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428 results on '"Ostergaard, Mikkel"'

151. MOR103, a human monoclonal antibody to granulocyte–macrophage colony-stimulating factor, in the treatment of patients with moderate rheumatoid arthritis:results of a phase Ib/IIa randomised, double-blind, placebo-controlled, dose-escalation trial

Author

Behrens, Frank, Tak, Paul P, Ostergaard, Mikkel, Stoilov, Rumen, Wiland, Piotr, Huizinga, Thomas W, Berenfus, Vadym Y, Vladeva, Stoyanka, Rech, Juergen, Rubbert-Roth, Andrea, Korkosz, Mariusz, Rekalov, Dmitriy, Zupanets, Igor A, Ejbjerg, Bo J, Geiseler, Jens, Fresenius, Julia, Korolkiewicz, Roman P, Schottelius, Arndt J, Burkhardt, Harald, Behrens, Frank, Tak, Paul P, Ostergaard, Mikkel, Stoilov, Rumen, Wiland, Piotr, Huizinga, Thomas W, Berenfus, Vadym Y, Vladeva, Stoyanka, Rech, Juergen, Rubbert-Roth, Andrea, Korkosz, Mariusz, Rekalov, Dmitriy, Zupanets, Igor A, Ejbjerg, Bo J, Geiseler, Jens, Fresenius, Julia, Korolkiewicz, Roman P, Schottelius, Arndt J, and Burkhardt, Harald

Abstract

OBJECTIVES: To determine the safety, tolerability and signs of efficacy of MOR103, a human monoclonal antibody to granulocyte-macrophage colony-stimulating factor (GM-CSF), in patients with rheumatoid arthritis (RA).METHODS: Patients with active, moderate RA were enrolled in a randomised, multicentre, double-blind, placebo-controlled, dose-escalation trial of intravenous MOR103 (0.3, 1.0 or 1.5 mg/kg) once a week for 4 weeks, with follow-up to 16 weeks. The primary outcome was safety.RESULTS: Of the 96 randomised and treated subjects, 85 completed the trial (n=27, 24, 22 and 23 for pooled placebo and MOR103 0.3, 1.0 and 1.5 mg/kg, respectively). Treatment emergent adverse events (AEs) in the MOR103 groups were mild or moderate in intensity and generally reported at frequencies similar to those in the placebo group. The most common AE was nasopharyngitis. In two cases, AEs were classified as serious because of hospitalisation: paronychia in a placebo subject and pleurisy in a MOR103 0.3 mg/kg subject. Both patients recovered fully. In exploratory efficacy analyses, subjects in the MOR103 1.0 and 1.5 mg/kg groups showed significant improvements in Disease Activity Score-28 scores and joint counts and significantly higher European League Against Rheumatism response rates than subjects receiving placebo. MOR103 1.0 mg/kg was associated with the largest reductions in disease activity parameters.CONCLUSIONS: MOR103 was well tolerated and showed preliminary evidence of efficacy in patients with active RA. The data support further investigation of this monoclonal antibody to GM-CSF in RA patients and potentially in those with other immune-mediated inflammatory diseases.TRIAL REGISTRATION NUMBER: NCT01023256.

Published
2015

152. Colaboradores

Author

Abramson, Steven, An, KaiNan, Andrade, Felipe, Ardoin, Stacy P., Barton, Anne, Baughman, Robert P., Beaton, Dorcas E., Beere, Helen M., Beltran, Javier, Bending, David, Bennett, Robert M., Bermas, Bonnie L., Bertsias, George, Bhardwaj, Nina, Bijlsma, Johannes W.J., Bockenstedt, Linda K., Boers, Maarten, Boilard, Eric, Boin, Francesco, Boumpas, Dimitrios T., Boyle, David L., Bradley, Sean, Brown, Matthew, Buch, Maya, Buckley, Christopher D., Budd, Ralph C., Burg, Nathalie, Burns, Christopher M., Cannella, Amy C., Carter, John D., Chakravarty, Eliza F., Chakravarty, Soumya D., Chang, Christopher, Cheng, Joseph S., Chiodo, Christopher P., Chung, Sharon, Cleland, Leslie G., Cohen, Stanley, Colbert, Robert A., Cook, Paul P., Craft, Joseph E., Crofford, Leslie J., Cronstein, Bruce N., Crow, Mary K., Crowson, Cynthia S., Culley, Kirsty L., Cunnane, Gaye, Dall’Era, Maria, Darrah, Erika, Davis, John M., III, De Bari, Cosimo, Dell’Accio, Francesco, Diamond, Betty, Di Cesare, Paul E., Dixit, Rajiv, Drenth, Joost P.H., Dustin, Michael L., El-Gabalawy, Hani S., Elmamoun, Musaab, Erickson, Alan R., Erkan, Doruk, Eyre, Stephen, Fanouriakis, Antonis, Felson, David T., Field, Max, Filer, Andrew, Firestein, Gary S., Fishman, Felicity G., FitzGerald, Oliver, Flaherty, John P., Nieves, César E. Fors, Fortner, Karen A., Gabriel, Sherine E., Gasque, Philippe, Gershwin, M. Eric, Gladue, Heather S., Goldring, Mary B., Goldring, Steven R., Golightly, Yvonne M., Goodman, Stuart, Gordon, Siamon, Grassi, Walter, Green, Douglas R., Greenspan, Adam, Gregersen, Peter, Grimaldi, Christine, Guilherme, Luiza, Hajj-Ali, Rula A., Haudenschild, Dominik R., Hellmann, David B., Holmdahl, Rikard, Hsu, Joyce J., Huddleston, James I., III, Hudson, Alan P., Huizinga, Thomas W.J., Hunder, Gene G., Iversen, Maura D., Jacobs, Johannes W.G., Jen, Ho, Jordan, Joanne M., Jorizzo, Joseph L., Kalil, Jorge, Kaufman, Kenton, Kaufman, William S., Kavanaugh, Arthur, Keenan, Robert T., Kenna, Tony, Kerr, Darcy A., Koch, Alisa E., Kono, Dwight H., Korsten, Peter, Krakow, Deborah, Krasnokutsky, Svetlana, Lafeber, Floris P.J.G., Lambert, Robert G.W., Lane, Nancy E., Langford, Carol A., Laskin, Daniel M., Layh-Schmitt, Gerlinde, Lee, Lela A., Lee, Tzielan C., Lockshin, Michael D., Lozada, Carlos J., Lundberg, Ingrid E., Luqmani, Raashid, Luyten, Frank P., Mader, Reuven, Maksymowych, Walter, Markenson, Joseph A., Martin, Scott David, Matteson, Eric L., McGregor, Laura, McInnes, Iain B., McNamara, Elizabeth K., Mikuls, Ted R., Miller, Mark S., Ming, Pedro Azevedo, Moder, Kevin G., Monach, Paul A., Moulton, Vaishali R., Nagaraju, Kanneboyina, Nelson, Amanda E., Nigrovic, Peter A., Nistala, Kiran, O’Dell, James R., Okada, Yasunori, Østergaard, Mikkel, Otero, Miguel, Palmer, Bradley M., Panush, Richard S., Peng, Stanford L., Pillai, Shiv, Pillinger, Michael H., Plüddemann, Annette, Polston, Gregory R., Porcelli, Steven A., Price, Mark D., Reed, Ann M., Reveille, John D., Robinson, Angela B., Robinson, Philip, Robinson, William H., Roosendaal, Goris, Rosen, Antony, Rosenbaum, James T., Rosenberg, Andrew E., Ruderman, Eric M., Saag, Kenneth G., Salmon, Jane E., Sammaritano, Lisa R., Samuels, Jonathan, Sandborg, Christy I., Sawalha, Amr H., Saxena, Amit, Schett, Georg, Schutgens, Roger E.G., Seldin, David C., Shah, Binita, Sikora, Keith A., Simon, Anna, Siraj, Dawd S., Sorkin, Linda S., Clair, E. William St., Stamp, Lisa K., Stone, John H., Suarez-Fueyo, Abel, Svensson, Camilla I., Sweiss, Nadera J., Swigart, Carrie R., Szekanecz, Zoltán, Tait, Stephen, Tanne, Antoine, Taylor, Peter C., Terkeltaub, Robert, Theofilopoulos, Argyrios N., Thornhill, Thomas S., Torok, Kathryn S., Toth, Michael J., Tozman, Elaine C., Trouw, Leendert A., Tsokos, George C., Tugwell, Peter, Tutuncu, Zuhre, Upadhyaya, Shivam, Van Der Helm-Van Mil, Annette H.M., van der Linden, Sjef, Van Der Meer, Jos W.M., Van Laar, Jacob M., Van Meter, Heather, van Vollenhoven, Ronald F., van Vulpen, Lize F.D., Varga, John, Vaseer, Samera, Vasquez-Castellanos, Raul, Veale, Douglas J., Wakefield, Richard J., Wallace, Mark S., Wang, Ruoning, Wang, Tingting, Warshaw, David M., Wedderburn, Lucy R., Werth, Victoria P., Wigley, Fredrick M., Wofsy, David, Wollheim, Frank A., Wondimu, Elisabeth, Wong, Cyrus, Wortmann, Robert L., Yelin, Edward, Zayat, Ahmed, Zou, Yong-Rui, and Zurier, Robert B.

Published
2018
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154. Brief report:M-ficolin levels reflect disease activity and predict remission in early rheumatoid arthritis

Author

Ammitzbøll, Christian G, Thiel, Steffen, Jensenius, Jens C, Ellingsen, Torkell, Hørslev-Petersen, Kim, Hetland, Merete Lund, Junker, Michael Peter, Krogh, Niels Steen, Ostergaard, Mikkel, and Stengaard-Pedersen, Kristian

Subjects
musculoskeletal diseases, skin and connective tissue diseases
Abstract

To assess plasma M-ficolin concentrations in disease-modifying antirheumatic drug (DMARD)-naive patients with early rheumatoid arthritis (RA), to investigate the correlation of M-ficolin concentrations with disease activity markers, and to determine the predictive value of M-ficolin with respect to the Disease Activity Score in 28 joints (DAS28).

Published
2013
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155. Imaging in rheumatoid arthritis, psoriatic arthritis, axial spondyloarthritis, and osteoarthritis: An international viewpoint on the current knowledge and future research priorities.

