle, A., additional, Krishan, P., additional, Garg, N., additional, McGowan, S. P., additional, Gerrard, D. T., additional, Chinoy, H., additional, Ollier, W. E., additional, Cooper, R. G., additional, Lamb, J. A., additional, Taborda, L., additional, Correia Azevedo, P., additional, Isenberg, D., additional, Leyland, K. M., additional, Judge, A., additional, Hunter, D., additional, Hart, D., additional, Javaid, M. K., additional, Edwards, M. H., additional, Litwic, A. E., additional, Jameson, K. A., additional, Deeg, D., additional, Cushnaghan, J., additional, Aihie Sayer, A., additional, Jagannath, D., additional, Parsons, C., additional, Stoppiello, L., additional, Mapp, P., additional, Ashraf, S., additional, Wilson, D., additional, Hill, R., additional, Scammell, B., additional, Wenham, C., additional, Shore, P., additional, Hodgson, R., additional, Grainger, A., additional, Aaron, J., additional, Hordon, L., additional, Conaghan, P., additional, Bar-Ziv, Y., additional, Beer, Y., additional, Ran, Y., additional, Benedict, S., additional, Halperin, N., additional, Drexler, M., additional, Mor, A., additional, Segal, G., additional, Lahad, A., additional, Haim, A., additional, Rath, U., additional, Morgensteren, D. M., additional, Salai, M., additional, Elbaz, A., additional, Vasishta, V. G., additional, Derrett-Smith, E., additional, Hoyles, R., additional, Khan, K., additional, Ezeonyeji, A., additional, Takhar, G., additional, Ong, V., additional, Loughrey, L., additional, Bissell, L.-A., additional, Hensor, E., additional, Abignano, G., additional, Redmond, A., additional, Del Galdo, F., additional, Hall, F. C., additional, Malaviya, A., additional, Baker, S., additional, Furlong, A., additional, Mitchell, A., additional, Godfrey, A. L., additional, Ruddlesden, M., additional, Hadjinicolaou, A., additional, Hughes, M., additional, Moore, T., additional, O'Leary, N., additional, Tracey, A., additional, Ennis, H., additional, Dinsdale, G., additional, Roberts, C., additional, Herrick, A., additional, Denton, C. P., additional, Guillevin, L., additional, Hunsche, E., additional, Rosenberg, D., additional, Schwierin, B., additional, Scott, M., additional, Krieg, T., additional, Anderson, M., additional, Matucci-Cerinic, M., additional, Alade, R., additional, Xu, S., additional, Nihtyanova, S., additional, Clark, K. E., additional, Tam, F. W. K., additional, Unwin, R., additional, Stratton, R. J., additional, Schreiber, B., additional, Seng Edwin Lim, C., additional, Corsiero, E., additional, Sutcliffe, N., additional, Wardemann, H., additional, Pitzalis, C., additional, Bombardieri, M., additional, Tahir, H., additional, Donnelly, S., additional, Greenwood, M., additional, Smith, T. O., additional, Easton, V., additional, Bacon, H., additional, Jerman, E., additional, Armon, K., additional, Poland, F., additional, Macgregor, A., additional, van der Heijde, D., additional, Sieper, J., additional, Elewaut, D., additional, Pangan, A. L., additional, Nguyen, D., additional, Badenhorst, C., additional, Kirby, S., additional, White, D., additional, Harrison, A., additional, Garcia, J. A., additional, Stebbings, S., additional, MacKay, J. W., additional, Aboelmagd, S., additional, Gaffney, K., additional, Deodhar, A., additional, Braun, J., additional, Mack, M., additional, Hsu, B., additional, Gathany, T., additional, Han, C., additional, Inman, R. D., additional, Cooper-Moss, N., additional, Packham, J., additional, Strauss, V., additional, Freeston, J. E., additional, Coates, L., additional, Nam, J., additional, Moverley, A. R., additional, Helliwell, P., additional, Wakefield, R., additional, Mease, P., additional, Fleischmann, R., additional, Wollenhaupt, J., additional, Kielar, D., additional, Woltering, F., additional, Stach, C., additional, Hoepken, B., additional, Arledge, T., additional, Gladman, D., additional, Coteur, G., additional, Kavanaugh, A., additional, Purcaru, O., additional, McInnes, I., additional, Gottlieb, A. B., additional, Puig, L., additional, Rahman, P., additional, Ritchlin, C., additional, Li, S., additional, Wang, Y., additional, Mendelsohn, A., additional, Doyle, M., additional, Tillett, W., additional, Jadon, D., additional, Shaddick, G., additional, Cavill, C., additional, Robinson, G., additional, Sengupta, R., additional, Korendowych, E., additional, de Vries, C., additional, Thomas, R. C., additional, Shuto, T., additional, Busquets-Perez, N., additional, Marzo-Ortega, H., additional, McGonagle, D., additional, Richards, G., additional, Bingham, S., additional, John