Is possible to rule out clinically significant prostate cancer using PI-RADS v2 for the assessment of prostate MRI?

Viana, Publio Cesar Cavalcanti; Horvat, Natally; Santos, Valter Ribeiro dos; Lima, Thais Carneiro; Romão, Davi dos Santos; Cerri, Luciana Mendes de Oliveira; Castro, Marilia Germanos de; Vargas, Herbert Alberto; Miranda, Júlia Azevedo; Leite, Claudia da Costa; Cerri, Giovanni Guido

doi:10.1590/S1677-5538.IBJU.2018.0382

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Sumário

ORIGINAL ARTICLE • Int. braz j urol 45 (4) • Jul-Aug 2019 • https://doi.org/10.1590/S1677-5538.IBJU.2018.0382 copy

Is possible to rule out clinically significant prostate cancer using PI-RADS v2 for the assessment of prostate MRI?

Authorship SCIMAGO INSTITUTIONS RANKINGS

ABSTRACT

Objectives

To evaluate the diagnostic performance and interobserver agreement of PI-RADS v2.

Materials and Methods

In this Institutional Review Board approved single-center retrospective study, 98 patients with clinically suspected PCa who underwent 3-T multiparametric MRI followed by MRI/TRUS fusion-guided prostate biopsy were included from June 2013 to February 2015. Two radiologists (R1 and R2) with 8 and 1 years of experience in abdominal radiology reviewed the MRI scans and assigned PI-RADS v2 scores in all prostate zones. PI-RADS v2 were compared to MRI/TRUS fusion-guided biopsy results, which were classified as negative, PCa, and significant PCa (sPCa).

Results

Sensitivity, specificity, NPV, PPV and accuracy for PCa was 85.7% (same for all metrics) for R1 and 81.6%, 79.6%, 81.2%, 80.0% and 80.6% for R2. For detecting sPCa, the corresponding values were 95.3%, 85.4%, 95.9%, 83.7% and 89.8% for R1 and 93.0%, 81.8%, 93.7%, 86.7% and 86.7% for R2. There was substantial interobserver agreement in assigning PI-RADS v2 score as negative (1, 2, 3) or positive (4, 5) (Kappa=0.78). On multivariate analysis, PI-RADS v2 (p <0.001) was the only independent predictor of sPCa compared with age, abnormal DRE, prostate volume, PSA and PSA density.

Conclusions

Our study population demonstrated that PI-RADS v2 had high diagnostic accuracy, substantial interobserver agreement, and it was the only independent predictor of sPCa.

Prostate; Magnetic Resonance Imaging; Neoplasms; Prostatic Neoplasms

Parameter	Axial T2WI	Axial DWI (B50 / 1500 /2000)	Multi plane T2 3D	Axial Dixon Pelvis	Axial DCE
Repetition time (msec)	7500	5500	1200	5.73	3.80
Echo time (msec)	116	84	126	2.46 and 3.69	1.41
Flip angle (degrees)	150	-	120	90	150
Field of view (mm)	150	300	300	280	180
Acquisition matrix	218 x 256	144 x 160	256 x 256	192 x 256	154 x 192
Section thickness (mm), no gaps	3	3.5	1.17	3.0	3.5
Reconstruction voxel imaging resolution (mm/pixel)	0.3 x 0.3	1.5 x 1.5	0.59 x 0.59	1.1 x 1.1	0.9 x 0.9
Acquisition time (min:sec)	04:15	08:43	06:59	00:16	04:58

Parameter	% (n/total)
DRE abnormal	34.8% (15/43)
Gleason score > 6	88.4% (38/43)
PSA > 10 ng/mL	55.8% (24/43)
PSA density ≥ 0.15 ng/mL/g	72.1% (31/43)
Three or greater than 3 prostate biopsy cores positives	90.7% (39/43)
> 50% cancer in any biopsy core	83.7% (36/43)

Parameters	% (n/total)
Gleason 6	5/43 (11.6%)
Gleason 7	19/43 (44.1%)
Gleason 8	10/43 (23.2%)
Gleason 9	9/43 (20.9%)