Author

Baraliakos, Xenofon, Conaghan, Philip G., D'Agostino, Maria-Antonietta, Maksymowych, Walter, Naredo, Esperanza, Ostergaard, Mikkel, Schett, Georg, and Emery, Paul

Abstract

Imaging is increasingly used in the routine management of rheumatic diseases as well as in the clinical trials of these disorders. This viewpoint, authored by a group of international imaging experts following two meetings dedicated to imaging in rheumatology, reports a consensus about the current knowledge and addresses where further research should be focused based on the views of the international imaging experts and discussion of the evidence with attending imaging practitioners. The goal was to maximize the potential of imaging to improve the clinical management of four rheumatic diseases. These rheumatic diseases include rheumatoid arthritis, psoriatic arthritis, axial spondyloarthritis, and osteoarthritis. [ABSTRACT FROM AUTHOR]

Published
2018
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156. A Treat-To-Target Strategy With Methotrexate and Intra-Articular Triamcinolone With Or Without Added Adalimumab Reduces Synovitis, Osteitis and Tenosynovitis and Halts Structural Damage Progression In Early Rheumatoid Arthritis:The Opera Magnetic Resonance Imaging Sub-Study

Author

Axelsen, Mette Bjorndal, Eshed, Iris, Horslev-Petersen, Kim, Steengaard-Petersen, Kristian, Hetland, Merete L., Moller, Jakob M., Junker, Peter, Podenphant, Jan, Ellingsen, Torkell, Ahlquist, Palle, Hanne Merete Lindegaard, Linauskas, Asta, Schlemmer, Annette, Dam, Mette Yde, Hansen, Ib, Horn, Hans Chr, Ammitzboll, Christian G., Jorgensen, Anette, Krintel, Sophine B., Raun, Johnny, Johansen, Julia S., Krogh, Niels Steen, and Ostergaard, Mikkel

Published
2013
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157. Very High Remission Rates Are Achieved By Methotrexate and Intraarticular Glucocorticoids Independent Of Induction Therapy With Adalimumab; Year 2 Clinical Results Of An Investigator-Initiated Randomised, Controlled Clinical Trial Of Early, Rheumatoid Arthritis (OPERA)

Author

Horslev-Petersen, Kim, Hetland, Merete L., Junker, Peter, Podenphant, Jan, Ellingsen, Torkell, Ahlqvist, Palle, Hanne Merete Lindegaard, Linauskas, Asta, Schlemmer, Annette, Dam, Mette Y., Hansen, Ib, Lottenburger, Tine, Jorgensen, Anette, Krintel, Sophine B., Raun, Johnny, Ammitzboll, Christian G., Johansen, Julia, Ostergaard, Mikkel, and Stengaard-Pedersen, Kristian

Published
2013
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158. Induction Therapy With Adalimumab On Top Of An Aggressive Treat-To-Target Strategy With Methotrexate and Intraarticular Corticosteroid Reduces Radiographic Erosive Progression In Early Rheumatoid Arthritis, Even After Withdrawal Of Adalimumab. Results Of a 2-Year Trial (OPERA)

Author

Horslev-Petersen, Kim, Ornbjerg, Lykke Midtboll, Hetland, Merete L., Junker, Peter, Podenphant, Jan, Ellingsen, Torkell, Ahlqvist, Palle, Hanne Merete Lindegaard, Linauskas, Asta, Schlemmer, Annette, Dam, Mette Y., Hansen, Ib, Lottenburger, Tine, Jorgensen, Anette, Krintel, Sophine B., Raun, Johnny, Ammitzboll, Christian G., Johansen, Julia, Ostergaard, Mikkel, and Stengaard-Pedersen, Kristian

Published
2013
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159. First in Patient Study of Anti-GM-CSF Monoclonal Antibody (MOR103) in Active Rheumatoid Arthritis: Results of a Phase 1b/2a Randomized, Double-Blind, Placebo-Controlled Trial

Author

Behrens, Frank, Ostergaard, Mikkel, Stoilov, Rumen, Wiland, Piotr, Tom Huizinga, Berenfus, Vadym Y., Tak, Paul-Peter, Vladeva, Stoyanka, Rech, Juergen, Rubbert-Roth, Andrea, Korkosz, Mariusz, Rekalov, Dmitriy, Zupanets, Igor A., Ejbjerg, Bo J., Geiseler, Jens, Fresenius, Julia, Korolkiewicz, Roman P., Schottelius, Arndt J., and Burkhardt, Harald

Published
2012

162. Patterns of magnetic resonance imaging bone erosion in rheumatoid arthritis - which bones are most frequently involved and show the most change?

Author

Ostergaard, Mikkel, Møller Døhn, Uffe, Duer-Jensen, Anne, Hetland, Merete Lund, Hørslev-Petersen, Kim, Stengaard-Pedersen, Kristian, Junker, Peter, Pødenphant, Jan, and Ejbjerg, Bo

Subjects
musculoskeletal diseases
Abstract

To investigate by magnetic resonance imaging (MRI) which bones in wrists and metacarpophalangeal (MCP) joints most frequently show bone erosions, and which most frequently demonstrate erosive progression, in early and established rheumatoid arthritis (RA).

Published
2011
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163. Treating rheumatoid arthritis to target: 2014 update of the recommendations of an international task force

Author

Smolen, Josef S, primary, Breedveld, Ferdinand C, additional, Burmester, Gerd R, additional, Bykerk, Vivian, additional, Dougados, Maxime, additional, Emery, Paul, additional, Kvien, Tore K, additional, Navarro-Compán, M Victoria, additional, Oliver, Susan, additional, Schoels, Monika, additional, Scholte-Voshaar, Marieke, additional, Stamm, Tanja, additional, Stoffer, Michaela, additional, Takeuchi, Tsutomu, additional, Aletaha, Daniel, additional, Andreu, Jose Louis, additional, Aringer, Martin, additional, Bergman, Martin, additional, Betteridge, Neil, additional, Bijlsma, Hans, additional, Burkhardt, Harald, additional, Cardiel, Mario, additional, Combe, Bernard, additional, Durez, Patrick, additional, Fonseca, Joao Eurico, additional, Gibofsky, Alan, additional, Gomez-Reino, Juan J, additional, Graninger, Winfried, additional, Hannonen, Pekka, additional, Haraoui, Boulos, additional, Kouloumas, Marios, additional, Landewe, Robert, additional, Martin-Mola, Emilio, additional, Nash, Peter, additional, Ostergaard, Mikkel, additional, Östör, Andrew, additional, Richards, Pam, additional, Sokka-Isler, Tuulikki, additional, Thorne, Carter, additional, Tzioufas, Athanasios G, additional, van Vollenhoven, Ronald, additional, de Wit, Martinus, additional, and van der Heijde, Desirée, additional

Published
2015
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164. Health-Related Quality of Life:Validity, Reliability, and Responsiveness of SF-36, EQ-15D, EQ-5D, RAQoL, and HAQ in Patients with Rheumatoid Arthritis

Author

Linde, Louise, Sørensen, Jan, Ostergaard, Mikkel, Hørslev-Petersen, Kim, and Hetland, Merete Lund

Abstract

Udgivelsesdato: Aug OBJECTIVE: To compare validity, reliability, and responsiveness of generic and disease specific health-related quality of life (HRQOL) instruments in rheumatoid arthritis (RA). METHODS: Two samples of patients completed the Medical Outcomes Study Short Form-36 Health Survey (SF-36), EuroQol (EQ)-5D, 15D, Rheumatoid Arthritis Quality of Life Scale (RAQoL), Health Assessment Questionnaire (HAQ), and visual analog scales (VAS) for pain, fatigue, and global RA. Validity (convergent, discriminant, and known-groups) was evaluated in a cross-section of 200 patients. Reliability was evaluated by agreement (intraclass correlation coefficient; baseline to 2 weeks) and internal consistency (Cronbach's alpha); and responsiveness by the standardized response mean stratified on improvement, status quo, or deterioration in health status after 6 months in 150 patients followed longitudinally. Followup questionnaires (at 2 weeks and 6 months) included questions about changes in health status since baseline. RESULTS: The cross-sectional sample included 77% women, median age 57 years (range 19-87), disease duration 6 years (0-58), with Disease Activity Score 28-joint count (DAS28) of 3.10 (1.21-6.47). The longitudinal sample included 80% women, median age 60 years (22-82). Validity: all instruments discriminated between low, moderate, and high DAS28. Reliability: RAQoL and HAQ displayed good repeatability (ICC > 0.95) and internal consistency (Cronbach's alpha > 0.90). Responsiveness: SF-36 bodily pain scale and VAS pain were responsive to both improvement and deterioration. CONCLUSION: All instruments were valid measures for HRQOL in RA. The RAQoL and HAQ displayed the best reliability, while the SF-36 bodily pain scale and VAS pain were the most responsive. The choice of instrument should depend on the study objectives.

Published
2008

165. Aggressive combination therapy with intraarticular glucocorticoid injections and conventional DMARDs in early rheumatoid arthritis:Two Year Clinical and Radiographic Results From The CIMESTRA Study

Author

Hetland, Merete Lund, Stengaard-Pedersen, Kristian, Junker, Peter, Lottenburger, Tine, Hansen, Ib, Andersen, Lis Smedegaard, Tarp, Ulrik, Svendsen, Anders, Pedersen, Jens K, Skjødt, Henrik, Lauridsen, Ulrik B, Ellingsen, Torkell, van Overeem Hansen, Gert, Lindegaard, Hanne, Vestergaard, Aage, Jurik, Anne Grethe, Ostergaard, Mikkel, and Hørslev-Petersen, Kim

Abstract

Udgivelsesdato: Sep-18 OBJECTIVE: To investigate whether clinical and radiographic disease control can be achieved and maintained in patients with early, active rheumatoid arthritis (RA) during the 2nd year of aggressive treatment with conventional DMARD and intraarticular corticosteroid. This paper presents the results of the 2nd year of the randomized, controlled double-blind CIMESTRA study. METHODS: 160 patients with early RA (

Published
2007
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166. Testing of the preliminary OMERACT validation criteria for a biomarker to be regarded as reflecting structural damage endpoints in rheumatoid arthritis clinical trials: the example of C-reactive protein

Author

Keeling, Stephanie O., Landewe, Robert, van der Heijde, Desiree, Bathon, Joan, Boers, Maarten, Garnero, Patrick, Geusens, Piet, El-Gabalawy, Hani, Inman, Robert D., Kraus, Virginia B., Kvien, Tore K., Mease, Philip J., Ostergaard, Mikkel, Ritchlin, Chris, Syversen, Silje W., Maksymowych, Walter P., and Other departments

Abstract

A list of 14 criteria for guiding the validation of a soluble biomarker as reflecting structural damage endpoints in rheumatoid arthritis (RA) clinical trials was drafted by an international working group after a Delphi consensus exercise. C-reactive protein (CRP), a soluble biomarker extensively studied in RA, was then used to test these criteria. Our objectives were: (1) To assess the strength of evidence in support of CRP as a soluble biomarker reflecting structural damage in RA according to the draft validation criteria. (2) To assess the strength of recommendation for inclusion of individual criteria in the draft set. A systematic literature review was conducted to elicit evidence in support of each specific criterion composing the 14-criteria draft set. A summary of the key literature findings per criterion was presented to both the working group and to participants in a special interest soluble biomarker group at OMERACT 8. Participants at OMERACT 8 were asked to rate the strength of evidence and the strength of the recommendation in support of each individual criterion on a 0-10 numerical rating scale. Working group members not present at OMERACT voted by a Web-based survey. Minimal data were extracted from the literature pertaining to those criteria listed under the category of truth. Ratings for strength of evidence were moderate to low ( 7) except for those criteria listed under the category of truth. The draft criteria serve as a useful template in the evaluation of the strength of evidence in support of a particular soluble biomarker as reflecting structural damage in RA

