Literature DB >> 30502398

Current strategies for Site-Directed RNA Editing using ADARs.

Maria Fernanda Montiel-Gonzalez1, Juan Felipe Diaz Quiroz1, Joshua J C Rosenthal2.   

Abstract

Adenosine Deaminases that Act on RNA (ADARs) are a group of enzymes that catalyze the conversion of adenosines (A's) to inosines (I's) in a process known as RNA editing. Though ADARs can act on different types of RNA, editing events in coding regions of mRNA are of particular interest as I's base pair like guanosines (G's). Thus, every A-to-I change catalyzed by ADAR is read as an A-to-G change during translation, potentially altering protein sequence and function. This ability to re-code makes ADAR an attractive therapeutic tool to correct genetic mutations within mRNA. The main challenge in doing so is to re-direct ADAR's catalytic activity towards A's that are not naturally edited, a process termed Site-Directed RNA Editing (SDRE). Recently, a handful of labs have taken up this challenge and two basic strategies have emerged. The first involves redirecting endogenous ADAR to new sites by making editable structures using antisense RNA oligonucleotides. The second also utilizes antisense RNA oligonucleotides, but it uses them as guides to deliver the catalytic domain of engineered ADARs to new sites, much as CRISPR guides deliver Cas nucleases. In fact, despite the intense current focus on CRISPR-Cas9 genome editing, SDRE offers a number of distinct advantages. In the present review we will discuss these strategies in greater detail, focusing on the concepts on which they are based, how they were developed and tested, and their respective advantages and disadvantages. Though the precise and efficient re-direction of ADAR activity still remains a challenge, the systems that are being developed lay the foundation for SDRE as a powerful tool for transient genome editing.
Copyright © 2018 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  ADAR; Antisense oligo; Guide RNA; Off-target events; RNA editing

Mesh:

Substances:

Year:  2018        PMID: 30502398      PMCID: PMC6814296          DOI: 10.1016/j.ymeth.2018.11.016

Source DB:  PubMed          Journal:  Methods        ISSN: 1046-2023            Impact factor:   3.608


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