Hamlin, P., additional, Adshead, R., additional, Cambridge, S., additional, Suppiah, P., additional, Cullinan, M., additional, Nolan, A., additional, Thompson, W. M., additional, Mathieson, H. R., additional, Mackie, S. L., additional, Bryer, D., additional, Krutikov, M., additional, Gray, L., additional, Bruce, E., additional, Keat, A., additional, Innes, W., additional, Pandit, R., additional, Kay, L., additional, Lapshina, S., additional, Myasoutova, L., additional, Erdes, S., additional, Wallis, D., additional, Waldron, N., additional, Thorne, I., additional, Harris, C., additional, Vohra, K., additional, Khinchi, D., additional, Kaur, L., additional, Jones, A., additional, Harrison, N., additional, Harris, D., additional, Jones, T., additional, Rees, J., additional, Bennett, A., additional, Fazal, S., additional, Tugnet, N., additional, Barkham, N., additional, Basu, N., additional, McClean, A., additional, Harper, L., additional, Amft, E. N., additional, Dhaun, N., additional, Luqmani, R. A., additional, Little, M. A., additional, Jayne, D. R., additional, Flossmann, O., additional, McLaren, J., additional, Kumar, V., additional, Reid, D. M., additional, Macfarlane, G. J., additional, Jones, G., additional, Yates, M., additional, Watts, R. A., additional, Igali, L., additional, Mukhtyar, C., additional, Doll, H., additional, Yew, S., additional, Suppiah, R., additional, Hoglund, P., additional, Jayne, D., additional, Westman, K., additional, Win Maw, W., additional, Patil, P., additional, Williams, M., additional, Adizie, T., additional, Christidis, D., additional, Borg, F., additional, Robertson, A., additional, Croft, A. P., additional, Smith, S., additional, Carr, S., additional, Youssouf, S., additional, Salama, A., additional, Pusey, C., additional, and Morgan, M., additional
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- 2013
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26. Painful knee but not hand osteoarthritis is an independent predictor of mortality over 23 years follow-up of a population-based cohort of middle-aged women.
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Kluzek, S., Sanchez-Santos, M. T., Leyland, K. M., Judge, A., Spector, T. D., Hart, D., Cooper, C., Newton, J., and Arden, N. K.
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CARDIOVASCULAR disease related mortality ,CAUSES of death ,HAND ,KNEE ,KNEE diseases ,LONGITUDINAL method ,OSTEOARTHRITIS ,RADIOGRAPHY ,TUMORS ,JOINT pain - Abstract
Unlabelled: To assess whether joint pain or radiographic osteoarthritis (ROA) of the knee and hand is associated with all-cause and disease-specific mortality in middle-aged women.Methods: Four subgroups from the prospective community-based Chingford Cohort Study were identified based on presence/absence of pain and ROA at baseline: (Pain-/ROA-; Pain+/ROA-; Pain-/ROA+; Pain+/ROA+). Pain was defined as side-specific pain in the preceding month, while side-specific ROA was defined as Kellgren-Lawrence grade ≥2. All-cause, cardiovascular disease (CVD) and cancer-related mortality over the 23-year follow-up was based on information collected by the Office for National Statistics. Associations between subgroups and all-cause/cause-specific mortality were assessed using Cox regression, adjusting for age, body mass index, typical cardiovascular risk factors, occupation, past physical activity, existing CVD disease, glucose levels and medication use.Results: 821 and 808 women were included for knee and hand analyses, respectively. Compared with the knee Pain-/ROA- group, the Pain+/ROA- group had an increased risk of CVD-specific mortality (HR 2.93 (95% CI 1.47 to 5.85)), while the knee Pain+/ROA+ group had an increased HR of 1.97 (95% CI 1.23 to 3.17) for all-cause and 3.57 (95% CI 1.53 to 8.34) for CVD-specific mortality. We found no association between hand OA and mortality.Conclusion: We found a significantly increased risk of all-cause and CVD-specific mortality in women experiencing knee pain with or without ROA but not ROA alone. No relationship was found between hand OA and mortality risk. This suggests that knee pain, more than structural changes of OA is the main driver of excess mortality in patients with OA. [ABSTRACT FROM AUTHOR]- Published
- 2016
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27. Tinkering at the edges : post-politics and the promulgation of National Planning Policy in New Zealand
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Leyland, Kate
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- 2022
28. 407 A COMPARISON OF FOUR RADIOGRAPHIC SCORING METHODS FOR KNEE OSTEOARTHRITIS – SHORT AND MEDIUM TERM REPRODUCIBILITY
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Leyland, K., primary, Bottomley, N., additional, Judge, A., additional, Spector, T., additional, Hart, D., additional, Javaid, M.K., additional, and Arden, N.K., additional
- Published
- 2011
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29. An inherited dystrophin deletion without muscle weakness.
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Collins, A L, primary, Leyland, K G, additional, Kennedy, C R, additional, Robinson, D, additional, and Spratt, H C, additional
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- 1994
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30. Capillary TSH screening programme for Down's syndrome in Scotland, 1997-2009.
