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Asian Journal of Urology, 2023, 10(3): 317-328    doi: 10.1016/j.ajur.2022.01.002
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Clinicopathological and oncological significance of persistent prostate-specific antigen after radical prostatectomy: A systematic review and meta-analysis
Shulin Wuab,Sharron X. Lina,Kristine M. Cornejob,Rory K. Crottyb,Michael L. Blutea,Douglas M. Dahla,Chin-Lee Wuab*()
a Department of Urology, Massachusetts General Hospital, Harvard Medical School, Boston, MA, USA
b Department of Pathology, Massachusetts General Hospital, Harvard Medical School, Boston, MA, USA
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Abstract: 

Objective To investigate the association of persistently elevated prostate-specific antigen (PSA) after radical prostatectomy (RP) with clinicopathological features and long-term oncological prognosis for the development of a potential management strategy.
Methods A systematic literature search was performed using PubMed and Web of Science up to June 2021 to identify the eligible studies focusing on understanding the impact of persistent PSA in patients who underwent RP for localized prostate cancer. Meta-analyses were performed on parameters with available information.
Results A total of 32 RP studies were identified, of which 11 included 26 719 patients with consecutive cohorts and the remaining 21 comprised 24 177 patients with cohorts carrying specific restrictions. Of the 11 studies with consecutive cohorts, the incidence of persistent PSA varied between 3.1% and 34.6% with a median of 11.0%. Meta-analyses revealed patients with persistent PSA consistently showed unfavorable clinicopathological features and a more than 3.5-fold risk of poorer biochemical recurrence, metastasis, and prostate cancer-specific mortality prognosis independently, when compared to patients with undetectable PSA. Similarly, cases with persistent PSA in different specific patient cohorts with a higher risk of prostate cancer also showed a trend of worse outcomes.
Conclusion We found that the frequency of persistent PSA was about 11.0% in consecutive RP cohorts. Persistent PSA was significantly associated with unfavorable clinicopathological characteristics and worse oncological outcomes. Patients with persistent PSA after RP may benefit from early salvage treatment to delay or prevent biochemical recurrence, improving oncological outcomes for these patients. Further prospective randomized controlled trials are warranted to understand optimal systemic therapy in these patients.

