Combined MR direct thrombus imaging and non-contrast magnetic resonance venography reveal the evolution of deep vein thrombosis: a feasibility study

Thirteen patients (mean age 61 years, range 18–78 years; M/F = 11:2) with ultrasound-proven above-knee DVT (in the femoral vein and/or proximal popliteal vein) and no previous history of venous thrombosis or contraindications for MRI were recruited from the DVT service in our institution. The local ethics committee approved the study and all patients gave informed consent before undergoing MR imaging. The initial diagnosis of DVT was made on CUS by experienced sonographers as part of routine standard of care. Following patient recruitment, a member of the research team with ultrasound experience repeated the CUS study and the following parameters were recorded: the date/time of onset of symptoms, the patient’s (pro-thrombotic) risk factors, the length of thrombus and its relationship to the inguinal ligament and knee joint space. CUS was also performed at 3 months (visit 2) and 6 months (visit 3) on the same day as the MRI follow-up. On these visits, CUS was only used to establish the presence of the thrombus.

MR imaging was performed on a 1.5-T scanner (Discovery MR450, GE Healthcare, Waukesha, WI) using a 12-channel phased array coil. The first examination (visit 1) was within 7 days of diagnosis, and further examinations were performed after 3 months (visit 2) and 6 months (visit 3). During this 6-month period all the patients received standard anticoagulant therapy (warfarin) in accordance with local protocols.

For each examination, NC-MRV was acquired using Acceleration-Dependent Vascular Anatomy for Non-Contrast-Enhanced MR Venography (ADVANCE-MRV) [22, 23]. This technique uses subtraction of velocity- and acceleration-dependent angiography methods, as described previously [24, 25]. Dark-vein images are subtracted from bright-vein images to obtain vein-only images. The bright-vein images were acquired using an acceleration-sensitized acquisition to suppress the arterial blood, without suppressing venous blood [22, 23]. The dark-vein (velocity-sensitized) images were acquired using two consecutive velocity-sensitization modules with differing effective first gradient moments [22, 23]. To further ensure good venous suppression, four of these dark-vein image volumes were automatically acquired together and combined to give homogeneous venous signal [22, 23]. The effective first gradient moments used to generate the dark-vein image volumes were 1.2, 0.6, 0.3 and 0.15 μTs²/m. Additionally, a bright-artery image volume was acquired and used to generate an artery-only image volume by automated subtraction of the dark-artery (bright vein) images described above.

For these acquisitions, the image readout was a 3D balanced-SSFP (oblique coronal orientation, flip angle 65°, echo time (TE) 1.7 ms, repetition time (TR) 3.7 ms, acquisition matrix 288 × 288 × 20, reconstruction matrix 512 × 512 × 40, field of view (FoV) 40 × 40 cm, slice thickness 2.4 mm). The acquisition was cardiac gated using peripheral-pulse triggering with a trigger delay set to peak arterial flow. Parallel imaging (ASSET) was used with an acceleration factor of 2. The acquisition time was 40 heartbeats per volume, or 240 heartbeats for one bright-vein, four dark-vein and one bright-artery image volumes. To avoid flow and heterogeneity-related artefacts near the edges of the field of view, two separate acquisitions covering the upper and lower halves of the thigh were performed, with a combined acquisition time of 480 heartbeats (8 min at 60 bpm). Based on the above matrix sizes, the acquired and reconstructed voxel dimensions were 1.38 × 1.38 × 2.4 mm³ and 0.78 × 0.78 × 1.2 mm³ respectively.

MR-DTI was performed using a 3D inversion-prepared fast gradient-echo acquisition with a water-selective excitation (1-2-1 binomial pulse sequence). The image volumes were acquired in coronal orientation and the image parameters were optimized by numerical simulation to ensure high signal from short-T1 thrombus while suppressing the signal from long-T1 blood [26]. The acquisition used centric k-space ordering, acquiring half the slice-encodes from each read-slice k-space plane per shot. The acquisition parameters were inversion time (TI) 340 ms, TE 6.3 ms, TR 12.2 ms, flip angle 25°, centric ordering, acquisition matrix 320 × 288 × 96, FoV 40 × 40 cm², slice thickness 2 mm, 320 ms delay after each shot. Parallel imaging (ASSET) was used with an acceleration factor of 2. Zero-filling interpolation was used in-plane to give a reconstructed volume size of 512 × 512 × 96. The acquisition time was 5 min 59 s.

The MR-DTI volumes were reformatted to match the NC-MRV images. An experienced radiologist (DJL) assessed the NC-MRV images using an Osirix workstation (Pixmeo, Berne, CH) to determine the location and length of the venous occlusion (complete or partial, above-knee only). This assessment was performed principally using the subtracted NC-MRV images; however, the arterial images, as well as the unsubtracted bright- and dark-vein images, were also available to aid the diagnosis where needed.

Subsequently, an assessment of the location and length of any high-signal regions on the matching MR-DTI images was performed and these were compared with the NC-MRV images to evaluate to what extent thrombus length and location matched on both techniques. The individual-slice images were evaluated with reference to curved-reformat images, as required where the thrombi curved significantly out of the image plane. Any mismatch in thrombus extent or location was recorded. All discontinuities in high signal T1 regions were noted and the tract lengths were summed over the affected region on the matching NC-MRV.