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Enregistrement W2138232309 · doi:10.1002/art.21291

International consensus guidelines for trials of therapies in the idiopathic inflammatory myopathies

2005· article· en· W2138232309 sur OpenAlex

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Notice bibliographique

RevueArthritis & Rheumatism · 2005
Typearticle
Langueen
DomaineMedicine
ThématiqueInflammatory Myopathies and Dermatomyositis
Établissements canadiensUniversity of TorontoSickKids FoundationHospital for Sick Children
Organismes subventionnairesNational Institute of Arthritis and Musculoskeletal and Skin Diseases
Mots-clésMedicineDermatomyositisInclusion body myositisPolymyositisMyositisAzathioprineDermatologyRashInflammatory myopathyEtiologyJuvenile dermatomyositisInternal medicineDisease

Résumé

récupéré en direct d'OpenAlex

Polymyositis (PM), dermatomyositis (DM), and inclusion body myositis (IBM) are acquired inflammatory muscle disorders of unknown etiology that are currently classified under the rubric of idiopathic inflammatory myopathy (IIM). All forms of IIM are characterized clinically by muscle weakness and pathologically by chronic muscle inflammation, although systemic manifestations involving many organ systems are common. Clinical subgroups have been recognized for many years and include adult-onset and juvenile-onset forms of PM and DM, myositis associated with another connective tissue disorder or malignancy, and the more recently recognized entity termed inclusion body myositis (1, 2). The presence of characteristic cutaneous features such as Gottron's papules and sign or the classic heliotrope rash distinguish DM from PM, and skin lesions may dominate the clinical presentation in some instances. Although the IIMs are rare diseases with an estimated incidence of 10 cases per million per year (3), they are associated with substantial morbidity and mortality. Currently available treatment of IIM is unsatisfactory. Corticosteroids are the only agents approved by the US Food and Drug Administration (FDA) for myositis. However, anecdotal reports and reports of case series do support the use of other immunosuppressive agents such as methotrexate and azathioprine in the treatment of myositis. Because of the rarity and heterogeneity of IIM, there is a paucity of controlled prospective clinical trials, and most published studies are from single referral centers reporting retrospectively on small numbers of patients followed up for relatively brief periods of time. Furthermore, accurate assessment of the effects of therapeutic interventions in IIM has been hampered by unreliable and insensitive outcome measures, as well as the challenge of distinguishing active and reversible disease from irreversible damage to muscle and other organs. Although previously published trials have utilized predefined outcome measures, no uniform criteria have been used to guide the conduct of these trials. As a result, different inclusion and exclusion criteria, trial duration, frequency of assessments, concomitant therapies, safety monitoring procedures, outcome measures, definitions of responses and disease flares, and stratifications of patients at outcome analysis have been used in almost all trials. Thus, it has been difficult to compare results from any two myositis trials even when the same agent is being studied, resulting in the current uncertainty regarding the safety and efficacy of most agents. In an effort to standardize the conduct and reporting of clinical studies in all forms of adult and juvenile IIM, and to coordinate and facilitate future clinical trials, an international multidisciplinary group, the International Myositis Assessment and Clinical Studies Group (IMACS), was founded in 2000. The IMACS consortium consists of more than 100 adult and pediatric specialists—including rheumatologists, neurologists, dermatologists, rehabilitation medicine physicians, statisticians, nurses, and others—with expertise in myositis. The coordination of studies of juvenile and adult-onset disease has been emphasized because of recent National Institutes of Health and FDA encouragement of parallel investigations in children and adults (4). IMACS has achieved a number of milestones toward its goals, which include the following: development of consensus on core set outcome measures to comprehensively describe myositis disease activity (5) (that are similar to those of another international group [6]); development of preliminary definitions of improvement, which reflect clinically meaningful change in the core set measures, for use as clinical trial end points, (7); and development and validation of new tools to assess myositis disease activity and damage (7, 8). Another goal of IMACS is to develop multidisciplinary, international consensus on the conduct of multicenter international trials of therapies for adult and juvenile IIM. This report describes the current IMACS consensus guidelines for the design and conduct of clinical trials in adult and pediatric patients with myositis. Given the limited number of controlled trials that have been conducted and the variability in expert opinion in the field, however, it is not the purpose of this report to propose a dogmatic approach to such issues. Rather, guidelines that are more structured in some aspects of trial design where consensus has been achieved, but less structured in other areas where data-driven evidence is lacking, are provided. In an effort to develop a consensus approach for the conduct of adult and juvenile myositis clinical trials, the design and features of 26 prospective treatment trials in IIM were reviewed (9-34). These included 14 trials of adult PM and DM, 5 of adult IBM, 5 prospective series of patients with juvenile DM, and 2 studies that combined adult PM, DM, and IBM patients. It was concluded that there is a clear lack of consistency in the design and conduct of clinical trials in adult and juvenile IIM, necessitating consensus among clinical investigators. The process to develop consensus for the design of adult and juvenile myositis clinical trials is described immediately below, with further detail provided in Appendix A. Several