Prostate Imaging Using MRI +/- Contrast Enhancement
500 patients around the world
Available in Argentina, United States, Brazil, Spain
The PRECISION study (NCT02380027) has established that multiparametric MRI +/- targeted
biopsy of suspicious areas identified on MRI is superior to standard 12 core TRUS biopsy in
the detection of clinically significant prostate cancer (Gleason > 3+ 4) (38% vs 26%), in
reducing the detection of clinically insignificant prostate cancer (Gleason 3 + 3) (9% vs
22%) and in maximising the proportion of cores positive for prostate cancer (44% vs 19%).
Multiparametric MRI (mpMRI) typically uses T2-weighted (T2W), diffusion-weighted (DWI) and
dynamic contrast enhanced (DCE) sequences. As a mpMRI is a precious resource, due to capacity
and resource limitations, one of the major challenges across institutions is delivering a
health service with pre-biopsy MRI before a biopsy in all men with suspected prostate cancer.
However, biparametric MRI (bpMRI), that is, a combination of T2W and DWI, which does not use
the DCE sequences, has demonstrated similar detection rates of prostate cancer as mpMRI in
some studies and there is a debate about the necessity of the DCE sequence.
The potential advantages of avoiding the DCE sequence include avoiding the cost associated
with it, shorter scan time, avoiding the need for medical practitioner attendance, and
avoiding putative basal ganglia accumulation and the possibility of adverse neurological
effect. Thus, a bpMRI approach may be more feasible and have health-economic benefits over a
mpMRI approach and may thus increase the accessibility of this resource to men who need it.
PRIME is a multi-centre study. Men referred with clinical suspicion of prostate cancer based
on raised prostate specific antigen (PSA) or abnormal digital rectal examination (DRE) who
have had no prior biopsy undergo mpMRI. The DCE sequence is blinded from the radiologist who
reports the bpMRI first. After reporting the bpMRI, the DCE sequence is made available to the
radiologist who reports the mpMRI. The MRIs and lesions are scored on 1-5 scales of suspicion
for the likelihood that clinically significant cancer is present:
1. - Very low (clinically significant cancer is highly unlikely to be present)
2. - Low (clinically significant cancer is unlikely to be present)
3. - Intermediate (the presence of clinically significant cancer is equivocal)
4. - High (clinically significant cancer is likely to be present)
5. - Very high (clinically significant cancer is highly likely to be present)
Men with non-suspicious MRI on bpMRI and mpMRI and low clinical risk of prostate cancer will
be counselled by their clinical teams as per routine clinical care. In routine clinical
practice these men typically do not undergo prostate biopsy.
Suspicious areas scoring 3, 4 or 5 on either bpMRI or mpMRI will undergo targeted and
systematic biopsy using the information from the mpMRI to influence biopsy conduct.
Suspicious areas will be labelled by their MRI score, with their location according to sector
diagrams.
The proportion of patients with clinically significant prostate cancer will be ascertained
and compared between bpMRI and mpMRI.
Treatment eligibility decisions without the DCE information will be made and once the
clinicians are unblinded to the DCE sequence the impact that this information makes on the
treatment decision will be evaluated.