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. 2012 Dec;44(12):1289-91.
doi: 10.1038/ng.2473.

TDP-43 toxicity and the usefulness of junk

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TDP-43 toxicity and the usefulness of junk

Shuying Sun et al. Nat Genet. 2012 Dec.

Abstract

A new study shows that loss of the lariat debranching enzyme Dbr1 suppresses TDP-43 toxicity. The accumulated intronic lariat RNAs, which are normally degraded after splicing, likely act as decoys to sequester TDP-43 away from binding to and disrupting functions of other RNAs.

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Figure 1
Figure 1
Model for suppressing TDP-43 toxicity by loss of Dbr1. (a) Dbr1 normally converts intronic lariats into linear RNAs that are subsequently degraded by exonucleases. Cytoplasmic TDP-43 aggregates sequester normal RNAs/RNA-binding proteins, thereby reducing their function. (b) Without Dbr1, lariats accumulate cytoplasmically, sequestering TDP-43 and diminishing its interference with normal RNAs.

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