Platinum Chemotherapy Induces Lymphangiogenesis in Cancerous and Healthy Tissues That Can be Prevented With Adjuvant Anti-VEGFR3 Therapy

Author:

Harris Alexandra R.,Esparza Savieay,Azimi Mohammad S.,Cornelison Robert,Azar Francesca N.,Llaneza Danielle C.,Belanger Maura,Mathew Alexander,Tkachenko Svyatoslav,Perez Matthew J.,Rosean Claire Buchta,Bostic Raegan R.,Cornelison R. Chase,Tate Kinsley M.,Peirce-Cottler Shayn M.,Paquette Cherie,Mills Anne,Landen Charles N.,Saucerman Jeff,Dillon Patrick M.,Pompano Rebecca R.,Rutkowski Melanie A.,Munson Jennifer M.

Abstract

Chemotherapy has been used to inhibit cancer growth for decades, but emerging evidence shows it can affect the tumor stroma, unintentionally promoting cancer malignancy. After treatment of primary tumors, remaining drugs drain via lymphatics. Though all drugs interact with the lymphatics, we know little of their impact on them. Here, we show a previously unknown effect of platinums, a widely used class of chemotherapeutics, to directly induce systemic lymphangiogenesis and activation. These changes are dose-dependent, long-lasting, and occur in healthy and cancerous tissue in multiple mouse models of breast cancer. We found similar effects in human ovarian and breast cancer patients whose treatment regimens included platinums. Carboplatin treatment of healthy mice prior to mammary tumor inoculation increased cancer metastasis as compared to no pre-treatment. These platinum-induced phenomena could be blocked by VEGFR3 inhibition. These findings have implications for cancer patients receiving platinums and may support the inclusion of anti-VEGFR3 therapy into treatment regimens or differential design of treatment regimens to alter these potential effects.

Publisher

Frontiers Media SA

Subject

Cancer Research,Oncology

Reference70 articles.

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