Published
2007

167. Contributors

Author

Abramson, Steven, An, KaiNan, Andrade, Felipe, Ardoin, Stacy P., Barton, Anne, Baughman, Robert P., Beaton, Dorcas E., Beere, Helen M., Beltran, Javier, Bending, David, Bennett, Robert M., Bermas, Bonnie L., Bertsias, George, Bhardwaj, Nina, Bijlsma, Johannes W.J., Bockenstedt, Linda K., Boers, Maarten, Boilard, Eric, Boin, Francesco, Boumpas, Dimitrios T., Boyle, David L., Bradley, Sean, Brown, Matthew, Buch, Maya, Buckley, Christopher D., Budd, Ralph C., Burg, Nathalie, Burns, Christopher M., Cannella, Amy C., Carter, John D., Chakravarty, Eliza F., Chakravarty, Soumya D., Chang, Christopher, Cheng, Joseph S., Chiodo, Christopher P., Chung, Sharon, Cleland, Leslie G., Cohen, Stanley, Colbert, Robert A., Cook, Paul P., Craft, Joseph E., Crofford, Leslie J., Cronstein, Bruce N., Crow, Mary K., Crowson, Cynthia S., Culley, Kirsty L., Cunnane, Gaye, Dall'Era, Maria, Darrah, Erika, Davis, John M., III, Bari, Cosimo De, Dell'Accio, Francesco, Diamond, Betty, Di Cesare, Paul E., Dixit, Rajiv, Drenth, Joost P.H., Dustin, Michael L., El-Gabalawy, Hani S., Elmamoun, Musaab, Erickson, Alan R., Erkan, Doruk, Eyre, Stephen, Fanouriakis, Antonis, Felson, David T., Field, Max, Filer, Andrew, Firestein, Gary S., Fishman, Felicity G., FitzGerald, Oliver, Flaherty, John P., Fors, César E., Fortner, Karen A., Gabriel, Sherine E., Gasque, Philippe, Gershwin, M. Eric, Gladue, Heather S., Goldring, Mary B., Goldring, Steven R., Golightly, Yvonne M., Goodman, Stuart, Gordon, Siamon, Grassi, Walter, Green, Douglas R., Greenspan, Adam, Gregersen, Peter, Grimaldi, Christine, Guilherme, Luiza, Hajj-Ali, Rula A., Haudenschild, Dominik R., Hellmann, David B., Holmdahl, Rikard, Hsu, Joyce J., Huddleston, James I., III, Hudson, Alan P., Huizinga, Thomas W.J., Hunder, Gene G., Iversen, Maura D., Jacobs, Johannes W.G., Jen, Ho, Jordan, Joanne M., Jorizzo, Joseph L., Kalil, Jorge, Kaufman, Kenton, Kaufman, William S., Kavanaugh, Arthur, Keenan, Robert T., Kenna, Tony, Kerr, Darcy A., Koch, Alisa E., Kono, Dwight H., Korsten, Peter, Krakow, Deborah, Krasnokutsky, Svetlana, Lafeber, Floris P.J.G., Lambert, Robert G.W., Lane, Nancy E., Langford, Carol A., Laskin, Daniel M., Layh-Schmitt, Gerlinde, Lee, Lela A., Lee, Tzielan C., Lockshin, Michael D., Lozada, Carlos J., Lundberg, Ingrid E., Luqmani, Raashid, Luyten, Frank P., Mader, Reuven, Maksymowych, Walter, Markenson, Joseph A., Martin, Scott David, Matteson, Eric L., McGregor, Laura, McInnes, Iain B., McNamara, Elizabeth K., Mikuls, Ted R., Miller, Mark S., Ming, Pedro Azevedo, Moder, Kevin G., Monach, Paul A., Moulton, Vaishali R., Nagaraju, Kanneboyina, Nelson, Amanda E., Nigrovic, Peter A., Nistala, Kiran, O'Dell, James R., Okada, Yasunori, Østergaard, Mikkel, Otero, Miguel, Palmer, Bradley M., Panush, Richard S., Peng, Stanford L., Pillai, Shiv, Pillinger, Michael H., Plüddemann, Annette, Polston, Gregory R., Porcelli, Steven A., Price, Mark D., Reed, Ann M., Reveille, John D., Robinson, Angela B., Robinson, Philip, Robinson, William H., Roosendaal, Goris, Rosen, Antony, Rosenbaum, James T., Rosenberg, Andrew E., Ruderman, Eric M., Saag, Kenneth G., Salmon, Jane E., Sammaritano, Lisa R., Samuels, Jonathan, Sandborg, Christy I., Sawalha, Amr H., Saxena, Amit, Schett, Georg, Schutgens, Roger E.G., Seldin, David C., Shah, Binita, Sikora, Keith A., Simon, Anna, Siraj, Dawd S., Sorkin, Linda S., St. Clair, E. William, Stamp, Lisa K., Stone, John H., Suarez-Fueyo, Abel, Svensson, Camilla I., Sweiss, Nadera J., Swigart, Carrie R., Szekanecz, Zoltán, Tait, Stephen, Tanne, Antoine, Taylor, Peter C., Terkeltaub, Robert, Theofilopoulos, Argyrios N., Thornhill, Thomas S., Torok, Kathryn S., Toth, Michael J., Tozman, Elaine C., Trouw, Leendert A., Tsokos, George C., Tugwell, Peter, Tutuncu, Zuhre, Upadhyaya, Shivam, Van, Annette H.M., van der Linden, Sjef, Van, Jos W.M., Van, Jacob M., Meter, Heather Van, van Vollenhoven, Ronald F., van Vulpen, Lize F.D., Varga, John, Vaseer, Samera, Vasquez-Castellanos, Raul, Veale, Douglas J., Wakefield, Richard J., Wallace, Mark S., Wang, Ruoning, Wang, Tingting, Warshaw, David M., Wedderburn, Lucy R., Werth, Victoria P., Wigley, Fredrick M., Wofsy, David, Wollheim, Frank A., Wondimu, Elisabeth, Wong, Cyrus, Wortmann, Robert L., Yelin, Edward, Zayat, Ahmed, Zou, Yong-Rui, and Zurier, Robert B.

Published
2017
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168. Musculoskeletal ultrasound including definitions for ultrasonographic pathology

Author

Wakefield, Richard J, Balint, Peter V, Szkudlarek, Marcin, Filippucci, Emilio, Backhaus, Marina, D'Agostino, Maria Antonietta, Sanchez, Esperanza Naredo, Iagnocco, Annamaria, Schmidt, Wolfgang A, Bruyn, George A W, Bruyn, George, Kane, David, O'Connor, Philip J, Manger, Bernhard, Joshua, Fred, Koski, Juhani, Grassi, Walter, Lassere, Marissa N D, Swen, Nanno, Kainberger, Franz, Klauser, Andrea, Ostergaard, Mikkel, Brown, Andrew K, Machold, Klaus P, and Conaghan, Philip G

Subjects
Settore MED/16 - REUMATOLOGIA, Synovitis, ultrasound, enthesopathy, erosions, synovitis, tenosynovitis, Synovial Membrane, Hypertrophy, Tenosynovitis, Arthritis, Rheumatoid, Terminology as Topic, Humans, Joints, Musculoskeletal System, Ultrasonography
Abstract

Ultrasound (US) has great potential as an outcome in rheumatoid arthritis trials for detecting bone erosions, synovitis, tendon disease, and enthesopathy. It has a number of distinct advantages over magnetic resonance imaging, including good patient tolerability and ability to scan multiple joints in a short period of time. However, there are scarce data regarding its validity, reproducibility, and responsiveness to change, making interpretation and comparison of studies difficult. In particular, there are limited data describing standardized scanning methodology and standardized definitions of US pathologies. This article presents the first report from the OMERACT ultrasound special interest group, which has compared US against the criteria of the OMERACT filter. Also proposed for the first time are consensus US definitions for common pathological lesions seen in patients with inflammatory arthritis.

Published
2005

172. Updating the OMERACT Filter: Core Areas as a Basis for Defining Core Outcome Sets

Author

Kirwan, John R., primary, Boers, Maarten, additional, Hewlett, Sarah, additional, Beaton, Dorcas, additional, Bingham, Clifton O., additional, Choy, Ernest, additional, Conaghan, Philip G., additional, D’Agostino, Maria-Antonietta, additional, Dougados, Maxime, additional, Furst, Daniel E., additional, Guillemin, Francis, additional, Gossec, Laure, additional, van der Heijde, Désirée M., additional, Kloppenburg, Margreet, additional, Kvien, Tore K., additional, Landewé, Robert B.M., additional, Mackie, Sarah L., additional, Matteson, Eric L., additional, Mease, Philip J., additional, Merkel, Peter A., additional, Ostergaard, Mikkel, additional, Saketkoo, Lesley Ann, additional, Simon, Lee, additional, Singh, Jasvinder A., additional, Strand, Vibeke, additional, and Tugwell, Peter, additional

Published
2014
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173. Can erosions on MRI of the sacroiliac joints be reliably detected in patients with ankylosing spondylitis? - A cross-sectional study

Author

Weber, Ulrich, Pedersen, Susanne J, Ostergaard, Mikkel, Rufibach, Kaspar, Lambert, Robert Gw, Maksymowych, Walter P, Weber, Ulrich, Pedersen, Susanne J, Ostergaard, Mikkel, Rufibach, Kaspar, Lambert, Robert Gw, and Maksymowych, Walter P

Abstract

INTRODUCTION: Erosions of the sacroiliac joints (SIJ) on pelvic radiographs of patients with ankylosing spondylitis (AS) are an important feature of the modified New York classification criteria. However, radiographic SIJ erosions are often difficult to identify. Recent studies have shown that erosions can be detected also on magnetic resonance imaging (MRI) of the SIJ early in the disease course before they can be seen on radiography. The goals of this study were to assess the reproducibility of erosion and related features, namely, extended erosion (EE) and backfill (BF) of excavated erosion, in the SIJ using a standardized MRI methodology. METHODS: Four readers independently assessed T1-weighted and short tau inversion recovery sequence (STIR) images of the SIJ from 30 AS patients and 30 controls (15 patients with non-specific back pain and 15 healthy volunteers) ≤45 years old. Erosions, EE, and BF were recorded according to standardized definitions. Reproducibility was assessed by percentage concordance among six possible reader pairs, kappa statistics (erosion as binary variable) and intraclass correlation coefficient (ICC) (erosion as sum score) for all readers jointly. RESULTS: SIJ erosions were detected in all AS patients and six controls by ≥2 readers. The median number of SIJ quadrants affected by erosion recorded by four readers in 30 AS patients was 8.6 in the iliac and 2.1 in the sacral joint portion (P < 0.0001). For all 60 subjects and for all four readers, the kappa value for erosion was 0.72, 0.73 for EE, and 0.63 for BF. ICC for erosion was 0.79, 0.72 for EE, and 0.55 for BF, respectively. For comparison, the kappa and ICC values for bone marrow edema were 0.61 and 0.93, respectively. CONCLUSIONS: Erosions can be detected on MRI to a comparable degree of reliability as bone marrow edema despite the significant heterogeneity of their appearance on MRI.

Published
2012

174. Algorithm for identification of undifferentiated peripheral inflammatory arthritis : a multinational collaboration through the 3e initiative.

Author

UCL - (SLuc) Service de rhumatologie, UCL - SSS/IREC/RUMA - Pôle de Pathologies rhumatismales, Hazlewood, Glen, Aletaha, Daniel, Carmona, Loreto, Landewé, Robert B M, van der Heijde, Désirée M, Bijlsma, Johannes W J, Bykerk, Vivian P, Canhão, Helena, Catrina, Anca I, Durez, Patrick, Edwards, Christopher J, Leeb, Burkhard F, Mjaavatten, Maria D, Martinez-Osuna, Pindaro, Montecucco, Carlomaurizio, Ostergaard, Mikkel, Serra-Bonett, Natali, Xavier, Ricardo M, Zochling, Jane, Machado, Pedro, Thevissen, Kristof, Vercoutere, Ward, Bombardier, Claire, UCL - (SLuc) Service de rhumatologie, UCL - SSS/IREC/RUMA - Pôle de Pathologies rhumatismales, Hazlewood, Glen, Aletaha, Daniel, Carmona, Loreto, Landewé, Robert B M, van der Heijde, Désirée M, Bijlsma, Johannes W J, Bykerk, Vivian P, Canhão, Helena, Catrina, Anca I, Durez, Patrick, Edwards, Christopher J, Leeb, Burkhard F, Mjaavatten, Maria D, Martinez-Osuna, Pindaro, Montecucco, Carlomaurizio, Ostergaard, Mikkel, Serra-Bonett, Natali, Xavier, Ricardo M, Zochling, Jane, Machado, Pedro, Thevissen, Kristof, Vercoutere, Ward, and Bombardier, Claire

Abstract

To develop an algorithm for identification of undifferentiated peripheral inflammatory arthritis (UPIA).