IMACS investigators outlined general topics regarding myositis clinical trial design issues that required consensus. An initial survey was then sent by e-mail to IMACS investigators (who included rheumatologists, neurologists, dermatologists, and physiatrists), and 41 adult and 29 pediatric specialists responded. Comments were reviewed and responses collated from both the adult and pediatric respondents to establish areas of both consensus (defined as agreement by at least two-thirds of the respondents) and lack of consensus. A second, focused survey, concentrating on major areas for which consensus was not achieved from the first survey, was sent by e-mail to the initial respondents and 7 additional investigators. Thirty-six adult and 31 pediatric specialists returned the second survey. The clinical trial design issues on which consensus was not achieved were then discussed at the third IMACS outcomes workshop, utilizing consensus-building approaches including nominal group and Delphi techniques (35). IMACS members who participated in the surveys and workshops are listed in Appendix B. Adult and pediatric working groups, each comprising 15 myositis experts, discussed these items, with ≥70% agreement required for consensus at this workshop. Both the adult and the pediatric specialists discussed issues of general applicability jointly, while issues that pertained exclusively to either group were discussed separately. Both adult and pediatric specialists agreed that the Bohan and Peter criteria (36, 37) should be utilized for the enrollment of adult and juvenile PM and DM patients into clinical trials and that probable or definite DM as defined by these criteria would be required. In accordance with these criteria, a diagnosis of probable or definite PM and DM requires that all other forms of myopathy, including infectious, metabolic, dystrophic, endocrine, and inclusion body myopathies, be excluded by appropriate clinical, laboratory, genetic, or pathologic techniques (36-38). There was some difference of opinion between the adult and pediatric specialists regarding the specifics of the required criteria, as discussed below. Dermatomyositis. Consensus was reached by both adult and pediatric specialists that the presence of Gottron's papules or heliotrope rash alone was sufficient to distinguish DM from PM; pediatric specialists also believed Gottron's sign was sufficient to distinguish juvenile DM from juvenile PM. It was decided that other criteria are necessary to enroll either adult DM or juvenile DM patients into a clinical trial. Pediatric specialists agreed that the criteria for probable juvenile DM were adequate and a muscle biopsy prior to entry was not necessary. Adult specialists did not come to consensus that a pathognomonic DM rash plus 2 other elements of the Bohan and Peter criteria were sufficient for enrollment of adult DM patients into a clinical trial, and adult specialists would leave this decision up to the investigators in individual clinical trials. Polymyositis. Adult and pediatric specialists agreed that an abnormal muscle biopsy result consistent with PM was necessary to enroll adult and juvenile PM patients into a clinical trial, due to concern about inadvertent inclusion of patients with non–immune-mediated myopathies (i.e., atypical dystrophies or toxic myopathies). Thus, patients without the pathognomonic rash of DM can be enrolled in a myositis trial and be considered to meet probable criteria only if one element of the criteria that are met is an abnormal muscle biopsy result consistent with PM. Other forms of myositis. It was the consensus that malignancy-associated myositis and myositis associated with another connective tissue disease (CTD) should be studied in separate clinical trials, but the definition of an associated CTD and the inclusion of such patients in a trial would be left to the trial's principal investigators so as not to exclude potentially eligible patients for study. IBM, defined according to the criteria for possible or definite IBM described by Griggs et al (2), should be studied separately from other myositis subgroups given the fact that it has distinguishing clinicopathologic characteristics and responses to treatment that differ from those of PM or DM. Subjects who develop myositis in association with an environmental exposure recognized as a probable risk factor for disease should also be studied separately. Consensus was achieved that clinical trials of refractory disease in adult and pediatric patients should include patients with muscle weakness of predetermined severity so response to the therapeutic agent can be adequately quantitated. Although patients who have chronic muscle weakness due to damage but do not have active disease will need to be excluded, the method of excluding such patients is not yet validated and will be decided by the investigators organizing the trial. Current approaches that appear promising (if available to investigators) include muscle biopsy, magnetic resonance imaging of muscle, and the use of the Myositis Disease Activity Assessment Tool and Myositis Damage Index (39, 40). Refractory disease was defined as disease with inadequate response to first-line agents such as corticosteroids and methotrexate (or another conventional immunosuppressive agent). It was agreed that, in order to assess corticosteroid treatment failure, adult patients had to have received 60 mg/day for at least 2 months, and pediatric patients had to have received 2.0 mg/kg/day prednisone for at least 2.5 months. It was further agreed that methotrexate treatment failure in pediatric patients could be defined as inadequate response to 25 mg/m2/week given parenterally for at least 3 months, but consensus regarding a definition of methotrexate failure in adult patients was not achieved. For other agents, the treatment regimen prior to trial entry was not agreed upon and should be decided by the team of investigators designing the trial. Patients with myositis-related organ dysfunction (e.g., cardiac, pulmonary, gastrointestinal, or cutaneous involvement) can be included in trials if the therapeutic agent under study is not toxic to the affected organ system. The