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Browsing by Author "Naredo, Esperanza (6602827091)"

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    An OMERACT reliability exercise of inflammatory and structural abnormalities in patients with knee osteoarthritis using ultrasound assessment
    (2016)
    Bruyn, George A. W. (7006486448)
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    Naredo, Esperanza (6602827091)
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    Damjanov, Nemanja (8503557800)
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    Bachta, Artur (9635500400)
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    Baudoin, Paul (56615335900)
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    Hammer, Hilde Berner (7102733905)
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    Lamers-Karnebeek, Femke B. G. (56020036000)
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    Parera, Ingrid Moller (12142507400)
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    Richards, Bethan (19737986700)
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    Taylor, Mihaela (14826071200)
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    Ben-Artzi, Ami (55232661600)
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    D'Agostino, Maria-Antonietta (26643055600)
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    Garrido, Jesus (7202779769)
    ;
    Iagnocco, Annamaria (6603972277)
    Objective To assess whether ultrasonography (US) is reliable for the evaluation of inflammatory and structural abnormalities in patients with knee osteoarthritis (OA). Methods Thirteen patients with early knee OA were examined by 11 experienced sonographers during 2 days. Dichotomous and semiquantitative scoring was performed on synovitis characteristics in various aspects of the knee joint. Semiquantitative scoring was done of osteophytes at the medial and lateral femorotibial joint space or cartilage damage of the trochlea and on medial meniscal damage bilaterally. Intra-and interobserver reliability were computed by use of unweighted and weighted ê coefficients. Results Intra-and interobserver reliability scores were moderate to good for synovitis (mean κ 0.67 and 0.52, respectively) as well as moderate to good for the global synovitis (0.70 and 0.50, respectively). Mean intra-and interobserver reliability κ for cartilage damage, medial meniscal damage and osteophytes ranged from fair to good (0.55 and 0.34, 0.75 and 0.56, 0.73 and 0.60, respectively). Conclusions Using a standardised protocol, dichotomous and semiquantitative US scoring of pathological changes in knee OA can be reliable.
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    An OMERACT reliability exercise of inflammatory and structural abnormalities in patients with knee osteoarthritis using ultrasound assessment
    (2016)
    Bruyn, George A. W. (7006486448)
    ;
    Naredo, Esperanza (6602827091)
    ;
    Damjanov, Nemanja (8503557800)
    ;
    Bachta, Artur (9635500400)
    ;
    Baudoin, Paul (56615335900)
    ;
    Hammer, Hilde Berner (7102733905)
    ;
    Lamers-Karnebeek, Femke B. G. (56020036000)
    ;
    Parera, Ingrid Moller (12142507400)
    ;
    Richards, Bethan (19737986700)
    ;
    Taylor, Mihaela (14826071200)
    ;
    Ben-Artzi, Ami (55232661600)
    ;
    D'Agostino, Maria-Antonietta (26643055600)
    ;
    Garrido, Jesus (7202779769)
    ;
    Iagnocco, Annamaria (6603972277)
    Objective To assess whether ultrasonography (US) is reliable for the evaluation of inflammatory and structural abnormalities in patients with knee osteoarthritis (OA). Methods Thirteen patients with early knee OA were examined by 11 experienced sonographers during 2 days. Dichotomous and semiquantitative scoring was performed on synovitis characteristics in various aspects of the knee joint. Semiquantitative scoring was done of osteophytes at the medial and lateral femorotibial joint space or cartilage damage of the trochlea and on medial meniscal damage bilaterally. Intra-and interobserver reliability were computed by use of unweighted and weighted ê coefficients. Results Intra-and interobserver reliability scores were moderate to good for synovitis (mean κ 0.67 and 0.52, respectively) as well as moderate to good for the global synovitis (0.70 and 0.50, respectively). Mean intra-and interobserver reliability κ for cartilage damage, medial meniscal damage and osteophytes ranged from fair to good (0.55 and 0.34, 0.75 and 0.56, 0.73 and 0.60, respectively). Conclusions Using a standardised protocol, dichotomous and semiquantitative US scoring of pathological changes in knee OA can be reliable.