Published
2011

175. Changes in plasma IL-6, plasma VEGF and serum YKL-40 during Treatment with Etanercept and Methotrexate or Etanercept alone in Patients with Active Rheumatoid Arthritis Despite Methotrexate Therapy

Author

Knudsen, Lene Surland, Hetland, Merete Lund, Johansen, Julia Sidenius, Skjødt, Henrik, Peters, Niels Daugaard, Colic, Ada, Grau, Karin, Nielsen, Hans Jørgen, Østergaard, Mikkel, Ostergaard, Mikkel, Knudsen, Lene Surland, Hetland, Merete Lund, Johansen, Julia Sidenius, Skjødt, Henrik, Peters, Niels Daugaard, Colic, Ada, Grau, Karin, Nielsen, Hans Jørgen, Østergaard, Mikkel, and Ostergaard, Mikkel

Abstract

Udgivelsesdato: 2009, Changes in plasma IL-6, plasma VEGF and serum YKL-40 were determined in rheumatoid arthritis (RA) patients during treatment with etanercept alone or in combination with methotrexate. Twenty-five patients with active RA (DAS28 >/= 3.2) were randomized to receive etanercept (25 mg sc. biweekly) plus methotrexate (n = 12) or etanercept alone (n = 13). Plasma IL-6, plasma VEGF and serum YKL-40 were determined by ELISA. The 3 biomarkers and DAS28 scores were evaluated at baseline and after 4, 8, 12 and 16 weeks of treatment. At inclusion all patients had significantly (p < 0.001) elevated plasma IL-6, plasma VEGF and serum YKL-40 compared to healthy subjects. Eighteen patients responded to treatment (pooled data from both treatment groups), and they had significant (p < 0.05 to p < 0.001) decreases in plasma IL-6, plasma VEGF, serum YKL-40, ESR and DAS28 after 4 weeks of treatment and throughout the study (except serum YKL-40 at week 16). Plasma IL-6 showed the largest reductions. Non-responders had unchanged biomarkers. At week 16 the patients with DAS28 < 3.2 had lower levels compared to baseline values in plasma IL-6 (p = 0.005), plasma VEGF (p = 0.014), and ESR (p = 0.024).Plasma IL-6, plasma VEGF and serum YKL-40, which reflect different aspects of the inflammatory process, may provide useful information regarding early differentiation of responders from non-responders.

Published
2009

176. Reducing invasiveness, duration, and cost of magnetic resonance imaging in rheumatoid arthritis by omitting intravenous contrast injection -- Does it change the assessment of inflammatory and destructive joint changes by the OMERACT RAMRIS?

Author

Østergaard, Mikkel, Conaghan, Philip G, O'Connor, Philip, Szkudlarek, Marcin, Klarlund, Mette, Emery, Paul, Peterfy, Charles, Genant, Harry, McQueen, Fiona M, Bird, Paul, Lassere, Marissa, Ejbjerg, Bo, Ostergaard, Mikkel, Østergaard, Mikkel, Conaghan, Philip G, O'Connor, Philip, Szkudlarek, Marcin, Klarlund, Mette, Emery, Paul, Peterfy, Charles, Genant, Harry, McQueen, Fiona M, Bird, Paul, Lassere, Marissa, Ejbjerg, Bo, and Ostergaard, Mikkel

Abstract

Udgivelsesdato: 2009-Aug, OBJECTIVE: Gadolinium (Gd)-enhanced magnetic resonance imaging (MRI) provides highly sensitive assessment of inflammatory and destructive changes in rheumatoid arthritis (RA) joints, but intravenous (IV) Gd injection prolongs examination time and increases cost, invasiveness, and patient discomfort. We explored to what extent RA joint pathologies in wrists and metacarpophalangeal (MCP) joints can be reliably assessed by unenhanced MRI images compared with Gd-enhanced MRI as the reference method. METHODS: MRI data sets from 2 RA substudies were scored according to preliminary OMERACT RA MRI scoring system (RAMRIS): Substudy A included 1.0 T/1.5 T MR images from 40 RA patients, which were scored twice by 2 experienced readers. Substudy B included 0.2 T dedicated extremity MRI (E-MRI) images from 55 patients, scored twice by one experienced reader. The first reading included only unenhanced images, whereas complete image sets were available for the second reading. RESULTS: Gd contrast injection appeared unimportant to MRI scores of bone erosions and bone edema in RA wrist and MCP joints. However, when post-Gd MRI was considered the standard reference, MRI without Gd provided only moderate to high agreement concerning assessment of synovitis, and omitting the post-Gd acquisitions increased the interreader variation on synovitis scores. Low-field (0.2 T) E-MRI in these exercises provided a lower sensitivity of unenhanced imaging for synovitis than MRI using higher-field strengths. CONCLUSION: Omitting IV contrast injection did not change scores of bone erosions and bone edema, but decreased the reliability of synovitis scores. However, this disadvantage may for some purposes be outweighed by the possibility to assess more joints and/or greater feasibility.

Published
2009

177. Reumatologien i fortsat hastig udvikling

Author

Madsen, Ole Rintek, Terslev, Lene, Tarp, Ulrik, Jacobsen, Søren, Ostergaard, Mikkel, Madsen, Ole Rintek, Terslev, Lene, Tarp, Ulrik, Jacobsen, Søren, and Ostergaard, Mikkel

Abstract

Udgivelsesdato: 2009-Mar-23

Published
2009

178. Guidelines for initiation of antitumour necrosis factor therapy in rheumatoid arthritis: Similarities and differences across europe

Author

Emery, P., Van Vollenhoven, Ronald, Ostergaard, Mikkel, Choy, Ernest, Combe, Bernard, Graninger, W., Krueger, K., Matucci-Cerinic, Marco Matucci, Navarro, F., Van Riel, P. C L M, Settas, Lucas, Steinfeld, Serge, Emery, P., Van Vollenhoven, Ronald, Ostergaard, Mikkel, Choy, Ernest, Combe, Bernard, Graninger, W., Krueger, K., Matucci-Cerinic, Marco Matucci, Navarro, F., Van Riel, P. C L M, Settas, Lucas, and Steinfeld, Serge

Abstract

SCOPUS: re.j, info:eu-repo/semantics/published

Published
2009

179. Monitoring anti-TNF{alpha} treatment in RA: Responsiveness of magnetic resonance imaging and ultrasonography of the dominant wrist compared to conventional measures of disease activity and structural damage

Author

Haavardsholm, Espen A, Ostergaard, Mikkel, Hammer, Hilde Berner, Bøyesen, Pernille, Boonen, Annelies, van der Heijde, Désirée, Kvien, Tore K, Haavardsholm, Espen A, Ostergaard, Mikkel, Hammer, Hilde Berner, Bøyesen, Pernille, Boonen, Annelies, van der Heijde, Désirée, and Kvien, Tore K

Abstract

Udgivelsesdato: 2008-Nov-19, OBJECTIVES: The objective of this study was to evaluate the responsiveness of magnetic resonance imaging (MRI) and ultrasonography (US) compared to conventional measures of disease activity and structural damage in RA patients during the first year of anti-TNFalpha treatment. METHODS: A cohort of RA patients (N=36, median age 53 years, disease duration 7.6 years and DAS28 5.7) was evaluated by core measures of disease activity, US (one wrist), MRI (one wrist) and conventional radiography (CR, both hands and wrists) at initiation of treatment with anti-TNFalpha agents and after 3, 6 and 12 months. Responsiveness was assessed by standardized response means (SRM). Accepted thresholds were applied to classify responsiveness as trivial, low, moderate or good. RESULTS: MRI synovitis (SRM between -0.79 and -0.92) and the MRI total inflammation score comprising synovitis, tenosynovitis and bone marrow edema (SRM between -1.05 and -1.24) were highly responsive. Moderate to high responsiveness was found for MRI tenosynovitis and bone marrow edema, all the composite indices (DAS28, SDAI and CDAI) and the 28-swollen joint count. US displayed low to moderate responsiveness. The MRI erosion score displayed low responsiveness, but was more responsive than CR measures at 3 and 6 months follow-up. MRI and CR measures of annual progression rates of damage performed similarly, and were highly responsive. CONCLUSIONS: The most responsive measure of inflammation when evaluating anti-TNFalpha medication was a composite measure comprising MRI synovitis, tenosynovitis and bone marrow edema, and this may be a promising outcome measure in clinical studies.

Published
2008

180. Magnetic resonance imaging findings in 84 patients with early rheumatoid arthritis: bone marrow oedema predicts erosive progression.

Author

Haavardsholm, Espen A, Bøyesen, Pernille, Ostergaard, Mikkel, Schildvold, Arnulf, Kvien, Tore K, Haavardsholm, Espen A, Bøyesen, Pernille, Ostergaard, Mikkel, Schildvold, Arnulf, and Kvien, Tore K

Abstract

Objectives: To examine the spectrum and severity of magnetic resonance imaging (MRI) findings in patients with early rheumatoid arthritis (RA), and to investigate the predictive value of MRI findings for subsequent development of conventional radiographic (CR) damage and MRI erosions. Methods: 84 consecutive patients with RA with disease duration <1 year were enrolled. Patients were treated according to standard clinical practice, and evaluated at baseline, 3, 6 and 12 months by core measures of disease activity, conventional radiographs of both hands and wrists and MRI of the dominant wrist. MR images were scored according to the OMERACT rheumatoid arthritis magnetic resonance imaging score (RAMRIS), and conventional radiographs according to the van der Heijde modified Sharp score. Results: MRI findings reflecting inflammation (synovitis, bone marrow oedema and tenosynovitis) decreased during follow-up, while there was a small increase in MRI erosion score and CR damage. The proportion of patients with erosive progression at 1 year was 48% for conventional radiography and 66% for MRI. Baseline MRI bone marrow oedema (score >2 RAMRIS units) was identified as an independent predictor of both CR (odds ratio = 2.77 (95% confidence interval (CI) 1.06 to 7.21)) and MRI erosive progression (B = 0.21 (95% CI 0.08 to 0.34)). Conclusions: MRI findings were common in early RA, and MRI bone marrow oedema was an independent predictor of radiographic damage. These results suggest that MRI scans of the dominant wrist may help clinicians to determine which patients need early and aggressive treatment to, Objectives: To examine the spectrum and severity of magnetic resonance imaging (MRI) findings in patients with early rheumatoid arthritis (RA), and to investigate the predictive value of MRI findings for subsequent development of conventional radiographic (CR) damage and MRI erosions. Methods: 84 consecutive patients with RA with disease duration <1 year were enrolled. Patients were treated according to standard clinical practice, and evaluated at baseline, 3, 6 and 12 months by core measures of disease activity, conventional radiographs of both hands and wrists and MRI of the dominant wrist. MR images were scored according to the OMERACT rheumatoid arthritis magnetic resonance imaging score (RAMRIS), and conventional radiographs according to the van der Heijde modified Sharp score. Results: MRI findings reflecting inflammation (synovitis, bone marrow oedema and tenosynovitis) decreased during follow-up, while there was a small increase in MRI erosion score and CR damage. The proportion of patients with erosive progression at 1 year was 48% for conventional radiography and 66% for MRI. Baseline MRI bone marrow oedema (score >2 RAMRIS units) was identified as an independent predictor of both CR (odds ratio = 2.77 (95% confidence interval (CI) 1.06 to 7.21)) and MRI erosive progression (B = 0.21 (95% CI 0.08 to 0.34)). Conclusions: MRI findings were common in early RA, and MRI bone marrow oedema was an independent predictor of radiographic damage. These results suggest that MRI scans of the dominant wrist may help clinicians to determine which patients need early and aggressive treatment to

Published
2008

181. Erosive progression is minimal, but erosion healing rare, in rheumatoid arthritis patients treated with adalimumab. A 1 year investigator-initiated follow-up study using high-resolution computed tomography as the primary outcome measure

Author

Møller Døhn, Uffe, Boonen, Annelies, Hetland, Merete Lund, Hansen, Michael Sejer, Knudsen, Lene Surland, Hansen, Annette, Madsen, Ole Rintek, Hasselquist, Maria, Møller, Jakob M, Ostergaard, Mikkel, Møller Døhn, Uffe, Boonen, Annelies, Hetland, Merete Lund, Hansen, Michael Sejer, Knudsen, Lene Surland, Hansen, Annette, Madsen, Ole Rintek, Hasselquist, Maria, Møller, Jakob M, and Ostergaard, Mikkel

