Enhanced anti-tumor and anti-angiogenic efficacy of a novel liposomal fenretinide on human neuroblastoma

被引:37
作者
Di Paolo, Daniela [1 ]
Pastorino, Fabio [1 ]
Zuccari, Guendalina [2 ]
Caffa, Irene [1 ]
Loi, Monica [1 ]
Marimpietri, Danilo [3 ]
Brignole, Chiara [1 ]
Perri, Patrizia [1 ]
Cilli, Michele [4 ]
Nico, Beatrice [5 ,6 ]
Ribatti, Domenico [5 ,6 ]
Pistoia, Vito [3 ]
Ponzoni, Mirco [1 ]
Pagnan, Gabriella [1 ]
机构
[1] Ist Giannina Gaslini, Lab Oncol, Expt Therapies Unit, I-16148 Genoa, Italy
[2] Univ Bologna, Dept Life Qual Studies, I-47921 Rimini, Italy
[3] Ist Giannina Gaslini, Lab Oncol, I-16148 Genoa, Italy
[4] IRCCS Azienda Osped Univ San Martino, IST Ist Nazl Ric Canc, Anim Facil, I-16132 Genoa, Italy
[5] Univ Bari, Sch Med, Sect Human Anat & Histol, Dept Basic Med Sci Neurosci & Sensory Organs, I-70124 Bari, Italy
[6] Natl Canc Inst Giovanni Paolo II, I-70124 Bari, Italy
关键词
Nanoliposomes; Fenretinide; Neuroblastoma; Vascular targeting; Targeted therapy; PHASE-I TRIAL; ANTISENSE OLIGODEOXYNUCLEOTIDES; INDUCED APOPTOSIS; RETINOIC ACID; CELLS; CHILDREN; GROWTH; N-(4-HYDROXYPHENYL)RETINAMIDE; IMMUNOLIPOSOMES; CHEMOTHERAPY;
D O I
10.1016/j.jconrel.2013.06.015
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
Neuroblastoma is an embryonal tumor originating from the simpatico-adrenal lineage of the neural crest. It approximately accounts for about 15% of all pediatric oncology deaths. Despite advances in multimodal therapy, metastatic neuroblastoma tumors at diagnosis remain a clinical challenge. Retinoids are a class of compounds known to induce both terminal differentiation and apoptosis/necrosis of neuroblastoma cells. Among them, fenretinide (HPR) has been considered one of the most promising anti-tumor agent but it is partially efficacious due to both poor aqueous solubility and rapid metabolism. Here, we have developed a novel HPR formulation, bywhich the drug was encapsulated into sterically stabilized nanoliposomes (NL[HPR]) according to the Reverse Phase Evaporation method. This procedure led to a higher structural integrity of liposomes in organic fluids for a longer period of time, in comparison with our previous liposomal formulation developed by the film method. Moreover, NL[HPR] were further coupled with NGR peptides for targeting the tumor endothelial cell marker, aminopeptidase N (NGR-NL[HPR]). Orthotopically xenografted neuroblastoma-bearing mice treated with NGR-NL [HPR] lived statistically longer than mice untreated or treated with free HPR (NGR-NL[HPR] vs both control and HPR: P < 0.0001). Also, NL[HPR] resulted in a statistically improved survival (NL[HPR] vs both control and HPR: P < 0.001) but to a less extent if compared with that obtained with NGR-NL[HPR] (NGR-NL[HPR] vs NL[HPR]: P < 0.01). Staining of tumor sections with antibodies specific for neuroblastoma and for either pericytes or endothelial cells evidenced that HPR reduced neuroblastoma growth through both anti-tumor and anti-angiogenic effects, mainly when delivered by NGR-NL[HPR]. Indeed, in this group of mice a marked reduction of tumor progression, of intra-tumoral vessel counts and VEGF expression, together with a marked down-modulation of matrix metalloproteinases MMP2 and MMP9, was observed. In conclusion, the use of this novel targeted delivery system for the apoptotic and antiangiogenic drug, fenretinide, could be considered as an adjuvant tool in the future treatment of neuroblastoma patients. (C) 2013 Elsevier B. V. All rights reserved.
引用
收藏
页码:445 / 451
页数:7
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