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Characteristics of screen-failures in prostate cancer screening

Sammanfattning
ABSTRACT Although prostate-specific antigen (PSA)-based screening has been shown to reduce prostate cancer (PC)-specific mortality with large variations in mortality reduction with different screening algorithms, the optimal screening strategy has not yet been established. This thesis aims at exploring aspects of underdiagnosis in PC screening, focusing on the impact of screening failures on screening effectiveness. All of its papers are based on the Göteborg randomized PC screening trial except for Paper I, which also includes data from the Dutch center of the European Randomized Study of Screening for Prostate Cancer (ERSPC). Paper I analyzes the frequency of interval cancers (IC) between a 2- and a 4-year screening interval, as high IC rates are recognized as a limitation for screening effectiveness in screening for other cancers. Extremely few IC cases were detected and no difference was found in cumulative incidences of IC with a 2- and 4-year interval. In Paper II, the risk of PC death is compared between attendees and nonattendees in screening. A large proportion of PC deaths occurred in nonattendees, and the majority of attendees dying from PC were men aged ≥60 years when detected at their first (prevalence) screen. Paper III analyzes the PC incidence after screening cessation (due to upper age limit). Compared to the control arm, the incidence of potentially aggressive PC was reduced in the screening arm up to 9 years post-screening but thereafter approached the incidence of the control group. In Paper IV, multiparametric magnetic resonance imaging (mpMRI) was evaluated as a screening tool. A lowered PSA cut-off (1.8 ng/ml) + mpMRI followed by targeted biopsy yielded a higher detection rate of clinically significant PC compared with “conventional” screening (PSA, cut-off ≥3 ng/ml followed by systematic biopsy), requiring a decreased number of biopsies. In conclusion, better screening strategies are needed to improve on screening failures. One option may be to lower the PSA cut-off and introduce sequential testing with mpMRI to decide which men to refer for biopsy. Age at screening start and cessation greatly impacts efficiency; starting at age 60 is probably too late, and stopping at age 70 for all men is probably too early.
Delarbeten
I. Roobol M, Grenabo A et al. Interval cancers in prostate cancer screening: comparing 2- and 4- year screening intervals in the European Randomised Study of Screening for Prostate Cancer, Gothenburg and Rotterdam. J Natl Cancer Inst 2007; 99: 1296-303 ::PMID::17728218
 
II. Grenabo Bergdahl A, Aus G et al. Risk of dying from prostate cancer in men randomised to screening: differences between attendees and nonattendees. Cancer 2009; 115: 5672-9 ::PMID::19813273
 
III. Grenabo Bergdahl A, Holmber E et al. Incidence of prostate cancer after termination of screening in a population-based randomised screening trial. Eur Urol 2013; 64: 703-9 ::PMID::23721957
 
IV. Grenabo Bergdahl A, Wilderäng U et al. Role fo MRI in prostate cancer screening: results from a pilot study nested within the Göteborg randomized screening trial (manuscript)
 
Examinationsnivå
Doctor of Philosophy (Medicine)
Universitet
University of Gothenburg. Sahlgrenska Academy
Institution
Institute of Clincial Sciences. Department of Urology
Disputation
Fredagen den 17 april 2015, kl. 9.00, Hörsal Arvid Carlsson, Academicum, Medicinaregatan 3.
Datum för disputation
2015-04-17
E-post
anna.grenabo@vgregion.se
URL:
http://hdl.handle.net/2077/38003
Samlingar
  • Doctoral Theses / Doktorsavhandlingar Institutionen för kliniska vetenskaper
  • Doctoral Theses from Sahlgrenska Academy
  • Doctoral Theses from University of Gothenburg / Doktorsavhandlingar från Göteborgs universitet
Fil(er)
Thesis frame (2.687Mb)
Abstract (254.1Kb)
Datum
2015-03-30
Författare
Grenabo Bergdahl, Anna
Nyckelord
screening
prostate cancer
screening failures
antigen
age
interval cancer
multiparametric magnetic resonance imaging
non-attendees
prostate cancer screening
Publikationstyp
Doctoral thesis
ISBN
978-91-628-9331-6
978-91-628-9330-9 (printed edition)
Språk
eng
Metadata
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