Abstract

Udgivelsesdato: 2008-Nov-19, OBJECTIVE: With computed tomography (CT) and radiography to investigate if repair of bone erosions, defined as regression of erosion scores, occurs during adalimumab-treatment of rheumatoid arthritis (RA) patients. METHODS: Fifty-two RA patients, naïve to biologics, with at least two low-grade radiographic erosions in the wrist or metacarpophalangeal (MCP) joints in the same (index) hand, initiated adalimumab 40 mg sc. eow. Thirty-five patients completed the study (median age 61 years (range 19-86), disease duration 8 years (0-36)). CT of index wrist and MCP2-5 and radiographs of hands and forefeet were obtained at baseline, 6 and 12 months. Images were evaluated blinded to chronology and clinical data, and assessed according to Sharp/van der Heijde (radiographs) and OMERACT RA MRI scoring (CT) methods. RESULTS: All investigated parameters of disease activity had decreased at 6 and 12 months (P<0.001). No significant change in any imaging parameters of joint destruction was observed at 6 and 12 months. High intrareader agreements were reached (mean intraobserver intraclass coefficients: 0.96 (CT) and 0.97 (radiography)). The number of patients with change scores exceeding the smallest detectable change (SDC) was comparable on CT and radiography, as were proportions of patients progressing/regressing. Decreased erosion scores at 12 months were registered in 1.6% and 1.8% of sites assessed on CT and radiography respectively. CONCLUSION: Repair of erosions in adalimumab-treated RA patients is rare, but erosive regression, exceeding the SDC, on CT and radiography occurred. The very limited overall erosive progression supports that joint destruction is minimal during adalimumab treatment of RA patients.

Published
2008

182. Health-related quality of life: validity, reliability, and responsiveness of SF-36, 15D, EQ-5D [corrected] RAQoL, and HAQ in patients with rheumatoid arthritis

Author

Linde, Louise, Sørensen, Jan, Ostergaard, Mikkel, Hørslev-Petersen, Kim, Hetland, Merete Lund, Linde, Louise, Sørensen, Jan, Ostergaard, Mikkel, Hørslev-Petersen, Kim, and Hetland, Merete Lund

Abstract

Udgivelsesdato: 2008-Aug, OBJECTIVE: To compare validity, reliability, and responsiveness of generic and disease specific health-related quality of life (HRQOL) instruments in rheumatoid arthritis (RA). METHODS: Two samples of patients completed the Medical Outcomes Study Short Form-36 Health Survey (SF-36), EuroQol (EQ)-5D, 15D, Rheumatoid Arthritis Quality of Life Scale (RAQoL), Health Assessment Questionnaire (HAQ), and visual analog scales (VAS) for pain, fatigue, and global RA. Validity (convergent, discriminant, and known-groups) was evaluated in a cross-section of 200 patients. Reliability was evaluated by agreement (intraclass correlation coefficient; baseline to 2 weeks) and internal consistency (Cronbach's alpha); and responsiveness by the standardized response mean stratified on improvement, status quo, or deterioration in health status after 6 months in 150 patients followed longitudinally. Followup questionnaires (at 2 weeks and 6 months) included questions about changes in health status since baseline. RESULTS: The cross-sectional sample included 77% women, median age 57 years (range 19-87), disease duration 6 years (0-58), with Disease Activity Score 28-joint count (DAS28) of 3.10 (1.21-6.47). The longitudinal sample included 80% women, median age 60 years (22-82). Validity: all instruments discriminated between low, moderate, and high DAS28. Reliability: RAQoL and HAQ displayed good repeatability (ICC > 0.95) and internal consistency (Cronbach's alpha > 0.90). Responsiveness: SF-36 bodily pain scale and VAS pain were responsive to both improvement and deterioration. CONCLUSION: All instruments were valid measures for HRQOL in RA. The RAQoL and HAQ displayed the best reliability, while the SF-36 bodily pain scale and VAS pain were the most responsive. The choice of instrument should depend on the study objectives.

Published
2008

183. Does low-field dedicated extremity MRI (E-MRI) reliably detect RA bone erosions? A comparison of two different E-MRI units and conventional radiography with high resolution CT

Author

Duer, Anne, Ejbjerg, Bo, Albrecht-Beste, Elisabeth, Vestergaard, Aage, Møller Døhn, Uffe, Lund Hetland, Merete, Ostergaard, Mikkel, Duer, Anne, Ejbjerg, Bo, Albrecht-Beste, Elisabeth, Vestergaard, Aage, Møller Døhn, Uffe, Lund Hetland, Merete, and Ostergaard, Mikkel

Abstract

Udgivelsesdato: 2008-Aug-21, OBJECTIVES: To compare the ability of 2 different E-MRI units and conventional radiography (CR) to identify bone erosions in rheumatoid arthritis (RA) metacarpophalangeal (MCP) and wrist joints, with computed tomography (CT) as standard reference method. METHODS: 20 RA patients and 5 controls underwent, within 2 weeks, CR, CT and two E-MRI (Esaote Biomedica; Artoscan and MagneVu; MV1000) examination of one hand. In all modalities each bone of wrist and (MCP) joints was blindedly evaluated for erosions. Furthermore, MagneVu images were assessed for the proportion of each bone being visualized. RESULTS: 550 bones were examined. CT, Artoscan, MagneVu and CR detected 188, 116, 55 and 45 bones with erosions, respectively. The majority were located in the carpal bones. The sensitivity of Artoscan for detecting erosions was higher than of MagneVu and CR (MCP joints: 0.68, 0.54 and 0.57, respectively; wrists: 0.50, 0.23 and 0.29). Corresponding specificities for detecting erosions were 0.94, 0.93 and 0.99, respectively, in the MCP joints and 0.92, 0.98 and 0.98 in the wrist. The MagneVu allowed visualization of 1.5 cm of the ventral-dorsal diameter of the bone. In the wrist 31.6% of bones were visualized entirely and 37.9% of bones were 67-99% visualized. In MCP joints, 84.2% of bones were visualized entirely and 15.8% of bones were 67-99% visualized. CONCLUSION: With CT as reference method for detecting erosions in RA hands, Artoscan showed higher sensitivity than MagneVu and CR. All imaging modalities revealed high specificities. The better performance of Artoscan should be considered when selecting imaging method in RA.

Published
2008

184. Aggressive combination therapy with intraarticular glucocorticoid injections and conventional DMARDs in early rheumatoid arthritis Two Year Clinical and Radiographic Results From The CIMESTRA Study.

Author

Hetland, Merete, Stengaard-Pedersen, Kristian, Junker, Peter, Lottenburger, Tine, Andersen, Lis Smedegaard, Hansen, Ib, Tarp, Ulrik, Svendsen, Anders, Pedersen, Jens K, Skjødt, Henrik, Lauridsen, Ulrik Birk, Ellingsen, Torkell, van Overeem Hansen, Gert, Lindegaard, Hanne, Vestergaard, Aage, Jurik, Anne Grethe, Ostergaard, Mikkel, Hørslev-Petersen, Kim, Hetland, Merete Lund, Hetland, Merete, Stengaard-Pedersen, Kristian, Junker, Peter, Lottenburger, Tine, Andersen, Lis Smedegaard, Hansen, Ib, Tarp, Ulrik, Svendsen, Anders, Pedersen, Jens K, Skjødt, Henrik, Lauridsen, Ulrik Birk, Ellingsen, Torkell, van Overeem Hansen, Gert, Lindegaard, Hanne, Vestergaard, Aage, Jurik, Anne Grethe, Ostergaard, Mikkel, Hørslev-Petersen, Kim, and Hetland, Merete Lund

Abstract

OBJECTIVE: To investigate whether clinical and radiographic disease control can be achieved and maintained in patients with early, active rheumatoid arthritis (RA) during the 2nd year of aggressive treatment with conventional DMARD and intraarticular corticosteroid. This paper presents the results of the 2nd year of the randomized, controlled double-blind CIMESTRA study. METHODS: 160 patients with early RA (<6 months' duration) were randomized to receive intraarticular betamethasone in any swollen joint in combination with step-up treatment with either methotrexate and placebo-cyclosporine (monotherapy) or methotrexate plus cyclosporine (combination therapy) during the first 76 weeks. At week 68 hydroxychlorochine 200 mg daily was added. From week 76-104 cyclosporine/placebo-cyclosporine was tapered to zero. RESULTS: ACR20, ACR50 and ACR70 were achieved in 88%, 79% and 59% of patients in the combination vs. 72%, 62% and 54% in the monotherapy group (p= 0.03, 0.02 and 0.6 between groups). Patient's global declined from 50 to 12 vs. 52 to 9, 51% and 50% were in DAS-remission, respectively. Mean+/-SD progressions in total Sharp/vdHeijde score were 1.42+/-3.52 and 2.03+/-5.86 in combination and monotherapy groups, respectively (NS). Serum creatinine levels increased by 7% in the combination group (4% in monotherapy), but hypertension was not more prevalent. CONCLUSION: Continuous methotrexate and intraarticular corticosteroid treatment resulted in excellent clinical reponse and disease control at 2 years, and the radiographic erosive progression was minimal. Addition of cyclosporine during the first 76 weeks resulted in significantly better ACR20 and ACR50 responses, but did not have any additional effect on remission rate and radiographic outcome. Udgivelsesdato: 2008-Sep-18, OBJECTIVE: To investigate whether clinical and radiographic disease control can be achieved and maintained in patients with early, active rheumatoid arthritis (RA) during the 2nd year of aggressive treatment with conventional DMARD and intraarticular corticosteroid. This paper presents the results of the 2nd year of the randomized, controlled double-blind CIMESTRA study. METHODS: 160 patients with early RA (<6 months' duration) were randomized to receive intraarticular betamethasone in any swollen joint in combination with step-up treatment with either methotrexate and placebo-cyclosporine (monotherapy) or methotrexate plus cyclosporine (combination therapy) during the first 76 weeks. At week 68 hydroxychlorochine 200 mg daily was added. From week 76-104 cyclosporine/placebo-cyclosporine was tapered to zero. RESULTS: ACR20, ACR50 and ACR70 were achieved in 88%, 79% and 59% of patients in the combination vs. 72%, 62% and 54% in the monotherapy group (p= 0.03, 0.02 and 0.6 between groups). Patient's global declined from 50 to 12 vs. 52 to 9, 51% and 50% were in DAS-remission, respectively. Mean+/-SD progressions in total Sharp/vdHeijde score were 1.42+/-3.52 and 2.03+/-5.86 in combination and monotherapy groups, respectively (NS). Serum creatinine levels increased by 7% in the combination group (4% in monotherapy), but hypertension was not more prevalent. CONCLUSION: Continuous methotrexate and intraarticular corticosteroid treatment resulted in excellent clinical reponse and disease control at 2 years, and the radiographic erosive progression was minimal. Addition of cyclosporine during the first 76 weeks resulted in significantly better ACR20 and ACR50 responses, but did not have any additional effect on remission rate and radiographic outcome.

