Comprehensive analysis of the BC200 ribonucleoprotein reveals a reciprocal regulatory function with CSDE1/UNR

Booy, Evan P.; McRae, Ewan K.S.; Ezzati, Peyman; Choi, Taegi; Gussakovsky, Daniel; McKenna, Sean Andrew

doi:10.1093/nar/gky860

Cited by 14 publications

(19 citation statements)

References 59 publications

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“…Immunoprecipitation assays showed that knocking down Unrip had a negligible impact on lncBC200 binding to CSDE1. However, knocking down CSDE1 in MCF-7 cells reduced Unrip binding on lncBC200 by more than 80% [64]. These results suggest the existence of a sequential connection of "Unrip-CSDE1-lncBC200".…”

Section: Sequential Connectionsmentioning

confidence: 81%

“…LncBC200 is a 200-nucleotide ncRNA that is normally highly expressed in the brain, but it is aberrantly expressed in various cancers [63]. In MCF-7 cells, CSDE1 could maintain the stability of lncBC200 by binding to the 3' A-rich region, while knocking down CSDE1 reduced the half-life of lncBC200 by 40% and decreased its expression [64].…”

Section: Increasing and Decreasing Rna Abundancementioning

confidence: 99%

“…In this mechanism, CSDE1 facilitates the binding of other regulators to RNA by adjusting the IRES structure [39,42]. In a few cases, CSDE1 connects indirect regulators with their target RNAs based on the sequential connection mode [64]. For all modes, CSDE1 binds RNAs directly and cooperates with other regulators in direct or indirect ways.…”

Section: Facilitating Connectionsmentioning

confidence: 99%

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The role of CSDE1 in translational reprogramming and human diseases

2020

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CSDE1 (cold shock domain containing E1) plays a key role in translational reprogramming, which determines the fate of a number of RNAs during biological processes. Interestingly, the role of CSDE1 is bidirectional. It not only promotes and represses the translation of RNAs but also increases and decreases the abundance of RNAs. However, the mechanisms underlying this phenomenon are still unknown. In this review, we propose a "protein-RNA connector" model to explain this bidirectional role and depict its three versions: sequential connection, mutual connection and facilitating connection. As described in this molecular model, CSDE1 binds to RNAs and cooperates with other protein regulators. CSDE1 connects with different RNAs and their regulators for different purposes. The triple complex of CSDE1, a regulator and an RNA reprograms translation in different directions for each transcript. Meanwhile, a number of recent studies have found important roles for CSDE1 in human diseases. This model will help us to understand the role of CSDE1 in translational reprogramming and human diseases.

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Section: Sequential Connectionsmentioning

confidence: 81%

Section: Increasing and Decreasing Rna Abundancementioning

confidence: 99%

Section: Facilitating Connectionsmentioning

confidence: 99%

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The role of CSDE1 in translational reprogramming and human diseases

2020

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“…The DIG-labelled RNA probe can then be incubated with cellular extract, and then placed to incubate onto magnetic beads. These magnetic beads are conjugated with a chemiluminescent anti-DIG antibody that is used to immunoprecipitate the potential RBPs associated with the DIG-labelled RNA (Booy et al 2018). Herranz and Pallás (2004) demonstrated, using DIG-labelled riboprobes, that the movement protein interacts with the Prunis necoritic ringsport viral ssRNA.…”

Section: Digoxigenin Labellingmentioning

confidence: 99%

Current approaches for RNA-labelling to identify RNA-binding proteins

Gemmill

D’souza

Meier-Stephenson

et al. 2020

Biochem. Cell Biol.

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RNA is involved in all domains of life, playing critical roles in a host of gene expression processes, host-defense mechanisms, cell proliferation, and diseases. A critical component in many of these events is the ability for RNA to interact with proteins. Over the past few decades, our understanding of such RNA–protein interactions and their importance has driven the search and development of new techniques for the identification of RNA-binding proteins. In determining which proteins bind to the RNA of interest, it is often useful to use the approach where the RNA molecule is the “bait” and allow it to capture proteins from a lysate or other relevant solution. Here, we review a collection of methods for modifying RNA to capture RNA-binding proteins. These include small-molecule modification, the addition of aptamers, DNA-anchoring, and nucleotide substitution. With each, we provide examples of their application, as well as highlight their advantages and potential challenges.

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“…Native RNA immunoprecipitations were performed on one 150 mm dish of HEK293T cells as previously described 45 degrees Celsius in TBST+ 5% milk, GAPDH and tubulin primary antibodies were incubated for 1 hour at room temperature in TBST+5% milk. Three sequential 5-minute washes with 5% TBS-T were followed by 1-hour incubation with secondary antibodies (1:10000) in TBST+5% milk and then 4 more 10-minute washes with TBS-T.…”

Section: Protein-rna Cop-immunoprecipitation and Rt-qpcrmentioning

confidence: 99%

An RNA guanine quadruplex regulated pathway to TRAIL-sensitization by DDX21

McRae

Dupas

Booy

et al. 2019

Preprint

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DDX21 is a newly discovered RNA G-quadruplex (rG4) binding protein with no known biological rG4 targets. In this study we identified 26 proteins that are expressed at significantly different levels in cells expressing wild type DDX21 relative to an rG4 binding deficient DDX21 (M4). From this list we validate MAGED2 as a protein that is regulated by DDX21 through rG4 in its 5'UTR. MAGED2 protein levels, but not mRNA levels, are reduced by half in cells expressing only DDX21 M4. MAGED2 has a repressive effect on TRAIL-R2 expression that is relieved under these conditions, resulting in elevated TRAIL-R2 mRNA and protein in cells expressing only DDX21 M4, and rendering previously resistant cells sensitive to TRAIL mediated apoptosis. Our work identifies the role of DDX21 in regulation at the translational level through biologically relevant rG4 and shows that MAGED2 protein levels are regulated, at least in part, by a rG4 forming potential in their 5'UTRs.

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Comprehensive analysis of the BC200 ribonucleoprotein reveals a reciprocal regulatory function with CSDE1/UNR

Cited by 14 publications

References 59 publications

The role of CSDE1 in translational reprogramming and human diseases

The role of CSDE1 in translational reprogramming and human diseases

Current approaches for RNA-labelling to identify RNA-binding proteins

An RNA guanine quadruplex regulated pathway to TRAIL-sensitization by DDX21

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