Targeting Cancer Chemotherapy Resistance by Precision Medicine-Driven Nanoparticle-Formulated Cisplatin | Zendy

Svenja Siemer | Zendy; Tobias Bauer | Zendy; Paul Scholz | Zendy; Christina Breder | Zendy; Federico Fenaroli | Zendy; Gregory S. Harms | Zendy; Dimo Dietrich | Zendy; Jörn Dietrich | Zendy; Christine Rosenauer | Zendy; Matthias Barz | Zendy; Sven Becker | Zendy; Sebastian Strieth | Zendy; Christoph Reinhardt | Zendy; Torsten Fauth | Zendy; Jan Hagemann | Zendy; Roland H. Stauber | Zendy

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Targeting Cancer Chemotherapy Resistance by Precision Medicine-Driven Nanoparticle-Formulated Cisplatin

Author(s) -

Svenja Siemer,

Tobias Bauer,

Paul Scholz,

Christina Breder,

Federico Fenaroli,

Gregory S. Harms,

Dimo Dietrich,

Jörn Dietrich,

Christine Rosenauer,

Matthias Barz,

Sven Becker,

Sebastian Strieth,

Christoph Reinhardt,

Torsten Fauth,

Jan Hagemann,

Roland H. Stauber

Publication year - 2021

Publication title -

acs nano

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 5.554

H-Index - 382

eISSN - 1936-086X

pISSN - 1936-0851

DOI - 10.1021/acsnano.1c08632

Subject(s) - cisplatin , cancer research , medicine , chemistry , pharmacology , chemotherapy

Therapy resistance is the major cause of cancer death. As patients respond heterogeneously, precision/personalized medicine needs to be considered, including the application of nanoparticles (NPs). The success of therapeutic NPs requires to first identify clinically relevant resistance mechanisms and to define key players, followed by a rational design of biocompatible NPs capable to target resistance. Consequently, we employed a tiered experimental pipeline from in silico o analytical and in vitro o overcome cisplatin resistance. First, we generated cisplatin-resistant cancer cells and used next-generation sequencing together with CRISPR/Cas9 knockout technology to identify the ion channel LRRC8A as a critical component for cisplatin resistance. LRRC8A's cisplatin-specificity was verified by testing free as well as nanoformulated paclitaxel or doxorubicin. The clinical relevance of LRRC8A was demonstrated by its differential expression in a cohort of 500 head and neck cancer patients, correlating with patient survival under cisplatin therapy. To overcome LRRC8A-mediated cisplatin resistance, we constructed cisplatin-loaded, polysarcosine-based core cross-linked polymeric NPs (NP Cis , Ø ∼ 28 nm) with good colloidal stability, biocompatibility (low immunogenicity, low toxicity, prolonged in vivo circulation, no complement activation, no plasma protein aggregation), and low corona formation properties. 2D/3D-spheroid cell models were employed to demonstrate that, in contrast to standard of care cisplatin, NP Cis significantly ( p < 0.001) eradicated all cisplatin-resistant cells by circumventing the LRRC8A-transport pathway via he endocytic delivery route. We here identified LRRC8A as critical for cisplatin resistance and suggest LRRC8A-guided patient stratification for ongoing or prospective clinical studies assessing therapy resistance to nanoscale platinum drug nanoformulations versus current standard of care formulations.

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