A computationally-enhanced hiCLIP atlas reveals Staufen1-RNA binding features and links 3′ UTR structure to RNA metabolism

Author:

Chakrabarti Anob M1ORCID,Iosub Ira A1ORCID,Lee Flora C Y12ORCID,Ule Jernej123ORCID,Luscombe Nicholas M14ORCID

Affiliation:

1. The Francis Crick Institute , London , NW1 4AT , UK

2. Department of Neuromuscular Diseases, UCL Queen Square Institute of Neurology , London , WC1N 3BG , UK

3. UK Dementia Research Institute at King's College London, Institute of Psychiatry , Psychology and Neuroscience, London , SE5 9RX , UK

4. Okinawa Institute of Science and Technology Graduate University , Onna-son, Okinawa 904-0495 , Japan

Abstract

Abstract The structure of mRNA molecules plays an important role in its interactions with trans-acting factors, notably RNA binding proteins (RBPs), thus contributing to the functional consequences of this interplay. However, current transcriptome-wide experimental methods to chart these interactions are limited by their poor sensitivity. Here we extend the hiCLIP atlas of duplexes bound by Staufen1 (STAU1) ∼10-fold, through careful consideration of experimental assumptions, and the development of bespoke computational methods which we apply to existing data. We present Tosca, a Nextflow computational pipeline for the processing, analysis and visualisation of proximity ligation sequencing data generally. We use our extended duplex atlas to discover insights into the RNA selectivity of STAU1, revealing the importance of structural symmetry and duplex-span-dependent nucleotide composition. Furthermore, we identify heterogeneity in the relationship between transcripts with STAU1-bound 3′ UTR duplexes and metabolism of the associated RNAs that we relate to RNA structure: transcripts with short-range proximal 3′ UTR duplexes have high degradation rates, but those with long-range duplexes have low rates. Overall, our work enables the integrative analysis of proximity ligation data delivering insights into specific features and effects of RBP-RNA structure interactions.

Funder

Wellcome Trust

Francis Crick Institute

Cancer Research UK

UK Medical Research Council

Crick Postdoctoral Clinical Fellowship and Academy of Medical Sciences Starter Grant for Clinical Lecturers

Wellcome Trust Four-Year PhD Studentship

Wellcome Trust Joint Investigator Awards

Okinawa Institute of Science & Technology Graduate University

Publisher

Oxford University Press (OUP)

Subject

Genetics

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