Abstrakti
To compare the survival between screen-detected and clinically detected cancers, we applied a series of non-homogeneous stochastic processes to deal with leadtime, length bias, and over-detection by using full information on detection modes obtained from the Finnish randomized controlled trial for prostate cancer screening. The results show after 9-year follow-up the hazard ratio of prostate cancer death for screen-detected cases against clinically detected cases increased from 0.24 (95% CI: 0.16-0.35) without correction for these biases, to 0.76 after correction for leadtime and length biases, and finally to 1.03 (95% CI: 0.79-1.33) for a further adjustment for over-detection. Adjustment for leadtime and length bias but no over-detection led to a 24% reduction in prostate cancer death as a result of prostate-specific antigen test. The further calibration of over-detection indicates no gain in survival of screen-detected prostate cancers (excluding over-detected case as stayer considered in the mover-stayer model) as compared with the control group in the absence of screening that is considered as the mover. However, whether the model assumption on over-detection is robust should be validated with other data sets and longer follow-up.
Alkuperäiskieli | Englanti |
---|---|
Sivut | 20-44 |
Sivumäärä | 25 |
Julkaisu | Biometrical Journal |
Vuosikerta | 54 |
Numero | 1 |
DOI - pysyväislinkit | |
Tila | Julkaistu - 2012 |
OKM-julkaisutyyppi | A1 Alkuperäisartikkeli tieteellisessä aikakauslehdessä |
Tutkimusalat
- Leadtime and length bias
- Mass screening
- Prostate neoplasms
- Prostate-specific antigen
- Stochastic processes
Julkaisufoorumi-taso
- Jufo-taso 1