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    Criterion validity of ultrasound in the identification of calcium pyrophosphate crystal deposits at the knee: an OMERACT ultrasound study
    (2021)
    Filippou, Georgios (57877288000)
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    Scanu, Anna (24345141600)
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    Adinolfi, Antonella (55123782700)
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    Toscano, Carmela (57188961588)
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    Gambera, Dario (6508122469)
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    Largo, Raquel (7005741188)
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    Naredo, Esperanza (6602827091)
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    Calvo, Emilio (7101608122)
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    Herrero-Beaumont, Gabriel (56216985100)
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    Zufferey, Pascal (6701310829)
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    Bonjour, Christel Madelaine (57219344858)
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    Maccarter, Daryl K (56739051000)
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    Makman, Stanley (57219341531)
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    Weber, Zachary (57219340181)
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    Figus, Fabiana (57189377404)
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    Möller, Ingrid (7103192512)
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    Gutierrez, Marwin (26635137500)
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    Pineda, Carlos (55989786100)
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    Clavijo Cornejo, Denise (55573688100)
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    Garcia, Hector (57219341101)
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    Ilizaliturri, Victor (6603190347)
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    Mendoza Torres, Jaime (55319151000)
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    Pichardo, Raul (57219343630)
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    Rodriguez Delgado, Luis Carlos (57219339578)
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    Filippucci, Emilio (6603881110)
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    Cipolletta, Edoardo (57201023875)
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    Serban, Teodora (57195419051)
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    Cirstoiu, Catalin (22955383600)
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    Vreju, Florentin Ananu (55862189100)
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    Grecu, Dan (14050021400)
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    Mouterde, Gaël (23027881800)
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    Govoni, Marcello (20634216400)
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    Punzi, Leonardo (7005080858)
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    Damjanov, Nemanja S (8503557800)
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    Keen, Helen Isobel (15051832900)
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    Bruyn, George A.W. (7006486448)
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    Terslev, Lene (55949307900)
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    D'agostino, Maria-Antonietta (26643055600)
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    Scirè, Carlo Alberto (6505840565)
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    Iagnocco, Annamaria (6603972277)
    Objective To evaluate the discriminatory ability of ultrasound in calcium pyrophosphate deposition disease (CPPD), using microscopic analysis of menisci and knee hyaline cartilage (HC) as reference standard. Methods Consecutive patients scheduled for knee replacement surgery, due to osteoarthritis (OA), were enrolled. Each patient underwent ultrasound examination of the menisci and HC of the knee, scoring each site for presence/absence of CPPD. Ultrasound signs of inflammation (effusion, synovial proliferation and power Doppler) were assessed semiquantitatively (0-3). The menisci and condyles, retrieved during surgery, were examined microscopically by optical light microscopy and by compensated polarised microscopy. CPPs were scored as present/absent in six different samples from the surface and from the internal part of menisci and cartilage. Ultrasound and microscopic analysis were performed by different operators, blinded to each other's findings. Results 11 researchers from seven countries participated in the study. Of 101 enrolled patients, 68 were included in the analysis. In 38 patients, the surgical specimens were insufficient. The overall diagnostic accuracy of ultrasound for CPPD was of 75% -sensitivity of 91% (range 71%-87% in single sites) and specificity of 59% (range 68%-92%). The best sensitivity and specificity were obtained by assessing in combination by ultrasound the medial meniscus and the medial condyle HC (88% and 76%, respectively). No differences were found between patients with and without CPPD regarding ultrasound signs of inflammation. Conclusion Ultrasound demonstrated to be an accurate tool for discriminating CPPD. No differences were found between patents with OA alone and CPPD plus OA regarding inflammation. © Author(s) (or their employer(s)) 2021. No commercial re-use. See rights and permissions. Published by BMJ.
