Table 2.
A standard table for reporting the use of blinding in randomized trials of pharmaceutical interventions
| Group or individual blindeda | Information withheldb | Method of blindingc,d | Blinding compromised |
|---|---|---|---|
| Required fields to be completed for all trials described as blinded | |||
| Person assigning participants to groups | Group assignment | Concealed allocation schedule | No |
| Participants | Group assignment | Placebo medications; sham surgeries | No |
| Care providers | Group assignment | Not told of group assignment | No |
| Data collectors and managers | Group assignment | Not told of group assignment | No |
| Outcome assessors | Purpose of study; group assignment; participant characteristics | Participants given numerical identifiers | No |
| Statisticians | Participant and group identities | Participants and groups given numerical identifiers | No |
| Supplemental fields for all blinded groups or individuals not mentioned above | |||
| Trial manager | Not applicable | . . . | . . . |
| Pharmacists | Not applicable | . . . | . . . |
| Laboratory technicians | Participant identities | Participants given numerical identifiers | |
| Outcome adjudicators | Group assignment | Groups given numerical identifiers | Yes [put details in text] |
| Data monitoring and safety committees | Not applicable | . . . | . . . |
| Manuscript writers | Not blinded | . . . | . . . |
aOther groups or individuals in a trial that were capable of being blinded should be listed in the table, and whether or not they were blinded in the study should be indicated. Individuals with dual responsibilities, such as caregiving and data collecting, should be identified by combining the entries in the same row heading
bAlthough group assignment is the information most commonly withheld in a blinded trial, data assessors, such as pathologists and radiologists, are often blinded to the purpose of the trial, group assignment, and the demographic and clinical characteristics of participants whose biopsy samples or images they are interpreting
cIn many cases, authors should determine before the trial begins whether the method of blinding had a reasonable chance of being effective, including establishing the similarity between active and placebo preparations and the bioequivalent availability for two or more active drugs [33]. Testing the effectiveness of blinding after the trial has ended is uninformative because the results cannot be separated from pre-trial expectations of the success of the intervention [32]
dIf blinding has been compromised, authors should report the fact and indicate the potential implications the loss of blinding might have for interpreting the results