Regulation of human interferon signaling by transposon exonization. Journal Article uri icon

Overview

abstract

  • Innate immune signaling is essential for clearing pathogens and damaged cells, and must be tightly regulated to avoid excessive inflammation or autoimmunity. Here, we found that the alternative splicing of exons derived from transposable elements is a key mechanism controlling immune signaling in human cells. By analyzing long-read transcriptome datasets, we identified numerous transposon exonization events predicted to generate functional protein variants of immune genes, including the type I interferon receptor IFNAR2. We demonstrated that the transposon-derived isoform of IFNAR2 is more highly expressed than the canonical isoform in almost all tissues, and functions as a decoy receptor that potently inhibits interferon signaling including in cells infected with SARS-CoV-2. Our findings uncover a primate-specific axis controlling interferon signaling and show how a transposon exonization event can be co-opted for immune regulation.

publication date

  • September 15, 2023

has restriction

  • green

Date in CU Experts

  • October 26, 2023 8:47 AM

Full Author List

  • Pasquesi GIM; Allen H; Ivancevic A; Barbachano-Guerrero A; Joyner O; Guo K; Simpson DM; Gapin K; Horton I; Nguyen L

author count

  • 17

Other Profiles

Electronic International Standard Serial Number (EISSN)

  • 2692-8205