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McGowan S, Jones J, Brown A, Reynolds L, Leyland K, Charleton P, Rahim M, Mansor M, Ritha S, Donaldson M, and Scottish Down Syndrome Thyroid Screening Group
- Abstract
OBJECTIVES: To assess uptake of community-based capillary thyroid stimulating hormone (TSH) screening in Scotland and determine the optimal frequency of screening, the justification for preschool screening and strategies for treatment. METHODS: Subjects with Down's syndrome aged 1-19 years underwent capillary TSH measurement. Clinical and biochemical data were collected using proformas. RESULTS: 5742 capillary TSH tests were performed on 1329 children in 1997-2009, increasing from 183 children from two health boards tested in 1997 to 630 from 13 health boards tested in 2009. Of 132 children referred by the screening laboratory with elevated capillary TSH, 98 (M:F ratio 1:1.2, median (range) age 8.9 (0.9-17.9) years) had adequate documentation and 76 had thyroid dysfunction (defined as venous TSH >6 mU/l), giving a prevalence of not less than 5.7%. Fifty-six (57%) had tested negative during the previous year, 8 (8%) tested positive on their first screening test and 23/67 (34%) were thyroid peroxidase autoantibody negative on initial venous blood. Two of the 13 (13%) preschool children were severely hypothyroid (venous TSH 71 and 283 mU/l). Of patients with venous TSH 6-10.9 (n=27), 11.0-20.9 (n=25) and >= 21.0 mU/l (n=24) following referral, initial/subsequent treatment with thyroxine was given in 3/8, 15/5 and 21/1, respectively. CONCLUSION: Capillary TSH screening in Down's syndrome is eminently feasible and should be performed annually from 1 year of age. Nearly all subjects with initial venous TSH >= 11.0 mU/l will require thyroxine treatment but most with TSH 6-10 mU/l only require surveillance initially. [ABSTRACT FROM AUTHOR]
- Published
- 2011
31. Medium-term neurological outcome in survivors of primary brain tumors in childhood
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Kennedy, C.R. and Leyland, K.
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Brain tumors -- Patient outcomes ,Tumors in children -- Patient outcomes ,Cancer survivors -- Research ,Business ,Health care industry - Abstract
AUTHORS: C.R. Kennedy and K. Leyland. Royal Marsden Hospital, London, United Kingdom. According to an abstract submitted by the authors to the 6th International Symposium on Pediatric Neuro -Oncology, held [...]
- Published
- 1994
32. P07 Splanchnic steal in patients with liver disease: a 3T MRI study of visceral blood flow.
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McAvoy, N, Leyland, K A, Richards, J M J, Semple, S I K, Patel, D, Newby, D E, and Hayes, P C
- Abstract
Introduction Liver cirrhosis and the development of portal hypertension is associated with significant morbidity and mortality. It is widely accepted that patients with liver disease have a hyperdynamic circulation that is associated with an increased cardiac output. We have previously proposed that, rather than a generalised systemic vasodilatation, there is selective splanchnic vasodilatation with concomitant vasoconstriction in other vascular beds: the so-called “splanchnic steal” phenomenon. Aim To measure regional visceral blood flow using 3T magnetic resonance imaging in patients with liver disease. Method Single centre pilot study of 19 subjects (10 healthy controls, nine patients with liver disease). Arterial and venous phase magnetic resonance angiograms were obtained using a Siemens 3T Verio MR scanner with gadolinium contrast. From these MRA's, ECG-gated phase contrast flow measurement MR data were then positioned and measured in the hepatic artery, portal vein, superior mesenteric artery, descending thoracic aorta, distal abdominal aorta, and the renal and carotid arteries. Results Mean MELD score in patient group was 14 (range 7–21) with a range of aetiologies: alcoholic (6), non-alcoholic fatty (1), autoimmune (1), hepatitis C virus (1). In comparison to controls, flow in the descending thoracic aorta was increased by 43% in patients with liver disease (4.74 vs 3.32 L/min; p=0.021) consistent with an increased cardiac output. Hepatic artery flow showed a trend towards increase in patients (0.47 vs 0.27 L/min; p=0.11) whereas portal vein flow decreased dramatically (0.20 vs 1.20 L/min; p=0.006). Overall, in patients with liver disease, there was a 46% reduction in total liver blood flow (0.67 vs 1.47 L/min; p=0.037) and a reversal of hepatic artery/portal vein flow ratio (4.15 vs 0.33 L/min; p=0.009). Although superior mesenteric artery flow was three times greater in patients (0.54 vs 0.15 L/min; p=0.001), renal blood flow showed a trend towards reduction of 32% (0.42 vs 0.62 L/min; p=0.053), no change in carotid blood flow (0.75 vs 0.62 L/min; p=0.129) and no change in inferior aortic flow (1.45 vs 1.12 L/min; p=0.28). Conclusion There are marked derangements in regional visceral blood flow in patients with liver cirrhosis. Our findings strongly support the splanchnic steal hypothesis that dysregulated splanchnic vasodilatation and porto-systemic shunting induce a high cardiac output state associated with extra-splanchnic vasoconstriction including the renal circulation. [ABSTRACT FROM PUBLISHER]
- Published
- 2010
33. Hyporesponsiveness to Erythropoiesis-Stimulating Agents in Dialysis-Dependent Patients with Anaemia of Chronic Kidney Disease: A Retrospective Observational Study.
