Comparison of axial and coronal acquisitions by non-contrast-enhanced renal 3D MR angiography using flow-in time-spatial labeling inversion pulse

This retrospective study was approved by the institutional review board (IRB) of our hospital and informed consent was obtained from all subjects. This retrospective study was performed on 128 subjects (88 men and 40 women, age range 29–85 years, average 62.1 ± 11.1 years) for evaluation by non-contrast-enhanced real artery MRA screening at Toranomon Health Management and Diagnostic Imaging Center (Tokyo, Japan) enrolled from January through September of 2015.

All MRA examinations were performed with a commercial 1.5-T scanner (Canon Medical Systems Corp., Tochigi, Japan) equipped with a 16-element ATLAS body-coil. Non-contrast-enhanced MRA was performed using segmented 3D imaging with a flow-in bSSFP sequence, with Time-SLIP. The Time-SLIP pulse utilized a slice-selective IR (sIR) pulse that inverts all spins of the tagged region to − 180° in the longitudinal magnetization (− Mz). During the TI interval, the spins exponentially recover via T1-relaxation, and untagged fresh blood travels from the aorta into the tagged region, where the renal arteries are located. The bSSFP sequence consists of a preparation pulse, dummy pulses, and fully balanced gradients in all three directions, which provide a high signal-to-noise ratio (SNR) in bright-blood images, due to intrinsic T2/T1 contrast. The detailed pulse sequence diagram and the relationship between the untagged blood and tagged region with magnetization state are shown in Ref. [19] and Fig. 4a.

Prior to these studies, we had optimized the axial acquisition using this technique by means of varying TI times, flip angle, and the number of segmentations for fat suppression were performed to depict the renal artery branches, within a reasonable scan time, which has been used in these studies [22].

Before each examination, we have instructed all subjects to have regular breathing and remain awake throughout the experiment. We also used an abdominal respiration belt in all subjects, and wrapped around the abdomen to control their expiration and suppress breathing-related motion of the abdomen [23]. The abdominal aorta and renal arteries were first localized using two-dimensional (2D) bSSFP coronal breath-hold scout imaging and then the axial breath-hold scout imaging with the following parameters: repetition time/echo time (TR/TE) = 4.4/2.2 milliseconds (ms), flip angle = 70°, matrix = 256 × 256, field-of-view (FOV) = 35 cm × 35 cm, slice thickness (ST) = 6 mm, number of slices = 16, and acquisition time (AT) = 16 s, without applying fat suppression. Following the 2D scout imaging, a spatial slice-selective Time-SLIP pulse (slice thickness of 240 mm) with a TI of 1500 ms was applied in the transverse plane. In most cases, the Time-SLIP pulse was placed immediately above the superior poles of both kidneys and was large enough to cover the vasculature of interest (aorta to renal arteries). A pre-saturation band pulse was applied to reduce the undesired signal of inflowing blood from the inferior vena cava. The position of the Time-SLIP pulse was graphically localized to suppress signals from background tissues within the imaging volume, as shown in Fig. 1. Data acquisition was accelerated with a parallel imaging (PI) factor of two in the phase-encoding (PE) direction. Depending on the acquired number of imaging sections and TI, the axial acquisition time ranged from 4.2 to 13.0 min and the coronal acquisition time ranged from 3.2 to 13.8 min. The imaging parameters were as follows: TR/TE = 4.3/2.2 ms, flip angle = 120°, matrix = 256 × 256 (interpolated to 512 × 512), TI = 1500 ms, FOV = 35 cm × 35 cm, 3-mm axial section slices (interpolated to eighty 1.5-mm section slices, resolution of 0.68 × 0.68/1.5 mm) or 2.5-mm coronal slices (interpolated to eighty 1.25-mm section slices, resolution of 0.68 × 0.68/1.25 mm), PI = 2.0, Time-SLIP tag-slice thickness = 240 mm, and segmentation of k-space = 2, using respiratory gating. The axial acquisition was performed using a CHESS fat-suppression technique and the coronal acquisition was performed using the STIR pulse with an inversion duration of 190 ms. The coronal 3D bSSFP acquisition required uniform fat suppression in a large coverage in the Z-direction without having banding artifacts, whereas the axial 3D bSSFP acquisition required a relatively smaller Z-directional coverage, and CHESS worked well.

