ATP-activated decrosslinking and charge-reversal vectors for siRNA delivery and cancer therapy

Zhanwei Zhou; Qingyan Zhang; Minghua Zhang; Huipeng Li; Gang Chen; Chenggen Qian; David Oupicky; Minjie Sun

doi:10.7150/thno.26889

ATP-activated decrosslinking and charge-reversal vectors for siRNA delivery and cancer therapy

Theranostics. 2018 Sep 9;8(17):4604-4619. doi: 10.7150/thno.26889. eCollection 2018.

Authors

Zhanwei Zhou¹, Qingyan Zhang¹, Minghua Zhang¹, Huipeng Li¹, Gang Chen¹, Chenggen Qian¹, David Oupicky^{1

2}, Minjie Sun¹

Affiliations

¹ State Key Laboratory of Natural Medicines, Department of Pharmaceutics, China Pharmaceutical University, 24 Tong Jia Xiang, Nanjing 210009, P. R. China.
² Center for Drug Delivery and Nanomedicine Department of Pharmaceutical Sciences University of Nebraska Medical Center Omaha, NE 68198, USA.

Abstract

Stimuli-responsive polycations have been developed for improved nucleic acid transfection and enhanced therapeutic efficacy. The most reported mechanisms for controlled release of siRNA are based on polyelectrolyte exchange reactions in the cytoplasm and the degradation of polycations initiated by specific triggers. However, the degradation strategy has not always been sufficient due to unsatisfactory kinetics and binding of cationic fragments to siRNA, which limits the gene silencing effect. In this study, a new strategy that combines degradation and charge reversal is proposed. Methods: We prepared a polycation (CrossPPA) by crosslinking of phenylboronic acid (PBA)-grafted 1.8k PEI with alginate. It was compared with 25k PEI, 1.8k PEI and 1.8k PEI-PBA on siRNA encapsulation, ATP-responsive behavior and mechanism, cytotoxicity, cell uptake, siRNA transfection, in vivo biodistribution and in vivo anti-tumor efficacy. The in vitro and in vivo experiments were performed on 4T1 murine breast cancer cells and 4T1 tumor model separately. Results: The crosslinking strategy obviously improve the siRNA loading ability of 1.8k PEI. We validated that intracellular levels of ATP could trigger CrossPPA disassembly and charge reversal, which resulted in efficient and rapid siRNA release due to electrostatic repulsion. Besides, CrossPPA/siRNA showed strong cell uptake in 4T1 cells compared with 1.8k PEI/siRNA. Notably, the cytotoxicity of CrossPPA was pretty low, which was owing to its biodegradability. Furthermore, the crosslinked polyplexes significantly enhanced siRNA transfection and improved tumor accumulation. The high gene silencing ability of CrossPPA polyplex led to strong anti-tumor efficacy when using Bcl2-targeted siRNA. Conclusion: These results indicated that the ATP-triggered disassembly and charge reversal strategy provided a new way for developing stimuli-responsive siRNA carriers and showed potential for nucleic acid delivery in the treatment of cancer.

Keywords: ATP-responsive; cancer therapy; charge reversal; phenylboronic acid; siRNA delivery.

MeSH terms

Adenosine Triphosphate / metabolism*
Animals
Antineoplastic Agents / administration & dosage*
Antineoplastic Agents / pharmacokinetics
Antineoplastic Agents / toxicity
Cell Line, Tumor
Drug Delivery Systems / methods*
Gene Silencing
Genetic Therapy / methods*
Mammary Neoplasms, Animal / therapy*
Mice
Molecular Targeted Therapy / methods
RNA, Small Interfering / administration & dosage*
RNA, Small Interfering / pharmacokinetics
RNA, Small Interfering / toxicity
Rodent Diseases / therapy*
Transfection / methods
Treatment Outcome

Substances

Antineoplastic Agents
RNA, Small Interfering
Adenosine Triphosphate