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Group-Randomized Trials

Group-Randomized Trials. Distinguishing characteristics The unit of assignment is an identifiable group. Different groups are allocated to each condition. The units of observation are members of the groups. The number of groups allocated to each condition is usually limited.

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Group-Randomized Trials

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  1. Group-Randomized Trials • Distinguishing characteristics • The unit of assignment is an identifiable group. • Different groups are allocated to each condition. • The units of observation are members of the groups. • The number of groups allocated to each condition is usually limited.

  2. Group-Randomized Trials • Primary advantages • Randomization provides the statistical basis for the assumption of independence at the group level. • With proper randomization and enough groups… • Potential sources of bias are fairly distributed across the study conditions. • Inferences based on a valid analysis can be as strong as those obtained from a randomized clinical trial. • For this reason, the GRT is the gold standard for design in public health and medicine when allocation of identifiable groups is necessary.

  3. Group-Randomized Trials • Primary disadvantages • There is extra variation attributable to the groups. • This increases the standard error of the intervention effect. • The number of groups is often limited. • This limits error degrees of freedom and reduces the effectiveness of randomization. • Together, these problems can threaten internal validity and power in small trials. • At the same time, logistics and cost can threaten the viability of large trials.

  4. The Warning • Randomization by cluster accompanied by an analysis appropriate to randomization by individual is an exercise in self-deception, however, and should be discouraged. Cornfield (1978)

  5. Progress Addressing the Major Disadvantages • Extra variation • Regression adjustment for covariates • Modeling time • Limited degrees of freedom • Proper planning • Borrowing information from similar studies

  6. Other Recent Methodological Developments • Analysis methods • Small sample corrections for GEE • Methods for survival analysis • Improved power for permutation tests • Mediation models • Missing data • Nonlinear mixed models • Reference • Murray, D. M., Varnell, S. P., & Blitstein, J. L. (2004). Design and analysis of group-randomized trials: A review of recent methodological developments. AJPH, 94(3), 423-432.

  7. State of the Practice • How are we doing? • Sample size estimation • Analysis methods • 58 GRTs published in AJPH and Prev Med, 1998-2002 • Reference • Varnell, S., Murray, D. M., Janega, J. B., & Blitstein, J. L. (2004). Design and analysis of group-randomized trials: A review of recent practices. AJPH,94(3), 393-399.

  8. Findings • Only 16% reported evidence of using appropriate methods for sample size calculations. • Similar to 19% in Simpson et al., 1995 review • 54% reported only analyses judged to be appropriate. • Similar to 57% in Simpson et al., 1995 review • That figure rises to 68% if we use Simpson et al.'s criteria • 19% reported only analyses deemed invalid. • 26% reported a mix of methods. • Some progress since 1995, but still need for improvement, especially with regard to more recent findings.

  9. Summary and Recommendations • Many questions do not require a GRT. • Formative research • Other questions may require a GRT design but not a full-blown GRT analysis. • Feasibility or preliminary evidence of efficacy • Here, estimate effect and/or ICC, but avoid causal inference. • Other questions cannot be addressed using a GRT. • Policy change at large aggregate level • Use quasi- or natural experiments if they will provide useful information efficiently. • Do not ignore the design and analytic challenges inherent in nested designs. • For efficacy studies, use individual-level randomization whenever possible.

  10. Summary and Recommendations • Reserve GRTs for situations in which… • Experimental evidence is needed for causal inference, • Individual randomization is not possible, • There is preliminary evidence for feasibility and efficacy, • There is sufficient information available to size the study. • Use the available tools to do the best job possible. • Match the design to the research question. • Use appropriate analysis methods. • Ensure adequate power. • Choose a valid analysis that minimizes the SE for the intervention effect. • Build in sufficient replication at the group level.

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