	WITHOUT PCa			TOTAL CANCER			sPCa			PCa
	RAD 1	RAD 2	RAD 1		RAD 2	RAD 1		RAD 2	RAD 1		RAD 2
PI-RADS 1 or 2	28/49 (57.1%)	32/49 (65.3%)	3/49 (6.1%)		6/49 (12.2%)	0/43 (0%)		1/43 (2.3%)	3/6 (50%)		5/6 (83.3%)
PI-RADS 3	13/49 (26.5%)	7/49 (14.2%)	4/49 (8.1%)		3/49 (6.1%)	2/43 (4.6%)		2/43 (4.6%)	2/6 (33.3%)		1/6 (16.6%)
PI-RADS 4	5/49 (10.2%)	10/49 (20.4%)	23/49 (46.9%)		18/49 (36.7%)	22/43 (51.1%)		18/43 (41.8%)	1/6 (16.6%)		0/6 (0%)
PI-RADS 5	2/49 (4%)	0/49 (0%)	19/49 (38.7%)		22/49 (44.8%)	19/43 (44.1%)		22/43 (51.1%)	0/6 (0%)		0/6 (0%)

	WITHOUT PCa			TOTAL CANCER			sPCa			PCa
	RAD 1	RAD 2	RAD 1		RAD 2	RAD 1		RAD 2	RAD 1		RAD 2

PI-RADS 1, 2 or 3	42/49 (85.7%)	39/49 (79.6%)	7/49 (14.3%)		9/49 (18.4%)	2/43 (4.7%)		3/43 (7%)	5/6 (83.3%)		6/6 (100%)
PI-RADS 4 or 5	7/49 (14.3%)	10/49 (20.4%)	42/49 (85.7%)		40/49 (81.6%)	41/43 (95.3%)		40/43 (93%)	1/6 (16.6%)		0/6 (0%)

	RADIOLOGIST 1		RADIOLOGIST 2

	PCa % (CI)	sPCa % (CI)	PCa % (CI)	sPCa % (CI)
Accuracy	85.7% (77.4–91.3)	89.8% (82.2 – 94.4)	80.6% (71.7–87.2)	86.7% (78.6–92.1)
Sensitivity	85.7% (73.3–92.9)	95.4% (84.5 – 98.7)	81.6% (68.6–90.0)	93.0% (81.4–97.6)
Specificity	85.7% (73.3–92.9)	85.4% (73.8 – 92.4)	79.6% (66.4–88.5)	81.8% (69.7–89.8)
NPV	85.7% (73.3–92.9)	95.9% (86.3 – 98.9)	81.2% (68.1–89.8)	93.7% (83.2–97.8)
PPV	85.7% (73.3–92.9)	83.7% (71.0 – 91.5)	80.0% (67.0–88.8)	86.7% (78.6–92.1)

	Patients with sPCa	Patients without sPCa	p-value

	Frequency (%)	Frequency (%)
PIRADS (RAD 1)
Positive (4 or 5)	41 (95.3%)	8 (14.5%)	<0.001
Negative (1,2 or 3)	2 (4.7%)	47 (85.5%)
PIRADS (RAD 2)
Positive (4 or 5)	40 (93.0%)	10 (18.2%)	<0.001
Negative (1, 2 or 3)	3 (7.0%)	45 (81.8%)

	Patients with PCa	Patients without PCa	p-value

	Frequency (%)	Frequency (%)

PIRADS (RAD 1)
Positive (4 or 5)	42 (85.7%)	7 (14.3%)	<0.001
Negative (1, 2 or 3)	7 (14.3%)	42 (85.7%)
PIRADS (RAD 2)
Positive (4 or 5)	40 (8.6%)	10 (20.4%)	<0.001
Negative (1,2 or 3)	9 (18.4%)	39 (79.6%)

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[1] Correspondence address: Julia Azevedo Miranda, MD Departamento de Radiologia do Hospital Sírio-Libanês Rua: Adma Jafet, nº 74, Bela Vista São Paulo, SP, 01308-050, Brasil E-mail: juazevedomiranda@gmail.com