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    Criterion validity of ultrasound in the identification of calcium pyrophosphate crystal deposits at the knee: an OMERACT ultrasound study
    (2021)
    Filippou, Georgios (57877288000)
    ;
    Scanu, Anna (24345141600)
    ;
    Adinolfi, Antonella (55123782700)
    ;
    Toscano, Carmela (57188961588)
    ;
    Gambera, Dario (6508122469)
    ;
    Largo, Raquel (7005741188)
    ;
    Naredo, Esperanza (6602827091)
    ;
    Calvo, Emilio (7101608122)
    ;
    Herrero-Beaumont, Gabriel (56216985100)
    ;
    Zufferey, Pascal (6701310829)
    ;
    Bonjour, Christel Madelaine (57219344858)
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    Maccarter, Daryl K (56739051000)
    ;
    Makman, Stanley (57219341531)
    ;
    Weber, Zachary (57219340181)
    ;
    Figus, Fabiana (57189377404)
    ;
    Möller, Ingrid (7103192512)
    ;
    Gutierrez, Marwin (26635137500)
    ;
    Pineda, Carlos (55989786100)
    ;
    Clavijo Cornejo, Denise (55573688100)
    ;
    Garcia, Hector (57219341101)
    ;
    Ilizaliturri, Victor (6603190347)
    ;
    Mendoza Torres, Jaime (55319151000)
    ;
    Pichardo, Raul (57219343630)
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    Rodriguez Delgado, Luis Carlos (57219339578)
    ;
    Filippucci, Emilio (6603881110)
    ;
    Cipolletta, Edoardo (57201023875)
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    Serban, Teodora (57195419051)
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    Cirstoiu, Catalin (22955383600)
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    Vreju, Florentin Ananu (55862189100)
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    Grecu, Dan (14050021400)
    ;
    Mouterde, Gaël (23027881800)
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    Govoni, Marcello (20634216400)
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    Punzi, Leonardo (7005080858)
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    Damjanov, Nemanja S (8503557800)
    ;
    Keen, Helen Isobel (15051832900)
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    Bruyn, George A.W. (7006486448)
    ;
    Terslev, Lene (55949307900)
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    D'agostino, Maria-Antonietta (26643055600)
    ;
    Scirè, Carlo Alberto (6505840565)
    ;
    Iagnocco, Annamaria (6603972277)
    Objective To evaluate the discriminatory ability of ultrasound in calcium pyrophosphate deposition disease (CPPD), using microscopic analysis of menisci and knee hyaline cartilage (HC) as reference standard. Methods Consecutive patients scheduled for knee replacement surgery, due to osteoarthritis (OA), were enrolled. Each patient underwent ultrasound examination of the menisci and HC of the knee, scoring each site for presence/absence of CPPD. Ultrasound signs of inflammation (effusion, synovial proliferation and power Doppler) were assessed semiquantitatively (0-3). The menisci and condyles, retrieved during surgery, were examined microscopically by optical light microscopy and by compensated polarised microscopy. CPPs were scored as present/absent in six different samples from the surface and from the internal part of menisci and cartilage. Ultrasound and microscopic analysis were performed by different operators, blinded to each other's findings. Results 11 researchers from seven countries participated in the study. Of 101 enrolled patients, 68 were included in the analysis. In 38 patients, the surgical specimens were insufficient. The overall diagnostic accuracy of ultrasound for CPPD was of 75% -sensitivity of 91% (range 71%-87% in single sites) and specificity of 59% (range 68%-92%). The best sensitivity and specificity were obtained by assessing in combination by ultrasound the medial meniscus and the medial condyle HC (88% and 76%, respectively). No differences were found between patients with and without CPPD regarding ultrasound signs of inflammation. Conclusion Ultrasound demonstrated to be an accurate tool for discriminating CPPD. No differences were found between patents with OA alone and CPPD plus OA regarding inflammation. © Author(s) (or their employer(s)) 2021. No commercial re-use. See rights and permissions. Published by BMJ.
