Literature DB >> 33203873

The use of prostate specific antigen density to predict clinically significant prostate cancer.

Igor Yusim1, Muhammad Krenawi1, Elad Mazor1, Victor Novack2, Nicola J Mabjeesh3.   

Abstract

The purpose of this study was to assess the predictive value of prostate specific antigen density (PSAD) for detection of clinically significant prostate cancer in men undergoing systematic transrectal ultrasound (TRUS)-guided prostate biopsy. We retrospectively analyzed data of men who underwent TRUS-guided prostate biopsy because of elevated PSA (≤ 20 ng/ml) or abnormal digital rectal examination. Receiver operating characteristic curve analysis to compare PSA and PSAD performance and chi-square automatic interaction detector methodologies were used to identify predictors of clinically significant cancer (Gleason score ≥ 7 or international society of urological pathology grade group ≥ 2). Nine-hundred and ninety-two consecutive men with a median age of 66 years (IQR 61-71) were included in the study. Median PSAD was 0.10 ng/ml2 (IQR 0.10-0.22). Prostate adenocarcinoma was diagnosed in 338 men (34%). Clinically significant prostate adenocarcinoma was diagnosed in 167 patients (50% of all cancers and 17% of the whole cohort). The AUC to predict clinically significant prostate cancer was 0.64 for PSA and 0.78 for PSAD (P < 0.001). The highest Youden's index for PSAD was at 0.20 ng/ml2 with 70% sensitivity and 79% specificity for the diagnosis of clinically significant cancer. Men with PSAD < 0.09 ng/ml2 had only 4% chance of having clinically significant disease. The detection rate of clinically significant prostate cancer in patients with PSAD between 0.09 and 0.19 ng/ml2 was significantly higher when prostate volume was less than 33 ml. In conclusion, PSAD was a better predictor than PSA alone of clinically significant prostate cancer in patients undergoing TRUS-guided biopsy. Patients with PSAD below 0.09 ng/ml2 were unlikely to harbor clinically significant prostate cancer. Combining PSAD in the gray zone (0.09-0.19) with prostate volume below 33 ml adds diagnostic value of clinically significant prostate cancer.

Entities:  

Mesh:

Substances:

Year:  2020        PMID: 33203873      PMCID: PMC7672084          DOI: 10.1038/s41598-020-76786-9

Source DB:  PubMed          Journal:  Sci Rep        ISSN: 2045-2322            Impact factor:   4.379


Introduction

Prostate cancer is recognized as one of the (leading) diseases in the male population [1]. Early detection of clinically significant prostate cancer is very important in order to achieve high rates of cure and local disease control. Historically, digital rectal examination (DRE) was the only tool used in the diagnosis of prostate cancer and in particular locally advanced disease. The accuracy of DRE in detecting prostate cancer is very low and it is rather used for clinical staging [2]. After prostate-specific antigen (PSA) emerged, its use was immediately coupled with DRE to improve the detection of prostate cancer unfortunately this resulted in unnecessary earlier diagnosis and over treatment of patients with very low and low risk disease [3]. Therefore, several measures have been proposed to improve the specificity of the PSA test, including, PSA velocity, free-to-total PSA ratio and PSA density (PSAD). Since PSAD introduction in the early 1990s by Benson et al., [4] it has been demonstrated to be a better predictor of prostate cancer than PSA but its application was not consistent in daily practice over the years [5,6]. At the same time in the modern era of the emerging role of prebiopsy diagnostic MRI to evaluate potential prostate pathology, noninvasive methods that reduce unnecessary biopsies are warranted. The need for such methods is higher in populations where MRI availability is limited. As the PSA blood test nowadays is part of our daily practice and the calculation of prostate volume is relatively simple, the application of PSAD would be possible in order to identify high risk prostate cancer. A similar trend was recently shown when the Stockholm-3 model, combining clinical, genomic variables and blood biomarkers, was thoroughly analyzed it found PSAD to improve the total performance of the model [7]. A number of recent reports also reexamined the added value of PSAD to detect clinically significant cancer and further refining a PSAD cutoff for this purpose [8−12]. In this current study, we evaluated the value of PSAD in predicting clinically significant prostate cancer in our population.

