Abstract
The selective delivery of bioactive agents to tumors reduces toxicity and enhances the efficacy of anticancer therapies. In this study, we show that the antibody F8, which recognizes perivascular and stromal EDA-fibronectin (EDA-Fn), when conjugated to interleukin-2 (F8-IL2) can effectively inhibit the growth of EDA-Fn-expressing melanomas in combination with paclitaxel. We obtained curative effects with paclitaxel administered before the immunocytokine. Coadministration of paclitaxel increased the uptake of F8 in xenografted melanomas, enhancing tumor perfusion and permeability. Paclitaxel also boosted the recruitment of F8-IL2-induced natural killer (NK) cells to the tumor, suggesting a host response as part of the observed therapeutic benefit. In support of this likelihood, NK cell depletion impaired the antitumor effect of paclitaxel plus F8-IL2. Importantly, this combination reduced both the tumor burden and the number of pulmonary metastatic nodules. The combination did not cause cumulative toxicity. Together, our findings offer a preclinical proof that by acting on the tumor stroma paclitaxel potentiates the antitumor activity elicited by a targeted delivery of IL2, thereby supporting the use of immunochemotherapy in the treatment of metastatic melanoma.
Highlights
Melanoma is the most common nonhematopoietic cancer in young adults, and the incidence of the disease is increasing at an alarming pace worldwide [1]
We show that human metastatic melanoma lesions express high levels of perivascular and stromal EDAFn, which is detectable with the recombinant antibody F8, and that the immunocytokine F8-IL2 administrated in combination with paclitaxel significantly inhibits [60%–80% complete regressions (CR)] the growth of a human xenografted melanoma expressing a high level of EDA-Fn in nude mice
The WM1552/5 and the A375M metastatic melanoma were chosen to evaluate the therapeutic activity of the F8-IL2 immunocytokine in preclinical models
Summary
Melanoma is the most common nonhematopoietic cancer in young adults, and the incidence of the disease is increasing at an alarming pace worldwide [1]. In a meta-analysis of 42 phase II cooperative group trials, median survival in metastatic stage IV melanoma was only 6.2 months, with a mean 1-year overall survival (OS) rate of 25.5% regardless of treatment regimen [2]. 3)—metastatic melanoma remains a solid malignancy that deserves therapeutic options. Authors' Affiliations: Departments of 1Oncology and 2Neuroscience, Mario Negri Institute for Pharmacological Research; 3Dipartimento di Fisica, Politecnico di Milano, Milan, Italy; 4Institute of Pathology, University Hospital Jena, Jena, Germany; 5Centro Ricerche Bracco–Bracco Imaging Spa, Colleretto Giacosa, Italy; 6Philochem AG; 7Institute of Pharmaceutical Sciences, ETH Zu€rich, Zu€rich, Switzerland; and 8Institute of Pathology, Helios-Klinikum Erfurt, Erfurt, Germany. Note: Supplementary data for this article are available at Cancer Research Online (http://cancerres.aacrjournals.org/).
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