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    Development of semiquantitative ultrasound scoring system to assess cartilage in rheumatoid arthritis
    (2019)
    Mandl, Peter (56632095700)
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    Studenic, Paul (55260230400)
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    Filippucci, Emilio (6603881110)
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    Bachta, Artur (9635500400)
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    Backhaus, Marina (55357052600)
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    Bong, David (6603031463)
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    Bruyn, George A. W (7006486448)
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    Collado, Paz (7004139223)
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    Damjanov, Nemanja (8503557800)
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    Dejaco, Christian (11641035700)
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    Delle-Sedie, Andrea (6506743522)
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    De Miguel, Eugenio (7007026871)
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    Duftner, Christina (8426993500)
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    Gessl, Irina (56248033200)
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    Gutierrez, Marwin (26635137500)
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    Hammer, Hilde B (7102733905)
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    Hernandez-Diaz, Cristina (25824331600)
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    Iagnocco, Annmaria (6603972277)
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    Ikeda, Kei (7404891581)
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    Kane, David (35787288500)
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    Keen, Helen (15051832900)
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    Kelly, Stephen (26642867500)
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    Kovári, Eszter (55206601500)
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    Möller, Ingrid (7103192512)
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    Møller-Dohn, Uffe (15046519200)
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    Naredo, Esperanza (6602827091)
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    Nieto, Juan C (55674555600)
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    Pineda, Carlos (55989786100)
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    Platzer, Alex (56178456400)
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    Rodriguez, Ana (59157930200)
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    Schmidt, Wolfgang A (7404056149)
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    Supp, Gabriela (55814504000)
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    Szkudlarek, Marcin (6603855651)
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    Terslev, Lene (55949307900)
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    Thiele, Ralf (55949550900)
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    Wakefield, Richard J (7006151013)
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    Windschall, Daniel (6506976907)
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    D'Agostino, Maria-Antonietta (26643055600)
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    Balint, Peter V (7005110127)
    To develop and test the reliability of a new semiquantitative scoring system for the assessment of cartilage changes by ultrasound in a web-based exercise as well as a patient exercise of patients with RA. Methods: A taskforce of the Outcome Measures in Rheumatology Ultrasound Working Group performed a systematic literature review on the US assessment of cartilage in RA, followed by a Delphi survey on cartilage changes and a new semiquantitative US scoring system, and finally a web-based exercise as well as a patient exercise. For the web-based exercise, taskforce members scored a dataset of anonymized static images of MCP joints in RA patients and healthy controls, which also contained duplicate images. Subsequently, 12 taskforce members used the same US to score cartilage in MCP and proximal interphalangeal joints of six patients with RA in in a patient reliability exercise. Percentage agreement and prevalence of lesions were calculated, as intrareader reliability was assessed by weighted kappa and interreader reliability by Light's kappa. Results: The three-grade semiquantitative scoring system demonstrated excellent intrareader reliability (kappa: 0.87 and 0.83) in the web-based exercise and the patient exercise, respectively. Interreader reliability was good in the web-based exercise (kappa: 0.64) and moderate (kappa: 0.48) in the patient exercise. Conclusion: Our study demonstrates that ultrasound is a reliable tool for evaluating cartilage changes in the MCP joints of patients with RA and supports further development of a new reliable semiquantitative ultrasound scoring system for evaluating cartilage involvement in RA. © 2019 The Author(s) 2019. Published by Oxford University Press on behalf of the British Society for Rheumatology. All rights reserved.