inclusion of patients with non–myositis-related systemic illnesses is also reasonable if the organ system involved does not preclude adequate assessment of the myositis and is not adversely affected by the agent being studied. Inclusion of patients with hepatic disease, however, is problematic due to the difficulty of assessing transaminase (aspartate aminotransferase, alanine aminotransferase), aldolase, and lactate dehydrogenase elevations, which may be due to either hepatitis or myositis. There was consensus that additional inclusion criteria would be trial-specific and determined based on the therapeutic agent being studied. Examples of such criteria are a specified level of functional disability, inadequate response to other therapeutic agents, unacceptable corticosteroid toxicity, and persistence of cutaneous or other extramuscular manifestations. In trials involving patients with new-onset disease, adult specialists agreed that these patients should meet definite Bohan and Peter criteria and pediatric specialists agreed on probable Bohan and Peter criteria. The initial treatment regimen prior to trial entry was not agreed upon but should be decided by the team of clinical investigators designing the trial. Both adult and pediatric specialists agreed that concomitant corticosteroid treatment should be allowed in a clinical trial, but that tapering should take place according to a standardized dosage reduction regimen. At this time, there is no agreed-upon regimen for corticosteroid dosage reduction, and this should be determined by the investigator and may vary based on the agent being studied and the design of the trial. If methotrexate or another immunosuppressive agent is to be continued during a trial, the dosage should generally be held constant. Pediatric specialists agreed that methotrexate at a dosage of up to 30 mg/m2/week (maximum 50 mg/week) could be allowed as concomitant therapy in a myositis clinical trial. However, if methotrexate or another immunosuppressive agent is to be discontinued before a patient is enrolled in a trial, a pre-enrollment washout period of at least 1 month for methotrexate and 2–3 months for other immunosuppressive agents was suggested. The group reached consensus that it was appropriate to continue concomitant physical and occupational therapy in trials as long as these interventions were kept constant. It was agreed to exclude complementary and alternative medicines that may have potential effects on muscle, such as creatine, coenzyme Q, adrenal extracts, niacin, and anabolic/male steroids. The use of placebos in clinical trials is controversial, and may be an even more contentious issue for pediatric studies. However, it is important to note that, depending on the design of a trial, “placebo” does not necessarily mean “no therapy”; it may refer to the use of placebo in addition to background therapy maintained at a constant dosage, which is often viewed as more acceptable by physicians enrolling patients in a clinical trial. In fact, adult and pediatric specialists did not find it acceptable for patients with refractory myositis to be receiving no background therapy while enrolled in a trial. Nevertheless, the use of a placebo for a limited period of time in both adult and pediatric myositis trials was deemed acceptable. The median allowable time according to adult specialists was 8 weeks, while pediatricians agreed that a median of 6 weeks for placebo administration was more appropriate for trials involving children with IIM. The design of placebo-controlled trials should take these time points into consideration so that patients with evidence of or lack of response to therapy may appropriate and treatment for active The of a clinical trial the time in which the is as well as a period of appropriate determined based on the agent being studied, safety or other issues such as the of the trial. It was the consensus of the adult specialists that a of 6 months was the time acceptable for therapeutic trials in PM and DM. However, depending on the being studied, the could 6 months. Pediatric specialists agreed on a mean trial of 5 months for both and (i.e., studies to assess and of an but that trials be with a mean of months. There was consensus among both adult and pediatric specialists that the frequency of assessment should be for both safety and monitoring in trials of adult and juvenile DM and PM. The use of trial such as or placebo and the study of agents with more response could for the placebo use without assessment of the end points in myositis trials or safety may be conducted time However, it should be that if a trial a result but a is included for only 6 or 8 weeks, may regarding the efficacy of use of the (i.e., the or period The study of efficacy is of for to efficacy time. for use in are studied in controlled trials of months (4). A of the study may be used to evidence of The National has defined the to standardize of in clinical trials, and consensus was reached to this system for assessing and in adult and pediatric IIM patients enrolled in trials. It was decided that, of the regimen in a myositis trial, be determined according to the agent being studied and the design of the should continue to be during the Adult and pediatric specialists agreed that these should be at for a of months, but the guidelines for will on the of the agent studied during the initial treatment As discussed IBM is viewed as a clinically myositis due to its generally and the difficulty in assessing its response to adult specialists a mean treatment of at least months in IBM clinical trials. outcome efficacy measures can be further and should be at The IMACS core set disease activity measures and preliminary definitions of should be used in trials of adult and juvenile DM and PM. These should include the definition for adult disease and for pediatric as a of improvement, that 3 of any 6 core set measures by with no more than 2 by that include muscle that investigators designing clinical trials in myositis this published definition of as the outcome measures of could also include any of the other IMACS preliminary definitions of improvement, as well as individual core set measures of or other