Structural Basis of Lariat RNA Recognition by the Intron Debranching Enzyme Dbr1

Overview

Journal Nucleic Acids Res

Publisher Oxford University Press

Specialty Biochemistry

Date 2014 Aug 16

PMID 25123664

Citations 26

Authors

Eric J Montemayor

Adam Katolik

Nathaniel E Clark

Alexander B Taylor

Jonathan P Schuermann

D Joshua Combs

Richard Johnsson

Stephen P Holloway

Scott W Stevens

Masad J Damha

P John Hart

Affiliations

Soon will be listed here.

Abstract

The enzymatic processing of cellular RNA molecules requires selective recognition of unique chemical and topological features. The unusual 2',5'-phosphodiester linkages in RNA lariats produced by the spliceosome must be hydrolyzed by the intron debranching enzyme (Dbr1) before they can be metabolized or processed into essential cellular factors, such as snoRNA and miRNA. Dbr1 is also involved in the propagation of retrotransposons and retroviruses, although the precise role played by the enzyme in these processes is poorly understood. Here, we report the first structures of Dbr1 alone and in complex with several synthetic RNA compounds that mimic the branchpoint in lariat RNA. The structures, together with functional data on Dbr1 variants, reveal the molecular basis for 2',5'-phosphodiester recognition and explain why the enzyme lacks activity toward 3',5'-phosphodiester linkages. The findings illuminate structure/function relationships in a unique enzyme that is central to eukaryotic RNA metabolism and set the stage for the rational design of inhibitors that may represent novel therapeutic agents to treat retroviral infections and neurodegenerative disease.

Citing Articles

Intron lariat spliceosomes convert lariats to true circles: implications for intron transposition.

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Intron-lariat spliceosomes convert lariats to true circles: implications for intron transposition.

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