Modular degradable dendrimers enable small RNAs to extend survival in an aggressive liver cancer model

Author:

Zhou Kejin,Nguyen Liem H.,Miller Jason B.,Yan Yunfeng,Kos Petra,Xiong Hu,Li Lin,Hao Jing,Minnig Jonathan T.,Zhu HaoORCID,Siegwart Daniel J.

Abstract

RNA-based cancer therapies are hindered by the lack of delivery vehicles that avoid cancer-induced organ dysfunction, which exacerbates carrier toxicity. We address this issue by reporting modular degradable dendrimers that achieve the required combination of high potency to tumors and low hepatotoxicity to provide a pronounced survival benefit in an aggressive genetic cancer model. More than 1,500 dendrimers were synthesized using sequential, orthogonal reactions where ester degradability was systematically integrated with chemically diversified cores, peripheries, and generations. A lead dendrimer, 5A2-SC8, provided a broad therapeutic window: identified as potent [EC50 < 0.02 mg/kg siRNA against FVII (siFVII)] in dose–response experiments, and well tolerated in separate toxicity studies in chronically ill mice bearing MYC-driven tumors (>75 mg/kg dendrimer repeated dosing). Delivery of let-7g microRNA (miRNA) mimic inhibited tumor growth and dramatically extended survival. Efficacy stemmed from a combination of a small RNA with the dendrimer’s own negligible toxicity, therefore illuminating an underappreciated complication in treating cancer with RNA-based drugs.

Funder

Cancer Prevention and Research Institute of Texas

Welch Foundation

American Cancer Society

HHS | National Institutes of Health

Mary Kay Foundation

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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