Multimodal Tetrahedral DNA Nanoplatform for Surprisingly Rapid and Significant Treatment of Acute Liver Failure

Author:

Wei Hongyan123,Yi Ke1,Li Fenfang1,Li Di4,Yang Jiazhen4,Shi Run5,Jin Yuanyuan1,Wang Haixia1,Ding Jianxun4,Tao Yu12,Li Mingqiang12ORCID

Affiliation:

1. Laboratory of Biomaterials and Translational Medicine Center for Nanomedicine Sun Yat‐sen University 600 Tianhe Road Guangzhou 510630 P. R. China

2. Guangdong Provincial Key Laboratory of Liver Disease 600 Tianhe Road Guangzhou 510630 P. R. China

3. Department of Obstetrics and Gynecology Chongqing Medical University 120 Longshan Road Chongqing 401147 P. R. China

4. Key Laboratory of Polymer Ecomaterials Changchun Institute of Applied Chemistry Chinese Academy of Sciences 5625 Renmin Street Changchun 130022 P. R. China

5. Department of Oncology The First Affiliated Hospital of Nanjing Medical University 300 Guangzhou Road Nanjing 210029 P. R. China

Abstract

AbstractAcute liver failure (ALF) is a life‐threatening disease associated with the rapid development of inflammatory storms, reactive oxygen species (ROS) level elevation, and hepatocyte necrosis, which results in high short‐term mortality. Except for liver transplantation, no effective strategies are available for ALF therapy due to the rapid disease progression and narrow therapeutic time window. Therefore, there is an urgent demand to explore fast and effective modalities for ALF treatment. Herein, a multifunctional tetrahedral DNA nanoplatform (TDN) is constructed by incorporating the tumor necrosis factor‐α siRNA (siTNF‐α) through DNA hybridization and antioxidant manganese porphyrin (MnP4) via π−π stacking interaction with G‐quadruplex (G4) for surprisingly rapid and significant ALF therapy. TDN‐siTNF‐α/‐G4‐MnP4 silences TNF‐α of macrophages by siTNF‐α and polarizes them to the anti‐inflammatory M2 phenotype, providing appropriate microenvironments for hepatocyte viability. Additionally, TDN‐siTNF‐α/‐G4‐MnP4 scavenges intracellular ROS by MnP4 and TDN, protecting hepatocytes from oxidative stress‐associated cell death. Furthermore, TDN itself promotes hepatocyte proliferation via modulating the cell cycle. TDN‐siTNF‐α/‐G4‐MnP4 shows almost complete liver accumulation after intravenous injection and exhibits excellent therapeutic efficacy of ALF within 2 h. The multifunctional DNA nanoformulation provides an effective strategy for rapid ALF therapy, expanding its application for innovative treatments for liver diseases.This article is protected by copyright. All rights reserved

Publisher

Wiley

Subject

Mechanical Engineering,Mechanics of Materials,General Materials Science

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