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    Performance of ultra-high-frequency ultrasound in the evaluation of skin involvement in systemic sclerosis: A preliminary report
    (2020)
    Naredo, Esperanza (6602827091)
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    Pascau, Javier (6603062222)
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    Damjanov, Nemanja (8503557800)
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    Lepri, Gemma (55588064900)
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    Gordaliza, Pedro M (56491169700)
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    Janta, Iustina (55930777100)
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    Ovalles-Bonilla, Juan Gabriel (55638537700)
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    López-Longo, Francisco Javier (6603414978)
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    Matucci-Cerinic, Marco (7005642558)
    High frequency ultrasound allows visualization of epidermis, dermis and hypodermis, precise measurement of skin thickness, as well as assessment of skin oedema, fibrosis and atrophy. The aim of this pilot cross-sectional observational study was to assess the performance and multiobserver variability of ultra-high-frequency (UHF) (50 MHz) ultrasound (US) in measuring skin thickness as well as the capacity of UHF-derived skin features to differentiate SSc patients from healthy controls. Methods: Twenty-one SSc patients (16 limited and five diffuse SSc) and six healthy controls were enrolled. All subjects underwent US evaluation by three experts at three anatomical sites (forearm, hand and finger). Dermal thickness was measured and two rectangular regions of interest, one in dermis and one in hypodermis, were established for texture feature analysis. Results: UHF-US allowed a precise identification and measurement of the thickness of the dermis. The dermal thickness in the finger was significantly higher in patients than in controls (P < 0.05), while in the forearm it was significantly lower in patients than in controls (P < 0.001). Interobserver variability for dermal thickness was good to excellent [forearm intraclass correlation coefficient (ICC) = 0.754; finger ICC = 0.699; hand ICC = 0.602]. Texture computed analysis of dermis and hypodermis was able to discriminate between SSc and healthy subjects (area under the curve >0.7). Conclusion: These preliminary data show that skin UHF-US allows a very detailed imaging of skin layers, a reliable measurement of dermal thickness, and a discriminative capacity between dermis and hypodermis texture features in SSc and healthy subjects. © 2019 The Author(s) 2019. Published by Oxford University Press on behalf of the British Society for Rheumatology. All rights reserved.
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    The 2017 EULAR standardised procedures for ultrasound imaging in rheumatology
    (2017)
    Möller, Ingrid (7103192512)
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    Janta, Iustina (55930777100)
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    Backhaus, Marina (55357052600)
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    Ohrndorf, Sarah (13205334300)
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    Bong, David A. (6603031463)
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    Martinoli, Carlo (7005449059)
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    Filippucci, Emilio (6603881110)
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    Sconfienza, Luca Maria (24448438200)
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    Terslev, Lene (55949307900)
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    Damjanov, Nemanja (8503557800)
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    Hammer, Hilde Berner (7102733905)
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    Sudol-Szopinska, Iwona (7003455916)
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    Grassi, Walter (7005496865)
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    Balint, Peter (7005110127)
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    Bruyn, George A.W. (7006486448)
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    D'Agostino, Maria Antonietta (26643055600)
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    Hollander, Diana (57199077688)
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    Siddle, Heidi J. (26650180700)
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    Supp, Gabriela (55814504000)
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    Schmidt, Wolfgang A. (7404056149)
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    Iagnocco, Annamaria (6603972277)
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    Koski, Juhani (7005081297)
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    Kane, David (35787288500)
