Targeted siRNA nanocarrier: a platform technology for cancer treatment

Author:

Bäumer Nicole,Tiemann Jessica,Scheller Annika,Meyer TheresaORCID,Wittmann Lisa,Suburu Matias Ezequiel GutierrezORCID,Greune Lilo,Peipp Matthias,Kellmann Neele,Gumnior Annika,Brand Caroline,Hartmann Wolfgang,Rossig Claudia,Müller-Tidow CarstenORCID,Neri Dario,Strassert Cristian A.,Rüter Christian,Dersch Petra,Lenz GeorgORCID,Koeffler H. Phillip,Berdel Wolfgang E.,Bäumer SebastianORCID

Abstract

AbstractThe small arginine-rich protein protamine condenses complete genomic DNA into the sperm head. Here, we applied its high RNA binding capacity for spontaneous electrostatic assembly of therapeutic nanoparticles decorated with tumour-cell-specific antibodies for efficiently targeting siRNA. Fluorescence microscopy and DLS measurements of these nanocarriers revealed the formation of a vesicular architecture that requires presence of antibody-protamine, defined excess of free SMCC-protamine, and anionic siRNA to form. Only these complex nanoparticles were efficient in the treatment of non-small-cell lung cancer (NSCLC) xenograft models, when the oncogene KRAS was targeted via EGFR-mediated delivery. To show general applicability, we used the modular platform for IGF1R-positive Ewing sarcomas. Anti-IGR1R-antibodies were integrated into an antibody-protamine nanoparticle with an siRNA specifically against the oncogenic translocation product EWS/FLI1. Using these nanoparticles, EWS/FLI1 knockdown blocked in vitro and in vivo growth of Ewing sarcoma cells. We conclude that these antibody-protamine-siRNA nanocarriers provide a novel platform technology to specifically target different cell types and yet undruggable targets in cancer therapy by RNAi.

Funder

Deutsche Forschungsgemeinschaft

Wilhelm Sander-Stiftung

Publisher

Springer Science and Business Media LLC

Subject

Cancer Research,Genetics,Molecular Biology

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