Vascular Damage and Anti-angiogenic Effects of Tumor Vessel-Targeted Liposomal Chemotherapy

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Vascular Damage and Anti-angiogenic Effects of Tumor Vessel-Targeted Liposomal Chemotherapy¹

Fabio Pastorino, Chiara Brignole, Danilo Marimpietri, Michele Cilli, Claudio Gambini, Domenico Ribatti, Renato Longhi, Theresa M. Allen, Angelo Corti and Mirco Ponzoni²

Differentiation Therapy Unit, Laboratory of Oncology [F. P., C. B., D. M., M. P.] and Laboratory of Pathology [C. G.], G. Gaslini Children’s Hospital, 16148 Genoa, Italy; Animal Research Facility, Istituto Nazionale per la Ricerca sul Cancro, 16100, Genoa, Italy [M. C.]; Department of Human Anatomy and Histology, University of Bari, 70100 Bari, Italy [D. R.]; Istituto di Chimica del Riconoscimento Molecolare, Consiglio Nazionale delle Ricerche, 20131 Milan, Italy [R. L.]; Department of Pharmacology, University of Alberta, T6G 2H7 Edmonton, Canada [T. M. A.]; and Immunobiotechnology Unit, San Raffaele Institute, 20132 Milan, Italy [A. C.]

The poor selective toxicity of chemotherapeutic anticancer drugsleads to dose-limiting side effects that compromise clinicaloutcome. Solid tumors recruit new blood vessels to support tumorgrowth, and unique epitopes expressed on tumor endothelial cellscan function as targets for the anti-angiogenic therapy of cancer.An NGR peptide that targets aminopeptidase N, a marker of angiogenicendothelial cells, was coupled to the surface of liposomal doxorubicin(NGR-SL[DXR]) and was used to treat orthotopic neuroblastoma(NB) xenografts in SCID mice. Pharmacokinetic studies indicatedthat liposomes coupled to NGR peptide had long-circulating profilesin blood. Their uptake into NB tumor was time dependent, beingat least 10 times higher than that of nontargeted liposomes(SL[DXR]) after 24 h, with DXR spreading outside the blood vesselsand into the tumors. No uptake was observed into tumors of micetreated with the mismatched peptide ARA-targeted SL[DXR]. Tumor-specificDXR uptake was completely blocked when mice were coinjectedwith a 50-fold molar excess of the soluble NGR peptide. Adrenaltumor-bearing mice treated with 2 mg/kg/week/x3 of NGR-SL[DXR]partly outlived the control mice (P < 0.001), whereas doses> 3 mg/kg/week/x3 were toxic. Histopathological analysisof cryosections taken from treated mice revealed pronounceddestruction of the tumor vasculature with a marked decreasedin vessel density. Double staining of tumors with terminal deoxynucleotidyltransferase-mediated nick end labeling and antifactor VIII antibodyor antihuman NB demonstrated endothelial cell apoptosis in thevasculature, as well as increased tumor cell apoptosis. Moreover,mice injected with 3 mg/kg/week/x3 of NGR-SL[DXR] displayedrapid tumor regression, as well as inhibition of metastasesgrowth (P = 0.0002). One day after the third treatment, fourof six mice showed no evidence of tumors, and the two othersshowed a >80% reduction in tumor mass and a >90% suppressionof blood vessel density (P < 0.01). In contrast, mice treatedwith ARA-SL[DXR] formed large well-vascularized tumors. Finally,a metronomic administration of NGR-SL[DXR] (1 mg/kg/every other2 days x 9) induced complete tumor eradication in all animals(P < 0.0001). Our strategy markedly enhanced the therapeuticindex of DXR and enabled metronomic administration of therapeuticdoses. A dual mechanism of action is proposed: indirect tumorcell kill via the destruction of tumor endothelium by NGR-targetedliposomes and direct tumor cell kill via localization of liposomalDXR to the tumor interstitial space. This combined strategyhas the potential to overcome some major limitations of conventionalchemotherapy.

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