The general transcription factor TFIIB is a target for transcriptome control during cellular stress and viral infection.

Published in: bioRxiv : the preprint server for biology (2024)

Transcription by RNA polymerase II (RNAPII) synthesizes all cellular protein-coding mRNA. Many cellular stressors and viral infections dampen RNAPII activity, though the processes underlying this are not fully understood. Here we describe a two-pronged degradation strategy by which cells respond to stress by depleting the abundance of the key RNAPII general transcription factor, TFIIB. We further demonstrate that an oncogenic human gammaherpesvirus antagonizes this process, retaining enough TFIIB to support its own robust viral transcription. Thus, modulation of RNAPII machinery plays a crucial role in dictating the outcome of cellular perturbation.

Keyphrases

transcription factor
sars cov
dna binding
induced apoptosis
endothelial cells
gene expression
binding protein
cell death
genome wide identification
rna seq
signaling pathway
stress induced
cell cycle arrest
antibiotic resistance genes
endoplasmic reticulum stress
microbial community
induced pluripotent stem cells