Published
2008

185. Biomarkers of inflammation in patients with unclassified polyarthritis and early rheumatoid arthritis. Relationship to disease activity and radiographic outcome

Author

Knudsen, L.S., Klarlund, M., Skjodt, H., Jensen, Tim, Østergaard, Morten, Jensen, Karl Erik, Hansen, Michael Sejer, Hetland, Merete Lund, Nielsen, Hans Jørgen, Johansen, J.S., Knudsen, Lene S, Klarlund, Mette, Skjødt, Henrik, Jensen, Trine, Ostergaard, Mikkel, Hansen, Michael S, Hetland, Merete L, Nielsen, Hans J, Johansen, Julia S, Knudsen, L.S., Klarlund, M., Skjodt, H., Jensen, Tim, Østergaard, Morten, Jensen, Karl Erik, Hansen, Michael Sejer, Hetland, Merete Lund, Nielsen, Hans Jørgen, Johansen, J.S., Knudsen, Lene S, Klarlund, Mette, Skjødt, Henrik, Jensen, Trine, Ostergaard, Mikkel, Hansen, Michael S, Hetland, Merete L, Nielsen, Hans J, and Johansen, Julia S

Abstract

Objective. To determine plasma interleukin 6 (pIL-6), plasma vascular endothelial growth factor (pVEGF), and serum (s) YKL-40 in patients with early rheumatoid arthritis (RA) and unclassified polyarthritis (PA), and investigate their relationship with radiographic outcome. Methods. pIL-6 and pVEGF were determined by ELISA and sYKL-40 by an in-house radioimmunoassay in 51 patients with early RA and 21 with PA. Patients were followed with clinical and biochemical measurement every month for 2 years. Conventional radiographs of hands, wrists, and forefeet were scored according to the Larsen method, and magnetic resonance imaging of 2nd to 5th metacarpophalangeal joints of the dominant hand were evaluated for presence or absence of bone erosions. Results. Baseline pIL-6, pVEGF, sYKL-40, C-reactive protein (CRP), and erythrocyte sedimentation rate (ESR) were elevated in RA patients compared to healthy persons (p < 0.001), but were not in patients with PA. Patients with early RA had higher pIL-6 (p = 0.007), pVEGF (p = 0.02), and sYKL-40 (p = 0.024) compared to PA patients. pIL-6, sYKL-40, CRP, and ESR but not pVEGF decreased in patients that responded to treatment after 2 years. The mean value of pIL-6 during the first and second year were higher in patients with early RA with progression in bone erosions (n = 14) compared to early RA patients without progression (n = 30; first year 8.4 vs 2.8 ng/l, p = 0.04; second year 6.1 vs 3.6 ng/l, p = 0.03). Conclusion. Plasma IL-6 was the only biomarker related to treatment response and progressive erosive disease in patients with early RA, but it may not give additional information compared to CRP in relation to disease activity and treatment response Udgivelsesdato: 2008/7, OBJECTIVE: To determine plasma interleukin 6 (pIL-6), plasma vascular endothelial growth factor (pVEGF), and serum (s) YKL-40 in patients with early rheumatoid arthritis (RA) and unclassified polyarthritis (PA), and investigate their relationship with radiographic outcome. METHODS: pIL-6 and pVEGF were determined by ELISA and sYKL-40 by an in-house radioimmunoassay in 51 patients with early RA and 21 with PA. Patients were followed with clinical and biochemical measurement every month for 2 years. Conventional radiographs of hands, wrists, and forefeet were scored according to the Larsen method, and magnetic resonance imaging of 2nd to 5th metacarpophalangeal joints of the dominant hand were evaluated for presence or absence of bone erosions. RESULTS: Baseline pIL-6, pVEGF, sYKL-40, C-reactive protein (CRP), and erythrocyte sedimentation rate (ESR) were elevated in RA patients compared to healthy persons (p < 0.001), but were not in patients with PA. Patients with early RA had higher pIL-6 (p = 0.007), pVEGF (p = 0.02), and sYKL-40 (p = 0.024) compared to PA patients. pIL-6, sYKL-40, CRP, and ESR but not pVEGF decreased in patients that responded to treatment after 2 years. The mean value of pIL-6 during the first and second year were higher in patients with early RA with progression in bone erosions (n = 14) compared to early RA patients without progression (n = 30; first year 8.4 vs 2.8 ng/l, p = 0.04; second year 6.1 vs 3.6 ng/l, p = 0.03). CONCLUSION:Plasma IL-6 was the only biomarker related to treatment response and progressive erosive disease in patients with early RA, but it may not give additional information compared to CRP in relation to disease activity and treatment response.

Published
2008

186. MRI bone oedema is the strongest predictor of subsequent radiographic progression in early rheumatoid arthritis. Results from a 2 year randomized controlled trial (CIMESTRA)

Author

Hetland, M L, Ejbjerg, B, Hørslev-Petersen, K, Jacobsen, S, Vestergaard, A, Jurik, A G, Stengaard-Pedersen, K, Junker, P, Lottenburger, T, Hansen, I, Andersen, L S, Tarp, U, Skjødt, H, Pedersen, J K, Majgaard, O, Svendsen, A J, Ellingsen, T, Lindegaard, H, Christensen, A F, Vallø, J, Torfing, T, Narvestad, E, Thomsen, H S, Ostergaard, M, Hetland, Merete Lund, Ejbjerg, Bo Jannik, Hørslev-Petersen, Kim, Jacobsen, Søren, Vestergaard, Aage, Jurik, Anne Grethe, Stengaard-Pedersen, Kristian, Junker, Peter, Lottenburger, Tine, Hansen, Ib, Andersen, Lis Smedegaard, Tarp, Ulrik, Skjødt, Henrik, Pedersen, Jens K, Majgaard, Ole, Svendsen, Anders J, Ellingsen, Torkell, Lindegaard, Hanne M, Christensen, Anne F, Vallø, Jørgen, Torfing, Trine, Narvestad, Eva, Thomsen, Henrik S, Ostergaard, Mikkel, Hetland, M L, Ejbjerg, B, Hørslev-Petersen, K, Jacobsen, S, Vestergaard, A, Jurik, A G, Stengaard-Pedersen, K, Junker, P, Lottenburger, T, Hansen, I, Andersen, L S, Tarp, U, Skjødt, H, Pedersen, J K, Majgaard, O, Svendsen, A J, Ellingsen, T, Lindegaard, H, Christensen, A F, Vallø, J, Torfing, T, Narvestad, E, Thomsen, H S, Ostergaard, M, Hetland, Merete Lund, Ejbjerg, Bo Jannik, Hørslev-Petersen, Kim, Jacobsen, Søren, Vestergaard, Aage, Jurik, Anne Grethe, Stengaard-Pedersen, Kristian, Junker, Peter, Lottenburger, Tine, Hansen, Ib, Andersen, Lis Smedegaard, Tarp, Ulrik, Skjødt, Henrik, Pedersen, Jens K, Majgaard, Ole, Svendsen, Anders J, Ellingsen, Torkell, Lindegaard, Hanne M, Christensen, Anne F, Vallø, Jørgen, Torfing, Trine, Narvestad, Eva, Thomsen, Henrik S, and Ostergaard, Mikkel

Abstract

OBJECTIVE: To identify predictors of radiographic progression in a 2-year randomized, double-blind clinical study (CIMESTRA) of patients with early rheumatoid arthritis (RA). METHODS: Early RA patients (N=130) were treated with methotrexate, intra-articular betamethasone and cyclosporine/placebo-cyclosporine. Baseline magnetic resonance imaging (MRI) of the wrist (wrist-only-group:N=130) or MRI of wrist and MCP-joints (wrist+MCP-group:N=89) (OMERACT RAMRIS), x-rays of hands, wrists and forefeet (Sharp/vdHeijde Score (TSS)), disease activity score (DAS28), anti-cyclic-citrullinated-peptide-antibodies (anti-CCP), HLA-DRB1-shared-epitope (SE) and smoking status were assessed. Multiple regression analysis was performed with delta-TSS (0-2 years) as dependent variable, and baseline DAS28, TSS, MRI bone oedema score, MRI synovitis score, MRI erosion score, anti-CCP, smoking, SE, age and gender as explanatory variables. RESULTS: Baseline values: median DAS28: 5.6 (range: 2.4-8.0); anti-CCP positive: 61%; radiographic erosions: 56%. At 2 years: DAS28: 2.0 (0.5-5.7), in DAS-remission: 56%, radiographic progression: 26% (wrist+MCP-group, similar for wrist-only-group). MRI bone oedema score was the only independent predictor of delta-TSS (wrist+MCP-group: coefficient=0.75 (95%CI: 0.56-0.97), p<0.00001; wrist-only-group: coefficient=0.56 (0.41-0.77), p<0.00001). Bone oedema score explained 41% of the variation in the progression of TSS (wrist+MCP-group), 25% in wrist-only-group, (Pearson's r=0.64 and r=0.50, respectively). The results were confirmed by sensitivity analyses. CONCLUSION: In a RCT aiming at remission in early RA patients, baseline RAMRIS MRI bone oedema score of MCP and wrist joints (and of wrist only) was the strongest independent predictor of radiographic progression in hands, wrists and forefeet after 2 years. MRI synovitis score, MRI erosion score, DAS28, anti-CCP, SE, smoking, age and gender were not independent risk factors Udgivelsesdato: 2008/4, OBJECTIVE: To identify predictors of radiographic progression in a 2-year randomized, double-blind clinical study (CIMESTRA) of patients with early rheumatoid arthritis (RA). METHODS: Early RA patients (N=130) were treated with methotrexate, intra-articular betamethasone and cyclosporine/placebo-cyclosporine. Baseline magnetic resonance imaging (MRI) of the wrist (wrist-only-group:N=130) or MRI of wrist and MCP-joints (wrist+MCP-group:N=89) (OMERACT RAMRIS), x-rays of hands, wrists and forefeet (Sharp/vdHeijde Score (TSS)), disease activity score (DAS28), anti-cyclic-citrullinated-peptide-antibodies (anti-CCP), HLA-DRB1-shared-epitope (SE) and smoking status were assessed. Multiple regression analysis was performed with delta-TSS (0-2 years) as dependent variable, and baseline DAS28, TSS, MRI bone oedema score, MRI synovitis score, MRI erosion score, anti-CCP, smoking, SE, age and gender as explanatory variables. RESULTS: Baseline values: median DAS28: 5.6 (range: 2.4-8.0); anti-CCP positive: 61%; radiographic erosions: 56%. At 2 years: DAS28: 2.0 (0.5-5.7), in DAS-remission: 56%, radiographic progression: 26% (wrist+MCP-group, similar for wrist-only-group). MRI bone oedema score was the only independent predictor of delta-TSS (wrist+MCP-group: coefficient=0.75 (95%CI: 0.56-0.97), p<0.00001; wrist-only-group: coefficient=0.56 (0.41-0.77), p<0.00001). Bone oedema score explained 41% of the variation in the progression of TSS (wrist+MCP-group), 25% in wrist-only-group, (Pearson's r=0.64 and r=0.50, respectively). The results were confirmed by sensitivity analyses. CONCLUSION: In a RCT aiming at remission in early RA patients, baseline RAMRIS MRI bone oedema score of MCP and wrist joints (and of wrist only) was the strongest independent predictor of radiographic progression in hands, wrists and forefeet after 2 years. MRI synovitis score, MRI erosion score, DAS28, anti-CCP, SE, smoking, age and gender were not independent risk factors.

Published
2008

187. Methodologies for Semiquantitative Evaluation of Hip Osteoarthritis by Magnetic Resonance Imaging: Approaches Based on the Whole Organ and Focused on Active Lesions

Author

Jaremko, Jacob L., primary, Lambert, Robert G.W., additional, Zubler, Veronika, additional, Weber, Ulrich, additional, Loeuille, Damien, additional, Roemer, Frank W., additional, Cibere, Jolanda, additional, Pianta, Marcus, additional, Gracey, David, additional, Conaghan, Philip, additional, Ostergaard, Mikkel, additional, and Maksymowych, Walter P., additional

Published
2013
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188. Definitions and validation criteria for biomarkers and surrogate endpoints: development and testing of a quantitative hierarchical levels of evidence schema.

