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Chromosome fusions triggered by noncoding RNA

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Publisher DOI
10.1080/15476286.2016.1195940
PubMed ID
27267579
Description
Chromosomal fusions are common in normal and cancer cells and can produce aberrant gene products that promote transformation. The mechanisms driving these fusions are poorly understood, but recurrent fusions are widespread. This suggests an underlying mechanism, and some authors have proposed a possible role for RNA in this process. The unicellular eukaryote Oxytricha trifallax displays an exorbitant capacity for natural genome editing, when it rewrites its germline genome to form a somatic epigenome. This developmental process provides a powerful model system to directly test the influence of small noncoding RNAs on chromosome fusion events during somatic differentiation. Here we show that small RNAs are capable of inducing chromosome fusions in four distinct cases (out of four tested), including one fusion of three chromosomes. We further show that these RNA-mediated chromosome fusions are heritable over multiple sexual generations and that transmission of the acquired fusion is associated with endogenous production of novel piRNA molecules that target the fused junction. We also demonstrate the capacity of a long noncoding RNA (lncRNA) to induce chromosome fusion of two distal germline loci. These results underscore the ability of short-lived, aberrant RNAs to act as drivers of chromosome fusion events that can be stably transmitted to future generations.
Date of Publication
2016-06-07
Publication Type
Article
Subject(s)
500 Science > 570 Life sciences; biology
Keyword(s)
Chromosome fusion
•
Oxytricha
•
long noncoding RNA
•
piRNAs
Language(s)
en
Contributor(s)
Bracht, John R
Wang, Xing
Shetty, Keerthi
Chen, Xiao
Uttarotai, Grace J
Callihan, Evan C
McCloud, Sierra S
Clay, Derek M
Wang, Jingmei
Nowacki, Mariusz
Institut für Zellbiologie (IZB)
Landweber, Laura F
Additional Credits
Institut für Zellbiologie (IZB)
Series
RNA biology
Publisher
Landes Bioscience
ISSN
1547-6286
Access(Rights)
metadata.only
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