Flexible nano-liposomes-encapsulated recombinant UL8-siRNA (r/si-UL8) based on bioengineering strategy inhibits herpes simplex virus-1 infection

Jiawei Pei, Ye Tian, Yamei Dang, Wei Ye, Xiaoqian Liu, Ningbo Zhao, Jiangfan Han, Yongheng Yang, Ziqing Zhou, Xudong Zhu, Hao Zhang, Arshad Ali, Yu Li, Fanglin Zhang, Yingfeng Lei, Airong Qian

Research output: Contribution to journalArticlepeer-review

Abstract

Herpes simplex virus-1 (HSV-1) infection can cause various diseases and the current therapeutics have limited efficacy. Small interfering RNA (siRNA) therapeutics are a promising approach against infectious diseases by targeting the viral mRNAs directly. Recently, we employed a novel tRNA scaffold to produce recombinant siRNA agents with few natural posttranscriptional modifications. In this study, we aimed to develop a specific prodrug against HSV-1 infection based on siRNA therapeutics by bioengineering technology. We screened and found that UL8 of the HSV-1 genome was an ideal antiviral target based on RNAi. Next, we used a novel bio-engineering approach to manufacture recombinant UL8-siRNA (r/si-UL8) in Escherichia coli with high purity and activity. The r/si-UL8 was selectively processed to mature si-UL8 and significantly reduced the number of infectious virions in human cells. r/si-UL8 delivered by flexible nano-liposomes significantly decreased the viral load in the skin and improved the survival rate in the preventive mouse zosteriform model. Furthermore, r/si-UL8 also effectively inhibited HSV-1 infection in a 3D human epidermal skin model. Taken together, our results highlight that the novel siRNA bioengineering technology is a unique addition to the conventional approach for siRNA therapeutics and r/si-UL8 may be a promising prodrug for curing HSV-1 infection.

Original languageEnglish
Article number105936
JournalAntiviral Research
Volume228
DOIs
StatePublished - Aug 2024

Keywords

  • Herpes simplex virus-1 (HSV-1)
  • r/si-UL8
  • Recombinant siRNA
  • SiRNA therapeutic

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