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Atzinger C, Arens HJ, Neri L, Arkossy O, Garbelli M, Jiletcovici A, Snijder R, Leyland K, Khalife N, Ali M, and Feuersenger A
- Abstract
Introduction: Hyporesponsiveness to erythropoiesis-stimulating agents (ESAs) in patients with anaemia of chronic kidney disease may lead to increased ESA doses to achieve target haemoglobin levels; however, elevated doses may be associated with increased mortality. Furthermore, patients with hyporesponsiveness to ESAs have poorer clinical outcomes than those who respond well to ESAs. Incidence and clinical characteristics of patients with ESA hyporesponsiveness were explored in a real-world setting., Methods: This was a retrospective study of electronic medical records of adults with stage 5 chronic kidney disease receiving renal replacement therapy and ESA treatment, from 1 January 2015 to 31 December 2021. The primary objective was ESA hyporesponsiveness rate/1000 days, with a hyporesponsive event defined as ESA use at an elevated dose, according to National Institute for Health and Care Excellence (NICE) criteria. Other hyporesponsiveness definitions applied were erythropoietin resistance index-defined ESA hyporesponsiveness (ERI) Kidney Disease Improving Global Outcomes (KDIGO) and a clinical practicality algorithm., Results: In total, 85,259 patients were included in the analysis; 59.9% were male, median (interquartile range) ESA starting dose was 733.3 (400.0, 1200.0) IU/week and follow-up duration was 2.2 (1.0, 4.2) years. Incidence of ESA hyporesponsiveness varied when applying different definitions; NICE 0.05/1000 days (5.2% of patients), ERI 0.40/1000 days (40.7%), KDIGO 0.15/1000 days (15.4%), and clinical practicality algorithm 0.48/1000 days (47.9%). ESA doses remained higher in hyporesponsive versus responsive patients, yet haemoglobin levels were similar between groups., Conclusion: The results from this study, which applied multiple hyporesponsiveness definitions to a large, geographically diverse population of patients with anaemia of CKD, showed variation in ESA hyporesponsiveness incidence rates depending on definitions used and higher ESA doses in hyporesponsive versus responsive patients. These results underscore the need for individualised clinical assessment and thorough evaluation when considering ESA dose adjustments to reach haemoglobin targets. Graphical abstract available for this article., Trial Registration: NCT05530291., Competing Interests: Declarations. Conflict of Interest: Hans-Jürgen Aren, Luca Neri, Astrid Feuersenger, Mario Garbelli and Otto Arkossy are employees of Fresenius Medical Care, contracted by Astellas Pharma Global Development Inc. to conduct the study. Hans-Jürgen Aren reports Fresenius Medical Care stock shares. Christopher Atzinger and Alina Jiletcovici are employees of Astellas Pharma Global Development Inc. Alina Jiletcovici reports Eli Lilly stock shares. Robert Snijder is an employee of Astellas Pharma Europe B.V. Kirsten Leyland, Najib Khalife and Mahmood Ali are employees of Astellas Pharma Europe Ltd. Ethical Approval: All data were pseudonymised and all patients provided written informed consent for access and secondary use of their pseudonymised clinical data for research purposes. According to the National Institutes of Health definition of human subject research, this study falls under the exempt human subjects research category [27]., (© 2024. The Author(s).)
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- 2024
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34. Clinical and molecular associations with outcomes at 2 years after acute knee injury: a longitudinal study in the Knee Injury Cohort at the Kennedy (KICK).
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Garriga C, Goff M, Paterson E, Hrusecka R, Hamid B, Alderson J, Leyland K, Honeyfield L, Greenshields L, Satchithananda K, Lim A, Arden NK, Judge A, Williams A, Vincent TL, and Watt FE
- Abstract
Background: Joint injury is a major risk factor for osteoarthritis and provides an opportunity to prospectively examine early processes associated with osteoarthritis. We investigated whether predefined baseline demographic and clinical factors, and protein analytes in knee synovial fluid and in plasma or serum, were associated with clinically relevant outcomes at 2 years after knee injury., Methods: This longitudinal cohort study recruited individuals aged 16-50 years between Nov 1, 2010, and Nov 28, 2014, across six hospitals and clinics in London, UK. Participants were recruited within 8 weeks of having a clinically significant acute knee injury (effusion and structural injury on MRI), which was typically treated surgically. We measured several predefined clinical variables at baseline (eg, time from injury to sampling, extent and type of joint injury, synovial fluid blood staining, presence of effusion, self-reported sex, age, and BMI), and measured 12 synovial fluid and four plasma or serum biomarkers by immunoassay at baseline and 3 months. The primary outcome was Knee Injury and Osteoarthritis Outcome Score (KOOS