measures as determined by the investigators in a given study. for disease in a clinical trial, to be used as the for treatment as and alternative therapies, were defined at the IMACS workshop. These include of the as by the by on a and of of muscle by or of extramuscular organ disease activity of gastrointestinal, pulmonary, and by on a or of any 3 of 6 IMACS core set activity measures by It was also that in cardiac, pulmonary, or should be considered as criteria for and could also to of patients from the trial or of treatment as Both adult and pediatric specialists agreed that further is to and the of and criteria to myositis disease the criteria for therapy were by the IMACS they were not consensus to the same as were the other guidelines in clinical response and clinical were defined in a similar to that used for juvenile idiopathic As in the case of these criteria do not imaging or biopsy due to the difficulty of these in multicenter international trials clinical response and clinical were as lack of evidence of active myositis while receiving therapy and lack of evidence of active myositis while not receiving any for a In order to clinical response and in IIM one the current of myositis disease activity to these There was consensus that lack of evidence of myositis disease activity is defined as by and extramuscular assessments, muscle and and muscle muscle and were defined as to change in the of the measures of these at least a It is possible that patients these definitions may continue to develop weakness due to damage or disease imaging or biopsy in a of in a trial would be in an of disease These clinical, definitions prospective that there would be no to the analysis of the in a clinical trial, adult and pediatric specialists agreed that patients should be for outcome may include IIM clinical of disease, and of muscle weakness or physical dysfunction at the time of and extramuscular organ such as disease and For adult and muscle were considered important and for juvenile cutaneous or and were as important to As outlined in there are a number of important issues to the design of clinical trials in adult and pediatric patients with inflammatory myopathy, which further These areas will need to be in future utilizing data-driven and other consensus-building The lack of consensus on the conduct and reporting of clinical trials in the IIMs has hampered therapeutic in the myositis and it difficult to compare studies. standardized outcome assessments, in other diseases such as systemic and have in consensus approaches to trial design issues A group of international myositis experts, termed has in an to develop for the conduct of studies in the inflammatory The results the first multidisciplinary effort to standardize the conduct of myositis clinical trials. these are they a for investigators in patients with utilizing a and All to this consensus however, the to assess these guidelines and to as trials are and The IMACS Clinical Studies will as a for such and in the for IIM corticosteroids and other immunosuppressive agents that have been studied of these and other or immunosuppressive in myositis are and propose these guidelines in order to and therapeutic agents in multicenter trials. The goal of IMACS has been to among members of all that and study patients with inflammatory myopathy and to and trials. The previously published IMACS with the guidelines set in this consensus the for such these guidelines are based on the of the IMACS that the of a trial may an In the first consensus guidelines for trials of interventions in IIM have been in an to standardize these for international in adults and These guidelines will be as additional All the need for coordination among all specialists for patients with the prospective validation of these and to the issues of trial design discussed are to other members of IMACS for and this The of and on the are also the for and without which these workshops could not have been Myositis and and of Health members of the Group for the process and and of the National of and and for are to the of these the National of Health the National of and and The of the National of and the Myositis and The Myositis The IMACS outlined the general topics regarding myositis clinical trial design issues in A survey in which all of these was sent by e-mail to all IMACS investigators. were received from 41 adult and 29 pediatric specialists neurologists, dermatologists, and In an IMACS members were of the for the survey develop consensus on clinical trial design issues as a first toward multicenter international trials of therapies for For each of the issues in IMACS investigators were provided background from the 26 prospective IIM studies published to to in the survey were that a second e-mail survey on the major areas of from the first survey would that at the IMACS outcomes workshops would consensus-building approaches including nominal group and Delphi and that the results of the consensus process would be The responses to the in survey 1 were collated to establish both areas of consensus (defined as at least two-thirds agreement utilizing a Delphi and areas of Comments were reviewed and the results were separately for the adult respondents and the pediatric specialists respondents clinical trial design issues were discussed by the of survey 1 and a second, and more survey was sent by e-mail to survey 1 and 7 additional investigators. Thirty-six adult and 31 pediatric specialists returned which were separately the same guidelines as for the first survey. A of the clinical trial design issues was at the second IMACS adult and pediatric working groups, each comprising 15 myositis experts, discussed the a nominal group and in an to The working of IMACS members of surveys 1 and and they were of the of both surveys by IMACS not all survey respondents the workshop. Consensus at this was defined as ≥70% of the issues were discussed by both the adult and pediatric while more topics were discussed separately. A consensus the guidelines for clinical trials in adult and juvenile which is the of this was of the International Myositis Assessment and Clinical Studies in addition to the of this are as Peter do

