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Dinucleotide Degradation by REXO2 Maintains Promoter Specificity in Mammalian Mitochondria.

Mol Cell. 2019; 
Nicholls Thomas J,Spåhr Henrik,Jiang Shan,Siira Stefan J,Koolmeister Camilla,Sharma Sushma,Kauppila Johanna H K,Jiang Min,Kaever Volkhard,Rackham Oliver,Chabes Andrei,Falkenberg Maria,Filipovska Aleksandra,Larsson Nils-Göran,Gustafsson Cla
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Mammalian Expression System Codon-optimized (Genscript) DNA constructs corresponding to amino acids 39-216 of human REXO2 was cloned in a pETM-11 vector (EMBL).  Get A Quote

摘要

Oligoribonucleases are conserved enzymes that degrade short RNA molecules of up to 5 nt in length and are assumed to constitute the final stage of RNA turnover. Here we demonstrate that REXO2 is a specialized dinucleotide-degrading enzyme that shows no preference between RNA and DNA dinucleotide substrates. A heart- and skeletal-muscle-specific knockout mouse displays elevated dinucleotide levels and alterations in gene expression patterns indicative of aberrant dinucleotide-primed transcription initiation. We find that dinucleotides act as potent stimulators of mitochondrial transcription initiation in vitro. Our data demonstrate that increased levels of dinucleotides can be used to initiate transcription, ... More

关键词

POLRMT,REXO2,RNA turnover,degradosome,mitochondria,mtDNA,oligoribonuclease,transcrip