Nanomicellar Lenalidomide-Fenretinide Combination Suppresses Tumor Growth in an MYCN Amplified Neuroblastoma Tumor

Isabella Orienti; Giovanna Farruggia; Ferro Nguyen; Peng Guan; Natalia Calonghi; Venkatadri Kolla; Michael Chorny; Garrett M Brodeur

doi:10.2147/IJN.S262032

Nanomicellar Lenalidomide-Fenretinide Combination Suppresses Tumor Growth in an MYCN Amplified Neuroblastoma Tumor

Int J Nanomedicine. 2020 Sep 16:15:6873-6886. doi: 10.2147/IJN.S262032. eCollection 2020.

Authors

Isabella Orienti¹, Giovanna Farruggia¹, Ferro Nguyen², Peng Guan², Natalia Calonghi¹, Venkatadri Kolla², Michael Chorny², Garrett M Brodeur²

Affiliations

¹ Department of Pharmacy and Biotechnology, University of Bologna, Bologna 40127, Italy.
² Divisions of Oncology and Cardiology, Children's Hospital of Philadelphia, Philadelphia, PA 19104, USA.

Abstract

Purpose: In a previous study, we demonstrated that the combination of fenretinide with lenalidomide, administered by a novel nanomicellar formulation (FLM), provided a strong antitumor effect in a neuroblastoma TrkB-expressing tumor. In this study, we tested the nanomicellar combination in an MYCN amplified neuroblastoma xenograft to assess its efficacy in different tumor genotypes and evaluate the interactions of the nanomicelles with the tumor cells.

Experimental design: FLM was administered to mice bearing human NLF xenografts to evaluate its efficacy in comparison with the nanomicelles containing fenretinide alone (FM). Confocal laser-scanning fluorescence microscopy images of the NLF cells treated with FLM and FM allowed us to estimate the nanomicelle ability to transport the encapsulated drugs inside the tumor cells. Flow cytometric analysis of the cells from treated tumors was performed to assess the effect of treatment on GD2 expression and NK cell infiltration.

Results: FLM and FM decreased the growth of NLF xenografts at comparable extents during the treatment period. Afterwards, FLM induced a progressive tumor regression without regrowth, while FM treatment was followed by regrowth within 15-20 days after the end of treatment. Both FLM and FM were able to penetrate the tumor cells transporting the encapsulated drugs. FLM transported higher amount of fenretinide inside the cells. Also, FLM treatment strongly increased GD2 expression in treated tumors and slightly decreased the NK infiltration compared to FM.

Conclusion: FLM treatment induced a superior antitumor response than FM in NLF xenografts, presumably due to the combined effects of fenretinide cytotoxicity and lenalidomide antiangiogenic activity. The ability of FLM to penetrate tumor cells, transporting the encapsulated drugs, substantially improved the therapeutic efficiency of this system. Moreover, the enhancement of GD2 expression in FLM treated tumors offers the possibility to further increase the antitumor effect by the use of anti-GD2 CAR-T cells and anti-GD2 antibodies in combination with FLM in multimodal therapies.

Keywords: GD2 increased expression.; antitumor activity; fenretinide–lenalidomide combination; nanomicelle penetration in tumor cells; nanomicelles; neuroblastoma.

MeSH terms

Animals
Antineoplastic Combined Chemotherapy Protocols / pharmacology*
Cell Line, Tumor
Drug Delivery Systems / methods
Female
Fenretinide / administration & dosage
Fenretinide / chemistry
Gene Expression Regulation, Neoplastic
Humans
Killer Cells, Natural / drug effects
Killer Cells, Natural / pathology
Lenalidomide / administration & dosage
Lenalidomide / chemistry
Mice, Nude
Micelles
Microscopy, Confocal
N-Myc Proto-Oncogene Protein / genetics*
Nanostructures / chemistry
Neuroblastoma / drug therapy*
Neuroblastoma / genetics
Neuroblastoma / pathology
Xenograft Model Antitumor Assays

Substances

MYCN protein, human
Micelles
N-Myc Proto-Oncogene Protein
Fenretinide
Lenalidomide