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Educação Continuada: Metodologia Científica

Loss to follow-up and missing data: important issues that can affect your study results

Perda de seguimento e dados faltantes: questões importantes que podem afetar os resultados do seu estudo

Juliana Carvalho Ferreira1,2,a, Cecilia Maria Patino1,3,b

DOI: http://dx.doi.org/10.1590/1806-3713/e20190091

Investigators used data from the São Paulo State Tuberculosis Control Program database to evaluate the association between the place of diagnosis and treatment outcomes. They reported that 25% of new tuberculosis cases were diagnosed in emergency facilities and that, in comparison with patients diagnosed in outpatient settings, they were more likely to have unsuccessful treatment outcomes, including loss to follow-up (in 12%) and death (in 10%).(1)



LOSS TO FOLLOW-UP AND TYPES OF MISSING DATA



To study associations of an exposure (in cohort studies) or of an intervention (in randomized controlled trials) with clinical outcomes prospectively, investigators collect exposure/intervention information at study entry and then follow study participants over time and collect outcome data. If follow-up is incomplete or interrupted, leading to missing data at the end of the study, this could impact the internal validity of the study. Participants with missing data, compared with those with complete data, may differ systematically, for example when loss to follow-up is related to the death of participants.



Missing data occur for multiple reasons: 1. the variable of interest is not measured by the research team (e.g., forgetting to measure weight at baseline); 2. the study participant misses a scheduled study visit or test; or 3. the variable is measured but the team fails to register the variable value on the data collection form. However, loss to follow-up, where patient data is not available until the end of the follow-up period, is the most critical mechanism of missing data, because it might include missing outcome data, which is crucial to answer the research question.



Missing data are classified as missing completely at random (MCAR), when missingness is not related to the exposure, covariates, or the outcome; missing at random (MAR), when missingness is related to the exposure or confounders, but not the outcome; and missing not at random (MNAR), when missingness might be related to the outcome (Chart 1).(2) Loss to follow-up and missing data can threaten the internal validity of a study even if the mechanism is MCAR, in which we consider that the remaining participants are a random sample of the initial study population, because the study power will be decreased. If the mechanism is MAR, adjustments and imputation methods can be used, but that might introduce biases to the study. If the mechanism is MNAR, there is a serious risk of biased results.(3)

 








HOW TO DEAL WITH LOSS TO FOLLOW-UP AND MISSING DATA



The best strategy to avert missing data is to prevent loss to follow-up. Designing the study carefully, training staff, implementing data quality procedures, and developing mechanisms to retain and contact participants are key. Additionally, there are statistical methods available to deal with missing data, but these procedures should be planned a priori and with consultation of a biostatistician. (3) However, there are situations when investigators might not overcome problems related to missing data because the mechanism of missingness is MNAR. In that case, losses to follow-up of 20%, for example, can result in serious biases and, therefore, should not be considered "acceptable". Remember, missing data are common and best practices include thinking about it early on when defining the research question and writing the protocol.



REFERENCES



1. Ranzani OT, Rodrigues LC, Waldman EA, Prina E, Carvalho CRR. Who are the patients with tuberculosis who are diagnosed in emergency facilities? An analysis of treatment outcomes in the state of São Paulo, Brazil. J Bras Pneumol. 2018;44(2):125-133. https://doi.org/10.1590/s1806-37562017000000384

2. Pedersen AB, Mikkelsen EM, Cronin-Fenton D, Kristensen NR, Pham TM, Pedersen L, et al. Missing data and multiple imputation in clinical epidemiological research. Clin Epidemiol. 2017;9:157-166. https://doi.org/10.2147/CLEP.S129785

3. Kristman V, Manno M, Côté P. Loss to follow-up in cohort studies: how much is too much? Eur J Epidemiol. 2004;19(8):751-60.

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