EGFP insertional mutagenesis reveals multiple FXR2P fibrillar states with differing ribosome association in neurons
Author(s) -
Emily E. Stackpole,
Michael R. Akins,
Maria Ivshina,
Anastasia C. Murthy,
Nicolas L. Fawzi,
Justin R. Fallon
Publication year - 2019
Publication title -
biology open
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.936
H-Index - 41
ISSN - 2046-6390
DOI - 10.1242/bio.046383
Subject(s) - biology , insertional mutagenesis , mutagenesis , association (psychology) , ribosome , green fluorescent protein , translation (biology) , genetics , microbiology and biotechnology , computational biology , bioinformatics , gene , mutation , messenger rna , rna , mutant , philosophy , epistemology
RNA-binding proteins (RBPs) function in higher-order assemblages such as RNA granules to regulate RNA localization and translation. The Fragile X homolog FXR2P is an RBP essential for formation of neuronal Fragile X granules that associate with axonal mRNA and ribosomes in the intact brain. However, the FXR2P domains important for assemblage formation in a cellular system are unknown. Here we used an EGFP insertional mutagenesis approach to probe for FXR2P intrinsic features that influence its structural states. We tested 18 different in-frame FXR2P EGFP fusions in neurons and found that the majority did not impact assemblage formation. However, EGFP insertion within a 23 amino acid region of the low complexity (LC) domain induced FXR2P EGFP assembly into two distinct fibril states that were observed in isolation or in highly-ordered bundles. FXR2P EGFP fibrils exhibited different developmental timelines, ultrastructures and ribosome associations. Formation of both fibril types was dependent on an intact RNA-binding domain. These results suggest that restricted regions of the LC domain, together with the RNA-binding domain, may be important for FXR2P structural state organization in neurons.
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