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EPV211/#493 Incomplete cycles of chemotherapy using weekly gemcitabine affecting prognosis of platinum-resistant ovarian cancer
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  1. A Seol1,
  2. SJ Park2,
  3. EJ Lee1,
  4. M Lee1,
  5. HS Kim1,
  6. HH Chung1,
  7. J-W Kim1,
  8. NH Park1 and
  9. Y-S Song1
  1. 1Seoul National University College of Medicine, Department of Obstetrics and Gynecology, Seoul, Korea, Republic of
  2. 2Seoul National University College of Medicine, Obstetrics and Gynecology, Seoul, Korea, Republic of

Abstract

Objectives To evaluate the risk of incomplete cycles of weekly gemcitabine on survival for patients with platinum-resistant ovarian cancer (PROC).

Methods We collected patients with PROC who received weekly gemcitabine (1000mg/m2; D1, D8 every 3 weeks or D1, D8, D15 every 4 weeks) between 2006–2018. We investigated rates of completed cycles, skipped cycles, dose reduction (DR) and prophylactic granulocyte colony-stimulating factor (G-CSF) usage, tumor response and factors affecting progression-free survival (PFS) and overall survival (OS).

Results A total of 101 patients with PROC received weekly gemcitabine. 58(57.4%) completed scheduled cycles without skip and 86 (85.1%) completed more than 80% of scheduled cycles. DR and the use of G-CSF were observed in 34(33.7%) and 25 patients (24.8%), respectively. Weekly gemcitabine was skipped because of grade3 or more hematologic toxicity(31.7%). Complete response, partial response, stable disease and progressive disease were identified in 1(1%), 12 (11.9%), 26 (25.7%) and 61 (60.4%). In terms of survival, the completion rate of scheduled cycles≥80% was a factor for better OS (median OS, the completion rate of scheduled cycles≥80% vs. <80%, 39.23 months vs. 8.97months, p=0.011), but not for better PFS (median PFS, the completion rate of scheduled cycles≥80% vs. <80%, 2.89months vs. 2.43months, p=0.238). Use of G-CSF was factor for better PFS and OS (median PFS, G-CSF group vs. non-G-CSF group, 2.53month vs. 2.07month, p=0.023; median OS, 39.23months vs. 14.72months, p=0.011)

Conclusions Incompletion of scheduled cycles of weekly gemcitabine may be associated with prognosis, and especially, the completion rate of scheduled cycles<80% may not improve survival in patients with PROC.

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