Author

Lassere, Marissa N, Johnson, Kent R, Boers, Maarten, Tugwell, Peter, Brooks, Peter, Simon, Lee, Strand, Vibeke, Conaghan, Philip G, Ostergaard, Mikkel, Maksymowych, Walter P, Landewe, Robert, Bresnihan, Barry, Tak, Paul-Peter, Wakefield, Richard, Mease, Philip, Bingham, Clifton O, Hughes, Michael, Altman, Doug, Buyse, Marc, Galbraith, Sally, Wells, George, Lassere, Marissa N, Johnson, Kent R, Boers, Maarten, Tugwell, Peter, Brooks, Peter, Simon, Lee, Strand, Vibeke, Conaghan, Philip G, Ostergaard, Mikkel, Maksymowych, Walter P, Landewe, Robert, Bresnihan, Barry, Tak, Paul-Peter, Wakefield, Richard, Mease, Philip, Bingham, Clifton O, Hughes, Michael, Altman, Doug, Buyse, Marc, Galbraith, Sally, and Wells, George

Abstract

OBJECTIVE: There are clear advantages to using biomarkers and surrogate endpoints, but concerns about clinical and statistical validity and systematic methods to evaluate these aspects hinder their efficient application. Our objective was to review the literature on biomarkers and surrogates to develop a hierarchical schema that systematically evaluates and ranks the surrogacy status of biomarkers and surrogates; and to obtain feedback from stakeholders. METHODS: After a systematic search of Medline and Embase on biomarkers, surrogate (outcomes, endpoints, markers, indicators), intermediate endpoints, and leading indicators, a quantitative surrogate validation schema was developed and subsequently evaluated at a stakeholder workshop. RESULTS: The search identified several classification schema and definitions. Components of these were incorporated into a new quantitative surrogate validation level of evidence schema that evaluates biomarkers along 4 domains: Target, Study Design, Statistical Strength, and Penalties. Scores derived from 3 domains the Target that the marker is being substituted for, the Design of the (best) evidence, and the Statistical strength are additive. Penalties are then applied if there is serious counterevidence. A total score (0 to 15) determines the level of evidence, with Level 1 the strongest and Level 5 the weakest. It was proposed that the term "surrogate" be restricted to markers attaining Levels 1 or 2 only. Most stakeholders agreed that this operationalization of the National Institutes of Health definitions of biomarker, surrogate endpoint, and clinical endpoint was useful. CONCLUSION: Further development and application of this schema provides incentives and guidance for effective biomarker and surrogate endpoint research, and more efficient drug discovery, development, and approval. Udgivelsesdato: 2007-Mar, OBJECTIVE: There are clear advantages to using biomarkers and surrogate endpoints, but concerns about clinical and statistical validity and systematic methods to evaluate these aspects hinder their efficient application. Our objective was to review the literature on biomarkers and surrogates to develop a hierarchical schema that systematically evaluates and ranks the surrogacy status of biomarkers and surrogates; and to obtain feedback from stakeholders. METHODS: After a systematic search of Medline and Embase on biomarkers, surrogate (outcomes, endpoints, markers, indicators), intermediate endpoints, and leading indicators, a quantitative surrogate validation schema was developed and subsequently evaluated at a stakeholder workshop. RESULTS: The search identified several classification schema and definitions. Components of these were incorporated into a new quantitative surrogate validation level of evidence schema that evaluates biomarkers along 4 domains: Target, Study Design, Statistical Strength, and Penalties. Scores derived from 3 domains the Target that the marker is being substituted for, the Design of the (best) evidence, and the Statistical strength are additive. Penalties are then applied if there is serious counterevidence. A total score (0 to 15) determines the level of evidence, with Level 1 the strongest and Level 5 the weakest. It was proposed that the term "surrogate" be restricted to markers attaining Levels 1 or 2 only. Most stakeholders agreed that this operationalization of the National Institutes of Health definitions of biomarker, surrogate endpoint, and clinical endpoint was useful. CONCLUSION: Further development and application of this schema provides incentives and guidance for effective biomarker and surrogate endpoint research, and more efficient drug discovery, development, and approval.

Published
2007

189. Testing of the preliminary OMERACT validation criteria for a biomarker to be regarded as reflecting structural damage endpoints in rheumatoid arthritis clinical trials: the example of C-reactive protein

Author

Keeling, Stephanie O, Landewe, Robert, van der Heijde, Desiree, Bathon, Joan, Boers, Maarten, Garnero, Patrick, Geusens, Piet, El-Gabalawy, Hani, Inman, Robert D, Kraus, Virginia B, Kvien, Tore K, Mease, Philip J, Ostergaard, Mikkel, Ritchlin, Chris, Syversen, Silje W, Maksymowych, Walter P, Keeling, Stephanie O, Landewe, Robert, van der Heijde, Desiree, Bathon, Joan, Boers, Maarten, Garnero, Patrick, Geusens, Piet, El-Gabalawy, Hani, Inman, Robert D, Kraus, Virginia B, Kvien, Tore K, Mease, Philip J, Ostergaard, Mikkel, Ritchlin, Chris, Syversen, Silje W, and Maksymowych, Walter P

Abstract

OBJECTIVE: A list of 14 criteria for guiding the validation of a soluble biomarker as reflecting structural damage endpoints in rheumatoid arthritis (RA) clinical trials was drafted by an international working group after a Delphi consensus exercise. C-reactive protein (CRP), a soluble biomarker extensively studied in RA, was then used to test these criteria. Our objectives were: (1) To assess the strength of evidence in support of CRP as a soluble biomarker reflecting structural damage in RA according to the draft validation criteria. (2) To assess the strength of recommendation for inclusion of individual criteria in the draft set. METHODS: A systematic literature review was conducted to elicit evidence in support of each specific criterion composing the 14-criteria draft set. A summary of the key literature findings per criterion was presented to both the working group and to participants in a special interest soluble biomarker group at OMERACT 8. Participants at OMERACT 8 were asked to rate the strength of evidence and the strength of the recommendation in support of each individual criterion on a 0-10 numerical rating scale. Working group members not present at OMERACT voted by a Web-based survey. RESULTS: Minimal data were extracted from the literature pertaining to those criteria listed under the category of truth. Ratings for strength of evidence were moderate to low (< 7) for CRP as a biomarker reflecting structural damage in RA; this was true for all criteria except those listed under the category of feasibility and 2 listed under the category of discrimination pertaining to assay reproducibility and evidence regarding sources of variability. Ratings for strength of recommendation for inclusion of each of the 14 criteria in the draft set were high (> 7) except for those criteria listed under the category of truth. CONCLUSION: The draft criteria serve as a useful template in the evaluation of the strength of evidence in support of a particular soluble, OBJECTIVE: A list of 14 criteria for guiding the validation of a soluble biomarker as reflecting structural damage endpoints in rheumatoid arthritis (RA) clinical trials was drafted by an international working group after a Delphi consensus exercise. C-reactive protein (CRP), a soluble biomarker extensively studied in RA, was then used to test these criteria. Our objectives were: (1) To assess the strength of evidence in support of CRP as a soluble biomarker reflecting structural damage in RA according to the draft validation criteria. (2) To assess the strength of recommendation for inclusion of individual criteria in the draft set. METHODS: A systematic literature review was conducted to elicit evidence in support of each specific criterion composing the 14-criteria draft set. A summary of the key literature findings per criterion was presented to both the working group and to participants in a special interest soluble biomarker group at OMERACT 8. Participants at OMERACT 8 were asked to rate the strength of evidence and the strength of the recommendation in support of each individual criterion on a 0-10 numerical rating scale. Working group members not present at OMERACT voted by a Web-based survey. RESULTS: Minimal data were extracted from the literature pertaining to those criteria listed under the category of truth. Ratings for strength of evidence were moderate to low (< 7) for CRP as a biomarker reflecting structural damage in RA; this was true for all criteria except those listed under the category of feasibility and 2 listed under the category of discrimination pertaining to assay reproducibility and evidence regarding sources of variability. Ratings for strength of recommendation for inclusion of each of the 14 criteria in the draft set were high (> 7) except for those criteria listed under the category of truth. CONCLUSION: The draft criteria serve as a useful template in the evaluation of the strength of evidence in support of a particular soluble

Published
2007

190. No erosive progression revealed by MRI in rheumatoid arthritis patients treated with etanercept, even in patients with persistent MRI and clinical signs of joint inflammation.

Author

Døhn, Uffe Møller, Skjødt, Henrik, Hetland, Merete, Vestergaard, Aage, Møller, Jakob M, Knudsen, Lene Surland, Ejbjerg, Bo Jannik, Thomsen, Henrik S, Ostergaard, Mikkel, Hetland, Merete Lund, Døhn, Uffe Møller, Skjødt, Henrik, Hetland, Merete, Vestergaard, Aage, Møller, Jakob M, Knudsen, Lene Surland, Ejbjerg, Bo Jannik, Thomsen, Henrik S, Ostergaard, Mikkel, and Hetland, Merete Lund

Abstract

The aim of this study is to investigate the course of magnetic resonance imaging (MRI) signs of inflammatory and destructive changes in rheumatoid arthritis (RA) wrist and metacarpophalangeal (MCP) joints during etanercept treatment. MRI of the non-dominant wrist and second to fifth MCP joints was performed in five clinical active RA patients before and 4 and 16 weeks after initiation of etanercept treatment. MRI was evaluated according to the EULAR-OMERACT RA MRI reference image atlas. The median 28-joint count disease activity score (DAS28; erythrocyte sedimentation rate based) was 5.6 (range 5.0-6.8) at baseline and 3.5 (1.5-4.1) at week 16 (decreased in all patients compared to baseline, Wilcoxon-Pratt, p < 0.05). The median MRI synovitis score was 18 (14-21), 18 (10-20) and 16 (10-20) at baseline, week 4 and 16, respectively (decreased in all patients compared to baseline, Wilcoxon-Pratt, p < 0.05), while corresponding MRI bone oedema scores were 4 (0-13), 3 (0-9) and 1 (0-3; NS). The median MRI bone erosion score was 27 (11-111; NS) at all time points. Four patients had identical total bone erosion scores at baseline and week 16, whereas one patient showed a reduced score. In conclusion, one patient showed erosive regression, while no patient showed erosive progression on MRI during 16 weeks of etanercept therapy; even though clinical and MRI signs of joint inflammation remained. This small study supports that erosive progression judged by MRI is minimal in RA patients treated with etanercept, even in joints with persistent inflammation. Udgivelsesdato: 2007-Nov, The aim of this study is to investigate the course of magnetic resonance imaging (MRI) signs of inflammatory and destructive changes in rheumatoid arthritis (RA) wrist and metacarpophalangeal (MCP) joints during etanercept treatment. MRI of the non-dominant wrist and second to fifth MCP joints was performed in five clinical active RA patients before and 4 and 16 weeks after initiation of etanercept treatment. MRI was evaluated according to the EULAR-OMERACT RA MRI reference image atlas. The median 28-joint count disease activity score (DAS28; erythrocyte sedimentation rate based) was 5.6 (range 5.0-6.8) at baseline and 3.5 (1.5-4.1) at week 16 (decreased in all patients compared to baseline, Wilcoxon-Pratt, p < 0.05). The median MRI synovitis score was 18 (14-21), 18 (10-20) and 16 (10-20) at baseline, week 4 and 16, respectively (decreased in all patients compared to baseline, Wilcoxon-Pratt, p < 0.05), while corresponding MRI bone oedema scores were 4 (0-13), 3 (0-9) and 1 (0-3; NS). The median MRI bone erosion score was 27 (11-111; NS) at all time points. Four patients had identical total bone erosion scores at baseline and week 16, whereas one patient showed a reduced score. In conclusion, one patient showed erosive regression, while no patient showed erosive progression on MRI during 16 weeks of etanercept therapy; even though clinical and MRI signs of joint inflammation remained. This small study supports that erosive progression judged by MRI is minimal in RA patients treated with etanercept, even in joints with persistent inflammation.

