Decreased A-to-I RNA Editing As a Source of Keratinocytes' DsRNA in Psoriasis

Overview

Journal RNA

Specialty Molecular Biology

Date 2018 Mar 30

PMID 29592874

Citations 23

Authors

Lea Shallev

Eli Kopel

Ariel Feiglin

Gil S Leichner

Dror Avni

Yechezkel Sidi

Eli Eisenberg

Aviv Barzilai

Erez Y Levanon

Shoshana Greenberger

Affiliations

Soon will be listed here.

Abstract

Recognition of dsRNA molecules activates the MDA5-MAVS pathway and plays a critical role in stimulating type-I interferon responses in psoriasis. However, the source of the dsRNA accumulation in psoriatic keratinocytes remains largely unknown. A-to-I RNA editing is a common co- or post-transcriptional modification that diversifies adenosine in dsRNA, and leads to unwinding of dsRNA structures. Thus, impaired RNA editing activity can result in an increased load of endogenous dsRNAs. Here we provide a transcriptome-wide analysis of RNA editing across dozens of psoriasis patients, and we demonstrate a global editing reduction in psoriatic lesions. In addition to the global alteration, we also detect editing changes in functional recoding sites located in the , , and genes. Accretion of dsRNA activates autoimmune responses, and therefore the results presented here, linking for the first time an autoimmune disease to reduction in global editing level, are relevant to a wide range of autoimmune diseases.

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