Type of anesthesia for cancer resection surgery: No differential impact on cancer recurrence in mouse models of breast cancer

Authors

Julia Dubowitz, Monash Institute of Pharmaceutical Sciences
Alexandra I. Ziegler, Monash Institute of Pharmaceutical Sciences
Richard Beare, Monash University
Fabian Jost-Brinkman, Monash Institute of Pharmaceutical Sciences
Adam K. Walker, Monash Institute of Pharmaceutical Sciences
Ryan D. Gillis, Monash Institute of Pharmaceutical Sciences
Aeson Chang, Monash Institute of Pharmaceutical Sciences
Ni Chun Chung, Monash Institute of Pharmaceutical Sciences
Olga A. Martin, University of Melbourne
Frédéric Hollande, University of Melbourne
Bernhard Riedel, Monash Institute of Pharmaceutical Sciences
Erica K. Sloan, Monash Institute of Pharmaceutical Sciences

Publication Name

PLoS ONE

Abstract

Background Surgery is essential for curative treatment of solid tumors. Evidence from recent retrospective clinical analyses suggests that use of propofol-based total intravenous anesthesia during cancer resection surgery is associated with improved overall survival compared to inhaled volatile anesthesia. Evaluating these findings in prospective clinical studies is required to inform definitive clinical guidelines but will take many years and requires biomarkers to monitor treatment effect. Therefore, we examined the effect of different anesthetic agents on cancer recurrence in mouse models of breast cancer with the overarching goal of evaluating plausible mechanisms that could be used as biomarkers of treatment response. Methods To test the hypothesis that volatile anesthesia accelerates breast cancer recurrence after surgical resection of the primary tumor, we used three mouse models of breast cancer. We compared volatile sevoflurane anesthesia with intravenous propofol anesthesia and used serial non-invasive bioluminescent imaging to track primary tumor recurrence and metastatic recurrence. To determine short-term perioperative effects, we evaluated the effect of anesthesia on vascular integrity and immune cell changes after surgery in animal models. Results Survival analyses found that the kinetics of cancer recurrence and impact on survival were similar regardless of the anesthetic agent used during cancer surgery. Vascular permeability, immune cell infiltration and cytokine profiles showed no statistical difference after resection with inhaled sevoflurane or intravenous propofol anesthesia. Conclusions These preclinical studies found no evidence that choice of anesthetic agent used during cancer resection surgery affected either short-term perioperative events or long-term cancer outcomes in mouse models of breast cancer. These findings raise the possibility that mouse models do not recapitulate perioperative events in cancer patients. Nonetheless, the findings suggest that future evaluation of effects of anesthesia on cancer outcomes should focus on cancer types other than breast cancer.

Open Access Status

This publication may be available as open access

Volume

18

Issue

11 November

Article Number

e0293905

Funding Number

1147498

Funding Sponsor

National Health and Medical Research Council