| Literature DB >> 31205032 |
Dipak Panigrahy1,2,3, Allison Gartung1,2,3, Jun Yang4, Haixia Yang1,2,3, Molly M Gilligan1,2,3, Megan L Sulciner1,2,3, Swati S Bhasin5, Diane R Bielenberg6, Jaimie Chang1,2,3, Birgitta A Schmidt7, Julia Piwowarski1,2,3, Anna Fishbein1,2,3, Dulce Soler-Ferran1,2,3, Matthew A Sparks8, Steven J Staffa9, Vidula Sukhatme10, Bruce D Hammock4, Mark W Kieran11,12, Sui Huang13, Manoj Bhasin5, Charles N Serhan14, Vikas P Sukhatme3,5,15.
Abstract
Cancer therapy is a double-edged sword, as surgery and chemotherapy can induce an inflammatory/immunosuppressive injury response that promotes dormancy escape and tumor recurrence. We hypothesized that these events could be altered by early blockade of the inflammatory cascade and/or by accelerating the resolution of inflammation. Preoperative, but not postoperative, administration of the nonsteroidal antiinflammatory drug ketorolac and/or resolvins, a family of specialized proresolving autacoid mediators, eliminated micrometastases in multiple tumor-resection models, resulting in long-term survival. Ketorolac unleashed anticancer T cell immunity that was augmented by immune checkpoint blockade, negated by adjuvant chemotherapy, and dependent on inhibition of the COX-1/thromboxane A2 (TXA2) pathway. Preoperative stimulation of inflammation resolution via resolvins (RvD2, RvD3, and RvD4) inhibited metastases and induced T cell responses. Ketorolac and resolvins exhibited synergistic antitumor activity and prevented surgery- or chemotherapy-induced dormancy escape. Thus, simultaneously blocking the ensuing proinflammatory response and activating endogenous resolution programs before surgery may eliminate micrometastases and reduce tumor recurrence.Entities:
Keywords: Cancer; Eicosanoids; Inflammation; Oncology; Surgery
Year: 2019 PMID: 31205032 PMCID: PMC6597207 DOI: 10.1172/JCI127282
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808