Abstract
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To understand the current role of prostate MRI for imaging-based targeted prostate biopsy, staging, and active surveillance
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To learn how to optimize the multiparametric prostate MR imaging protocol
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To illustrate how to use the PI-RADS classification for prostatic lesion assessment
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To understand the need of structured reporting in communicating with the urologists
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To discuss the most common pitfalls in multiparametric MRI of the prostate
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FormalPara Learning Objectives-
To understand the current role of prostate MRI for imaging-based targeted prostate biopsy, staging, and active surveillance
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To learn how to optimize the multiparametric prostate MR imaging protocol
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To illustrate how to use the PI-RADS classification for prostatic lesion assessment
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To understand the need of structured reporting in communicating with the urologists
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To discuss the most common pitfalls in multiparametric MRI of the prostate
11.1 Introduction
Over the past years, continuing technical innovation in combination with a broad research activity has resulted in a high diagnostic accuracy of magnetic resonance imaging (MRI) of the prostate. At the same time, the Prostate Imaging Reporting and Data System (PI-RADS) has standardized image acquisition and reporting and facilitated the communication of imaging findings to the urologist and can therefore be considered an obligatory key element in prostate MRI. This has had a tremendous impact on the diagnostic workup of patients with suspected prostate cancer, with MRI being incorporated in multiple prostate cancer guidelines (e.g., NICE, AUA, German S3-Guideline) by now. As a direct result, imaging-based targeted prostate biopsy has increased almost at the same speed, and urologists not only heavily rely on accurate interpretation of MRI of the prostate but actively claim high-quality MRI scans for their daily practice because prostate MRI has direct impact on their cancer detection rate. Furthermore, a paradigm shift is taking place in the urological community regarding the care of low-grade prostate cancer patients, where therapy is more and more replaced by active surveillance (AS). Prostate MRI plays an important role in AS not only during the initial assessment whether the patient is a candidate for AS but also during the surveillance of the disease.
Therefore, any abdominal and genitourinary radiologist if not already performing prostate MRI will subsequently be involved, and we forecast prostate MRI to be an indispensable diagnostic step for any patient with a clinical suspicion for prostate cancer or during surveillance of low-grade prostate cancer in the near future.
11.2 PI-RADS
The European Society of Uroradiology (ESUR) has introduced PI-RADS (Prostate Imaging Reporting and Data System) in 2012. An updated version (PI-RADS v2) was published in 2015 in collaboration with the American College of Radiology (ACR) and the AdMeTech Foundation. PI-RADS is not based on evidence from clinical research trials rather than on expert knowledge; however, several studies have confirmed that the PI-RADS system improves the diagnostic accuracy of mpMRI. The overall rationale for implementation of PI-RADS was to “improve detection, localization, characterization, and risk stratification in patients with suspected cancer in treatment naïve prostate glands.” PI-RADS is currently not applicable to assess treatment response in prostate cancer patients. The following specific definitions and aims regarding MR imaging and reporting are targeted by PI-RADS:
11.2.1 Clinical Considerations
Timing of mpMRI after prostate biopsy does not necessarily need to be postponed since clinically significant cancer is likely in a location not altered by post biopsy hemorrhage when the biopsy was negative. For local staging of prostate cancer, a delay of a minimum of 6 weeks might be advantageous. No specific patient preparation is necessary; however, the administration of a spasmolytic drug may be beneficial. Bowel cleaning is not recommended; however, the patient should evacuate the rectum if possible.
11.2.2 Technical Considerations
The field strengths of 1.5 and 3 T can both be adequate (even without an endorectal coil at 1.5 T) when the scan parameters are tailored to small field-of-view imaging of the prostate and contemporary scanner technology is used (specifically multichannel phased-array surface coils and high-performance gradients); however, 3 T is the preferred field strength (higher signal-to-noise ratio, shorter scan time).
Multiparametric MRI of the prostate should include the following sequences:
T2-weighted imaging: 2D turbo spin-echo sequence, slice thickness ≤3 mm (no interslice gap), and in-plane spatial resolution ≤0.7 mm (phase-encoding direction) x ≤ 0.4 mm (frequency-encoding direction).
Diffusion-weighted imaging (DWI): spin-echo EPI (echo planar imaging) sequence with fat saturation, slice thickness ≤4 mm (no interslice gap), in-plane spatial resolution ≤2.5 mm (phase- and frequency-encoding direction), and at least two b-values (low b-value of 50–100 s/mm2 and a high b-value of 800–1000 s/mm2) with consecutive calculation of an ADC map. If SNR allows, a very high b-value of 1400–2000 s/mm2 should be measured. An alternative is to calculate a high b-value, which is less SNR critical.
Dynamic contrast-enhanced (DCE) imaging: 2D or 3D gradient-echo sequence with a temporal resolution below 10 s (preferably below 7 s) per acquisition, slice thickness ≤ 3 mm (no interslice gap), and in-plane spatial resolution ≤2 mm (phase- and frequency-encoding direction).
Slice orientation and slice thickness should match for all mpMRI sequences to allow side-by-side comparison. Also, a large field-of-view sequence covering the pelvic lymph nodes and the skeleton should be acquired.
11.2.3 Assessment of Prostatic Lesions
One major key element of PI-RADS is scoring the likelihood of a prostatic lesion to be clinically significant prostate cancer on a 5-point Likert-type scale (Table 11.1).