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    Fodor, Daniela (24168513700)
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    Bruns, Alessandra (57207968067)
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    Mandl, Peter (56632095700)
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    Kaeley, Gurjit S. (6507369276)
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    Micu, Mihaela (36176375800)
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    Ho, Carmen (7404652632)
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    Vlad, Violeta (35724995700)
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    Chávez-López, Mario (55930446200)
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    Filippou, Georgios (57877288000)
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    Cerón, Carmen Elena (56585652100)
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    Nestorova, Rodina (24923396300)
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    Quintero, Maritza (12757057400)
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    Wakefield, Richard (7006151013)
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    Carmona, Loreto (35263586300)
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    Naredo, Esperanza (6602827091)
    Background In 2001, the European League Against Rheumatism developed and disseminated the first guidelines for musculoskeletal (MS) ultrasound (US) in rheumatology. Fifteen years later, the dramatic expansion of new data on MSUS in the literature coupled with technological developments in US imaging has necessitated an update of these guidelines. Objectives To update the existing MSUS guidelines in rheumatology as well as to extend their scope to other anatomic structures relevant for rheumatology. Methods The project consisted of the following steps: (1) a systematic literature review of MSUS evaluable structures; (2) a Delphi survey among rheumatologist and radiologist experts in MSUS to select MS and non-MS anatomic structures evaluable by US that are relevant to rheumatology, to select abnormalities evaluable by US and to prioritise these pathologies for rheumatology and (3) a nominal group technique to achieve consensus on the US scanning procedures and to produce an electronic illustrated manual (ie, App of these procedures). Results Structures from nine MS and non-MS areas (ie, shoulder, elbow, wrist and hand, hip, knee, ankle and foot, peripheral nerves, salivary glands and vessels) were selected for MSUS in rheumatic and musculoskeletal diseases (RMD) and their detailed scanning procedures (ie, patient position, probe placement, scanning method and bony/other landmarks) were used to produce the App. In addition, US evaluable abnormalities present in RMD for each anatomic structure and their relevance for rheumatology were agreed on by the MSUS experts. Conclusions This task force has produced a consensus-based comprehensive and practical framework on standardised procedures for MSUS imaging in rheumatology. © Article author(s) (or their employer(s) unless otherwise stated in the text of the article) 2017. All rights reserved. No commercial use is permitted unless otherwise expressly granted.
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    The 2017 EULAR standardised procedures for ultrasound imaging in rheumatology
    (2017)
    Möller, Ingrid (7103192512)
    ;
    Janta, Iustina (55930777100)
    ;
    Backhaus, Marina (55357052600)
    ;
    Ohrndorf, Sarah (13205334300)
    ;
    Bong, David A. (6603031463)
    ;
    Martinoli, Carlo (7005449059)
    ;
    Filippucci, Emilio (6603881110)
    ;
    Sconfienza, Luca Maria (24448438200)
    ;
    Terslev, Lene (55949307900)
    ;
    Damjanov, Nemanja (8503557800)
    ;
    Hammer, Hilde Berner (7102733905)
    ;
    Sudol-Szopinska, Iwona (7003455916)
    ;
    Grassi, Walter (7005496865)
    ;
    Balint, Peter (7005110127)
    ;
    Bruyn, George A.W. (7006486448)
    ;
    D'Agostino, Maria Antonietta (26643055600)
    ;
    Hollander, Diana (57199077688)
    ;
    Siddle, Heidi J. (26650180700)
    ;
    Supp, Gabriela (55814504000)
    ;
    Schmidt, Wolfgang A. (7404056149)
    ;
    Iagnocco, Annamaria (6603972277)
    ;
    Koski, Juhani (7005081297)
    ;
    Kane, David (35787288500)
    ;
    Fodor, Daniela (24168513700)
    ;
    Bruns, Alessandra (57207968067)
    ;
    Mandl, Peter (56632095700)
    ;
    Kaeley, Gurjit S. (6507369276)
    ;
    Micu, Mihaela (36176375800)
    ;
    Ho, Carmen (7404652632)
    ;
    Vlad, Violeta (35724995700)
    ;
    Chávez-López, Mario (55930446200)
    ;
    Filippou, Georgios (57877288000)
    ;
    Cerón, Carmen Elena (56585652100)
    ;
    Nestorova, Rodina (24923396300)
    ;
    Quintero, Maritza (12757057400)
    ;
    Wakefield, Richard (7006151013)
    ;
    Carmona, Loreto (35263586300)
    ;
    Naredo, Esperanza (6602827091)
