Projects:GroupwiseRegistration

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Non-rigid Groupwise Registration

We aim at providing efficient groupwise registration algorithms for population analysis of anatomical structures. Here we extend a previously demonstrated entropy based groupwise registration method to include a free-form deformation model based on B-splines. We provide an efficient implementation using stochastic gradient descents in a multi-resolution setting. We demonstrate the method in application to a set of 50 MRI brain scans and compare the results to a pairwise approach using segmentation labels to evaluate the quality of alignment. Our results indicate that increasing the complexity of the deformation model improves registration accuracy significantly, especially at cortical regions.

Description

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Objective Function


In order to align all subjects in the population, we consider sum of pixelwise entropies as a joint alignment criterion. The justification for this approach is that if the images are aligned properly, intensity values at corresponding coordinate locations from all the images will form a low entropy distribution. This approach does not require the use of a reference subject; all subjects are simultenously driven to the common tendency of the population.

We employ a Parzen window based density estimation scheme to estimate univariate entropies \cite{duda}: [math] f = -\sum_{v=1}^{V} \frac{1}{N} \sum_{i=1}^{N} \log \frac{1}{N}\sum_{j=1}^{N} G_\sigma(d_{ij}(x_v) ) [/math] where [math]d_{ij}(x)=I_i(T_i(x))-I_j(T_j(x))[/math] is the distance between intensity values of a pair of images evaluated at a point in the reference frame and [math]G_\sigma[/math] is a Gaussian kernel with variance $\sigma^2$. The objective function achieves its minimum when the intensity differences are small. Using the entropy measure we obtain a better treatment of transitions between different tissue types, such as gray matter-white matter transitions in the cortical regions where intensity distributions can be multi-modal. Parzen window density estimator allows us to obtain analytical expressions for the derivative of the objective function with respect to transform parameters

Deformation Model


For the nonrigid deformation model, we define a combined transformation consisting of a global and a local component [math] T(\mathbf{x}) = T_{local}({T_{global}(\mathbf{x})}) [/math]

where $T_{global}$ is a twelve parameter affine transform and $T_{local}$ is a deformation model based on B-splines.

Following Rueckert et al.'s formulation \cite{rueckert}, we let $\mathbf{\Phi}$ denote an $n_x \times n_y \times n_z $ grid of control points $\Phi_{i,j,k}$ with uniform spacing. The free form deformation can be written as the 3-D tensor product of 1-D cubic B-splines. [math] T_{local}(\mathbf{x}) = \mathbf{x} + \sum_{l=0}^3\sum_{m=0}^3\sum_{n=0}^3 B_l(u)B_m(v)B_n(w) \Phi_{i+l,j+m,k+n} [/math]

where

$\mathbf{x}=(x,y,z)$,

$i=\lfloor x/n_x \rfloor -1$, $j=\lfloor y/n_y\rfloor -1$, $k=\lfloor z/n_z\rfloor -1$, $u=x/n_x -\lfloor x/n_x\rfloor$, $v=y/n_y -\lfloor y/n_y\rfloor$, $w=z/n_z -\lfloor z/n_z\rfloor$ and where $B_l$ is $l$'th cubic B-spline basis function. Using the same expressions for $u,v$ and $w$ as above, the derivative of the deformation field with respect to B-spline coefficients can be given by [math] \frac{\partial T_{local}(x,y,z) }{\partial \Phi_{i,j,k}} = B_l(u)B_m(v)B_n(w) [/math] where $l=i-\lfloor x/n_x\rfloor+1$, $m=j-\lfloor y/n_y\rfloor+1$ and $n=k-\lfloor z/n_z\rfloor+1$. We consider $B_l(u) = 0$ for $l<0 $ and $l>3$. The derivative terms are nonzero only in the neighborhood of a given point. Therefore, optimization of the objective function using gradient descent can be implemented efficiently.


%The resolution of the deformation field %can be controlled by the grid size. %In order to capture shape variations at different resolution levels %we start the registration at a low resolution level with a coarse grid %and increase the resolution by refining the grid of control points. %Results of a registration at a coarse level are used to initialize %the grid of control points at a higher resolution level.

