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Proximity-labeling proteomics reveals remodeled interactomes and altered localization of pathogenic SHP2 variants

Author(s)
van Vlimmeren, Anne E.; Tang, Lauren C.; Jiang, Ziyuan; Iyer, Abhishek; Voleti, Rashmi; Krismer, Konstantin; Gaublomme, Jellert T.; Jovanovic, Marko; Shah, Neel H.; ... Show more Show less
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Abstract
Missense mutations in PTPN11, which encodes the protein tyrosine phosphatase SHP2, are common in several developmental disorders and cancers. While many mutations disrupt auto-inhibition and hyperactivate SHP2, several do not enhance catalytic activity. Both activating and non-activating mutations could potentially drive pathogenic signaling by altering SHP2 interactions or localization. We employed proximity-labeling proteomics to map the interaction networks of wild-type SHP2, ten clinically relevant mutants, and SHP2 bound to an inhibitor that stabilizes its auto-inhibited state. Our analyses reveal mutation- and inhibitor-dependent alterations in the SHP2 interactome, with several mutations also changing localization. Some mutants show increased mitochondrial localization and impact mitochondrial function. This study provides a resource for exploring SHP2 signaling and offers new insights into the molecular basis of SHP2-driven diseases. Furthermore, this work highlights the capacity for proximity-labeling proteomics to detect missense-mutation-dependent changes in protein interactions and localization.
Date issued
2025-12-22
URI
https://hdl.handle.net/1721.1/164519
Department
Koch Institute for Integrative Cancer Research at MIT
Journal
EMBO Reports
Publisher
Nature Publishing Group UK
Citation
van Vlimmeren, A.E., Tang, L.C., Jiang, Z. et al. Proximity-labeling proteomics reveals remodeled interactomes and altered localization of pathogenic SHP2 variants. EMBO Rep (2025).
Version: Final published version

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