Codelivery of HBx-siRNA and Plasmid Encoding IL-12 for Inhibition of Hepatitis B Virus and Reactivation of Antiviral Immunity

Yan Mu; Xiao-He Ren; Di Han; Ying-Ying Guan; Pei-Ling Liu; Si-Xue Cheng; Hong Liu

doi:10.3390/pharmaceutics14071439

Codelivery of HBx-siRNA and Plasmid Encoding IL-12 for Inhibition of Hepatitis B Virus and Reactivation of Antiviral Immunity

Pharmaceutics. 2022 Jul 9;14(7):1439. doi: 10.3390/pharmaceutics14071439.

Authors

Yan Mu^{1

2

3}, Xiao-He Ren⁴, Di Han⁴, Ying-Ying Guan^{1

2

3}, Pei-Ling Liu^{1

2

3}, Si-Xue Cheng⁴, Hong Liu^{1

2

3}

Affiliations

¹ National & Local Joint Engineering Research Center of High-Throughput Drug Screening Technology, College of Life Sciences, Hubei University, Wuhan 430062, China.
² Key Laboratory of Biotechnology of Chinese Traditional Medicine of Hubei Province, College of Life Sciences, Hubei University, Wuhan 430062, China.
³ Hubei Collaborative Innovation Center for Green Transformation of Bio-Resources, College of Life Sciences, Hubei University, Wuhan 430062, China.
⁴ Key Laboratory of Biomedical Polymers of Ministry of Education, Department of Chemistry, Wuhan University, Wuhan 430072, China.

Abstract

Chronic hepatitis B is a critical cause of many serious liver diseases such as hepatocellular carcinoma (HCC). The main challenges in hepatitis B treatment include the rebound of hepatitis B virus (HBV)-related antigen levels after drug withdrawal and the immunosuppression caused by the virus. Herein, we demonstrate that the HBV-related antigen can be effectively inhibited and antiviral immunity can be successfully reactivated through codelivery of the small interfering RNA (siRNA) targeting HBV X protein (HBx) and the plasmid encoding interleukin 12 (pIL-12) to hepatocytes and immune cells. After being treated by the siRNA/pIL-12 codelivery system, HBx mRNA and hepatitis B surface antigen (HBsAg) are dramatically reduced in HepG2.215 cells. More importantly, the downregulated CD47 and programmed death ligand 1 (PD-L1) and the upregulated interferon-β promoter stimulator-1 (IPS-1), retinoic acid-inducible gene-1 (RIG-1), CD80, and human leukocyte antigen-1 (HLA-1) in treated HepG2.215 cells indicate that the immunosuppression is reversed by the codelivery system. Furthermore, the codelivery system results in inhibition of extracellular regulated protein kinases (ERK) and phosphoinositide-3-kinase (PI3K)/protein kinase B (Akt) pathways, as well as downregulation of B-cell lymphoma-2 (Bcl-2) and upregulation of p53, implying its potential in preventing the progression of HBV-induced HCC. In addition, J774A.1 macrophages treated by the codelivery system were successfully differentiated into the M1 phenotype and expressed enhanced cytokines with anti-hepatitis B effects such as interleukin 6 (IL-6) and tumor necrosis factor-α (TNF-α). Therefore, we believe that codelivery of siRNA and pIL-12 can effectively inhibit hepatitis B virus, reverse virus-induced immunosuppression, reactivate antiviral immunity, and hinder the progression of HBV-induced hepatocellular carcinoma. This investigation provides a promising approach for the synergistic treatment of HBV infection.

Keywords: hepatitis B treatment; immune regulation; macrophage polarity; plasmid DNA; siRNA.

Grants and funding

20210201/Opening Project of Key Laboratory of Biomedical Polymers of Ministry of Education at Wuhan University