BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. CXCL2, glucose metabolic process, Arthritis, Stem cell, Anticancer prodrugs, Lipitor)
Bookmark Forward

Inhibition of human adenovirus replication by TRIM35-mediated degradation of E1A.

Nan Sun, Jikai Zhang, Chen Zhang, Tan Xie, Zeyu Zhang, Xueyan Wang, Wanjing Li, Yi Zhang, Zhaokai Chen, Junnian Zheng, Lin Fang, Gang Wang

Journal of virology 2023 Aug 31


filter terms:
  • adenovirus (4)
  • adenovirus e1a proteins (2)
  • apoptosis (2)
  • children (1)
  • E1A (8)
  • factors (1)
  • helps (1)
  • human (2)
  • human adenovirus (9)
  • proteins human (2)
  • TRIM35 (9)
  • trim35 protein human (1)
  • viral protein (1)
    • Sizes of these terms reflect their relevance to your search.

    Human adenovirus (HAdV) is ubiquitous in the human population, constituting a significant burden of global respiratory diseases. Children and individuals with low immunity are at risk of developing severe infections without approved antiviral treatment for HAdV. Our study demonstrated that TRIM35 inhibited HAdV-C5 early gene transcription, early protein expression, genome replication, and infectious virus progeny production. Furthermore, TRIM35 was found to inhibit HAdV replication by attenuating E1A expression. Mechanistically, TRIM35 interacts with and degrades E1A by promoting its K48-linked ubiquitination. Additionally, K253 and K285 are the key sites necessary for TRIM35 degradation. Moreover, an oncolytic adenovirus carrying shTRIM35 was constructed and observed to exhibit improved oncolysis in vivo, providing new ideas for clinical tumor treatment. Our results expand the broad antiviral activity of TRIM35 and mechanically support its application as a HAdV replication inhibitor. IMPORTANCE E1A is an essential human adenovirus (HAdV) protein responsible for the early replication of adenovirus while interacting with multiple host proteins. Understanding the interaction between HAdV E1A and TRIM35 helps identify effective antiviral therapeutic targets. The viral E1A protein is a crucial activator and regulator of viral transcription during the early infection stages. We first reported that TRIM35 interacts with E1A to resist adenovirus infection. Our study demonstrated that TRIM35 targets E1A to resist adenovirus, indicating the applicability of targeting virus-dependent host factors as a suitable antiviral strategy.

    Citation

    Nan Sun, Jikai Zhang, Chen Zhang, Tan Xie, Zeyu Zhang, Xueyan Wang, Wanjing Li, Yi Zhang, Zhaokai Chen, Junnian Zheng, Lin Fang, Gang Wang. Inhibition of human adenovirus replication by TRIM35-mediated degradation of E1A. Journal of virology. 2023 Aug 31;97(8):e0070023

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 37578239

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.