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بسم الله الرحمن الرحیم

بسم الله الرحمن الرحیم. HOW to use CONSORT. Randomisation. Population. Experimental intervention. Outcome. Sample. Outcome. Control intervention. Time. Randomised, controlled trial. scales and their modifications including:. Jadad Maastricht Delphi List PEDro

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بسم الله الرحمن الرحیم

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  1. بسم الله الرحمن الرحیم

  2. HOW to use CONSORT

  3. Randomisation Population Experimental intervention Outcome Sample Outcome Control intervention Time Randomised, controlled trial

  4. scales and their modifications including: Jadad Maastricht Delphi List PEDro Maastricht-Amsterdam List (MAL) Van Tulder Bizzini Chalmers Reisch Andrew Imperiale Detsky Cho and Bero Balas Sindhu Downs and Black Nguyen Oxford Pain ValidityScale (OPVS) Arrive´ CONSORT Yates

  5. http://www.consort-statement.org/

  6. How CONSORT began • In 1993, 30 experts comprised of medical journal editors, clinical trialists, epidemiologists, and methodologists met in Ottawa, Canada with the aim of developing a new scale to assess the quality of randomized controlled trial (RCT) reports • One outcome of the meeting was the Standardized Reporting of Trials (SORT) statement .This statement consisted of a 32-item checklist and flow diagram in which investigators were encouraged to report on the various aspects of how RCTs were conducted.

  7. Concurrently, and independently, another group of experts, the Asilomar Working Group on Recommendations for Reporting of Clinical Trials in the Biomedical Literature, convened in Asilomar (California), USA, were working on a similar mandate • At the suggestion of Drummond Rennie, Deputy Editor of JAMA, representatives from both groups met in 1996, in Chicago, USA.. The meeting resulted in the Consolidated Standards of Reporting Trials (CONSORT) Statement, which was first published in 1996 

  8. Influence on related reporting guidelines • PRISMA for systematic reviews of randomized trials; MOOSE for systematic reviews of observational studies; STARD for diagnostic accuracy studies; REMARK for tumor marker prognostic studies; TREND for non-randomized evaluations of behavioural and public health interventions; STROBE for observational studies.

  9. CONSORT……stands for • Consolidated Standards of Reporting Trials, encompasses various initiatives developed by the CONSORT Group to alleviate the problems arising from inadequate reporting of randomized controlled trials (RCTs).

  10. The main product of CONSORT • The CONSORT Statement comprises a 25-item checklist and a flow diagram, along with some brief descriptive text. The checklist items focus on reporting how the trial was designed, analyzed, and interpreted; the flow diagram displays the progress of all participants through the trial.

  11. Title and Abstract • Item 1a - Identification as a randomised trial in the title. • Item 1b - Structured summary of trial design, methods, results, and conclusions To help ensure that a study is appropriately indexed and easily identified, authors should use the word “randomised” in the title to indicate that the participants were randomly assigned to their comparison groups

  12. Introduction: Background-Objectives • Item 2a - Scientific background and explanation of rationale • Item 2b - Specific objectives or hypotheses

  13. Method: • Trial Design :Item 3a - Description of trial design (such as parallel, factorial) including allocation ratio • Changes to trial design: Item 3b - Important changes to methods after trial commencement (such as eligibility criteria), with reasons • Participants: Item 4a - Eligibility criteria for participants • Study settings: Item 4b- Settings and locations where the data were collected

  14. Interventions • Item 5 - The interventions for each group with sufficient details to allow replication, including how and when they were actually administered

  15. Outcomes • Item 6a - Completely defined pre-specified primary and secondary outcome measures, including how and when they were assessed • Changes to outcomes :Item 6b - Any changes to trial outcomes after the trial commenced, with reasons

  16. Sample size • Item 7a - How sample size was determined • Interim analyses and stopping guidelines:Item 7b - When applicable, explanation of any interim analyses and stopping guidelines

  17. Randomization: • sequence generationItem 8a - Method used to generate the random allocation sequence • Randomization: typeItem 8b - Type of randomisation; details of any restriction (such as blocking and block size)

  18. Randomisation: allocation concealment mechanism • Item 9 - Mechanism used to implement the random allocation sequence (such as sequentially numbered containers), describing any steps taken to conceal the sequence until interventions were assigned • Item 10 - Who generated the allocation sequence, who enrolled participants, and who assigned participants to interventions

  19. Blinding • Item 11a - If done, whowas blinded after assignment to interventions (for example, participants, care providers, those assessing outcomes) and how

  20. Blinding • Participants • Providers • Raters/data collectors • Data analysts

  21. Blinding • The term “blinding” or “masking” refers to withholding information about the assigned interventions from people involved in the trial who may potentially be influenced by this knowledge. • Blinding is an important safeguard against bias, particularly when assessing subjective outcomes

  22. Similarity of interventions • Item 11b - If relevant, description of the similarity of interventions

  23. Statistical methods • Item 12a - Statistical methods used to compare groups for primary and secondary outcomes • Additional analyses: • Item 12b - Methods for additional analyses, such as subgroup analyses and adjusted analyses

  24. Participant Flow • A diagram is strongly recommended. • Item 13a - For each group, the numbers of participants who were randomly assigned, received intended treatment, and were analyzed for the primary outcome

  25. Losses and exclusions • Item 13b - For each group, losses and exclusions after randomisation, together with reasons

  26. Recruitment • Item 14a - Dates defining the periods of recruitment and follow-up • Reason for stopped trial : • Item 14b - Why the trial ended or was stopped

  27. Baseline data • Item 15 - A table showing baseline demographic and clinical characteristics for each group

  28. Numbers analyzed • Item 16 - For each group, number of participants (denominator) included in each analysis and whether the analysis was by original assigned groups

  29. Outcomes and estimation • Item 17a - For each primary and secondary outcome, results for each group, and the estimated effect size and its precision (such as 95% confidence interval)

  30. Binary outcomes • Item 17b - For binary outcomes, presentation of both absolute and relative effect sizes is recommended

  31. Ancillary analyses • Item 18 - Results of any other analyses performed, including subgroup analyses and adjusted analyses, distinguishing pre-specified from exploratory

  32. Harms • Item 19 - All important harms or unintended effects in each group

  33. Limitations • Item 20 - Trial limitations, addressing sources of potential bias, imprecision, and, if relevant, multiplicity of analyses

  34. Medicine recommends that authors structure the Discussion section by presenting • (1) a brief synopsis of the key findings, • (2) consideration of possible mechanisms and explanations, • (3) comparison with relevant findings from other published studies

  35. (4) limitations of the present study (and methods used to minimise and compensate for those limitations) • (5) a brief section that summarises the clinical and research implications of the work, as appropriate

  36. Although discussion of limitations is frequently omitted from research reports, identification and discussion of the weaknesses of a study have particular importance

  37. Generalisability • Item 21 - Generalisability (external validity, applicability) of the trial findings

  38. Appraising Applicability • Is my patient similar to the study population? • Is the treatment feasible in my clinical setting? Will potential benefits of treatment outweigh potential harms of treatment for my patient?

  39. Interpretation • Item 22 - Interpretation consistent with results, balancing benefits and harms, and considering other relevant evidence

  40. Registration • Item 23 - Registration number and name of trial registry

  41. Protocol • Item 24 - Where the full trial protocol can be accessed, if available

  42. Funding • Item 25 - Sources of funding and other support (such as supply of drugs), role of funders

  43. همتم بدرقه راه کن ای طایر قدس که درازست ره مقصد و من نو سفرم ای نسیم سحری بندگی من برسان که فراموش مکن وقت دعای سحرم

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