    Background In 2001, the European League Against Rheumatism developed and disseminated the first guidelines for musculoskeletal (MS) ultrasound (US) in rheumatology. Fifteen years later, the dramatic expansion of new data on MSUS in the literature coupled with technological developments in US imaging has necessitated an update of these guidelines. Objectives To update the existing MSUS guidelines in rheumatology as well as to extend their scope to other anatomic structures relevant for rheumatology. Methods The project consisted of the following steps: (1) a systematic literature review of MSUS evaluable structures; (2) a Delphi survey among rheumatologist and radiologist experts in MSUS to select MS and non-MS anatomic structures evaluable by US that are relevant to rheumatology, to select abnormalities evaluable by US and to prioritise these pathologies for rheumatology and (3) a nominal group technique to achieve consensus on the US scanning procedures and to produce an electronic illustrated manual (ie, App of these procedures). Results Structures from nine MS and non-MS areas (ie, shoulder, elbow, wrist and hand, hip, knee, ankle and foot, peripheral nerves, salivary glands and vessels) were selected for MSUS in rheumatic and musculoskeletal diseases (RMD) and their detailed scanning procedures (ie, patient position, probe placement, scanning method and bony/other landmarks) were used to produce the App. In addition, US evaluable abnormalities present in RMD for each anatomic structure and their relevance for rheumatology were agreed on by the MSUS experts. Conclusions This task force has produced a consensus-based comprehensive and practical framework on standardised procedures for MSUS imaging in rheumatology. © Article author(s) (or their employer(s) unless otherwise stated in the text of the article) 2017. All rights reserved. No commercial use is permitted unless otherwise expressly granted.
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    The OMERACT ultrasound group: A report from the OMERACT 2016 meeting and perspectives
    (2017)
    Terslev, Lene (55949307900)
    ;
    Iagnocco, Annamaria (6603972277)
    ;
    Bruyn, George A.W. (7006486448)
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    Naredo, Esperanza (6602827091)
    ;
    Vojinovic, Jelena (6603423836)
    ;
    Collado, Paz (7004139223)
    ;
    Damjanov, Nemanja (8503557800)
    ;
    Filer, Andrew (6603511236)
    ;
    Filippou, Georgios (57877288000)
    ;
    Finzel, Stephanie (36703920200)
    ;
    Gandjbakhch, Frederique (23567463900)
    ;
    Ikeda, Kei (7404891581)
    ;
    Keen, Helen I. (15051832900)
    ;
    Kortekaas, Marion C. (36944035400)
    ;
    Magni-Manzoni, Silvia (6602281787)
    ;
    Ohrndorf, Sarah (13205334300)
    ;
    Pineda, Carlos (55989786100)
    ;
    Ravagnani, Viviana (23100930700)
    ;
    Richards, Bethan (19737986700)
    ;
    Sahbudin, Ilfita (56731080400)
    ;
    Schmidt, Wolfgang A. (7404056149)
    ;
    Siddle, Heidi J. (26650180700)
    ;
    Stoenoiu, Maria S. (6602649826)
    ;
    Szkudlarek, Marcin (6603855651)
    ;
    Tzaribachev, Nikolay (16837459300)
    ;
    D'Agostino, Maria-Antonietta (26643055600)
    Objective: To provide an update from the Outcome Measures in Rheumatology (OMERACT) Ultrasound Working Group on the progress for defining ultrasound (US) minimal disease activity threshold at joint level in rheumatoid arthritis (RA) and for standardization of US application in juvenile idiopathic arthritis (JIA). Methods: For minimal disease activity, healthy controls (HC) and patients with early arthritis (EA) who were naive to disease-modifying antirheumatic drugs were recruited from 2 centers. US was performed of the hands and feet, and scored semiquantitatively (0-3) for synovial hypertrophy (SH) and power Doppler (PD). Synovial effusion (SE) was scored a binary variable. For JIA, a Delphi approach and subsequent validation in static images and patient-based exercises were used to developed preliminary definitions for synovitis and a scoring system. Results: For minimal disease activity, 7% HC had at least 1 joint abnormality versus 30% in the EA group. In HC, the findings of SH and PD were predominantly grade 1 whereas all grades were seen in the EA cohort, but SE was rare. In JIA, synovitis can be diagnosed based on B-mode findings alone because of the presence of physiological vascularization. A semiquantitative scoring system (0-3) for synovitis for both B-mode and Doppler were developed in which the cutoff between Doppler grade 2 and grade 3 was 30%. Conclusion: The first step has been taken to define the threshold for minimal disease activity in RA by US and to define and develop a scoring system for synovitis in JIA. Further steps are planned for the continuous validation of US in these areas. The Journal of Rheumatology Copyright © 2017. All rights reserved.
