|
PATHOLOGY
doi: 10.1590/S1677-553820100003000020
Prostate-specific
antigen kinetics during follow-up are an unreliable trigger for intervention
in a prostate cancer surveillance program
Ross AE, Loeb S, Landis P, Partin AW, Epstein JI, Kettermann A, Feng Z,
Carter HB, Walsh PC
Departments of Urology and Pathology, The Johns Hopkins University School
of Medicine, The James Buchanan Brady Urological Institute, The Johns
Hopkins Hospital, Baltimore, MD, USA
J Clin Oncol. 2010; 28: 2810-6
- Purpose:
To assess the predictive ability of prostate-specific antigen (PSA)
velocity (PSAV) and doubling time (PSADT) for biopsy progression and
adverse pathology at prostatectomy among men with low-risk prostate
cancer enrolled on an active-surveillance program.
Methods: We evaluated 290 men who met criteria for active surveillance
(ie, PSA density < 0.15 ng/mL/cm(3) and Gleason score < or = 6
with no pattern > or = 4, involving < or = 2 cores with cancer,
and < or = 50% involvement of any core by cancer) with two or more
serial PSA measurements after diagnosis from 1994 to 2008. Follow-up
included twice-yearly digital rectal exam and PSA measurements and yearly
surveillance biopsy. Treatment was recommended for biopsy progression
(ie, Gleason score > or = 7, or > 2 positive cores, or > 50%
core involvement). Sensitivity and specificity of postdiagnostic PSAV
and PSADT were explored by using receiver operating characteristic (ROC)
analysis.
Results: Overall, 188 (65%) men remained on active surveillance, and
102 (35%) developed biopsy progression at a median follow-up of 2.9
years. PSADT was not significantly associated with subsequent adverse
biopsy findings (P = .83), and PSAV was marginally significant (P =
.06). No PSAV or PSADT cut point had both high sensitivity and specificity
(area under the curve, 0.61 and 0.59, respectively) for biopsy progression.
In those who eventually underwent radical prostatectomy, PSAV (P = .79)
and PSADT (P = .87) were not associated with the presence of unfavorable
surgical pathology.
Conclusion: Postdiagnostic PSA kinetics do not reliably predict adverse
pathology and should not be used to replace annual surveillance biopsy
for monitoring men on active surveillance.
- Editorial
Comment
This is an important study concluding that postdiagnostic PSA kinetics
do not reliably predict adverse pathology and should not be used to
replace annual surveillance biopsy for monitoring men on active surveillance.
At Johns Hopkins, the criteria for active surveillance are: PSA density
< 0.15 ng/mL/cm3, Gleason score = 6 with no pattern 4 or 5, involving
= 2 cores with cancer, and = 50% involvement of any core by cancer (1).
At Stanford, the criteria are: Gleason score = 6 with no pattern 4 or
5, one single core with cancer, linear extent of cancer = 3mm, and serum
PSA is not considered (2). It is controversial whether percentage or
linear extent is the best measure.
The follow-up included twice-yearly digital rectal exam and PSA measurements
and yearly surveillance biopsy. Tretament was recommended for biopsy
progression which was considered whenever Gleason score was = 7, >
2 positive cores, or > 50% core involvement. The important finding
in Ross et al. study was that PSA double time was not significantly
associated with subsequent adverse biopsy findings (p = 0.83) and PSA
velocity was marginally significant (p = 0.06).
References
- Bastian
PJ, Mangold LA, Epstein JI, Partin AW: Characteristics of insignificant
clinical T1c prostate tumors. A contemporary analysis. Cancer. 2004;
101: 2001-5.
- Noguchi
M, Stamey TA, McNeal JE, Yemoto CM: Relationship between systematic
biopsies and histological features of 222 radical prostatectomy specimens:
lack of prediction of tumor significance for men with nonpalpable prostate
cancer. J Urol. 2001; 166: 104-9; discussion 109-10.
Dr.
Athanase Billis
Full-Professor of Pathology
State University of Campinas, Unicamp
Campinas, São Paulo, Brazil
E-mail: athanase@fcm.unicamp.br
|