Abstract
Active surveillance (AS), where biopsies are conducted to detect cancer progression, has been acknowledged as an efficient way to reduce the overtreatment of prostate cancer. Most AS cohorts use fixed biopsy schedules for all patients. However, the ideal test frequency remains unknown, and the routine use of such invasive tests burdens the patients. An emerging idea is to generate personalized biopsy schedules based on each patient's progression-specific risk. To achieve that, we propose the interval-censored cause-specific joint model (ICJM), which models the impact of longitudinal biomarkers on cancer progression while considering the competing event of early treatment initiation. The underlying likelihood function incorporates the interval-censoring of cancer progression, the competing risk of treatment, and the uncertainty about whether cancer progression occurred since the last biopsy in patients that are right-censored or experience the competing event. The model can produce patient-specific risk profiles until a horizon time. If the risk exceeds a certain threshold, a biopsy is conducted. The optimal threshold can be chosen by balancing two indicators of the biopsy schedules: the expected number of biopsies and expected delay in detection of cancer progression. A simulation study showed that our personalized schedules could considerably reduce the number of biopsies per patient by 34%-54% compared to the fixed schedules, though at the cost of a slightly longer detection delay.
Original language | English |
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Number of pages | 33 |
Journal | arXiv preprint arXiv:2104.10751 |
DOIs | |
Publication status | Published - 3 Jan 2023 |
Bibliographical note
AcknowledgementsThe research was funded by the National Institutes of Health (the NIH CISNET Prostate Award CA253910).
The authors would also like to show our gratitude to the Canary PASS team and all study participants.