Since several different definitions of clinically significant prostate cancer exist, PI-RADS defines it as “Gleason score ≥7 (including 3+4 with prominent but not predominant Gleason 4 component), and/or volume ≥0.5 cc, and/or extra prostatic extension (EPE).” The scoring system is based on typical imaging findings on the respective multiparametric MR sequence (exact definitions according to PI-RADS, see Tables 11.2, 11.3 and 11.4; for examples, see Figs. 11.1, 11.2, 11.3, 11.4, 11.5, 11.6, 11.7, 11.8, 11.9, 11.10, 11.11, 11.12 and 11.13). For this purpose, typical examples for each score and sequence are included in the PI-RADS publication. The goal is to increase the diagnostic accuracy for detection of prostate cancer and to reduce the variability in image interpretation. Most preliminary studies report a good reader agreement which is higher for peripheral zone (PZ) lesions as compared to transition zone (TZ) lesions. Also, agreement is higher for PI-RADS score 4 and 5 compared to lower scores.
In the PI-RADS version 2, the diagnostic weighting of the multiparametric sequences has been changed compared to the first version. Now, a concept of a dominant sequence has been introduced. The dominant sequence depends on the prostatic zone the lesion is located; therefore identification of the zonal anatomy is crucial. The area at the base of the prostate where the central zone borders the peripheral zone and the anterior gland where the anterior horn of the peripheral zone borders the transition zone and the anterior fibromuscular stroma might be challenging in this respect. The DWI sequence is the dominant sequence for the peripheral zone where most prostate cancers are located. The T2-weighted sequence is the dominant sequence for the transition zone. The dominant sequence defines the final PI-RADS score with the exception of PI-RADS 3 lesions, where for the peripheral zone the DCE sequence and for the transition zone the DWI sequence defines the final PI-RADS score (see Tables 11.5 and 11.6).
If a particular sequence cannot be acquired or is nondiagnostic due to artifacts (e.g., DWI when certain hip implants are present), it should be marked with “x.” In this situation, the following rules apply:
Assessment without DWI (applies to PZ and TZ): the T2-weighted sequences define the final PI-RADS score with the exception of PI-RADS 3—if the lesion is DCE negative, the final score remains 3; if the lesion is DCE positive, the final score is 4.
Assessment without DCE (only applies to the peripheral zone since DCE is not needed for transition zone scoring): the DWI score represents the final PI-RADS score.
11.2.4 Structured Reporting
A very important task of PI-RADS is to “simplify and standardize the terminology and content of radiology reports” and to “enhance interdisciplinary communications with referring clinicians.” A comprehensive mpMRI report should therefore include the following contents:
The volume of prostate should be reported according to the ellipsoid formula: maximum AP diameter x maximum transverse diameter x maximum longitudinal diameter × 0.52.
The aforementioned PI-RADS score is assigned to up to four intraprostatic lesions with a score ≥3. In case of multiple lesions, an index lesion should be defined. The index lesion is the one with the highest PI-RADS score. In case multiple lesions qualify for the highest PI-RADS score, extraprostatic extension (EPE) outclasses lesion size. For each lesion a PI-RADS score is assigned to the series and the image number where the lesion is best visualized should be reported to assist the urologist in selecting optimal images for MRI/US fusion-guided prostate biopsy. The lesion size also needs to be reported. Measurement of each lesion is preferred on the axial images; the DWI sequence should be used for peripheral zone lesions and the T2-weighted images for transition zone lesions. If a lesion is not well delineated on the axial sequences, then another plain should be used.
Another crucial element of a full PI-RADS report is a sector map in which the lesions should be indicated, since this particularly enhances the communication with the urologist. For this matter, the prostate is subdivided into three axial heights, the base, the midgland, and the prostatic apex, respectively. The seminal vesicles should also be included for cases of extraprostatic extension. The zonal anatomy (peripheral zone, transition zone, central zone, and anterior fibromuscular stroma) and the urethra should also be incorporated into the sector map.
11.3 Concluding Remarks
Comprehensive multiparametric MRI of the prostate should include lesion scoring and reporting according to the PI-RADS system. This will assist to achieve a high level of diagnostic accuracy and assure a thriving communication with the urologist.
Key Points
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Continuing technical innovation and broad research activity have resulted in a high diagnostic accuracy of MRI of prostate.
-
Prostate MRI plays an important role for imaging-based targeted prostate biopsy.
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In patients undergoing active surveillance of prostate carcinoma, MRI has become indispensable for initial assessment as well as during the surveillance of the disease.
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PI-RADS standardizes image acquisition and facilitates communication with the urologists. It is considered an obligatory key element in prostate MRI.
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Comprehensive multiparametric MRI of the prostate should include lesion scoring and reporting according to the PI-RADS system.
Suggested Reading
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Barentsz JO, Richenberg J, Clements R, European Society of Urogenital Radiology, et al. ESUR prostate MR guidelines 2012. Eur Radiol. 2012;22:746–57.
Cash H, Günzel K, Maxeiner A, et al. Men with a negative real-time MRI/ultrasound-fusion guided targeted biopsy but prostate cancer detection on TRUS-guided random biopsy – what are the reasons for targeted biopsy failure? BJU Int. 2016;118:35–43.
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Hamm, B., Asbach, P. (2018). Magnetic Resonance Imaging of the Prostate in the PI-RADS Era. In: Hodler, J., Kubik-Huch, R., von Schulthess, G. (eds) Diseases of the Abdomen and Pelvis 2018-2021. IDKD Springer Series. Springer, Cham. https://doi.org/10.1007/978-3-319-75019-4_11
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