Literature DB >> 29685979

The past and presence of gene targeting: from chemicals and DNA via proteins to RNA.

T M Geel1, M H J Ruiters1, R H Cool2, L Halby3, D C Voshart1, L Andrade Ruiz1, K E Niezen-Koning4, P B Arimondo5, M G Rots6.   

Abstract

The ability to target DNA specifically at any given position within the genome allows many intriguing possibilities and has inspired scientists for decades. Early gene-targeting efforts exploited chemicals or DNA oligonucleotides to interfere with the DNA at a given location in order to inactivate a gene or to correct mutations. We here describe an example towards correcting a genetic mutation underlying Pompe's disease using a nucleotide-fused nuclease (TFO-MunI). In addition to the promise of gene correction, scientists soon realized that genes could be inactivated or even re-activated without inducing potentially harmful DNA damage by targeting transcriptional modulators to a particular gene. However, it proved difficult to fuse protein effector domains to the first generation of programmable DNA-binding agents. The engineering of gene-targeting proteins (zinc finger proteins (ZFPs), transcription activator-like effectors (TALEs)) circumvented this problem. The disadvantage of protein-based gene targeting is that a fusion protein needs to be engineered for every locus. The recent introduction of CRISPR/Cas offers a flexible approach to target a (fusion) protein to the locus of interest using cheap designer RNA molecules. Many research groups now exploit this platform and the first human clinical trials have been initiated: CRISPR/Cas has kicked off a new era of gene targeting and is revolutionizing biomedical sciences.This article is part of a discussion meeting issue 'Frontiers in epigenetic chemical biology'.
© 2018 The Author(s).

Entities:  

Keywords:  CRISPR/dCas; TALEs (transcription activator-like effectors); ZFPs (zinc finger proteins); genome editing; polyamides

Mesh:

Substances:

Year:  2018        PMID: 29685979      PMCID: PMC5915719          DOI: 10.1098/rstb.2017.0077

Source DB:  PubMed          Journal:  Philos Trans R Soc Lond B Biol Sci        ISSN: 0962-8436            Impact factor:   6.237


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