“Boundary residues” between the folded RNA recognition motif and disordered RGG domains are critical for FUS–RNA binding

Fused in sarcoma (FUS) is an abundant RNA-binding protein, which drives phase separation of cellular condensates and plays multiple roles in RNA regulation. The RNA-binding ability of FUS protein is crucial to its cellular function. Here, our molecular simulation study on the FUS–RNA complex provide...

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Veröffentlicht in:The Journal of biological chemistry 2023-12, Vol.299 (12), p.105392, Article 105392
Hauptverfasser: Balasubramanian, Sangeetha, Maharana, Shovamayee, Srivastava, Anand
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Sprache:eng
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Zusammenfassung:Fused in sarcoma (FUS) is an abundant RNA-binding protein, which drives phase separation of cellular condensates and plays multiple roles in RNA regulation. The RNA-binding ability of FUS protein is crucial to its cellular function. Here, our molecular simulation study on the FUS–RNA complex provides atomic resolution insights into the observations from biochemical studies and also illuminates our understanding of molecular driving forces that mediate the structure, stability, and interaction of the RNA recognition motif (RRM) and RGG domains of FUS with a stem–loop junction RNA. We observe clear cooperativity and division of labor among the ordered (RRM) and disordered domains (RGG1 and RGG2) of FUS that leads to an organized and tighter RNA binding. Irrespective of the length of RGG2, the RGG2–RNA interaction is confined to the stem–loop junction and the proximal stem regions. On the other hand, the RGG1 interactions are primarily with the longer RNA stem. We find that the C terminus of RRM, which make up the “boundary residues” that connect the folded RRM with the long disordered RGG2 stretch of the protein, plays a critical role in FUS–RNA binding. Our study provides high-resolution molecular insights into the FUS–RNA interactions and forms the basis for understanding the molecular origins of full-length FUS interaction with RNA.
ISSN:0021-9258
1083-351X
1083-351X
DOI:10.1016/j.jbc.2023.105392