4 ) at 2 years, adjusted for baseline score, assessed in all patients. Linear and logistic regression models adjusting for predefined covariates were used to assess associations between baseline variables and 2-year KOOS4 . This study is registered with ClinicalTrials.gov, number NCT02667756., Findings: We enrolled 150 patients at a median of 17 days (range 1-59, IQR 9-26) after knee injury. 123 (82%) were male, with a median age of 25 years (range 16-50, IQR 21-30). 98 (65%) of 150 participants completed a KOOS4 at 2 (or 3) years after enrolment (50 participants were lost to follow-up and two were withdrawn due to adverse events unrelated to study participation); 77 (51%) participants had all necessary variables available and were included in the core variable adjusted analysis. In the 2-year dataset mean KOOS4 improved from 38 (SD 18) at baseline to 79 (18) at 2 years. Baseline KOOS4, medium-to-large knee effusion, and moderate-to-severe synovial blood staining and their interaction significantly predicted 2-year KOOS4 (n=77; coefficient -20·5, 95% CI -34·8 to -6·18; p=0·0060). The only predefined biomarkers that showed independent associations with 2-year KOOS4 were synovial fluid MCP-1 (n=77; -0·015, 0·027 to -0·004 per change in 1 pg/mL units; p=0·011) and IL-6 (n=77; -0·0005, -0·0009 to -0·0001 per change in 1 pg/mL units; p=0·017). These biomarkers, combined with the interaction of effusion and blood staining, accounted for 39% of outcome variability. Two adverse events occurred that were linked to study participation, both at the time of blood sampling (one presyncopal episode, one tenderness and pain at the site of venepuncture)., Interpretation: The combination of effusion and haemarthrosis was significantly associated with symptomatic outcomes after acute knee injury. The synovial fluid molecular protein response to acute knee injury (best represented by MCP-1 and IL-6) was independently associated with symptomatic outcomes but not with structural outcomes, with the biomarkers overall playing a minor role relative to clinical predictors. The relationship between symptoms and structure after acute knee injury and their apparent dissociation early in this process need to be better understood to make clinical progress., Funding: Versus Arthritis, Kennedy Trust for Rheumatology Research, and NIHR Oxford Biomedical Research Centre., Competing Interests: TLV reports consultancy fees from GlaxoSmithKline, UCB, and Mundipharma and has also received research grants from Galapagos, Fidia, and Samumed. NKA reports consultancy fees from Pfizer/Lilly and received a grant in a related area of research from Merck. AJ reports consultancy fees from Freshfields Bruckhaus Deringer and from Anthera Pharmaceuticals. AW is a board member and holds stock in Fortius Clinic, has received research grants from Smith and Nephew, is a board member and shareholder in Innovate Orthopaedics, and a shareholder in DocComs. FEW has received clinical study grants from Pfizer and Astellas Pharma, reports consultancy fees from Pfizer, and is part of a consortium receiving some of its research funding from Galapagos, Fidia, and Samumed. All other authors report no competing interests., (© 2021 The Authors. Published by Elsevier Ltd. This is an Open Access article under the CC BY-NC-ND 4.0 license.)- Published
- 2021
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35. Differences between race and sex in measures of hip morphology: a population-based comparative study.
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Edwards K, Leyland KM, Sanchez-Santos MT, Arden CP, Spector TD, Nelson AE, Jordan JM, Nevitt M, Hunter DJ, and Arden NK
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- Acetabulum anatomy & histology, Black or African American, Aged, Asian People, Female, Femur Head anatomy & histology, Femur Neck anatomy & histology, Hip Joint anatomy & histology, Humans, Male, Middle Aged, Osteoarthritis, Hip epidemiology, Radiography, Sex Factors, White People, Acetabulum diagnostic imaging, Femur Head diagnostic imaging, Femur Neck diagnostic imaging, Hip Joint diagnostic imaging, Osteoarthritis, Hip ethnology
- Abstract
Objective: This paper aims to (i) identify differences in measures of hip morphology between four racial groups using anteroposterior (AP) hip x-rays, and (ii) examine whether these differences vary by sex., Methods: 912 hip x-rays (456 individuals) from four racial groups (European Caucasians, American Caucasians, African Americans and Chinese) were obtained. Males and females (45-75 years) with no radiographic hip OA (Kellgren and Lawrence < Grade 2 or Croft < Grade 1) were included. Eleven features of hip joint morphology were analysed. Linear regression with generalised estimating equations (GEE) was used to determine race and sex differences in hip morphology. Post-hoc Bonferroni procedure was used to adjust for multiple comparisons., Results: The final analysis included 875 hips. Chinese hips showed significant differences for the majority of measures to other racial groups. Chinese were characterised by more shallow and narrow acetabular sockets, reduced femoral head coverage, smaller femoral head diameter, and a lesser angle of alignment between the femoral neck and shaft. Variation was found between other racial groups, but with few statistically significant differences. The average of lateral centre edge angle, minimum neck width and neck length differed between race and sex (p-value for interaction < 0.05)., Conclusions: Significant differences were found in measures of morphology between Chinese hips compared to African Americans or Caucasian groups; these may explain variation in hip OA prevalence rates between these groups and the lower rate of hip OA in Chinese. Sex differences were also identified, which may further explain male-female prevalence differences for OA., (Copyright © 2019 The Authors. Published by Elsevier Ltd.. All rights reserved.)
- Published
- 2020
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36. Novel Approach to Estimate Osteoarthritis Progression: Use of the Reliable Change Index in the Evaluation of Joint Space Loss.
