Landmark-based evaluation of a deformable motion correction for DCE-MRI of the liver

Several image registration-based motion correction methods have been proposed for DCE-MRI series of the liver. In an early publication, Mainardi et al. corrected for organ motion of two subsequent phases by a rigid alignment of the liver followed by a slice-wise DIR [9]. Registration quality was assessed based on similarity after registration, leaving unclear whether the deformable transformation was physically plausible. Tokuda et al. used a different method to evaluate registration quality of a motion correction for large 2D time series [16]. They calculated a marker for liver function on the series using a pharmacokinetic model. The model-fit error before and after registration was used to assess the registration quality. A DIR for 3D time series was presented by Hamy et al. [5]. This method employs a robust principal component analysis to separate image changes induced by motion from those induced by the contrast agent, limiting it to series with high and constant temporal resolution. Besides qualitative measures, Hamy et al. use synthesized data to quantitatively evaluate their method. Registered non-contrast-enhanced time series are manually segmented and contrast enhancements within the different tissue classes are simulated based on pharmacokinetic modeling to generate a pseudo-ground truth. A DIR that is suitable for aligning both common clinical hepatic DCE-MRI as well as longer time series was proposed by Papiez et al. [12]. The method was evaluated based on manually annotated landmarks and an analysis of the deformation fields. For liver-applications, however, the method was only evaluated on two cases. Recently, Feng et al. proposed a manifold-based registration framework for liver DCE-MRI, that also relies on a decomposition of motion- and CA-related image changes [2]. Motion correction quality was assessed via time-intensity curves computed from manually annotated regions as well as by several visual and thus qualitative indicators.

Most publications assess performance via qualitative and indirect measures [6]. Indirect measures typically involve pharmacokinetic modeling and potentially introduce biases or are limited to certain scenarios. Motion corrections aiming at clinical applicability should further be evaluated on large datasets exhibiting realistic variety that may be problematic to synthesize.

A well-established direct method for registration evaluation is to sparsely generate transformation ground truth by annotating corresponding landmarks in the scans to be registered [1]. The distances between corresponding landmarks after registration, short landmark distances (LD), are then used to calculate a metric for registration quality. Castillo et al. formulated two requirements for a meaningful landmark-based evaluation of DIR methods: First, the landmarks should be spatially well distributed over the region of interest and second, the annotations should be numerous to ensure certain statistical criteria. They annotated numerous landmarks in some pairs and estimated the pooled standard deviation of landmark distance after registration \({\bar{s}}_{\texttt {DIR}}^{p}\). The number of annotations that are needed to ensure that a 95% confidence interval (CI) of size \(\pm d\) mm around the mean LD is then given byThe method of Castillo et al. is mostly used for evaluation of DIR algorithms on single image pairs. On evaluation datasets with multiple pairs it is assumed that the LD after registration is predominantly a property of the registration method and less dependent on differing motion between the pairs.

A common scheme for landmark annotation on time series is to automatically find distinctive features on a fixed image and to annotate them in the moving images to be registered [11]. Changing visibility of image features renders this strategy infeasible for early phases of hepatic DCE-MRI. Annotating numerous landmarks on multiple time points of multiple time series and by multiple observers is practically not feasible and thus rarely reported, as also pointed out in [6].

Landmark-based evaluation of DCE-MRI motion corrections is hampered by the excessive workload of ground truth generation. We propose a new annotation scheme for DCE-MRI that makes landmark-based ground truth generation practically feasible for datasets with a large number of cases. We apply the scheme to collect ground truth data from 26 DCE-MRI series. Further, we combine a state-of-the-art DIR, a linear preregistration, and a novel liver segmentation to several exemplary motion correction methods for hepatic DCE-MRI and evaluate them using the generated ground truth. The high number of annotated cases enables us to split the ground truth into a training and an evaluation dataset. We show how the training dataset can be used to optimize the parameters of the motion compensation.

Our method uses a sequence of pairwise registrations to correct for motion that occurs between the acquisition of the DCE-MRI volumes. We use the late-venous phase as the fixed image and employ a two-step pipeline: First, coarse differences in respiratory state are reduced by a rigid preregistration. Subsequently, organ deformations are corrected by a deformable registration. The preregistration step is restricted to the liver region by a coarse automatic liver segmentation that will be detailed below.

For deformable registration, we use a fast nonparametric method proposed by König et al. [8]. This method uses the similarity measure normalized gradient field (NGF) [4], which was successfully used for DCE-MRI of the kidney [6]. NGF has a parameter \(\eta \), that is used to control the influence of features with different gradient magnitude. A high \(\eta \) value will tend to diminish the influence of features with low gradients. Curvature regularization [3] is used as a regularization term. The influence of the regularization term is weighted by a factor \(\alpha \).

For rigid preregistration, we use a method of Rühaak et al. [14] that also uses NGF as a similarity measure. To focus the preregistration to the liver, we restrict the evaluation of the similarity measure to an automatically computed coarse liver segmentation.