Patients and methods

Patients

Soroka University Medical Center ethics committee approved the study and waived informed consent requirements and all methods were performed in accordance with the relevant guidelines and regulations. We retrospectively collected data on 1,226 consecutive men who underwent TRUS-guided prostate biopsy at our center between January 2014 and December 2018. Men with PSA levels of > 4 ng/ml, or with abnormal DRE findings, were referred for TRUS-guided prostate biopsy. Ideally, prostate biopsies were performed with 12 cores taken from both lobes, 6 from each side, under TRUS guidance; two specimens were obtained from the base of the prostate gland of each side, two from middle of the gland, and two from the apex. Occasionally, more cores were taken when suspicious lesion was noticed on ultrasonography. All biopsies were performed only by experienced senior urologists. Since repeat biopsies for the same patients were included in the database, we selected the first available biopsy for each patient performed at our center and we excluded all repeated biopsies. Biopsy specimens were reviewed by experienced pathologists. Our cohort included 992 men with the restriction of PSA ≤ 20 ng/ml measured prior to biopsy. Estimated prostate volume was measured by TRUS. The PSAD (ng/ml[2]) was calculated as PSA (ng/mL) divided by the prostate volume (ml).

Statistical analysis

Descriptive statistics of the study sample were used to summarize relevant participant characteristics. The Student’s t-test was used for comparison of the continuous variables. Chi-square and Fisher’s exact tests were used for comparison of the proportions. Receiver operating characteristic (ROC) curves were plotted as sensitivity vs. 1-specificity for PSA and PSAD for each outcome. Clinically significant prostate cancer is defined as Gleason score ≥ 7 or international society of urological pathology (ISUP) grade group 2 or greater. We calculated the PSA and PSAD AUC predicting clinically significant disease and overall prostate cancer vs. no cancer [13]. We have used Youden's index (sensitivity + specificity-1) for identification of the optimum cut-off point for PSAD to be used as a predictor of the significant finding. Classification and regression tree and χ2 automatic interaction detection (CHAID) methods were used to divide the predictors into categories on the basis of the clinically significant cancer detection status [14]. All tests were two-tailed and statistical significance was defined as a P < 0.05. Analyses were performed using SPSS Statistics for Windows, version 24 (IBM Corp., Armonk, N.Y., USA).

Results

Nine-hundred ninety-two consecutive men with a median age of 66 years (IQR 61–71) who had TRUS-guided prostate biopsy were included in the study. Median PSA was 6.2 ng/ml (IQR 5–8.3) and median prostate volume was 43 ml (IQR 31–59). Median PSAD was 0.10 ng/ml2 (IQR 0.10–0.22). Prostate adenocarcinoma was diagnosed in 338 men (34%). Table 1 summarizes the clinical and histopathological features of the men with cancer vs. men without cancer. Men with prostate cancer were slightly older (median age of 68 vs. 66) with significantly higher mean PSA and PSAD values but lower mean prostate volume. Of the men with cancer about 50% had clinically significant prostate cancer, ISUP grade group ≥ 2 (Gleason score ≥ 7).
Table 1

Clinical and pathological characteristics of study patients.

CharacteristicCancerNo cancerP-value
No. (%)338 (34)654 (66)
Age (years)
Mean ± SD67.9 ± 6.965.4 ± 6.9 < 0.001
Range45–8447–89
Median (IQR)68 (63–73)66 (61–70)
Suspicious DRE (%)28 (8.3)26 (4)0.007
PSA (ng/ml)
Mean ± SD8.02 ± 4.066.60 ± 2.83 < 0.001
Range1.2–200.4–19
Median (IQR)6.8 (5.2–9.5)5.9 (4.9–7.8)
Prostate volume (ml)
Mean ± SD37.90 ± 22.653.46 ± 25.30 < 0.001
Range10–19810–190
Median (IQR)32.5 (23–46)49 (36–65)
PSAD (ng/ml2)
Mean ± SD0.27 ± 0.20.14 ± 0.1 < 0.001
Range0.04–1.330.006–1.50
Median (IQR)0.21 (0.14–0.34)0.12 (0.09–0.17)
Prostate cancer histology
ISUP grade group(%)
149.8
221.6
36.6
415.4
56.6
Clinical stage(%)
T1c69
T2a24
T2b2
T2c4
T3a1

