abstract
OBJECTIVES:
While
primary treatment for high-grade
serous ovarian cancer tends to be
uniform - maximal debulking and platinum/taxane adjuvant chemotherapy -
there is little standardization of treatment in the recurrent setting
beyond the exhaustive use of platinum therapies. Using secondary data
from multiple centers participating in the Cancer Genome Atlas study
(TCGA), we seek to characterize clinical features, timing and serial
response data to provide empirical evidence for treatment expectations
in the recurrent setting.
METHODS:
We
conducted a retrospective survival analysis of TCGA study primary and
secondary patient chemotherapy regimens by characterizing the dynamics
of 1119 lines of therapy comprising the treatment of
461 high-grade
serous ovarian cancer patients. All patients with post-surgical drug
therapy information from the TCGA database were included in this study.
RESULTS:
A
complete response to adjuvant therapy led to longer overall survival,
but did not affect treatment free intervals (TFIs) after relapse of
disease. A strong predictor of the TFI on the next treatment regimen was
the previous TFI with a decaying effect. The number of previous
treatments, of platinum treatments, and the length of time from surgery
all have an exponentially decreasing effect on TFI. Re-treatment times
appear to cluster at predictable times following surgery.
CONCLUSIONS:
While
patients experience a consistent reduction in TFI with increasing
re-treatment,
the initial adjuvant interval is unrelated to later
interval lengths. Platinum re-treatment remained an effective option in
patients typically thought to be platinum resistant and the timing of
monitoring visits may drive overall re-treatment patterns.
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