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Multiple comparison correction

Multiple comparison correction. Klaas Enno Stephan Laboratory for Social and Neural Systems Research Institute for Empirical Research in Economics University of Zurich Functional Imaging Laboratory (FIL) Wellcome Trust Centre for Neuroimaging University College London.

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Multiple comparison correction

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  1. Multiple comparison correction Klaas Enno Stephan Laboratory for Social and Neural Systems Research Institute for Empirical Research in Economics University of Zurich Functional Imaging Laboratory (FIL) Wellcome Trust Centre for Neuroimaging University College London With many thanks for slides & images to: FIL Methods group Methods & models for fMRI data analysis18 March 2009

  2. Overview of SPM Design matrix Statistical parametric map (SPM) Image time-series Kernel Realignment Smoothing General linear model Gaussian field theory Statistical inference Normalisation p <0.05 Template Parameter estimates

  3. model specification parameter estimation hypothesis statistic Voxel-wise time series analysis Time Time BOLD signal single voxel time series SPM

  4. contrast ofestimatedparameters t = varianceestimate Inference at a single voxel NULL hypothesisH0: activation is zero u  = p(t > u | H0)  p-value: probability of getting a value of t at least as extreme as u. If  is small we reject the null hypothesis. We can choose u to ensure a voxel-wise significance level of . t distribution

  5. 0.4 n =1 0.35 n =2 n =5 0.3 n =10 n ¥ = 0.25 0.2 0.15 0.1 0.05 0 -5 -4 -3 -2 -1 0 1 2 3 4 5 Student's t-distribution • t-distribution is an approximation to the normal distribution for small samples • For high degrees of freedom (large samples), t approximates Z. Sn = sample standard deviation  = population standard deviation

  6. False positive (FP) Type I error α False negative (FN) Type II error β Types of error Actual condition H0 true H0 false True positive (TP) Reject H0 Test result Fail to reject H0 True negative (TN) specificity: 1- = TN / (TN + FP) = proportion of actual negatives which are correctly identified sensitivity (power): 1- = TP / (TP + FN) = proportion of actual positives which are correctly identified

  7. t > 0.5 t > 3.5 t > 5.5 Assessing SPMs High Threshold Med. Threshold Low Threshold Good SpecificityPoor Power(risk of false negatives) Poor Specificity(risk of false positives)Good Power

  8. Signal Inference on images Noise Signal+Noise

  9. Use of ‘uncorrected’ p-value, =0.1 11.3% 11.3% 12.5% 10.8% 11.5% 10.0% 10.7% 11.2% 10.2% 9.5% Percentage of Null Pixels that are False Positives Using an ‘uncorrected’ p-value of 0.1 will lead us to conclude on average that 10% of voxels are active when they are not. This is clearly undesirable. To correct for this we can define a null hypothesis for images of statistics.

  10. Family-wise null hypothesis FAMILY-WISE NULL HYPOTHESIS: Activation is zero everywhere. If we reject a voxel null hypothesis at any voxel, we reject the family-wise null hypothesis A false-positive anywhere in the image gives a Family Wise Error (FWE). Family-Wise Error (FWE) rate = ‘corrected’ p-value

  11. Use of ‘uncorrected’ p-value, =0.1 Use of ‘corrected’ p-value, =0.1 FWE

  12. The Bonferroni correction The family-wise error rate (FWE), , fora family of N independent voxels is α = Nv where v is the voxel-wise error rate. Therefore, to ensure a particular FWE, we can use v = α / N BUT ...

  13. The Bonferroni correction Independent voxels Spatially correlated voxels Bonferroni correction assumes independence of voxels  this is too conservative for smooth brain images !

