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68 Ga‐PSMA has a high detection rate of prostate cancer recurrence outside the prostatic fossa in patients being considered for salvage radiation treatment
Author(s) -
Leeuwen Pim J.,
Stricker Phillip,
Hruby George,
Kneebone Andrew,
Ting Francis,
Thompson Ben,
Nguyen Quoc,
Ho Bao,
Emmett Louise
Publication year - 2016
Publication title -
bju international
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.773
H-Index - 148
eISSN - 1464-410X
pISSN - 1464-4096
DOI - 10.1111/bju.13397
Subject(s) - medicine , biochemical recurrence , prostate cancer , prostatectomy , prostate specific antigen , urology , pathological , nuclear medicine , positron emission tomography , prostate , radiation therapy , glutamate carboxypeptidase ii , cancer , radiology
Objectives To examine the detection rates of 68 Ga‐ PSMA ‐positron emission tomography ( PET )/computed tomography ( CT ) in patients with biochemical recurrence ( BCR ) after radical prostatectomy ( RP ), and also the impact on their management. Materials and Methods A total of 300 consecutive patients with prostate cancer ( PC a) who underwent 68 Ga‐ PSMA ‐ PET / CT between February and July 2015 were prospectively included in the Prostate Cancer Imaging (ProCan‐I) database. For the present analysis, we included patients with BCR (prostate‐specific antigen [ PSA ] level ≥0.05 and <1.0 ng/ mL ) after RP , who were being considered for salvage radiation therapy ( RT ) according to the Faculty of Radiation Oncology Genito‐Urinary Group ( FROGG ) guidelines. Two readers assessed each 68 Ga‐ PSMA ‐ PET / CT , and all positive lesions were assigned to an anatomical location. For each patient, the clinical and pathological features were recorded, their association with pathological 68 Ga‐ PSMA uptake was investigated, and detection rates were determined according to PSA level. Results A total of 70 patients were included, and 53 positive 68 Ga‐ PSMA lesions were detected in 38 (54%) patients. Among patients with PSA levels 0.05–0.09 ng/mL, 8% were definitely positive; the corresponding percentages for the other PSA ranges were as follows: PSA 0.1–0.19 ng/mL, 23%; PSA 0.2–0.29 ng/ mL , 58%; PSA 0.3–0.49 ng/ mL , 36%; and PSA 0.5–0.99 ng/ mL , 57%. Eighteen of 70 patients (27%) had pathological 68 Ga‐ PSMA uptake in the prostatic fossa, 11 (14.3%) in the pelvic nodes, and five (4.3%) in both the fossa and pelvic lymph nodes. Finally, there was uptake outside the pelvis with or without a lesion in the fossa or pelvic lymph nodes in four cases (8.6%). As a result of the 68 Ga‐ PSMA findings there was a major management change in 20 (28.6%) patients. Conclusions 68 Ga‐ PSMA appears to be useful for re‐staging of PC a in patients with rising PSA levels who are being considered for salvage RT even at PSA levels <0.5 ng/mL. These results underline the need for further prospective trials to evaluate the changes in RT volume or management attributable to 68 Ga‐ PSMA findings.