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Parsons CM, Judge A, Leyland K, Bruyère O, Petit Dop F, Chapurlat R, Reginster JY, Edwards MH, Dennison EM, Cooper C, and Inskip H
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- Aged, Female, Humans, Male, Middle Aged, Osteoarthritis, Knee drug therapy, Osteoarthritis, Knee epidemiology, Reproducibility of Results, Bone Density Conservation Agents therapeutic use, Disease Progression, Knee Joint diagnostic imaging, Osteoarthritis, Knee diagnostic imaging, Severity of Illness Index, Thiophenes therapeutic use
- Abstract
Objective: Osteoarthritis-related changes in joint space measurements over time are small and sensitive to measurement error. The Reliable Change Index (RCI) determines whether the magnitude of change observed in an individual can be attributed to true change. This study aimed to examine the RCI as a novel approach to estimating osteoarthritis progression., Methods: Data were from 167 men and 392 women with knee osteoarthritis (diagnosed using the American College of Rheumatology criteria) randomized to the placebo arm of the 3-year Strontium Ranelate Efficacy in Knee Osteoarthritis trial (SEKOIA) and assessed annually. The RCI was used to determine whether the magnitude of change in joint space width (JSW) on radiographs between study years was likely to be true or due to measurement error., Results: Between consecutive years, 57-69% of participants had an apparent decrease (change <0) in JSW, while 31-43% of participants had annual changes indicating improvement in JSW. The RCI identified JSW decreases in only 6.0% of patients between baseline and year 1, and in 4.5% of patients between the remaining study years. The apparent increases in JSW were almost eliminated between baseline and year 1, and between years 1 and 2 only 1.3% of patients had a significant increase, dropping to 0.9% between years 2 and 3., Conclusion: The RCI provides a method to identify change in JSW, removing many apparent changes that are likely to be due to measurement error. This method appears to be useful for assessing change in JSW from radiographs in clinical and research settings., (© 2018, American College of Rheumatology.)
- Published
- 2019
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37. Harmonising measures of knee and hip osteoarthritis in population-based cohort studies: an international study.
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Leyland KM, Gates LS, Nevitt M, Felson D, Bierma-Zeinstra SM, Conaghan PG, Engebretsen L, Hochberg M, Hunter DJ, Jones G, Jordan JM, Judge A, Lohmander LS, Roos EM, Sanchez-Santos MT, Yoshimura N, van Meurs JBJ, Batt ME, Newton J, Cooper C, and Arden NK
- Subjects
- Aged, Canada, Cohort Studies, Consensus, Disability Evaluation, Disease Progression, Female, Follow-Up Studies, Humans, Internationality, Magnetic Resonance Imaging methods, Male, Middle Aged, Osteoarthritis, Hip pathology, Osteoarthritis, Knee diagnostic imaging, Osteoarthritis, Knee pathology, Severity of Illness Index, Time Factors, Tomography, X-Ray Computed methods, Osteoarthritis, Hip diagnostic imaging, Osteoarthritis, Hip physiopathology, Osteoarthritis, Knee physiopathology, Pain Measurement, Range of Motion, Articular physiology
- Abstract
Objective: Population-based osteoarthritis (OA) cohorts provide vital data on risk factors and outcomes of OA, however the methods to define OA vary between cohorts. We aimed to provide recommendations for combining knee and hip OA data in extant and future population cohort studies, in order to facilitate informative individual participant level analyses., Method: International OA experts met to make recommendations on: 1) defining OA by X-ray and/or pain; 2) compare The National Health and Nutrition Examination Survey (NHANES)-type OA pain questions; 3) the comparability of the Western Ontario & McMaster Universities Osteoarthritis Index (WOMAC) scale to NHANES-type OA pain questions; 4) the best radiographic scoring method; 5) the usefulness of other OA outcome measures. Key issues were explored using new analyses in two population-based OA cohorts (Multicenter Osteoarthritis Study; MOST and Osteoarthritis Initiative OAI)., Results: OA should be defined by both symptoms and radiographs, with symptoms alone as a secondary definition. Kellgren and Lawrence (K/L) grade ≥2 should be used to define radiographic OA (ROA). The variable wording of pain questions can result in varying prevalence between 41.0% and 75.4%, however questions where the time anchor is similar have high sensitivity and specificity (91.2% and 89.9% respectively). A threshold of 3 on a 0-20 scale (95% CI 2.1, 3.9) in the WOMAC pain subscale demonstrated equivalence with the preferred NHANES-type question., Conclusion: This research provides recommendations, based on expert agreement, for harmonising and combining OA data in existing and future population-based cohorts., (Copyright © 2018. Published by Elsevier Ltd.)
- Published
- 2018
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38. A comparison of radiographic anatomic axis knee alignment measurements and cross-sectional associations with knee osteoarthritis.
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Goulston LM, Sanchez-Santos MT, D'Angelo S, Leyland KM, Hart DJ, Spector TD, Cooper C, Dennison EM, Hunter D, and Arden NK
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- Adult, Aged, Anatomic Landmarks pathology, Bone Malalignment diagnostic imaging, Bone Malalignment pathology, Female, Humans, Knee Joint diagnostic imaging, Middle Aged, Osteoarthritis, Knee diagnostic imaging, Osteoarthritis, Knee pathology, Pain etiology, Prospective Studies, Radiographic Image Interpretation, Computer-Assisted methods, Radiography methods, Reproducibility of Results, Bone Malalignment complications, Knee Joint pathology, Osteoarthritis, Knee etiology
- Abstract
Objective: Malalignment is associated with knee osteoarthritis (KOA), however, the optimal anatomic axis (AA) knee alignment measurement on a standard limb radiograph (SLR) is unknown. This study compares one-point (1P) and two-point (2P) AA methods using three knee joint centre locations and examines cross-sectional associations with symptomatic radiographic knee osteoarthritis (SRKOA), radiographic knee osteoarthritis (RKOA) and knee pain., Methods: AA alignment was measured six different ways using the KneeMorf software on 1058 SLRs from 584 women in the Chingford Study. Cross-sectional associations with principal outcome SRKOA combined with greatest reproducibility determined the optimal 1P and 2P AA method. Appropriate varus/neutral/valgus alignment categories were established using logistic regression with generalised estimating equation models fitted with restricted cubic spline function., Results: The tibial plateau centre displayed greatest reproducibility and associations with SRKOA. As mean 1P and 2P values differed by >2°, new alignment categories were generated for 1P: varus <178°, neutral 178-182°, valgus >182° and for 2P methods: varus <180°, neutral 180-185°, valgus >185°. Varus vs neutral alignment was associated with a near 2-fold increase in SRKOA and RKOA, and valgus vs neutral for RKOA using 2P method. Nonsignificant associations were seen for 1P method for SRKOA, RKOA and knee pain., Conclusions: AA alignment was associated with SRKOA and the tibial plateau centre had the strongest association. Differences in AA alignment when 1P vs 2P methods were compared indicated bespoke alignment categories were necessary. Further replication and validation with mechanical axis alignment comparison is required., (Crown Copyright © 2015. Published by Elsevier Ltd. All rights reserved.)