PSA, prostate-specific antigen; PSAD, PSA density; ISUP, international society of urological pathology. SD, Standard deviation; IQR, interquartile range.

Clinical and pathological characteristics of study patients. PSA, prostate-specific antigen; PSAD, PSA density; ISUP, international society of urological pathology. SD, Standard deviation; IQR, interquartile range. The AUC to predict any prostate cancer was 0.60 (95% CI 0.56–0.63, P < 0.001) for PSA and 0.75 (95% CI 0.72–0.78, P < 0.001) for PSAD (Fig. 1A). The highest Youden's index was at PSAD of 0.15. At this point the diagnosis of cancer has 70% sensitivity and 70% specificity. On the other hand, the AUC to predict clinically significant prostate cancer was 0.64 (95% CI 0.59–0.69, P < 0.001) for PSA and 0.78 (95% CI 0.74–0.82) for PSAD (Fig. 1B). The highest Youden's index was at PSAD of 0.20. At this point the diagnosis of the clinically significant cancer has 70% sensitivity and 79% specificity.
Figure 1

ROC for the comparison between PSA and PSAD for the diagnosis of the prostate cancer. ROC curves comparing PSA and PSAD predictive accuracy to detect overall (A) and clinically significant (B) prostate cancer. P for comparison between the PSA and PSAD is < 0.001 in A and B. ROC, receiver operating characteristic; PSA, prostate-specific antigen; PSAD, PSA density.

ROC for the comparison between PSA and PSAD for the diagnosis of the prostate cancer. ROC curves comparing PSA and PSAD predictive accuracy to detect overall (A) and clinically significant (B) prostate cancer. P for comparison between the PSA and PSAD is < 0.001 in A and B. ROC, receiver operating characteristic; PSA, prostate-specific antigen; PSAD, PSA density. We next used the CHAID methodology to create a decision tree and found that patients with PSAD higher than 0.34 have 56.4% chance to be diagnosed with clinically significant cancer while patients with PSAD less than 0.09 have very low probability (4%) of having clinically significant prostate cancer (Table 2). Men with PSAD between 0.19 to 0.34 have 31.5% chance to be diagnosed with clinically significant prostate cancer. The chance of having clinically significant prostate cancer in men with PSAD between 0.09 and 0.19 is relatively low (8.5%). In this subgroup of patients, when PSAD is combined with prostate volume, the detection rate increases to 16.5% specifically in men having prostate volume less or equal to 33 ml while it drops to 6.8% when prostate volume is larger than 33 ml (Table 2).
Table 2

CHAID decision tree for the detection of clinically significant prostate cancer.

*, "Others" consists of patients without cancer and non-clinically significant cancer.

**, percent relates to total number of patients (992).

CHAID, chi-square automatic interaction detector; PSAD, prostate-specific antigen density; CS, clinically-significant.

CHAID decision tree for the detection of clinically significant prostate cancer. *, "Others" consists of patients without cancer and non-clinically significant cancer. **, percent relates to total number of patients (992). CHAID, chi-square automatic interaction detector; PSAD, prostate-specific antigen density; CS, clinically-significant.

