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False-positive neuroimaging: Undisclosed flexibility in testing spatial hypotheses allows presenting anything as a replicated finding

YongWook Hong, Yejong Yoo, Jihoon Han, View ORCID ProfileTor D. Wager, View ORCID ProfileChoong-Wan Woo
doi: https://doi.org/10.1101/514521
YongWook Hong
1Center for Neuroscience Imaging Research, Institute for Basic Science, South Korea
2Department of Biomedical Engineering, Sungkyunkwan University, South Korea
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Yejong Yoo
1Center for Neuroscience Imaging Research, Institute for Basic Science, South Korea
2Department of Biomedical Engineering, Sungkyunkwan University, South Korea
3Department of Biology, Taylor University, United States
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Jihoon Han
1Center for Neuroscience Imaging Research, Institute for Basic Science, South Korea
2Department of Biomedical Engineering, Sungkyunkwan University, South Korea
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Tor D. Wager
4Department of Psychology and Neuroscience, University of Colorado Boulder, United States
5Institute for Cognitive Sciences, University of Colorado Boulder, United States
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  • ORCID record for Tor D. Wager
Choong-Wan Woo
1Center for Neuroscience Imaging Research, Institute for Basic Science, South Korea
2Department of Biomedical Engineering, Sungkyunkwan University, South Korea
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  • ORCID record for Choong-Wan Woo
  • For correspondence: waniwoo@skku.edu
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Abstract

Hypothesis testing in neuroimaging studies relies heavily on treating named anatomical regions (e.g., “the amygdala”) as unitary entities. Though data collection and analyses are conducted at the voxel level, inferences are often based on anatomical regions. The discrepancy between the unit of analysis and the unit of inference leads to ambiguity and flexibility in analyses that can create a false sense of reproducibility. For example, hypothesizing effects on “amygdala activity” does not provide a falsifiable and reproducible definition of precisely which voxels or which patterns of activation should be observed. Rather, it comprises a large number of unspecified sub-hypotheses, leaving room for flexible interpretation of findings, which we refer to as “model degrees of freedom.” From a survey of 135 functional Magnetic Resonance Imaging studies in which researchers claimed replications of previous findings, we found that 42.2% of the studies did not report any quantitative evidence for replication such as activation peaks. Only 14.1% of the papers used exact coordinate-based or a priori pattern-based models. Of the studies that reported peak information, 42.9% of the ‘replicated’ findings had peak coordinates more than 15 mm away from the ‘original’ findings, suggesting that different brain locations were activated, even when studies claimed to replicate prior results. To reduce the flexible and qualitative region-level tests in neuroimaging studies, we recommend adopting quantitative spatial models and tests to assess the spatial reproducibility of findings. Techniques reviewed here include permutation tests on peak distance, Bayesian MANOVA, and a priori multivariate pattern-based models. These practices will help researchers to establish precise and falsifiable spatial hypotheses, promoting a cumulative science of neuroimaging.

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The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. It is made available under a CC-BY-NC-ND 4.0 International license.
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Posted March 27, 2019.
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False-positive neuroimaging: Undisclosed flexibility in testing spatial hypotheses allows presenting anything as a replicated finding
YongWook Hong, Yejong Yoo, Jihoon Han, Tor D. Wager, Choong-Wan Woo
bioRxiv 514521; doi: https://doi.org/10.1101/514521
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False-positive neuroimaging: Undisclosed flexibility in testing spatial hypotheses allows presenting anything as a replicated finding
YongWook Hong, Yejong Yoo, Jihoon Han, Tor D. Wager, Choong-Wan Woo
bioRxiv 514521; doi: https://doi.org/10.1101/514521

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