- Published
- 2016
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39. Measures of hip morphology are related to development of worsening radiographic hip osteoarthritis over 6 to 13 year follow-up: the Johnston County Osteoarthritis Project.
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Nelson AE, Stiller JL, Shi XA, Leyland KM, Renner JB, Schwartz TA, Arden NK, and Jordan JM
- Subjects
- Black or African American statistics & numerical data, Aged, Case-Control Studies, Disease Progression, Female, Femoracetabular Impingement complications, Femoracetabular Impingement diagnostic imaging, Femoracetabular Impingement ethnology, Follow-Up Studies, Hip Joint diagnostic imaging, Humans, Male, Middle Aged, Osteoarthritis, Hip ethnology, Osteoarthritis, Hip etiology, Radiography methods, Severity of Illness Index, Sex Factors, White People statistics & numerical data, Femoracetabular Impingement pathology, Hip Joint pathology, Osteoarthritis, Hip diagnostic imaging, Osteoarthritis, Hip pathology
- Abstract
Objectives: We sought to describe the effect of alterations in hip morphology with respect to worsening hip OA in a community-based sample including African American (AA) and white men and women., Methods: This nested case-control study defined case hips as Kellgren Lawrence grade (KLG) <3 on baseline supine pelvis radiographs and KLG ≥3 or THR for OA at the 1st or 2nd follow-up visit (mean 6 and 13 years, respectively); control hips had KLG <3 at both visits, with gender/race distribution similar to cases. Hip morphology was assessed using HipMorf software (Oxford, UK). Descriptive means and standard errors were obtained from generalized estimating equation (GEE) models. Sex-stratified GEE regression models (accounting for within-person correlation), adjusted for age, race, BMI, and side were then employed., Results: A total of 120 individuals (239 hips; 71 case/168 control) were included (25% male, 26% AA, mean age 62 years, BMI 30 kg/m(2)). Case hips tended to have greater baseline AP alpha angles, smaller minimum joint space width (mJSW) and more frequent triangular index signs. Adjusted results among men revealed that higher AP alpha angle, Gosvig ratio, and acetabular index were positively associated with case hips; coxa profunda was negatively associated. Among women, greater AP alpha angle, smaller mJSW, protrusio acetabuli, and triangular index sign were associated with case hips., Conclusions: We confirmed an increased risk of worsening hip OA due to baseline features of cam deformity among men and women, as well as protrusio acetabuli among women, and provide the first estimates of these measures in AAs., (Copyright © 2015 Osteoarthritis Research Society International. Published by Elsevier Ltd. All rights reserved.)
- Published
- 2016
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40. Screening for hypothyroidism in Down syndrome using the capillary thyroid stimulating hormone method.
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McGowan S, Jones J, McMillan D, McLaughlin K, Smith S, Leyland K, Charleton P, and Donaldson M
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- Adolescent, Child, Child, Preschool, Down Syndrome diagnosis, Down Syndrome epidemiology, Female, Follow-Up Studies, Humans, Hypothyroidism epidemiology, Hypothyroidism etiology, Incidence, Infant, Infant, Newborn, Male, Prevalence, Retrospective Studies, Scotland epidemiology, Down Syndrome complications, Hypothyroidism diagnosis, Neonatal Screening methods, Thyroid Function Tests methods, Thyrotropin blood
- Abstract
Objectives: To analyze data from the Scottish capillary thyroid stimulating hormone (TSH) screening program for hypothyroidism in Down syndrome to identify a threshold for capillary TSH elevation below which low venous free thyroxine (fT4) (<9 pmol/L) and/or frank venous TSH elevation (>10 mU/L) range is unlikely., Study Design: Review of proformas prospectively submitted on all children with Down syndrome referred via the screening program between 2003 and 2013., Results: Ninety-nine patients with Down syndrome (50 females, 49 males) were identified, 76 school-age (≥ 5 years) and 23 preschool (<5 years), mean (range) age at referral 9.4 (0.9-18.1) years. Pearson correlation between capillary TSH and venous TSH was 0.814; between capillary TSH and venous fT4 -0.522 (P = .01). Receiver operator curve analysis showed that capillary TSH values of 4 and 6 mU/L were 95.9% and 73.5% sensitive, 5.8% and 80.8% specific, respectively, in predicting venous TSH >10 mU/L. Fifty-three children had capillary TSH values of 4-5.9 mU/L of whom only one, a boy of 15.8 years, had subnormal venous fT4 (<9 pmol/L), and venous TSH >10 mU/L was found in 13 (4 preschool)., Conclusions: Venous fT4 is normal in almost all patients with Down syndrome with capillary TSH 4-6 mU/L. We propose an algorithm incorporating rescreening by finger prick after 6 months, rather than venepuncture, in school-aged children with borderline capillary TSH elevation. Further data are needed before this approach can be recommended for preschool children., (Copyright © 2015 Elsevier Inc. All rights reserved.)
