Automated 3D segmentation and diameter measurement of the thoracic aorta on non-contrast enhanced CT

Aortic aneurysm with the risk of acute dissection is an important cause of mortality in the western world [1]. The prevalence of thoracic aortic aneurysms is estimated around 0.3% in the normal population [2, 3]. Most patients with a dilated aorta or aortic aneurysm are asymptomatic. The diagnosis can be made as during screening in the context of a positive family history or by coincidence on imaging examinations performed for other purposes like lung cancer screening [4]. However, acute dissection is often the first presentation, in which case over 50% of all patients die within 30 days [5].

Because of this silent process with high risks, screening programs using non-contrast computed tomography (CT) could be considered. In patients with aortic aneurysms, the aortic size has a profound impact on the risk of dissection [6, 7]. Detecting aortic dilatation at an early stage enables preventive surgery, which might save lives. CT imaging of the thoracic aorta could become available as part of a comprehensive assessment of CT imaging performed for screening purposes including also other organs (lungs, coronary calcium, vertebral bone density, etc.) [4].

By measuring aortic dimensions in such screening cohorts we will also gain more information on normal values of aortic diameters, normal increase in diameters over time, and risk factors for dilatation, and a better insight in prognosis.

Besides its potential in screening, non-contrast CT is frequently used in diagnosis and follow-up of patients in clinical practice. It plays a central role in the imaging of the thoracic aorta because of the short time required for image acquisition, the ability to obtain a complete 3D view of the entire aorta, and its widespread availability. CT scans can be used for follow-up of patients with dilatation, especially in cases where echocardiography does not adequately visualize the dilatation. The ESC Guidelines and ACCF/AHA guidelines [8, 9] describe standard anatomical landmarks for reporting aortic diameters in CT in clinical practice.

Performing measurements of the aorta manually is labor intensive and subject to inter-observer variability. To assess aortic dilatation both in screening settings and in clinical practice, automated aorta segmentation and subsequent diameter analysis are therefore desirable. While automatic solutions for aortic measurements in CT angiography (CTA) exist [10‐14], automatic aorta segmentation in non-contrast CT scans is more challenging due to the lack of contrast between blood pool regions and surrounding soft tissue [15‐19].

The aim of the current study is to develop and validate an automatic method to robustly assess diameters of the ascending and descending aorta in non-ECG-gated, non-contrast CT without human interaction.

Figure 3 shows examples of segmentation results. Out of all 1334 CT scans only in two cases, the seed points at the descending aorta were extracted incorrectly. Centerline extraction further failed in seven cases, all of which were easily detected automatically. Average DSC for the entire aorta was 0.95 ± 0.01 (0.92–0.96) and MSD was 0.56 ± 0.08 (0.43–0.93) mm. The mean absolute distance between the manual and automatic landmark level of the pulmonary artery bifurcation was 2.55 ± 1.94 mm, with almost no bias (mean signed distance 0.45 ± 3.18 mm).

Box plots for the average manual and automatic diameters for each measuring level are shown in Fig. 4. Diameters measured at the different levels, for men and women separately, are shown in Table 2. High agreement between manually and automatically measured diameters was obtained, with an overall ICC and R² Pearson’s correlation of 0.97. The level-wise correlations together with the correlations separated per gender are shown in Table 3 (see supplementary Fig. S2 for scatter plots of each measuring level).

An average absolute diameter error of 1.09 ± 0.6 mm between manual and automatic diameters was obtained over all measuring levels, which showed a slight underestimation of the automated measurements compared to manual measurements (mean signed error − 0.97 ± 0.8 mm). As shown in box plots of the level-wise diameter errors in Fig. 5, larger errors (more than 3 mm) were extracted in 8 out of 100 scans. In four cases, a large error occurred due to motion artifacts at the ascending aorta (beneath the landmark level), and in three cases, it occurred at the aortic arch due to branching arteries. In one case, the error was along the entire aorta due to a 6-mm difference between the automatic and manual landmark levels. Bland-Altman plots of manual and automated diameter measurements are given in Fig. 6.

From the 617 subjects used to assess repeatability, 7 subjects had failed centerline or seed point extraction. From the remaining 610 subjects, ICC between the automatic diameters of the scan and rescan of each subject is shown in Table 4. From these 610 subjects, 72 subjects (12%) had an absolute diameter difference larger than 3 mm between the two time points at any of the measuring levels. In 35 out of 72 cases (48.6%), the segmentations appeared visually correct in both time points. In 17 cases of these 35 cases, a 2- or 3-mm difference between the extracted landmark level in one of the time points resulted in big diameter differences at 2 cm below the landmark level at the ascending aorta (in average 3.7 ± 0.5 mm). This is due to the aortic anatomy at the sinotubular junction where the aorta below this level is on average 3 mm larger than above [31]. In 5 out of 35 cases, there was more than 6-mm difference between the extracted landmark levels from the two time points, leading to a diameter measurement at very different levels along the entire aorta being compared (in average 3.4 ± 0.5 mm). The remaining 13 out of 35 cases appeared to have a slightly larger diameter at one of the time points (in average 3.7 ± 0.7 mm), possibly due to the aortic size changes during the cardiac cycle. In 37 out of 72 cases (51.4%), the average diameter difference (3.6 ± 0.6 mm) was due to segmentation error which mainly occurred at the aortic arch which was due to branching arteries, or was at the ascending aorta below the pulmonary artery bifurcation level which was due to heart motion artifacts caused by the non-ECG-gated data.