All MR images were transferred to a workstation (Zio station2; Ziosoft Corporation, Tokyo, Japan) for post-processing. Maximum image projection (MIP) images for the entire volume of the renal artery were obtained by an experienced radiological technologist with standardized post-processing procedures for both axial and coronal acquisitions. Entire volumetric MIP images were generated by rotating the 3D data set through 180° at 15° increments for assessing renal arteries. Source images were also used for this evaluation.

Image review and analysis were performed independently by two readers (a radiological technologist with 25 years of experience in MRI and a cardiologist with 10 years of experience in cardiovascular imaging). Both readers were blinded to the patient’s clinical information. Image quality was evaluated for both source and MIP images for renal arteries. Each artery was rated on a four-point scale: grade 3, excellent with high homogeneous signal intensity within the vessel lumen and good delineation of the vessel border, and no artifacts present; grade 2, good visualization of the vessel lumen, incomplete delineation of the vessel border, although some artifacts may be present; grade 1, fair visualization with low, inhomogeneous signal intensity, incomplete delineation of the vessel border, and diagnosis may be impaired; and grade 0, poor visualization and diagnosis not possible. Image quality scores of 2 or above were defined as acceptable image quality. The images were also assessed on a four-point scale for motion degradation at the renal arteries and branches: grade 3, no visible motion degradation; grade 2, minimal motion degradation; grade 1, moderate motion degradation with blurring of the vessel border, but diagnostic; and grade 0, severe motion degradation and non-diagnostic. In quantitative assessment, the number of branch vessels was assessed by counting on MIP images.

Region of interest (ROI) analysis was performed on the renal arterial signal intensity (SIA) and renal cortex, renal medulla, and muscle as background signal intensities (SIB) for both coronal and axial acquisitions. A ROI with 14.02 mm² area was placed manually on the renal artery and background. The relative signal contrast ratio between the artery and background signals, i.e., vessel-to-background ratio (VBR), VBR = (SIA − SIB)/SIA were measured from the source images.

Statistical analyses were performed using commercially available software, Statistical Package for Social Science (SPSS) for Windows, ver.13.0 (Chicago, IL USA).

Data were presented as means ± standard deviations. Paired Student’s t test was used to evaluate the contrast ratio. Wilcoxon’s signed-rank test was used for comparison of image quality, motion degradation, and the number of countable renal arterial branches. A p value of less than < 0.05 was considered to indicate a statistically significant difference.

The inter-reader agreement was calculated using Cohen’s kappa statistics with the following interpretation: poor, < 0.4; good, ≥ 0.4 and < 0.75; excellent, ≥ 0.75. We use same metrics (Cohen’s kappa) for the assessment of inter-reader agreement with both image quality and motion degradation. Reviewer scores were averaged, and statistical analyses of image quality and motion degradation were performed on both source and MIP images for each renal artery. We adopted the image score of reader 1 and compared inter-reader agreement with reader 2.

Visual evaluation of source and MIP images of renal arteries between the axial and coronal acquisitions is presented in Table 1. For both the right and left renal arteries, there was no statistically significant difference in the image quality between the axial and the coronal acquisitions. The results of Cohen’s kappa statistics are summarized in Table 2. Inter-reader agreement of source image evaluation was excellent in right and left renal arteries on both axial acquisition and coronal acquisition. For MIP images, kappa values were also excellent in right and left renal arteries on both axial acquisition and coronal acquisition, indicating excellent inter-reader agreement.

In source image evaluation, the motion degradation of coronal acquisitions was significantly greater (p < 0.01) than that of the axial acquisitions. In MIP images, the motion degradation and the number of visualized branches were significantly greater than those of the axial acquisition (p < 0.01). We use the same metrics (Cohen’s kappa) for the assessment of the inter-reader agreement with motion degradation. The kappa statistics was interpreted as follows: poor < 0.4, good ≥ 0.4, and excellent ≥ 0.75.

The contrast ratio between the artery and background signals is shown in Table 3. The contrast ratios measured in the coronal acquisitions were significantly higher (p < 0.01) than those of the axial acquisitions.