Key words:  Prostate cancer    Radical prostatectomy    Persistent prostate-specific antigen    Prognosis    Salvage    Systematic review    Meta-analysis
收稿日期:  2021-08-05           接受日期:  2022-01-25           发布日期:  2023-08-11      整期出版日期:  2023-07-20
引用本文:    
. [J]. Asian Journal of Urology, 2023, 10(3): 317-328.
Shulin Wu,Sharron X. Lin,Kristine M. Cornejo,Rory K. Crotty,Michael L. Blute,Douglas M. Dahl,Chin-Lee Wu. Clinicopathological and oncological significance of persistent prostate-specific antigen after radical prostatectomy: A systematic review and meta-analysis. Asian Journal of Urology, 2023, 10(3): 317-328.
链接本文:  
http://www.ajurology.com/CN/10.1016/j.ajur.2022.01.002  或          http://www.ajurology.com/CN/Y2023/V10/I3/317
Reference Year Group Period Total/persistent (n) RP cohort Persist cutoff (ng/mL) Persistent rate (%) BCR (ng/mL) F/U (M) NOS Clinical significance of persistent PSA after RP
Micoogullari et al. [8] 2021 Turkey 2009-2017 875/97 Consecutive ≥0.1 at 6-8 weeks 11.1 Two consecutive PSA≥0.2 18-24 9 -0.1-0.2 ng/mL associated with aggressive disease and BCR in UVa
Milonas et al. [9] 2021 Lithuania 2001-2019 1225/246 Consecutive ≥0.1 at 4-8 weeks 20.1 Two consecutive PSA>0.2 103 7 -Worse outcomes in high risk, worse BCR in intermedium in MVa
Preisser et al. [10] 2019 Germany 1992-2016 11 604/1025 Consecutive ≥0.1 at 6 weeks 8.8 Two consecutive PSA≥0.2 62 9 -Worse prognosis of Mets, OS, PCSM in MVa
Spratt et al. [11] 2018 USA 1990-2015 477/150 Consecutive ≥0.1 at 8 weeks 31.4 NA 77 8 -Worse prognosis of Mets in MVa
García-Barreras et al. [12] 2018 France 2000-2016 2500/229 Consecutive ≥0.1 at 6 weeks 9.2 PSA≥0.2 58 6 -Associated with aggressive disease
Kumar et al. [13] 2017 USA 2008-2013 5300/162 Consecutive ≥0.1 at 6 weeks 3.1 PSA≥0.2 38 7 -Associated with aggressive disease and BCR in UVa
Audenet et al. [14] 2012 France 1996-2006 240/83 Consecutive ≥0.1 at 6 weeks 34.6 PSA>0.2 44 8 -Worse prognosis of BCR in MVa
Eisenberg et al. [35] 2010 USA 1996-2006 525/69 Consecutive >0.05 at 4-12 weeks 13.1 Two consecutive PSA≥0.2 56 8 -Worse 5-year BCR prognosis in MVa
Moreira et al. [36] 2010 USA 2001-2008 901/230 Consecutive ≥0.03 at 4-24 weeks 25.5 PSA>0.2 ≥6 8 -≥0.03 ng/mL showed aggressive features and BCR outcome in MVa
Naselli et al. [15] 2009 Italy 2002-2007 318/33 Consecutive ≥0.1 at 6 weeks 10.3 PSA>0.4 5 8 -Associated with aggressive disease, worse BCR outcome in MVa
Sengupta et al. [16] 2006 USA 1990-1999 2754/303 Consecutive >0.1/0.15 at 8-16 weeks 11.0 NA 102 7 -Worse prognosis of Mets and PCSM in MVa
Sood et al. [37] 2020 USA NA NA/760 RTOG9601 >0.4 NA PSA 0.2-4.0 144 6 -Worse local recurrence, Mets, and OS than BCR patients in UVa
Venclovas et al. [17] 2019 Lithuania 2001-2017 433/130 High-risk PCa ≥0.1 at 6-8 weeks 30.0 Two consecutive PSA≥0.2 64 8 -Predict Mets and PCSM in UVa but not in MV; early BCR
Roy et al. [38] 2019 Canada 2005-2014 167/52 pN1 ≥0.2 at 4-8 weeks 31.1 >0.2 48 6 -Worse prognosis of Mets in MVa, not in OS
Kim et al. [18] 2019 Korea 2002-2014 96/52 pN1 ≥0.1 at 6 weeks 54.2 Two consecutive PSA>0.2 45 7 -Worse prognosis of Mets in MVa
Bartkowiak et al. [19] 2019 Germany 1997-2002 555/133 pN0, SRT ≥0.1 24.0 Two consecutive PSA≥0.2 73 7 -Worse PFS prognosis in UVa but not in MV by pre-SRT PSA
Xiang et al. [20] 2018 China 2009-2014 198/104 Persistent ≥0.1 and < 0.2 at 6-8 weeks NA Two consecutive PSA≥0.2 53 6 -RT and ADT control BCR progress well in MVa
Schmidt-Hegemann et al. [39] 2018 Germany 2014-2017 129/67 PSMA PET/CT RT Undefined 52.0 PSA>0.2 20 6 -With high-risk PCa and shorter time interval to BCR before Tx
McDonald et al. [40] 2018 USA 1982-2015 124/44 pN1 ≥0.2 35.5 PSA≥0.2 98 7 -Associated with Mets in MVa
Fossati et al. [21] 2018 Italy 1996-2009 925/324 SRT ≥0.1 at 4 weeks 35.0 PSA≥0.1 96 7 -Worse Mets prognosis treated with SRT in MVa
Gandaglia et al. [22] 2017 Italy 1994-2014 982/496 Persistent ≥0.1 at 6-8 weeks NA NA 110 6 -Worse PCSM prognosis in UVa, RT benefit
Bianchi et al. [23] 2016 Italy 1998-2013 391/83 pN1 ≥0.1 at 6 weeks 26.0 PSA≥0.2 53 7 -Worse Mets and PCSM prognosis in MVa
Ploussard et al. [24] 2013 France 1998-2011 9735/496 Persistent ≥0.1 at 6 weeks NA NA 27 6 -Worse BCR prognosis and worse salvage Tx outcome in MVa
Lohm et al. [25] 2013 Germany 1997-2004 159/72 BCR, SRT ≥0.1 45.3 PSA≥0.1 42 7 -Similar BCR prognosis as undetectable, SRT benefit
Rogers et al. [26] 2004 USA 1989-2002 2680/160 Persistent ≥0.1 at 12 weeks NA NA ≥12 6 -PSA change ≥0.05 ng/mL showed worse Mets prognosis in UVa
Song et al. [27] 2002 USA 1989-1999 NA/73 SRT ≥0.1 NA NA 36 6 -Worse disease PFS after RT in UVa
Catton et al. [41] 2001 Canada 1987-1994 113/21 ART, SRT ≥0.2 18.6 NA 44 6 -Worse BCR prognosis than undetectable in UVa
Garg et al. [42] 1998 USA 1991-1997 78/37 SRT ≥0.05 47.4 NA 27 7 -Similar 3 years disease-free survival as undetectable
Coetzee et al. [43] 1996 USA NA 45/15 PSM, ART ≥0.5 33.3 NA 33 6 -80% disease progress, may with micro Mets or local disease
Wu et al. [28] 1995 USA 1987-1993 53/38 RT Decreased from 0.3 to 0.1 82.6 NA 15 7 -Predict less undetectable PSA after RT in UVa but not in MV
Link et al. [44] 1991 USA 1984-1988 25/12 ART Undefined 48.0 NA 33 6 -Less durable response after RT
Hudson and Catalona [30] 1990 USA 1983-1988 80/21 RT >0.6 26.3 NA 13 6 -At risk of further progression
  