Récupéré en direct depuis OpenAlex et désinversé. Les résumés ne sont pas conservés dans cette base de données : les index inversés représentent 8,6 Go des 9,3 Go de texte de la base, et le serveur dispose de 13 Go libres.

Prédiction distillée sur la base complète

Imitation des enseignants

Ni prévalence calibrée, ni vérité terrain. Validation humaine à venir. Apprise à partir de 10 348 étiquettes directes de Codex et de 10 348 étiquettes directes de Gemma. Le mode candidate est l'union des têtes enseignantes seuillées; le consensus est leur intersection. Ces sorties portent le statut machine_predicted_unvalidated et ne sont ni des étiquettes humaines ni des étiquettes directes de modèles de pointe.

score de la tête « metaresearch » (Codex)0,004
score de la tête « metaresearch » (Gemma)0,003
Version: codex-gemma-dda1882f352aStatut de validation: machine_predicted_unvalidated
Catégories candidatesaucune
Catégories consensuellesaucune
DomaineSignal candidat: aucune · Signal consensuel: aucune
Devis d'étudeSignal candidat: Autre devis · Signal consensuel: aucune
GenreSignal candidat: Empirique · Signal consensuel: Empirique
Score de désaccord entre enseignants0,867
Score d'incertitude au seuil0,635

Scores Codex et Gemma par catégorie

CatégorieCodexGemma
Métarecherche0,0040,003
Méta-épidémiologie (sens strict)0,0000,000
Méta-épidémiologie (sens large)0,0010,000
Bibliométrie0,0000,000
Études des sciences et des technologies0,0000,000
Communication savante0,0000,000
Science ouverte0,0000,000
Intégrité de la recherche0,0000,000
Charge utile insuffisante (le modèle a refusé de juger)0,0000,000

Scores machine (provisoires)

Les deux têtes enseignantes du modèle étudiant, lues sur ce travail. Un score ordonne la base pour la relecture; il n'affirme jamais une catégorie, et le statut de validation accompagne chaque rangée tel quel.

Scores de référence d'un modèle non mature (critères de maturité non atteints, 7 itérations). Un score ordonne; il n'affirme jamais une catégorie.

Tête enseignante Opus0,059
Tête enseignante GPT0,341
Écart entre enseignants0,282 · la distance entre les deux têtes enseignantes sur ce seul travail
Statut de validationscore_only:v0-immature-baseline · tel quel depuis la passe de notation : score_only signifie que le nombre peut ordonner les travaux, et qu'aucune étiquette de catégorie n'en découle