Discussion

In the era of post PSA screening there is still great concern about the low reliability of PSA to detect clinically significant prostate cancer. The use of PSAD was first developed by Benson et al. to improve cancer detection rate when PSA ranged between 4 and 10 ng/ml (gray zone) [15]. Later on, Catalona et al. found high cancer detection performance (95% sensitivity) when they used a PSAD cutoff of 0.078 ng/ml2 in men with PSA values in this gray zone [16]. They found that 40% of cancer cases would have been missed with a cutoff of 0.15 ng/ml2 in this population. It should be taken into consideration that PSAD value was originally based on the sextant biopsy template described by Bazinet et al. [17], which is not the standard anymore. It is clear that the lower the threshold is set, the more biopsies are done and fewer cancers are missed but the rate of unnecessary biopsies and over detection of non-clinically significant disease are greater. Recently, Aminsharifi et al. studied the predictive accuracy of PSAD for the detection of clinically significant prostate cancer [8]. Interestingly, they found that using a PSAD cutoff of 0.08 ng/ml2 could have avoided 273 of 2,162 biopsies (13%), missing 48 of 622 non-clinically significant prostate cancers (ISUP grade group 1) (8%) and 10 of 499 clinically significant cancers (2%). Furthermore, Nordström et al. reported that using PSAD cutoffs of 0.1 and 0.15 ng/ml2 could lead to missing detection rate of 23% and 51%, respectively, for clinically significant cancers [9]. But, when they set a cutoff point of 0.07 ng/ml2, they were able to avoid about 20% of biopsies while missing only about 7% of clinically significant cancers in patients with PSA 3 ng/ml or greater. It should be kept in mind that these recent studies are based on a higher number of biopsies from the prostate compared to the classic sextant biopsy. In the current study, the performance of PSA was relatively poor compared with PSAD. Also in our population a cutoff point at PSAD of 0.15 gave the highest sensitivity (70%) and specificity (70%) for the detection of any prostate cancer, while at PSAD of 0.20 gave the highest sensitivity (70%) and specificity (79%) for the detection of clinically significant cancer (Fig. 1). In addition, we used the CHAID methodology to create a decision tree and found that patients with PSAD higher than 0.19 have 30% to 60% chance to be diagnosed with clinically significant cancer while patients with PSAD less than 0.09 have very low probability (4%) of having clinically significant prostate cancer (Table 2). Interestingly, the chance of having clinically significant prostate cancer in men with PSAD in a "gray zone" between 0.09 and 0.19 is relatively low (8.5%). In this subgroup of patients falling in the PSAD gray zone, the detection rate of clinically significant caner depends on prostate volume. When prostate volume is higher than 33 ml the detection rate is 6.8% whereas it increases more than two-fold to (17%) when prostate volume is smaller than 33 ml (Table 2). The chance of hitting a cancerous lesion is higher in smaller prostates than in larger ones . In our analysis, this was true and significant only in a subgroup of patients with PSAD values between 0.09 and 0.19 indicating that we are not dealing with an artifact. Otherwise, it would have be observed in each value of PSAD. Our findings are consistent with those recently described by Jue et al. who evaluated the predictive accuracy of PSAD to detect prostate cancer in 1,290 men with various PSA levels [10]. It should be emphasized that our cohort included patients with PSA levels ≤ 20 ng/ml. The tendency of PSAD to detect clinically significant prostate cancer has been shown in several clinical scenarios. For instance, the integration of PSAD into active surveillance protocols can be associated with improved enrollment criteria and a reduced rate of upgrading and reclassification down to 17.5% [11,12]. It is worth to mention that today there are additional commercially available blood tests to help diagnose clinically significant prostate cancer better than PSA such as 4Kscore and prostate health index (PHI) [18] as well as urine-based tests including PCA-3 [19] and SelectMDx [20]. The limitations of this study that it includes data specific to one population from one area located in southern Israel. Therefore, results may not be extrapolated completely to other populations. Second, this is an observational retrospective study lacking information on the indications for PSA testing which limits our conclusions since no prospective data was collected. Third, the results should be interpreted with caution, since prostate volume was determined only after referral of the patients to TRUS-guided prostate biopsy, but not for the purpose of calculating prostate volume before the decision on the biopsy had been made. Forth, it should be emphasized that only PSA and PSAD were used as predictive variables. Finally, we only included individuals with the first biopsy available without data on repeated biopsies. Therefore, performance and the cutoff point may not be generalizable to candidates for repeat biopsy although PSAD was shown to be a significant predictive factor for positive repeat biopsy [21]. In summary, PSAD was a better predictor than PSA alone of biopsy outcomes in patients undergoing transrectal prostate biopsy. Men with PSAD less than 0.09 ng/ml2 were unlikely to harbor ISUP grade group 2 or greater disease when PSA was ≤ 20 ng/ml. In patients having PSAD values between 0.09 and 0.19, adjunction of prostate volume increases the performance of PSAD for the detection of clinically significant disease. We propose testing PSAD prior to decision on prostate biopsy since it is a simple inexpensive and available tool that can be used to reduce over detection and morbidity of unnecessary biopsies.