Variable Study (n) I2 (%) Heterogeneity (p-value) OR 95% CI p-Value Effects model Reference
D'amico risk (H vs. M+L) 5 90 <0.001 3.11 1.78-5.45 <0.001 Random [9,[11], [12], [13],35]
GS (≥8 vs. <8) 7 92 <0.001 3.55 2.04-6.74 <0.001 Random [8,[10], [11], [12], [13], [14],16]
pT stage (≥T3 vs. T2) 8 93 <0.001 3.51 2.28-5.41 <0.001 Random [8,[10], [11], [12], [13], [14], [15], [16]]
EPE (+ vs. -) 5 83 <0.001 2.73 1.82-4.09 <0.001 Random [8,[11], [12], [13],36]
SVI (+ vs. -) 4 64 0.04 4.49 3.10-6.51 <0.001 Random [8,11,16,36]
Margin (PSM vs. NSM) 10 84 <0.001 2.99 2.28-3.92 <0.001 Random [8,[10], [11], [12], [13], [14], [15], [16],35,36]
LNI (+ vs. -) 8 89 <0.001 4.83 2.39-9.76 <0.001 Random [8,[10], [11], [12], [13],15,16,36]
SRT (with vs. without) 3 85 0.001 14.9 7.58-25.22 <0.001 Random [8,10,11]
  
Reference Log-rank test (K-M analysis), p-value Univariate HR (95% CI), p-value Multivariate HR (95% CI), p-value Covariate
Micoogullari et al. [8]
BCR p<0.001 (persistent worse) NA NA NA
Preisser et al. [10]
Mets p<0.001 (persistent worse) NA 3.59 (2.83-4.57), p<0.001 Year/age/pT/GG/pN1
Cancer-specific death p<0.001 (persistent worse) NA 3.15 (1.92-5.18), p<0.001 Year/pT/GG/PSM
All-cause death p<0.001 (persistent worse) NA 1.86 (1.41-2.45), p<0.001 Age/pT/GG/PSM/CCI
Spratt et al. [11]
Mets NA 2.36 (0.89-6.72), p=0.08 4.26 (1.16-21.8), p=0.03 Decipher risk/pN1
Kumar et al. [13]
BCR p<0.01 (persistent worse) NA NA NA
Audenet et al. [14]
BCR p<0.001 (persistent worse) NA NA NA
Eisenberg et al. [35]
BCR p<0.01 (persistent worse) NA NA NA
Naselli et al. [15]
BCR p<0.001 (persistent worse) NA 4.54 (2.35-8.78), p<0.001 pT/pN
Moreira et al. [36]
BCR p<0.001 (persistent worse) 3.88 (2.13-7.06), p<0.001 3.23 (1.62-6.48), p=0.001 BMI/GS/PSM
Sengupta et al. [16]
Mets p<0.001 (persistent worse) NA 3.58 (2.37-5.41), p<0.001 PSA (log2)/GS/SVI/PSM
Cancer-specific death p<0.001 (persistent worse) NA 4.26 (2.27-7.99), p<0.001 PSA (log2)/GS/SVI/PSM
  
  
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