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FMRP promotes RNA localization to neuronal projections through interactions between its RGG domain and G-quadruplex RNA sequences
by
Hudish, Laura I.
, Russ, Holger A.
, Taliaferro, J. Matthew
, Raj, Nisha
, Goering, Raeann
, Guzman, Bryan B.
, Bassell, Gary J.
, Dominguez, Daniel
in
Molecular Biology
2019
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FMRP promotes RNA localization to neuronal projections through interactions between its RGG domain and G-quadruplex RNA sequences
by
Hudish, Laura I.
, Russ, Holger A.
, Taliaferro, J. Matthew
, Raj, Nisha
, Goering, Raeann
, Guzman, Bryan B.
, Bassell, Gary J.
, Dominguez, Daniel
in
Molecular Biology
2019
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FMRP promotes RNA localization to neuronal projections through interactions between its RGG domain and G-quadruplex RNA sequences
by
Hudish, Laura I.
, Russ, Holger A.
, Taliaferro, J. Matthew
, Raj, Nisha
, Goering, Raeann
, Guzman, Bryan B.
, Bassell, Gary J.
, Dominguez, Daniel
in
Molecular Biology
2019
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FMRP promotes RNA localization to neuronal projections through interactions between its RGG domain and G-quadruplex RNA sequences
Paper
FMRP promotes RNA localization to neuronal projections through interactions between its RGG domain and G-quadruplex RNA sequences
2019
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Overview
The sorting of RNA molecules to distinct subcellular locations facilitates the activity of spatially restricted processes through local protein synthesis. This process affects thousands of transcripts yet precisely how these RNAs are trafficked to their destinations remains generally unclear. Here we have analyzed subcellular transcriptomes of FMRP-null mouse neuronal cells to identify transcripts that depend on FMRP for efficient transport to neurites. We found that these FMRP RNA localization targets contain a large enrichment of G-quadruplex sequences, particularly in their 3′ UTRs, suggesting that FMRP recognizes these sequences to promote the localization of transcripts that contain them. Fractionation of neurons derived from human Fragile X Syndrome patients revealed a high degree of conservation in the identity of FMRP localization targets between human and mouse as well as an enrichment of G-quadruplex sequences in human FMRP RNA localization targets. Using high-throughput RNA/protein interaction assays and single-molecule RNA FISH, we identified the RGG domain of FMRP as important for both interaction with G-quadruplex RNA sequences and the neuronal transport of G-quadruplex-containing transcripts. Finally, we used ribosome footprinting to identify translational regulatory targets of FMRP. The translational regulatory targets were not enriched for G-quadruplex sequences and were largely distinct from the RNA localization targets of FMRP, indicating that the two functions can be biochemically separated and are mediated through different target recognition mechanisms. These results establish a molecular mechanism underlying FMRP-mediated neuronal RNA localization and provide a framework for the elucidation of similar mechanisms governed by other RNA-binding proteins.
Publisher
Cold Spring Harbor Laboratory
Subject
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