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      Definition of levels of evidence (LoE) and overall strength of evidence (SoE)

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      Global Spine Journal
      Georg Thieme Verlag KG

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          Abstract

          Definition of the Different Levels of Evidence (LoE) Articles on treatment Studies of therapy Level Risk of bias Study design Criteria I Low risk Study adheres to commonly held tenets of high quality design, execution and avoidance of bias Good quality RCT • Random sequence generation • Allocation concealment• Intent-to-treat analysis• Blind or independent assessment for important outcomes• Co-interventions applied equally• F/U rate of 80%+• Adequate sample size II Moderately low risk Study has potential for some bias; study does not meet all criteria for level I, but deficiencies not likely to invalidate results or introduce significant bias Moderate or poor quality RCTGood quality cohort • Violation of one of the criteria for good quality RCT• Blind or independent assessment in a prospective study, or use of reliable dataa in a retrospective study• Co-interventions applied equally• F/U rate of 80%+• Adequate sample size• Controlling for possible confoundingb III Moderately high risk Study has significant flaws in design and/or execution that increase potential for bias that may invalidate study results Moderate or poor quality cohortCase-control • Violation of any of the criteria for good quality cohort• Any case-control design IV High risk Study has significant potential for bias; lack of comparison group precludes direct assessment of important outcomes Case series • Any case series design a Outcome assessment is independent of healthcare personnel judgment. Reliable data are data such as mortality or re-operation. b Authors must provide a description of robust baseline characteristics, and control for those that are unequally distributed between treatment groups. Articles on prognosis or risk Studies of prognosis Level Risk of bias Study design Criteria I Low risk Study adheres to commonly held tenets of high quality design, execution and avoidance of bias Good quality cohorta • Prospective design• Patients at similar point in the course of their disease or treatment• F/U rate of ≥ 80%b • Patients followed long enough for outcomes to occur • Accounting for other prognostic factorsc II Moderately low risk Study has potential for some bias; does not meet all criteria for level I but deficiencies not likely to invalidate results or introduce significant bias Moderate quality cohort • Prospective design, with violation of one of the other criteria for good quality cohort study • Retrospective design, meeting all the rest of the criteria in level I III Moderately high risk Study has flaws in design and/or execution that increase potential for bias that may invalidate study results Poor quality cohortGood quality case-control or cross-sectional study • Prospective design with violation of 2 or more criteria for good quality cohort, or• Retrospective design with violation of 1 or more criteria for good quality cohort• A good case-control studyd • A good cross-sectional studye IV High risk Study has significant potential for bias; does not include design features geared toward minimizing bias and/or does not have a comparison group Poor quality case-control or cross-sectionalCase seriesd • Other than a good case-control study• Other than a good cross-sectional study• Any case seriesf design a Cohort studies follow individuals with the exposure of interest over time and monitor for occurrence of the outcome of interest. b Applies to cohort studies only. c Authors must consider other factors that might influence patient outcomes and should control for them if appropriate. d A good case-control study must have the all of the following: all incident cases from the defined population over a specified time period, controls that represent the population from which the cases come, exposure that precedes an outcome of interest, and accounting for other prognostic factors. e A good cross-sectional study must have all of the following: a representative sample of the population of interest, an exposure that precedes an outcome of interest (e.g., sex, genetic factor), an accounting for other prognostic factors, and for surveys, at least a 80% return rate. f A case-series design for prognosis is one where all the patients in the study have the exposure of interest. Since all the patients have the exposure, risks of an outcome can be calculated only for those with the exposure, but cannot be compared with those who do not have the exposure. For example, a case-series evaluating the effect of smoking on spine fusion that only recruits patients who smoke can simply provide the risk of patients who smoke that result in pseudarthrosis but cannot compare this risk to those that do not smoke. Determination of Overall Strength of Evidence (SoE) After individual article evaluation, the overall body of evidence with respect to each outcome is determined based on precepts outlined by the Grades of Recommendation Assessment, Development and Evaluation (GRADE) Working Group and recommendations made by the Agency for Healthcare Research and Quality (AHRQ). Qualitative analysis is performed considering the AHRQ required and additional domains. The table below provides an outline of the method used to determine the final SoE. Strength of Evidence for Existing Systematic Reviews Level of evidence ratings for Cochrane reviews and other systematic reviews are assigned a baseline score of HIGH if RCTs were used, LOW if observational studies were used. The rating can be upgraded or downgraded based on adherence to the core criteria for methods, qualitative, and quantitative analyses for systematic reviews (there is a reference/evaluation table for this). The following four possible levels and their definition are reported: High: High confidence that the evidence reflects the true effect. Further research is very unlikely to change our confidence in the estimate of effect. Moderate: Moderate confidence that the evidence reflects the true effect. Further research may change our confidence in the estimate of effect and may change the estimate. Low: Low confidence that the evidence reflects the true effect. Further research is likely to change the confidence in the estimate of effect and likely to change the estimate. Insufficient or very low: Evidence either is unavailable or does not permit a conclusion. All AHRQ “required” and “additional” domainsa are assessed. Only those that influence the baseline grade are listed in table. Baseline strength: Risk of bias (including control of confounding) is accounted for in the individual article evaluations. High = majority of articles level I/II; low = majority of articles level III/IV Downgrade: Inconsistencyb of results (1 or 2); Indirectness of evidence (1 or 2); Imprecision of effect estimates (1 or 2); Sub-group analyses not stated apriori and no test for interaction (2) Upgrade: Large magnitude of effect (1 or 2); Dose response gradient (1) Outcome Strength of evidence Conclusions and comments Baseline Downgrade Upgrade Outcome High Summary of findings High Level I/II studies No Consistent, direct, and precise estimates No Outcome Moderate Summary of findings Low Level III studies No Consistent, direct, and precise estimates Yes Large effect Outcome Low Summary of findings High Level I/II studies Yes (2) InconsistentIndirect No a Required domains: risk of bias, consistency, directness, precision. Plausible confounding that would decrease observed effect is accounted for in our baseline risk of bias assessment through individual article evaluation. Additional domains: dose-response, strength of association, publication bias. b Single study = “consistency unknown.” Definitions of the Different Levels of Evidence for Reliability Studies Level Study type Criteria 1 Good quality study • Broad spectrum of persons with the expected condition• Adequate description of methods for replication• Blinded performance of tests, measurements or interpretation• Second test/interpretation performed independently of the first 2 Moderate quality • Violation of any one of the criteria for a good quality study 3 Poor quality study • Violation of any two of the criteria 4 Very poor quality study • Violation of all three of the criteria

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          Author and article information

          Journal
          Global Spine J
          Global Spine J
          10.1055/s-00000177
          Global Spine Journal
          Georg Thieme Verlag KG (Stuttgart · New York )
          2192-5682
          2192-5690
          December 2015
          : 5
          : 6
          : 539
          Article
          CoE
          10.1055/s-0035-1570346
          4671889
          26682110
          d8568f1c-97d2-44b2-8aa3-96431a2a4bdf
          © Thieme Medical Publishers
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