Published
2007

191. Consensus statement on blocking the effects of interleukin-6 and in particular by interleukin-6 receptor inhibition in rheumatoid arthritis and other inflammatory conditions

Author

Smolen, Josef S, primary, Schoels, Monika M, additional, Nishimoto, Norihiro, additional, Breedveld, Ferdinand C, additional, Burmester, Gerd R, additional, Dougados, Maxime, additional, Emery, Paul, additional, Ferraccioli, Gianfranco, additional, Gabay, Cem, additional, Gibofsky, Allan, additional, Gomez-Reino, Juan Jesus, additional, Jones, Graeme, additional, Kvien, Tore K, additional, Murakami, Miho, additional, Betteridge, Neil, additional, Bingham, Clifton O, additional, Bykerk, Vivian, additional, Choy, Ernest H, additional, Combe, Bernard, additional, Cutolo, Maurizio, additional, Graninger, Winfried, additional, Lanas, Angel, additional, Martin-Mola, Emilio, additional, Montecucco, Carlomaurizio, additional, Ostergaard, Mikkel, additional, Pavelka, Karel, additional, Rubbert-Roth, Andrea, additional, Sattar, Naveed, additional, Scholte-Voshaar, Marieke, additional, Tanaka, Yoshiya, additional, Trauner, Michael, additional, Valentini, Gabriele, additional, Winthrop, Kevin L, additional, de Wit, Maarten, additional, and van der Heijde, Désirée, additional

Published
2012
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192. After treat-to-target: can a targeted ultrasound initiative improve RA outcomes?: Table 1

Author

Wakefield, Richard J, primary, D'Agostino, Maria Antonietta, additional, Naredo, Esperanza, additional, Buch, Maya H, additional, Iagnocco, Annamaria, additional, Terslev, Lene, additional, Ostergaard, Mikkel, additional, Backhaus, Marina, additional, Grassi, Walter, additional, Dougados, Maxime, additional, Burmester, Gerd R, additional, Saleem, Benazir, additional, de Miguel, Eugenio, additional, Estrach, Cristina, additional, Ikeda, Kei, additional, Gutierrez, Marwin, additional, Thompson, Robert, additional, Balint, Peter, additional, and Emery, Paul, additional

Published
2012
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195. Greater body mass independently predicts less radiographic progression on X-ray and MRI over 1-2 years.

Author

Baker, Joshua F, Ostergaard, Mikkel, George, Michael, Shults, Justine, Emery, Paul, Baker, Daniel G, and Conaghan, Philip G

Abstract

Introduction: Greater body mass index (BMI) has been associated with less radiographic progression in rheumatoid arthritis (RA). We evaluated the association between BMI and joint damage progression as measured by X-ray and MRI.Methods: 1068 subjects with RA from two clinical trials of golimumab (GO-BEFORE and GO-FORWARD) had radiographs performed at weeks 0, 52 and 104 and evaluated using the van der Heijde-Sharp (vdHS) scoring system. Contrast-enhanced MRIs of the dominant wrist and hand were obtained at weeks 0, 12, 24, 52 and 104. Multivariable logistic regression evaluated the risk of radiographic progression for each BMI category (<25, 25-30, >30 kg/m(2)). Within GO-BEFORE, piecewise, robust generalised estimating equations marginal models assessed the probability of MRI erosion progression for each BMI category. Multivariable linear regression models assessed baseline associations between BMI and bone oedema (a precursor of bone erosion).Results: Higher BMI category was associated with a lower probability of progression in vdHS score at weeks 52 and 104 independent of potential confounders. Higher BMI was also independently associated with a lower probability of progression in MRI erosion score over 2 years. Subjects with greater BMI demonstrated less bone oedema independent of differences in other disease severity measures, including MRI synovitis in the same joints.Conclusions: Greater BMI is associated with a lower risk of progression on X-ray and MRI over 2 years. Subjects with greater BMI also demonstrate less bone oedema at baseline. Greater BMI may indicate a less aggressive RA phenotype and aid in risk stratification. [ABSTRACT FROM AUTHOR]

Published
2014
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196. Updating the OMERACT Filter: Implications for Imaging and Soluble Biomarkers.

Author

D'Agostino, Maria-Antonietta, Maarte n Boers, Kirwan, John, van der Heijde, Désirée, Ostergaard, Mikkel, Schett, Georg, Landewé, Robert B., R Maksymowych, Walter, Naredo, Esperanza, Dougados, Maxime, Iagnocco, Annamaria, Bingham III, Clifton O., Brooks, Peter M., Beaton, Dorcas E., Gandjbakhch, Frederique, Gossec, Laure, Guillemin, Francis, Hewlett, Sarah E., Kloppenburg, Margreet, and March, Lyn

Published
2014
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199. Contributors

Author

Abramson, Steven B., An, Kai-Nan, Andrade, Felipe, Atkinson, John P., Baeten, Dominique, Baughman, Robert P., Beaton, Dorcas E., Bennett, Robert, Benseler, Susanne M., Bertsias, George, Bhardwaj, Nina, Bijlsma, Johannes W.J., Bockenstedt, Linda K., Boers, Maarten, Boin, Francesco, Boumpas, Dimitrios T., Bresnihan, Barry, Brettler, Doreen B., Buckley, Christopher D., Budd, Ralph C., Burns, Christopher M., Cannella, Amy C., Chakravarty, Eliza F., Chang, Christopher, Cheng, Joseph S., Chiodo, Christopher P., Cleland, Leslie G., Clowse, Megan E., Cook, Paul P., Craft, Joseph E., Crofford, Leslie J., Cronstein, Bruce N., Crow, Mary K., Cunnane, Gaye, Cush, John J., Cutolo, Maurizio, Dall'Era, Maria, Dao, Kathryn H., Darrah, Erika, Davis, John M., III, DeGroot, Jeroen, Devin, Clint, Diamond, Betty, Díaz-González, Federico, Di Cesare, Paul E., Dixit, Rajiv, Drenth, Joost P.H., Dustin, Michael L., El-Gabalawy, Hani S., Elkon, Keith B., Erkan, Doruk, Fanouriakis, Antonios, Field, Max, Filer, Andrew, Firestein, Gary S., Fitzgerald, Oliver, Flaherty, John P., Flanagan, Adrienne M., Fortner, Karen A., Gabriel, Sherine E., Gaston, J.S. Hill, Gay, Steffen, Gershwin, M. Eric, Gibofsky, Allan, Ginsberg, Mark H., Goldring, Mary B., Goldring, Steven R., Golightly, Yvonne M., Goodman, Stuart, Gordon, Siamon, Grassi, Walter, Greenspan, Adam, Gregersen, Peter K., Grimaldi, Christine, Hajj-Ali, Rula A., Harper, Lorraine, Harris, Edward D., Jr., Haudenschild, Dominik R., Hellmann, David B., Holmdahl, Rikard, Hsu, Joyce J., Huddleston, James I., Huizinga, Thomas W.J., Hunder, Gene G., Hung, Emily W., Inman, Robert D., Iversen, Maura Daly, Jacobs, Johannes W.G., Jordan, Joanne M., Jorizzo, Joseph L., Kaufman, Kenton R., Kaufman, William S., Kavanaugh, Arthur, Keenan, Robert T., Khan, Shaukat, Koch, Alisa E., Kono, Dwight H., Krakow, Deborah, Lambert, Robert G.W., Landewé, Robert B.M., Lane, Nancy E., Langford, Carol A., Laskin, Daniel M., Laxer, Ronald M., Lee, David M., Lee, Lela A., Lee, Tzielan Chang, Lockshin, Michael D., Lories, Rik, Lozada, Carlos J., Lundberg, Ingrid E., Luqmani, Raashid, Luyten, Frank P., Mader, Reuven, Maksymowych, Walter P., Mandell, Brian, Martin, Scott David, Matteson, Eric L., McGirt, Matthew J., McInnes, Iain B., McNamara, Elizabeth Kaufman, Mikuls, Ted R., Miller, Mark S., Moder, Kevin G., Nagaraju, Kanneboyina, Naides, Stanley J., Nelson, Amanda E., Nigrovic, Peter A., Nistala, Kiran, Nowatzky, Johannes, O'Dell, James R., Okada, Yasunori, Orduño, Nataly Manjarrez, Ospelt, Caroline, Østergaard, Mikkel, Palmer, Bradley M., Panush, Richard S., Peng, Stanford L., Pillinger, Michael H., Polston, Gregory R., Porcelli, Steven A., Price, Mark D., Rasker, Johannes J., Reveille, John D., Roberts, W. Neal, Jr., Ronneberger, Monika, Rosen, Antony, Rosenbaum, James T., Rosenberg, Andrew E., Ruderman, Eric M., Ruutu, Merja, Salmon, Jane E., Samuels, Jonathan, Sandborg, Christy I., Savage, Caroline O.S., Saxena, Amit, Scher, Jose U., Schett, Georg, Seldin, David C., Simon, Anna, Siraj, Dawd S., Skinner, Martha, St. Clair, E. William, Stamp, Lisa K., Stone, John H., Straub, Rainer H., Sweeney, Susan E., Sweiss, Nadera J., Swigart, Carrie R., Symmons, Deborah, Szekanecz, Zoltan, Tak, Paul-Peter, Taylor, Peter C., Terkeltaub, Robert, Theofilopoulos, Argyrios N., Thomas, Ranjeny, Thornhill, Thomas S., Torralba, Karina D., Toth, Michael J., Tugwell, Peter, Tutuncu, Zuhre, Upchurch, Katherine S., van der Heijde, Désirée M.F.M., van der Helm-van Mil, Annette H.M., van der Linden, Sjef M., van der Meer, Jos W.M., van Laar, Jacob M., Varga, John, Wallace, Mark S., Warshaw, David M., Wedderburn, Lucy R., Werth, Victoria P., Wigley, Fredrick M., Wise, Christopher M., Wofsy, David, Wolfe, Frederick, Wollheim, Frank A., Wortmann, Robert L., Yelin, Edward, Yu, David, Zabriskie, John B., Zurier, Robert B., and Zuurmond, Anne-Marie

Published
2013
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200. After treat-to-target: can a targeted ultrasound initiative improve RA outcomes?

Author

Wakefield, Richard J, D'Agostino, Maria Antonietta, Naredo, Esperanza, Buch, Maya H, Iagnocco, Annamaria, Terslev, Lene, Ostergaard, Mikkel, Backhaus, Marina, Grassi, Walter, Dougados, Maxime, Burmester, Gerd R, Saleem, Benazir, de Miguel, Eugenio, Estrach, Cristina, Ikeda, Kei, Gutierrez, Marwin, Thompson, Robert, Balint, Peter, and Emery, Paul

Subjects
RHEUMATOID arthritis, ULTRASONIC imaging, SYNOVITIS, ARTHRITIS, AUTOIMMUNE diseases, SYNOVIAL membrane diseases
Abstract

For patients with rheumatoid arthritis (RA), remission can be achieved with tight control of inflammation and early use of disease modifying agents. The importance of remission as an outcome has been recently highlighted by European League Against Rheumatism recommendations. However, remission when defined by clinical remission criteria (disease activity score, simplified disease activity index, etc) does not always equate to the complete absence of inflammation as measured by new sensitive imaging techniques such as ultrasound (US) . There is evidence that imaging synovitis is frequently found in these patients and associated with adverse clinical and functional outcomes. This article reviews the data regarding remission, ultrasound imaging and outcomes in patients with RA to provide the background to a consensus statement from an international collaboration of ultrasonographers and rheumatologists who have recently formed a research network - the Targeted Ultrasound Initiative (TUI) group. The statement proposes that targeting therapy to PD activity provides superior outcomes compared with treating to clinical targets alone and introduces the rationale for a new randomised trial using targeted ultrasound in RA. [ABSTRACT FROM AUTHOR]

Published
2012
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