| Literature DB >> 24932281 |
Abstract
The role of fluorine-18 fluorodeoxyglucose (FDG) positron emission tomography (PET)-computed tomography (CT) in prostate cancer remains controversial due to a limited number of previous clinical investigations. The aim of the present retrospective study was to assess the diagnostic value of FDG PET-CT in prostate cancer, with an emphasis on the detection of metastatic disease. Twenty-five relevant cases of patients with newly diagnosed prostate cancer, referred for staging, or with a history of prostate cancer or recent prostate specific antigen (PSA) relapse, referred for the detection of metastatic disease, were included in the present study. None of the patients had known imaging or pathological evidence of metastatic disease prior to FDG PET-CT, however, the PSA levels had been recorded in all patients in the two months prior to FDG PET-CT imaging. Verification of the FDG PET-CT observations was made by biopsy, regional diagnostic CT and/or whole-body bone scintigraphy. The sensitivity of FDG PET-CT in identifying untreated primary lesions was only 33% (3/9). However, FDG PET-CT detected metastatic disease in six of the nine patients who underwent initial staging. Out of 16 patients with previous treatments and recent PSA relapse, FDG PET-CT successfully identified metastatic diseases in 12 and tumor recurrence within the prostatic fossa of two patients. The difference in the PSA levels was identified to be statistically significant between the FDG PET-CT-positive and -negative subgroups of the 16 restaging patients. The results indicated that FDG PET-CT is not useful for the diagnosis of prostate cancer, but may aid with the detection of metastatic disease in appropriately selected patients.Entities:
Keywords: fluorine-18 fluorodeoxyglucose positron emission tomography-computed tomography; metastasis; prostate cancer; prostate-specific antigen
Year: 2014 PMID: 24932281 PMCID: PMC4049681 DOI: 10.3892/ol.2014.1997
Source DB: PubMed Journal: Oncol Lett ISSN: 1792-1074 Impact factor: 2.967
Patient characteristics and FDG PET-CT observations.
| FDG PET-CT observation | ||||||||
|---|---|---|---|---|---|---|---|---|
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| ||||||||
| Patient no. | Age, years | Gleason score | Therapeutic history | PSA on imaging, ng/ml | Prostatic fossa | Lymph nodes | Bone (or other) | Confirmatory test |
| 1 | 59 | 7 | Initial staging | 6.8 | − | + | + | BS and CT |
| 2 | 61 | 9 | Initial staging | 14 | − | + | − | CT and PLND |
| 3 | 52 | 6 | Initial staging | 49 | + | − | − | CT and BS |
| 4 | 50 | 7 | Initial staging | 6.1 | − | − | − | CT and BS |
| 5 | 73 | 8 | Initial staging | 680 | + | + | + | CT and BS |
| 6 | 69 | 6 | Initial staging | 9.6 | − | − | − | CT |
| 7 | 53 | 8 | Initial staging | 511 | − | + | + | BS and CT |
| 8 | 59 | 7 | Initial staging | 369 | − | − | + | BS and CT |
| 9 | 71 | 9 | Initial staging | 980 | + | + | + | BS and CT |
| 10 | 64 | 6 | Prostatectomy | 3.1 | − | − | + | BS and CT |
| 11 | 63 | 6 | Prostatectomy | 22.5 | − | + | − | CT |
| 12 | 55 | 8 | Prostatectomy | 10.7 | − | + | − | CT |
| 13 | 70 | 7 | Prostatectomy | 67 | − | − | + | BS and CT |
| 14 | 72 | 6 | Prostatectomy | 15.4 | − | − | + (lung) | Lung Bx |
| 15 | 64 | 6 | Prostatectomy | 3.8 | − | − | − | CT and repeat PET |
| 16 | 68 | 7 | Prostatectomy | 14 | − | − | + | Bx |
| 17 | 72 | 7 | Prostatectomy | 8.4 | − | − | + | CT |
| 18 | 67 | 8 | Hormone | 11.5 | − | − | + | BS and CT |
| 19 | 60 | 9 | Brachytherapy | 15.7 | − | − | + | BS and CT |
| 20 | 70 | 8 | Brachytherapy | 5.5 | − | − | − | CT |
| 21 | 72 | 7 | Brachytherapy | 7.8 | + | − | − | Bx |
| 22 | 77 | 7 | Brachytherapy | 4.8 | − | − | − | None |
| 23 | 64 | 7 | Hormone + XRT | 41 | − | + | − | CT |
| 24 | 62 | 7 | Hormone + XRT | 680 | − | + | + | BS and CT |
| 25 | 57 | 8 | Orchiectomy + XRT | 671 | + | + | + | BS and CT |
FDG, fluorine-18 fluorodeoxyglucose; PET, positron emission tomography; CT, computed tomography; PSA, prostate-specific antigen; BS, bone scan; PLND, pelvic lymph node dissection; Bx, biopsy; XRT, radiation therapy; +, positive; −, negative.
Figure 1(A) Transaxial fluorine-18 fluorodeoxyglucose (FDG) positron emission tomography (PET)-computed tomography (CT) images of the upper chest of patient 13. The 70-year-old male exhibited a prostate-specific antigen relapse (PSA level, 67 ng/ml) five years following radical prostatectomy. The first bone scintigraphy and pelvic CT were obtained one month prior to the FDG PET-CT and the two were negative. FDG PET-CT demonstrated a small sclerotic density with mild uptake (SUVmax, 3.5), which indicated metastasis in the right-side of the T1 vertebral body (indicated by the arrows). (B) Repeat bone scintigraphy one month later confirmed the FDG PET-CT-identified lesion (indicated by the arrow).
Figure 2Transaxial fluorine-18 fluorodeoxyglucose (FDG) positron emission tomography (PET)-computed tomography (CT) images obtained from a 72-year-old male (patient 21) following external beam radiotherapy for prostate cancer. The patient’s series prostate-specific antigen (PSA) levels were unremarkable until two years later when the PSA level was 7.8 ng/ml. FDG PET-CT demonstrated an FDG-avid lesion in the left-side of the prostate (indicated by the arrows), which was confirmed as recurrent adenocarcinoma by transrectal biopsy.
Figure 3Mean PSA levels in the subgroups of patients. For primary prostate tumors in the initial staging group, the mean PSA level was 153±92 ng/ml in the FDG PET-CT-negative cases and 570±274 ng/ml in the FDG PET-CT-positive cases; the difference in the PSA levels was not identified to be statistically significant (P>0.05). The mean PSA levels in the restaging (metastatic) group were 4.7±0.49 ng/ml in the FDG PET-CT-negative cases and 120±68 ng/ml in the the FDG PET-CT-positive cases. The difference in the PSA levels was identified to be statistically significant (*P<0.05) between the two subgroups of restaging patients. FDG, fluorine-18 fluorodeoxyglucose; PET-CT, positron emission tomography-computed tomography; PSA, prostate-specific antigen.