Ethics approval

Soroka University Medical Center ethics committee approved the study and waived informed consent requirements. We confirm that all methods were performed in accordance with the relevant guidelines and regulations.
  20 in total

1.  Comparison Between the Four-kallikrein Panel and Prostate Health Index for Predicting Prostate Cancer.

Authors:  Tobias Nordström; Andrew Vickers; Melissa Assel; Hans Lilja; Henrik Grönberg; Martin Eklund
Journal:  Eur Urol       Date:  2014-08-20       Impact factor: 20.096

Review 2.  Overdiagnosis and overtreatment of prostate cancer.

Authors:  Stacy Loeb; Marc A Bjurlin; Joseph Nicholson; Teuvo L Tammela; David F Penson; H Ballentine Carter; Peter Carroll; Ruth Etzioni
Journal:  Eur Urol       Date:  2014-01-09       Impact factor: 20.096

3.  Comparing the areas under two or more correlated receiver operating characteristic curves: a nonparametric approach.

Authors:  E R DeLong; D M DeLong; D L Clarke-Pearson
Journal:  Biometrics       Date:  1988-09       Impact factor: 2.571

4.  Prostate-specific antigen density toward a better cutoff to identify better candidates for active surveillance.

Authors:  Yun-Sok Ha; Jihyeong Yu; Amirali Hassanzadeh Salmasi; Neal Patel; Jaspreet Parihar; Eric A Singer; Jeong Hyun Kim; Tae Gyun Kwon; Wun-Jae Kim; Isaac Yi Kim
Journal:  Urology       Date:  2014-06-10       Impact factor: 2.649

5.  Comparison of percent free PSA, PSA density, and age-specific PSA cutoffs for prostate cancer detection and staging.

Authors:  W J Catalona; P C Southwick; K M Slawin; A W Partin; M K Brawer; R C Flanigan; A Patel; J P Richie; P C Walsh; P T Scardino; P H Lange; G H Gasior; K G Loveland; K R Bray
Journal:  Urology       Date:  2000-08-01       Impact factor: 2.649

6.  Urine TMPRSS2:ERG Plus PCA3 for Individualized Prostate Cancer Risk Assessment.

Authors:  Scott A Tomlins; John R Day; Robert J Lonigro; Daniel H Hovelson; Javed Siddiqui; L Priya Kunju; Rodney L Dunn; Sarah Meyer; Petrea Hodge; Jack Groskopf; John T Wei; Arul M Chinnaiyan
Journal:  Eur Urol       Date:  2015-05-16       Impact factor: 20.096

7.  Prostate Specific Antigen Density as a Predictor of Clinically Significant Prostate Cancer When the Prostate Specific Antigen is in the Diagnostic Gray Zone: Defining the Optimum Cutoff Point Stratified by Race and Body Mass Index.

Authors:  Alireza Aminsharifi; Lauren Howard; Yuan Wu; Amanda De Hoedt; Charlotte Bailey; Stephen J Freedland; Thomas J Polascik
Journal:  J Urol       Date:  2018-07-06       Impact factor: 7.450

8.  Re-examining Prostate-specific Antigen (PSA) Density: Defining the Optimal PSA Range and Patients for Using PSA Density to Predict Prostate Cancer Using Extended Template Biopsy.