As none of the images are chosen as an anatomical reference, it is necessary to add a geometric constraint to define the reference coordinate frame. Similar to Bhatia et al. \cite{bhatia}, we define the reference frame by constraining the average deformation to be the identity transform: [math] \frac{1}{N}\sum_{n=1}^{N} T_n(\mathbf{x}) = \mathbf{x} [/math]

This constraint assures that the reference frame lies in the center of the population. In the case of B-splines, the constraint can be satisfied by constraining the sum of B-spline coefficients across images to be zero. In the gradient descent optimization scheme, the constraint can be forced by subtracting the mean from each update vector \cite{bhatia}.



Implementation

We provide an efficient optimization scheme by using line search with the gradient descent algorithm. For computational efficiency, we employ a stochastic subsampling procedure \cite{pluim}. In each iteration of the algorithm, a random subset is drawn from all samples and the objective function is evaluated only on this sample set. The number of samples to be used in this method depends on the number of the parameters of the deformation field. Using the number of samples on the order of the number of variables works well in practice.

To obtain a dense deformation field capturing anatomical variations at different scales, we gradually increase the complexity of the deformation field by refining the grid of B-spline control points. First, we perform a global registration with affine transforms. Then, we use affine transforms to initialize a low resolution deformation field at a grid spacing around $32$~voxels. We increase the resolution of the deformation field to $8$~voxels by using registration results at coarser grids to initialize finer grids.

As in every iterative search algorithm, local minima pose a significant problem. To avoid local minima we use a multi-resolution optimization scheme for each resolution level of the deformation field. The registration is first performed at a coarse scale by downsampling the input. Results from coarser scales are used to initialize optimization at finer scales. For each resolution level of the deformation field we used a multi-resolution scheme of three image resolution levels.

We implemented our groupwise registration method in a multi-threaded fashion using Insight Toolkit (ITK) and made the implementation publicly available \cite{itk}. We run experiments using a dataset of 50 MR images with $256\times256\times128$ voxels on a workstation with four CPUs and 8GB of memory. The running time of the algorithm is about 20 minutes for affine registration and two days for non-rigid registration of the entire dataset. The memory requirement of the algorithm depends linearly on the number of input images and was around 3GB for our dataset.


Progress

We tested the groupwise registration algorithm on a MR brain dataset and compared the results to a pairwise approach \cite{joshi}. The dataset consists of 50 MR brain images of three subgroups: schizophrenics, affected disorder and normal control patients. MR images are T1 scans with $256\times256\times128$ voxels and $0.9375\times0.9375\times1.5$~$\mbox{mm}^3$ spacing. MR images are preprocessed by skull stripping. To account for global intensity variations, images are normalized to have zero mean and unit variance. For each image in the dataset, an automatic tissue classification \cite{pohl} was performed, yielding gray matter (GM), white matter (WM) and cerebro-spinal fluid (CSF) labels. In addition, manual segmentations of four subcortical regions (left and right hippocampus and amygdala) and four cortical regions (left and right superior temporal gyrus and para-hippocampus) were available for each MR image.


The prediction accuracy reported in Table \ref{table:pred} is lower than what is typically achieved by segmentation methods. This is to be expected as our relatively simple label prediction method only considers voxelwise majority of the labels in the population and does not use the novel image intensity to predict the labels. Effectively, Table \ref{table:pred} reports the accuracy of the spatial prior (atlas) in predicting the labels before the local intensity is used to refine the segmentation. Increasing the complexity of the deformation model improves the accuracy of prediction. An interesting open problem is automatically identifying the appropriate deformation complexity before the registration overfits and the accuracy of prediction goes down. We also note that the alignment of the subcortical structures is much better than that of the cortical regions. It is not surprising as the registration algorithm does not use the information about geometry of the cortex to optimize the alignment of the cortex. In addition, it has been often observed that the cortical structures exhibit higher variability across subjects when considered in the 3D volume rather than modelled on the surface.

Our experiments highlight the need for further research in developing evaluation criteria for image alignment. We used the standard Dice measure, but it is not clear that this measurement captures all the nuances of the resulting alignment.

Comparing the groupwise registration to the pairwise approach, we observe that the sharpness of the mean images and the tissue overlaps in Figure~\ref{fig:mean} look visually similar. From Table~\ref{table:pred}, we note that groupwise registration performs slightly better than the pairwise setting in most of the cases, especially as we increase the complexity of the warp. This suggests that considering the population as a whole and registering subjects jointly brings the population into better alignment than matching each subject to a mean template image. However, the advantage shown here is only slight; more comparative studies are needed of the two approaches.

