Abstract

BackgroundInvestigate the impact of interval cytoreductive surgery (ICS) on progression in an orthotopic mouse model of ovarian cancer and the impact of chemotherapy delivered at various timelines following surgery.MethodsLuciferase-expressing ID8 murine ovarian cancer cells were implanted intra-bursally and IP to C57BL/7 mice. Once disease was established by bioluminescence, 2 cycles of neoadjuvant cisplatin were administered, and animals received either ICS (removal of the injected bursa/primary tumor) or anesthesia alone. Postsurgical chemotherapy was administered on the same day as the intervention (ICS/anesthesia), or on day 7 or day 28 following the intervention. Progression was quantified serially with in vivo bioluminescence imaging. Volume of ascitic fluid volume collected at necropsy was measured.ResultsAnimals were matched for tumor burden at stratification. There was no accelerated growth of residual tumor after interval cytoreduction compared to controls. Animals who received chemotherapy on postoperative day (POD) 7 had better disease control compared to standard-of-care POD 28. Animals who underwent surgery had less ascites at necropsy compared to those who had anesthesia alone.ConclusionsIn this animal model, surgical wounding with suboptimal cytoreduction after neoadjuvant chemotherapy did not cause accelerated expansion of residual disease. Surgical wounding appears to impair cisplatin activity when given at time of surgery.

Highlights

  • Investigate the impact of interval cytoreductive surgery (ICS) on progression in an orthotopic mouse model of ovarian cancer and the impact of chemotherapy delivered at various timelines following surgery

  • Using an ID8 syngeneic model of ovarian cancer [24, 25] modified to mimic residual disease following optimal primary cytoreduction, we demonstrated that incisional wounding accelerated tumor growth and decreased perioperative cisplatin efficacy [17]

  • We evaluated the impact of interval cytoreductive surgery (ICS) in an immunocompetent orthotopic mouse model of advanced ovarian cancer using the syngeneic ID8 murine ovarian cancer cell line and examined the impact on perioperative cisplatin treatment

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Summary

Introduction

Investigate the impact of interval cytoreductive surgery (ICS) on progression in an orthotopic mouse model of ovarian cancer and the impact of chemotherapy delivered at various timelines following surgery. Clark et al Journal of Ovarian Research (2021) 14:157 suboptimal cytoreduction, defined as residual disease at the conclusion of surgery of greater than 1 c­m3, offers no improvement in overall survival [5, 6]. Those patients who have presumed unresectable disease or who are judged to be poor surgical candidates are best offered neoadjuvant chemotherapy (NACT) followed by interval cytoreduction and post-operative adjuvant consolidation chemotherapy [7, 8]

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