Authors:  Joshua S Jue; Marcelo Panizzutti Barboza; Nachiketh S Prakash; Vivek Venkatramani; Varsha R Sinha; Nicola Pavan; Bruno Nahar; Pratik Kanabur; Michael Ahdoot; Yan Dong; Ramgopal Satyanarayana; Dipen J Parekh; Sanoj Punnen
Journal:  Urology       Date:  2017-04-18       Impact factor: 2.649

9.  Prostate specific antigen density: a means of distinguishing benign prostatic hypertrophy and prostate cancer.

Authors:  M C Benson; I S Whang; A Pantuck; K Ring; S A Kaplan; C A Olsson; W H Cooner
Journal:  J Urol       Date:  1992-03       Impact factor: 7.450

10.  The Stockholm-3 Model for Prostate Cancer Detection: Algorithm Update, Biomarker Contribution, and Reflex Test Potential.

Authors:  Peter Ström; Tobias Nordström; Markus Aly; Lars Egevad; Henrik Grönberg; Martin Eklund
Journal:  Eur Urol       Date:  2018-01-10       Impact factor: 20.096
View more
  7 in total

1.  Diagnostic value of combining PI-RADS v2.1 with PSAD in clinically significant prostate cancer.

Authors:  Xiaoting Wei; Jianmin Xu; Shuyuan Zhong; Jinsen Zou; Zhiqiang Cheng; Zhiguang Ding; Xuhui Zhou
Journal:  Abdom Radiol (NY)       Date:  2022-07-05

2.  Comparative Analysis of PSA Density and an MRI-Based Predictive Model to Improve the Selection of Candidates for Prostate Biopsy.

Authors:  Juan Morote; Angel Borque-Fernando; Marina Triquell; Anna Celma; Lucas Regis; Richard Mast; Inés M de Torres; María E Semidey; José M Abascal; Pol Servian; Anna Santamaría; Jacques Planas; Luis M Esteban; Enrique Trilla
Journal:  Cancers (Basel)       Date:  2022-05-11       Impact factor: 6.575

3.  PI-RADS v2.1 Combined With Prostate-Specific Antigen Density for Detection of Prostate Cancer in Peripheral Zone.

Authors:  Jing Wen; Tingting Tang; Yugang Ji; Yilan Zhang
Journal:  Front Oncol       Date:  2022-04-08       Impact factor: 5.738

Review 4.  Any Correlation Between Prostate Volume and Incidence of Prostate Cancer: A Review of Reported Data for the Last Thirty Years.

Authors:  Justine R Yamashiro; Werner T W de Riese
Journal:  Res Rep Urol       Date:  2021-10-10

5.  Clinicopathological factors associated with pathological upgrading from biopsy to prostatectomy in patients with ISUP grade group ≤2 prostate cancer.

Authors:  Xing Li; Zhi-Xian Wang; Yun-Peng Zhu; Jing Wang; Yi-Sheng Yin; Xiao-Yong Zeng
Journal:  Asian J Androl       Date:  2022 Sep-Oct       Impact factor: 3.054

Review 6.  Foundational Statistical Principles in Medical Research: Sensitivity, Specificity, Positive Predictive Value, and Negative Predictive Value.

Authors:  Thomas F Monaghan; Syed N Rahman; Christina W Agudelo; Alan J Wein; Jason M Lazar; Karel Everaert; Roger R Dmochowski
Journal:  Medicina (Kaunas)       Date:  2021-05-16       Impact factor: 2.430

Review 7.  Active Surveillance in Prostate Cancer: Role of Available Biomarkers in Daily Practice.

Authors:  Belén Pastor-Navarro; José Rubio-Briones; Ángel Borque-Fernando; Luis M Esteban; Jose Luis Dominguez-Escrig; José Antonio López-Guerrero
Journal:  Int J Mol Sci       Date:  2021-06-10       Impact factor: 5.923
  7 in total

北京卡尤迪生物科技股份有限公司 © 2022-2023.