%Average Dice measures in Table \ref{table:pred} indicate relatively low values, especially for %manual segmentations of cortical structures. %This is to be expected as our relatively simple label prediction method %only considers voxelwise majority of the labels in the population. %Higher overlap values can be obtained by using more advanced segmentation techniques which make us of the % shapes of the structures. %As our method keeps the voxelwise intensity distributions in the population, these distributions %can be used to supply prior information to a more advanced segmentation algorithm to increase %the segmentation accuracy.


%Evaluation of a groupwise registration %challenging task as it is hard to distinguish between registration inaccuracy and anatomical variability %by considering Dice measure as the only evaluation criterion. %However, comparing overlap measures relative to each other gives us useful information. %The blurriness of the mean images in figure \ref{fig:mean} indicate high anatomical variabilities %at cortical structures. %Part of this anatomical variability is captured by higher resolution levels of B-splines, %as can be observed from the increase in Dice measures for cortical structures in Table \ref{table:pred}. %White matter and grey matter tissue type have a significant component in cortical regions; therefore, %the overlap measures for these tissue types also increase as the resolution of the deformation field increases. %Label overlap values for subcortical structures do not improve significantly with an increase in the resolution of the %deformation field. %These structures do not highly correlate with local intensity variations; therefore, %we believe that %the low Dice measures are mostly due to anatomical variabilities in these structures.


%As for the comparison of groupwise to pairwise approach, %we can observe that the sharpness of the mean images and the tissue overlaps in figure \ref{fig:mean} look visually similar. %From figure \ref{table:pred} we note that groupwise registration performs %slightly better than the pairwise setting in most of the cases. %This suggests that considering the population as a whole and registering subjects jointly brings the population into better %alignment than matching each subject to a mean template image. %A mean template image cannot fully explain multi-modal distributions; our groupwise setting %captures the modes in the distributions by considering stack entropies as an alignment criterion.


We compare our groupwise algorithm to a pairwise method where we register each subject to the mean intensity using sum of square differences. The objective function for pairwise registration to the mean can be described as follows [math] f_{pair} = \sum_{n=1}^{N} ( I_n(T_n(x)) - \mu(x) )^2 [/math] where $\mu$ is defined as the mean of the intensities $\mu(x) = \frac{1}{N}\sum_{n=1}^{N} I_n(T_n(x))$. During each iteration we consider the mean image as a reference image and register every subject to the mean image using sum of squared differences. After each iteration the mean image is updated and pairwise registrations are performed until convergence.


The images in Figure \ref{fig:mean} show central slices of 3D images after registration. Visually, mean images get sharper and variance images becomes darker, especially around central ventricles and cortical regions. We can observe that anatomical variability at cortical regions causes significant blur for GM, WM and CSF structures using affine registration. Finer scales of B-spline deformation fields capture a significant part of this anatomical variability and the tissue label overlap images get sharper.


We evaluate registration results by measuring label prediction accuracy in a leave-one-out fashion for the two different sets of segmentation labels. To predict the segmentation labels of a subject, we use majority voting for the labels in the rest of the population. We compute the Dice measure between the predicted and the true labels and average

over the whole population.

%Table \ref{table:pred} shows average Dice measures for two automatically segmented %tissue types: grey matter (GM) and white matter (WM) in the first two columns. %We excluded cerebro-spinal fluid (CSF) from the evaluation because CSF labels %near the cortex get corrupted %after preprocessing the data with skull stripping. %In the last two columns of Table \ref{table:pred} we display average prediction values for %manual segmentations of the cortical structures: superior temporal gyrus and para-hippocampus in the %left and right hemispheres; the subcortical structures: amygdala and hippocampus in the left and %right hemispheres.

Key Investigators

  • MIT: Serdar K Balci, Polina Golland, Sandy Wells

Publications

  • S.K. Balci, P. Golland, M.E. Shenton, W.M. Wells III. Free-Form B-spline Deformation Model for Groupwise Registration. In Proceedings of MICCAI 2007 Statistical Registration Workshop: Pair-wise and Group-wise Alignment and Atlas Formation, 23-30, 2007.