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    Publication
    The OMERACT ultrasound group: A report from the OMERACT 2016 meeting and perspectives
    (2017)
    Terslev, Lene (55949307900)
    ;
    Iagnocco, Annamaria (6603972277)
    ;
    Bruyn, George A.W. (7006486448)
    ;
    Naredo, Esperanza (6602827091)
    ;
    Vojinovic, Jelena (6603423836)
    ;
    Collado, Paz (7004139223)
    ;
    Damjanov, Nemanja (8503557800)
    ;
    Filer, Andrew (6603511236)
    ;
    Filippou, Georgios (57877288000)
    ;
    Finzel, Stephanie (36703920200)
    ;
    Gandjbakhch, Frederique (23567463900)
    ;
    Ikeda, Kei (7404891581)
    ;
    Keen, Helen I. (15051832900)
    ;
    Kortekaas, Marion C. (36944035400)
    ;
    Magni-Manzoni, Silvia (6602281787)
    ;
    Ohrndorf, Sarah (13205334300)
    ;
    Pineda, Carlos (55989786100)
    ;
    Ravagnani, Viviana (23100930700)
    ;
    Richards, Bethan (19737986700)
    ;
    Sahbudin, Ilfita (56731080400)
    ;
    Schmidt, Wolfgang A. (7404056149)
    ;
    Siddle, Heidi J. (26650180700)
    ;
    Stoenoiu, Maria S. (6602649826)
    ;
    Szkudlarek, Marcin (6603855651)
    ;
    Tzaribachev, Nikolay (16837459300)
    ;
    D'Agostino, Maria-Antonietta (26643055600)
    Objective: To provide an update from the Outcome Measures in Rheumatology (OMERACT) Ultrasound Working Group on the progress for defining ultrasound (US) minimal disease activity threshold at joint level in rheumatoid arthritis (RA) and for standardization of US application in juvenile idiopathic arthritis (JIA). Methods: For minimal disease activity, healthy controls (HC) and patients with early arthritis (EA) who were naive to disease-modifying antirheumatic drugs were recruited from 2 centers. US was performed of the hands and feet, and scored semiquantitatively (0-3) for synovial hypertrophy (SH) and power Doppler (PD). Synovial effusion (SE) was scored a binary variable. For JIA, a Delphi approach and subsequent validation in static images and patient-based exercises were used to developed preliminary definitions for synovitis and a scoring system. Results: For minimal disease activity, 7% HC had at least 1 joint abnormality versus 30% in the EA group. In HC, the findings of SH and PD were predominantly grade 1 whereas all grades were seen in the EA cohort, but SE was rare. In JIA, synovitis can be diagnosed based on B-mode findings alone because of the presence of physiological vascularization. A semiquantitative scoring system (0-3) for synovitis for both B-mode and Doppler were developed in which the cutoff between Doppler grade 2 and grade 3 was 30%. Conclusion: The first step has been taken to define the threshold for minimal disease activity in RA by US and to define and develop a scoring system for synovitis in JIA. Further steps are planned for the continuous validation of US in these areas. The Journal of Rheumatology Copyright © 2017. All rights reserved.

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