- Published
- 2015
- Full Text
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41. Associations between body mass index and foot joint pain in middle-aged and older women: a longitudinal population-based cohort study.
- Author
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Gay A, Culliford D, Leyland K, Arden NK, and Bowen CJ
- Subjects
- Aged, Cohort Studies, Female, Humans, Longitudinal Studies, Middle Aged, Arthralgia physiopathology, Body Mass Index, Foot Joints physiopathology
- Abstract
Objective: To investigate the relationship between body mass index (BMI) and foot joint pain (FJP) over a 5-year period in a community-based cohort., Methods: We examined a subset of women from the Chingford Women's Study, a community cohort followed up for 20 years. From a baseline of 1,003 female participants, we reviewed data from 639 women (64%) for whom complete data sets for FJP and BMI were obtained over a 5-year period between year 10 (Y10) and year 15 (Y15). Descriptive statistics, binary regression modeling, and odds ratios (ORs) were used to examine the longitudinal relationship between BMI and FJP., Results: For Y10 and Y15, the median age was 61 years (interquartile range [IQR] 57-67) and 66 years (IQR 62-72), respectively, and the mean ± SD BMI was 26.7 ± 4.6 kg/m(2) and 27.2 ± 4.8 kg/m(2) , respectively. FJP prevalence was 21.6% at Y10 and 26.6% at Y15. Longitudinal analyses showed that both BMI and FJP increased significantly from Y10 to Y15 (P < 0.001). The odds of having FJP after a 5-year period increased by 4.9% for each BMI unit increase 5 years earlier (OR 1.049 [95% confidence interval (95% CI) 1.011-1.089], P = 0.012). This remained significant when adjusted for age, diabetes mellitus, and rheumatoid arthritis (OR 1.051 [95% CI 1.011-1.091], P = 0.012)., Conclusion: This is the first large longitudinal cohort study demonstrating that, in middle-aged women, a high BMI precedes and is predictive of FJP independent of age. Evidence from our findings can be used to identify those individuals at risk of developing FJP., (© 2014 The Authors. Arthritis Care & Research is published by Wiley Periodicals, Inc. on behalf of the American College of Rheumatology.)
- Published
- 2014
- Full Text
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42. Osteoarthritis year 2013 in review: clinical.
- Author
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Arden NK and Leyland KM
- Subjects
- Anti-Inflammatory Agents, Non-Steroidal therapeutic use, Arthroplasty, Replacement, Humans, Muscle Strength physiology, Obesity complications, Obesity epidemiology, Osteoarthritis etiology, Osteoarthritis therapy, Risk Factors, Treatment Outcome, Osteoarthritis epidemiology
- Abstract
Some major themes over the past year in clinical research of osteoarthritis (OA) include obesity, muscle strength, pain mechanisms, novel disease modifying drugs, and risk factors for poor outcomes of joint replacement surgery. A systematic literature search was performed using PubMed from January 2012 to December 2012. The articles selected for this review represent topics the authors thought best highlight recent clinical OA research., (Copyright © 2013 Osteoarthritis Research Society International. Published by Elsevier Ltd. All rights reserved.)
- Published
- 2013
- Full Text
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43. Comparison of screening instruments for disability and emotional/behavioral disorders with a generic measure of health-related quality of life in survivors of childhood brain tumors.
- Author
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Kennedy CR and Leyland K
- Subjects
- Adolescent, Child, Disabled Children, Humans, Survivors, Affective Symptoms diagnosis, Brain Neoplasms psychology, Child Behavior Disorders diagnosis, Health Status, Quality of Life
- Abstract
The sensory, motor, educational and emotional/behavioral outcomes in 32 survivors of childhood brain tumors were evaluated by examination, interview, questionnaires on emotion/behavior and the Health Utilities Index Mark 2 (HUI 2). Thirty-eight percent had moderate/severe disability, and this was associated closely with special educational provision. Pre- and peri-operative factors were the commonest determinants of disability. Fifty percent had a high score on the emotion/behavior questionnaires, suggesting a high risk of an emotional or behavioral problem. The HUI 2 discriminated well between those survivors who had and those who had not had special provision made for their education but poorly between those with high and those with low scores on the emotion/behavior questionnaires. Previous studies have found self-reported health-related quality of life to be related more closely to emotional/behavioral sequelae than to disability. Possible uses and limitations of the HUI 2 in this clinical context are discussed., (Copyright 1999 Wiley-Liss, Inc.)
- Published
- 1999
- Full Text
- View/download PDF
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