We presented a fully automatic method to segment the thoracic aorta and measure aortic diameters. In our evaluation on 100 non-ECG-gated, non-contrast CT scans, the 3D segmentation algorithm performed well with an average segmentation overlap of 0.95 ± 0.01 and a mean surface distance between manual and automatic segmentations of less than 1 voxel (0.56 mm).

The agreement with diameters obtained from manual segmentations was high, with an overall ICC of 0.97 and an average per-level ICC of 0.91 ± 0.03, which is similar to the agreement reported between observers in [32] (ICC = 0.94). The manual diameters were on average approximately 1 mm larger than automatic diameters. This bias is similar to inter-observer bias reported in [33] for mid-ascending aorta diameter measurement on CTA. Scan-rescan repeatability was high, with an overall ICC of 0.98 and an average per-level ICC of 0.94 ± 0.01.

The mean ascending aorta diameters measured at the pulmonary artery bifurcation level were 36.7 ± 3.5 mm for males and 33.9 ± 3.3 mm for females. These values are similar to those reported by Kalsch et al [3] (37.1 ± 4 mm for males and 34.5 ± 4 mm for females), while they were slightly greater than those reported by Wolak et al [34] (33.5 ± 4 mm for males and 31.4 ± 3 mm for females). These differences may be due to differences in the study populations, CT scan protocol, and measurement approach.

A significant diameter increase of on average 0.11 ± 1.0 mm was measured in repeated scans after 1 year. This agrees well with reported natural yearly aortic diameter growth of 0.1–0.2 mm per year in the healthy population [3, 30]. In 12% of repeat scan pairs (72 subjects), diameter changes larger than 3 mm were observed. In the majority of these cases (44 subjects), large diameter differences occur at the ascending aorta beneath the landmark level which is due to the anatomy and the difficulty of measuring these regions. Due to motion artifacts in the non-ECG-gated scans, segmentation of the proximal part of the aorta including the aortic root is difficult even for experienced radiologists. However, although isolated aortic root aneurysms are seen in patients with Marfan syndrome [9], it is less common than aneurysms of the ascending aorta more distal to the aortic root. Therefore, the aortic root segmentation is less important in our application than the ascending aorta. In the remaining 28 cases, the large diameter difference was either in the aortic arch (15) or in the descending aorta (8) or at multiple locations due to error in the extraction of the pulmonary artery bifurcation level (5). Diameters measured at the aortic arch were visually correct; however, slightly larger diameters were measured at the location of branching arteries. In descending aorta, the large diameter differences were mainly due to segmentation error.

In contrast with our study, in literature, most methods for automatic aorta segmentation were evaluated on CTA in which the aortic lumen is much more clearly visible [10‐14]. Few methods were proposed to segment the aorta in non-contrast CT [15‐19]. Compared to these previous works, shown in Table 5, our proposed method is evaluated on a larger dataset and shows better performance.

We proposed to measure aortic dimensions at fixed intervals with respect to a single anatomical landmark level, the pulmonary artery bifurcation. In clinical practice, multiple anatomical landmarks including locations in the aortic arch are used instead for reporting aortic diameters in CTA [8, 9, 35]. However, consistently extracting these landmarks especially in non-ECG-gated CT is difficult. Moreover, the aorta diameter is poorly defined at the locations of the brachiocephalic artery, left-common carotid artery, and left-subclavian artery. Consistent measurements in the arch require landmark points in between branches that are not affected by this issue; however, detecting such points automatically and robustly in non-contrast CT scans is difficult. Furthermore, aortic dilatation is less common in the arch than in the ascending and descending aorta. Therefore, in this paper, we focus on the ascending and descending aortas which clinically are of more interest. In non-contrast CT, diameters have been mainly measured at the pulmonary artery bifurcation level [2, 3, 34, 36, 37]. The measuring levels used in our study approximately cover the same area used in CTA [8, 9, 35] but are easier to extract reliably in non-contrast and non-ECG-gated CT.

A limitation of our study is that the method was validated only on a relatively healthy screening population. Further investigation would be required to evaluate the performance on abnormal aortic shapes or large aneurysms. However, in all cases with aortic dilatation as indicated in the original radiology reports, the obtained segmentation was correct. In our data, calcification in the aorta was assessed by the Agatston score [38]. Visual inspection of the scans with Agatston score higher than 1500 for the entire aorta (58 out of 742 subjects) showed that the proposed method segmented the calcifications correctly inside the vessel wall in all cases.

The proposed automatic method is a promising technique to accurately and reproducibly assess subtle signs of aorta dilatation in non-ECG-gated, non-contrast CT scans without any human interaction and could be used for efficient screening for aortic dilatation as well as for monitoring of aortic change in clinical practice as part of a comprehensive CT analysis including lung screening.