Is MRCP necessary to diagnose pancreas divisum?

This is a retrospective single center exploratory study on patients referred to standard 3D-MRCP without secretin enhancement at our institution between October 2016 and August 2017. The study was approved by the institutional review board, and informed consent was waived. Inclusion criteria were age of at least 18 years and availability of MRCP as a part of the individuals’ standard abdominal MRI work-up. Exclusion criteria were history of pancreaticobiliary surgery (excluding cholecystectomy) and incomplete MRI protocol lacking one or more of the sequences regularly included in the exam (see below). For patients who received more than one MRI with 3D-MRCP during the study period, only the first examination was considered.

Technical parameters of 3D-MRCP and non-MRCP T2-weighted sequences are summarized in Table 1. 3D-MRCP was a three-dimensional respiration-navigated T2-weighted turbo spin echo sequence in coronal orientation with a slice thickness of 1.5 mm. Non-MRCP T2-weighted sequences were: First, a multi-breathhold TIRM in coronal orientation with a slice thickness of 6 mm. Second, a multi-breathhold HASTE in transverse orientation with a slice thickness of 4 mm.

Other sequences in the MRI protocol were: First, a pre-contrast T1-weighted three-dimensional fast low angle shot volumetric interpolated breath-hold examination with controlled aliasing in parallel imaging (VIBE-CAIPIRINHA) and Dixon technique for fat suppression in transverse orientation (slice thickness, 3 mm). Second, pre- and post-contrast (arterial phase, portal-venous phase, delayed phase) VIBE-CAIPIRINHA with spectral fat suppression in transverse orientation (slice thickness, 3 mm). Gadopentetate-Dimeglumine (Gadovist, Bayer Healthcare, Berlin, Germany) was administered at a dose of 0.1 mmol/kg body weight and a flow rate of 2 ml/s, followed by a 30 ml saline flush using a power injector.

Images were analyzed using a picture archiving and communication system. 3D-MRCP, TIRM, and HASTE were assessed for presence of PD independently in a randomized manner by a single radiologist (reader 1). A panel consensus on presence of PD reached by two radiologists (reader 1 and reader 2) using the combination of 3D-MRCP, TIRM, HASTE, and the above mentioned other imaging sequences together was defined as the standard of reference. Reader 1 and reader 2 had 4 years and 12 years of experience in abdominal imaging, respectively, and were blinded to clinical information. Disagreement between two radiologists was managed by discussion.

PD was deemed to be present when the dorsal pancreatic duct crossed the common bile duct, opened into the duodenum via the minor papilla, and was separated from a smaller ventral duct.

If assessment of the pancreatic duct anatomy was not possible, it was assessed whether this was attributable either to motion artifacts or to insufficient duct visibility on images not compromised by motion artifacts. Image quality was determined by assessing the general magnitude of motion artifacts present on each image series and was subjectively scored using a Likert scale ranging from 0 (no artifacts) to 3 (severe artifacts).

All statistics were calculated using IBM SPSS Statistics release 23 (Statistical Package for the Social Sciences, IBM Corporation, Armonk, USA). The diagnostic performance of 3D-MRCP, TIRM, and HASTE for diagnosis of PD was determined in comparison with the standard of reference including sensitivity, specificity, and negative predictive value. A noninferiority test was performed to analyze similarity between 3D-MRCP on the one hand and HASTE and TIRM on the other hand for diagnosis of PD. Noninferiority was assumed if the sensitivity of the test method (non-MRCP T2-weighted sequences, P_T) was not worse than the sensitivity of the comparator method (3D-MRCP, P_C) by using a 1-sided test with a noninferiority margin of Δ. The primary hypothesis can be stated as H₀: P_T − P_C ≤ −Δ. Noninferiority of P_T to P_C is inferred when the lower bound of either confidence interval (CI) is above the noninferiority margin (−Δ) [11]. The margin Δ was defined to be 0.5 on the basis of the population and was confirmed by clinical estimates from prior research and institutional pilot data. Image quality assessments were compared between sequence protocols using paired t-tests.

During the study period, in 436 consecutive patients abdominal MRI including 3D-MRCP was performed. Eighty-eight patients had to be excluded due to history of pancreatobiliary surgery. Six patients had to be excluded due to incomplete MRI protocol. Thus, in total 342 patients were available for analysis (sex, 170 females; mean age, 51 ± 16 years). MRI with 3D-MRCP was performed for a variety of clinical indications, which are summarized in Table 2. Pancreatic findings observed in the study patients are summarized in Table 3.

Mean acquisition time of 3D-MRCP was 176 ± 66 s. Acquisition times per sequence protocol design were 55 s and 74 s for TIRM and HASTE, respectively.

Thirty-three of 342 patients (9.7%) were diagnosed with PD using the standard of reference.

Sensitivity and specificity of 3D-MRCP for diagnosing PD was 81.2 and 69.7% (p < 0.001). Sensitivity and specificity of TIRM for diagnosing PD was 92.5 and 93.9% (p < 0.001). Sensitivity and specificity of HASTE for diagnosing PD was 98.1 and 97.0% (p < 0.001). Grouped sensitivity and specificity of the combination of non-MRCP T2-weighted sequences was 99.8 and 91.0%. The negative predictive value of the combination of non-MRCP T2-weighted sequences was 99.9%.

Both TIRM alone (lower bound of 95% CI -0.03) and HASTE alone (lower bound of 95% CI 0.3) as well as the combination of TIRM and HASTE (lower bound of 95% CI 0.06) were noninferior to 3D-MRCP (lower bound of 95% CI -0.3) for diagnosis of PD (Fig. 1).

The mean general magnitude of motion artifacts was scored with 1.07 ± 0.86, 0.03 ± 0.19, and 0.10 ± 0.33 for 3D-MRCP, TIRM, and HASTE. The artifact scoring was better for both TIRM and HASTE than for 3D-MRCP (p < 0.001, each).

Assessment of pancreatic duct orifice anatomy was not possible in 20.2% (69/342), 7.3% (25/342), and 2.3% (8/342) of 3D-MRCP, TIRM, and HASTE, respectively. This was due to motion artifacts in 9.4% (32/342), 0.3% (1/342), and 0.0% (0/342) and due to insufficient duct depiction in 10.8% (37/342), 7.0% (24/342), and 2.3% (8/342) of 3D-MRCP, TIRM, and HASTE, respectively.

Figures 2 and 3 show representative examples of PD diagnosis in a patient with 3D-MRCP without artifacts (Fig. 2) and in a patient with 3D-MRCP with severe artifacts (Fig. 3).

There are limitations to our study. ERCP as the historical gold standard for assessment of pancreaticobiliary duct anatomy was not available in our patients, and we used a combination of all available image series to define the ground truth. Nowadays, the mainstay of endoscopic procedures is depicting the pancreatic and biliary system in patients with high pretest probability for necessity of a simultaneous endoscopic therapeutic procedure and are, thus, frequently limited to ERC to reduce complication rates. Taking this into account, MRCP techniques may be considered the de facto gold standard for assessing the pancreatic duct anatomy. Endosonography represents an endoscopic alternative to ERCP for PD assessment [29]. In the absence of a non-invasive reference standard for PD diagnosis different from MRI, all available imaging sequences including the investigational sequences were used to determine ground truth. This may lead to an incorporation bias resulting in potential overestimation of the diagnostic test’s accuracy. We only performed a single-reader analysis for assessment of PD and a two-person consensus panel defined the reference standard. Thus, information on reproducibility and inter-rater variability of our data cannot be inferred. As the number of cases positive for PD in our study is low, the results should be confirmed in a larger prospective trial.