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How Well do Polygenic Risk Scores Identify Men at High Risk for Prostate Cancer? Systematic Review and Meta-Analysis

Authors :
Aino Siltari
Ragnar Lönnerbro
Karl Pang
Kirill Shiranov
Alex Asiimwe
Susan Evans-Axelsson
Billy Franks
Amit Kiran
Teemu J. Murtola
Jack Schalken
Carl Steinbeisser
Anders Bjartell
Anssi Auvinen
J. N’Dow
E.J. Smith
R. Shepherd
M. Ribal
N. Mottet
L. Moris
M. Lardas
P-P. Willemse
G. Gandaglia
R. Campi
Rossella Nicoletti
M. Gacci
A. Briganti
M.M. Ratti
E. Alleva
L. Leardini
E.S. Sisca
R. Bangma
M. Roobol
S. Remmers
D. Tilki
T. Visakorpi
K. Talala
T. Tammela
M. van Hemelrijck
K. Bayer
S. Lejeune
S. Byrne
L. Fialho
P. Palaiologou B. De Meulder
C. Auffray
A. Hijazy
S. Power
N. Zounemat Kermani
K. van Bochove
M. Kalafati
M. Moinat
E. Voss
D. Horgan
L. Fullwood
M. Holtorf
D. Lancet
G. Bernstein
I. Omar
S. MacLennan
S. Maclennan
S. Tripathee
M. Wirth
M. Froehner
B. Brenner
A. Borkowetz
C. Thomas
F. Horn
K. Reiche
M. Kreux
A. Josefsson
D. Gasi Tandefekt
J. Hugosson
H. Huisman
J. Schalken
T. Hofmacher
P. Lindgren
E. Andersson
A. Fridhammar
J. Zong
J-E. Butler-Ransohoff
R. Herrera
M. Maass
P. Torremante
M.D. Voss
Z. Devecseri
T. Abbott
C. Dau
K. Papineni
R. Snijder
M. Lambrecht
R. Wolfinger
S. Rogiers
A. Servan
L. Antoni
K. Pacoe
P. Robinson
B. Jaton
D. Bakkard
H. Turunen
O. Kilkku
P. Pohjanjousi
O. Voima
L. Nevalaita
C. Reich
S. Araujo
E. Longden-Chapman
D. Burke
P. Agapow
S. Derkits
M. Licour
C. McCrea
S. Payne
A. Yong
L. Thompson
S. Le Mare
M Bussmann
D. Kotik
Source :
Clinical Genitourinary Cancer, 21, 2, pp. 316.e1-316.e11, Clinical Genitourinary Cancer, 21, 316.e1-316.e11
Publication Year :
2023

Abstract

Contains fulltext : 291547.pdf (Publisher’s version ) (Open Access) OBJECTIVES: Genome-wide association studies have revealed over 200 genetic susceptibility loci for prostate cancer (PCa). By combining them, polygenic risk scores (PRS) can be generated to predict risk of PCa. We summarize the published evidence and conduct meta-analyses of PRS as a predictor of PCa risk in Caucasian men. PATIENTS AND METHODS: Data were extracted from 59 studies, with 16 studies including 17 separate analyses used in the main meta-analysis with a total of 20,786 cases and 69,106 controls identified through a systematic search of ten databases. Random effects meta-analysis was used to obtain pooled estimates of area under the receiver-operating characteristic curve (AUC). Meta-regression was used to assess the impact of number of single-nucleotide polymorphisms (SNPs) incorporated in PRS on AUC. Heterogeneity is expressed as I(2) scores. Publication bias was evaluated using funnel plots and Egger tests. RESULTS: The ability of PRS to identify men with PCa was modest (pooled AUC 0.63, 95% CI 0.62-0.64) with moderate consistency (I(2) 64%). Combining PRS with clinical variables increased the pooled AUC to 0.74 (0.68-0.81). Meta-regression showed only negligible increase in AUC for adding incremental SNPs. Despite moderate heterogeneity, publication bias was not evident. CONCLUSION: Typically, PRS accuracy is comparable to PSA or family history with a pooled AUC value 0.63 indicating mediocre performance for PRS alone. 01 april 2023

Details

ISSN :
15587673
Volume :
21
Database :
OpenAIRE
Journal :
Clinical Genitourinary Cancer
Accession number :
edsair.doi.dedup.....aebe650dd619575ff9d0e1f7617b2c01