Kinase-mediated RAS signaling via membraneless cytoplasmic protein granules
Author(s) -
Asmin Tulpule,
Juan Guan,
Dana S. Neel,
Hannah R. Allegakoen,
Yone Phar Lin,
David T. Brown,
YuTing Chou,
Ann Heslin,
Nilanjana Chatterjee,
Shriya Perati,
Shruti Me,
Tan Nguyen,
Jayanta Debnath,
Alejandro Ramirez,
Xiaoyu Shi,
Bin Yang,
Siyu Feng,
Suraj Makhija,
Bo Huang,
Trever G. Bivona
Publication year - 2021
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2021.03.031
Subject(s) - biology , microbiology and biotechnology , signal transduction , grb2 , effector , anti apoptotic ras signalling cascade , gtpase , mapk/erk pathway , protein kinase a , receptor tyrosine kinase , cytoplasm , signal transducing adaptor protein , small gtpase , kinase
Receptor tyrosine kinase (RTK)-mediated activation of downstream effector pathways such as the RAS GTPase/MAP kinase (MAPK) signaling cascade is thought to occur exclusively from lipid membrane compartments in mammalian cells. Here, we uncover a membraneless, protein granule-based subcellular structure that can organize RTK/RAS/MAPK signaling in cancer. Chimeric (fusion) oncoproteins involving certain RTKs including ALK and RET undergo de novo higher-order assembly into membraneless cytoplasmic protein granules that actively signal. These pathogenic biomolecular condensates locally concentrate the RAS activating complex GRB2/SOS1 and activate RAS in a lipid membrane-independent manner. RTK protein granule formation is critical for oncogenic RAS/MAPK signaling output in these cells. We identify a set of protein granule components and establish structural rules that define the formation of membraneless protein granules by RTK oncoproteins. Our findings reveal membraneless, higher-order cytoplasmic protein assembly as a distinct subcellular platform for organizing oncogenic RTK and RAS signaling.
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