  14. Smoothness (or roughness) • roughness = 1/smoothness • intrinsic smoothness • some vascular effects have extended spatial support • extrinsic smoothness • resampling during preprocessing • matched filter theorem  deliberate additional smoothing to increase SNR • described in resolution elements: "resels" • resel = size of image part that corresponds to the FWHM (full width half maximum) of the Gaussian convolution kernel that would have produced the observed image when applied to independent voxel values • # resels is similar, but not identical to # independent observations • can be computed from spatial derivatives of the residuals

  15. Random Field Theory • Consider a statistic image as a discretisation of a continuous underlying random field with a certain smoothness • Use results from continuous random field theory Discretisation (“lattice approximation”)

  16. Euler characteristic (EC) Topological measure • threshold an image at u • EC=# blobs • at high u: p (blob) = E [EC] therefore (under H0) FWE,  = E [EC]

  17. Euler characteristic (EC) for 2D images R = number of resels ZT = Z value threshold We can determine that Z threshold for which E[EC] = 0.05. At this threshold, every remaining voxel represents a significant activation, corrected for multiple comparisons across the search volume. Example: For 100 resels, E [EC] = 0.049 for a Z threshold of 3.8. That is, the probability of getting one or more blobs where Z is greater than 3.8, is 0.049. Expected EC values for an image of 100 resels

  18. Euler characteristic (EC) for any image • Computation of E[EC] can be generalized to be valid for volumes of any dimensions, shape and size, including small volumes (Worsley et al. 1996, A unified statistical approach for determining significant signals in images of cerebral activation, Human Brain Mapping, 4, 58–83.) • When we have a good a priori hypothesis about where an activation should be, we can reduce the search volume: • mask defined by (probabilistic) anatomical atlases • mask defined by separate "functional localisers" • mask defined by orthogonal contrasts • spherical search volume around known coordinates small volume correction (SVC)

  19. Voxel, cluster and set level tests Regional specificity Sensitivity Voxel level test: intensity of a voxel Cluster level test: spatial extent above u Set level test: number of clusters above u  

  20. False Discovery Rate (FDR) • Familywise Error Rate (FWE) • probability of one or more false positive voxels in the entire image • False Discovery Rate (FDR) • FDR = E(V/R) (R voxels declared active, V falsely so) • proportion of activated voxels that are false positives

  21. False Discovery Rate - Illustration Noise Signal Signal+Noise

  22. 11.3% 11.3% 12.5% 10.8% 11.5% 10.0% 10.7% 11.2% 10.2% 9.5% 6.7% 10.5% 12.2% 8.7% 10.4% 14.9% 9.3% 16.2% 13.8% 14.0% Control of Per Comparison Rate at 10% Percentage of False Positives Control of Familywise Error Rate at 10% Occurrence of Familywise Error FWE Control of False Discovery Rate at 10% Percentage of Activated Voxels that are False Positives

  23. p(i) (i/V)q Benjamini & Hochberg procedure • Select desired limit q on FDR • Order p-values, p(1)p(2) ...  p(V) • Let r be largest i such that • Reject all null hypotheses corresponding top(1), ... , p(r). 1 p(i) p-value (i/V)q 0 0 1 i/V i/V = proportion of all selected voxels Benjamini & Hochberg, JRSS-B (1995) 57:289-300

  24. Real Data: FWE correction with RFT • Threshold • S = 110,776 • 2  2  2 voxels5.1  5.8  6.9 mmFWHM • u = 9.870 • Result • 5 voxels above the threshold -log10 p-value

  25. Real Data: FWE correction with FDR • Threshold • u = 3.83 • Result • 3,073 voxels abovethreshold

  26. Caveats concerning FDR • Current methodological discussions whether standard FDR implementations are valid for neuroimaging data • Some argue (Chumbley & Friston 2009, NeuroImage) that the fMRI signal is spatially extended, it does not have compact support → inference should therefore not be about single voxels, but about topological features of the signal (e.g. peaks or clusters) • In contrast, FDR=E(V/R), i.e. the expected fraction of all positive decisions R, that are false positive decisions V. To be applicable, this definition requires that a subset of the image is signal-free. In images with continuous signal (e.g. after smoothing), all voxels have signal and consequently there are no false positives; FDR (and FWE) must be zero. • Possible alternative: FDR on topological features (e.g. clusters)

  27. Conclusions • Corrections for multiple testing are necessary to control the false positive risk. • FWE • Very specific, not so sensitive • Random Field Theory • Inference about topological features (peaks, clusters) • Excellent for large sample sizes (e.g. single-subject analyses or large group analyses) • Afford littles power for group studies with small sample size  consider non-parametric methods (not discussed in this talk) • FDR • Less specific, more sensitive • Interpret with care! • represents false positive risk over whole set of selected voxels • voxel-wise inference (which has been criticised)

  28. Thank you

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