Our liver segmentation is based on the accumulation of CA in the liver (see Fig. 3). A mean intensity projection over all time points is computed giving an image with relatively high intensities in the liver and spleen regions (a). The liver region is emphasized over the spleen region by multiplying a linear ramp image to the projection that has its maximum value in the most anterior right position and its lowest value in the posterior left (b, c). After that, a region including the liver is extracted by applying a threshold at the \(90\%\) quantile of image values (d). Non-liver parts in the resulting mask are reduced by a morphological opening with a large kernel of 10 mm (e). The convex hull of the resulting mask gives the coarse liver segmentation (f). To include anatomies around the liver, the segmentation is again dilated with a kernel size of 5 mm (g).

We will denote the algorithm including all steps the full method and two variants, without masking the preregistration (RMwom), and without preregistration (RMwop) the reduced methods.

While landmarks are used to sparsely sample the transformation ground truth, they cannot be used to evaluate the physical plausibility of a registration. We thus augment the landmark-based evaluation by a check for foldings in the deformation field. Further, we evaluate the motion compensations over a qualitative measure.

Our landmark annotation scheme has two parameters, the number of landmarks per pair L and the number of pairs P. The parameter L is chosen to fulfill the requirement that landmarks should be well distributed over the region of interest. We choose \(L=10\) as a compromise between spatial coverage of the liver and induced workload.

For a coarse estimation of P we treat each pair as if it had only one annotation. Following the assumption that the LD after registration is mostly independent of the underlying motion we can then use Formula 1 to estimate the number of pairs that are necessary to ensure a certain size of a 95% CI. We aim on an evaluation method that has a 95% CI smaller than half the mean voxel diagonal and thus choose \(\pm d = 0.7925\). Further, we estimate the standard deviation of the LD after registration with FMemp by annotating a single case with 50 landmarks per time point and computing the standard deviation after motion compensation \({\bar{s}}_{\texttt {FMemp}}=3.07\). Using Formula 1 we calculate \(P>61\). To compensate for estimation errors we annotated 104 pairs. After annotation of the 104 pairs with 10 landmarks, we calculate the actual standard deviation of LD after the full method with empirical parameters to \(s_\mathrm{FMemp}= 1.9\) mm. We estimate the number of pairs necessary for a 95% CI of size \(2\times 0.7925\) as before and get \(P>23\) as a lower bound. Consequently, we chose a training dataset that contains 24 pairs, i.e., six cases.

In total, 990 landmarks were annotated on the 26 cases, each by two annotators. One hundred and two of those landmarks were marked as ‘uncertain’ and were thus excluded from the evaluation. Five time points exhibited strong intra-scan motion artifacts and could not be annotated at all. To give an estimate of the ground truth quality, we calculate the inter-observer distance (IOD), i.e., the distance between corresponding moving image landmarks of the two annotators. Mean IOD was 3.01 mm (median: 2.09 mm, min: 0 mm, max: 22.64 mm), which is smaller than the mean voxel diagonal. Overall annotation time per annotator for all landmarks was below 12 h, distributed over several sessions. Statistics for the spatial extent of fixed image landmarks as well as average normal liver extents reported in [7] are given in Table 1.

Mean LD was computed for 65 different parameter combinations of \(\alpha \) and \(\eta \) on the training data. Figure 4 shows the mean LD as contour plots for the broad and the focused search range. Foldings were detected for several parameter configurations with low \(\alpha \) and \(\eta \) values (below red line). Within the focused search range, mean LD was minimal at a combination of \(\alpha = 32\) and \(\eta = 2\). Those parameters were used for FMopt.

Table 2 lists LD statistics for our full method with optimal parameters (FMopt), the full method with empirically motivated parameters (\(\eta = 1, \alpha =100\)) (FMemp), the reduced versions without masking the preregistration (RMwom) and without preregistration (RMwop), as well as the landmark distances before registration. FMopt performs best on average as well as in the median and maximum LD. Both reduced methods only slightly reduce the maximum LD before registration and have elevated values in the 99% quantile. For the FMemp the median is slightly elevated (\(+\) 9%) as compared to the full method. With respect to the Wilcoxon signed-rank test with a significance threshold of 0.05, the difference between FMopt and FMemp is statistically significant, the difference of FMopt to both reduced methods is statistically not significant.

Per evaluation case, three TCI pairs before and after motion compensation with FMopt were visually compared. In 51 TCI pairs, temporal consistency was rated as improved, in nine pairs it was rated indifferent. In all cases, at least one TCI pair indicated an improvement. The TCI of FMopt were compared to the TCI of the other methods on a per case basis. The TCI were mostly rated indifferent, only few cases were rated worse (FMemp:0, RMwom:4, RMwop:2) and none better. Time cuts for three lines of an exemplary case are displayed in Fig. 5. In this case, the result of FMopt was rated as improved as compared to the before motion compensation and RMwop was rated worse than FMopt because of a misalignment of a single time point (blue arrow). The green and gray arrows point to anatomical structures that show the improvement in temporal consistency.

The phase images of a representative case, before and after motion correction, are provided in a video as supplementary material. While continuously looping through the phases, the image slice is swept through the volume in the axial direction.

Motion correction was performed on a desktop computer with standard hardware running Windows 10 (Intel Core I7 4770k, 32 GB RAM). Average computation time per scan pair was 62 and 246 s per case.