Uncovering key steps in FGF12 cellular release reveals a common mechanism for unconventional FGF protein secretion

Author:

Biadun MartynaORCID,Sochacka MartynaORCID,Kalka MartaORCID,Chorazewska AleksandraORCID,Karelus RadoslawORCID,Krowarsch DanielORCID,Opalinski LukaszORCID,Zakrzewska MalgorzataORCID

Abstract

AbstractFGF12 belongs to a subfamily of FGF proteins called FGF homologous factors (FHFs), which until recently were thought to be non-signaling intracellular proteins. Our recent studies have shown that although they lack a conventional signal peptide for secretion, they can reach the extracellular space, especially under stress conditions. Here, we unraveled that the long “a” isoform of FGF12 is secreted in a pathway involving the A1 subunit of Na(+)/K(+) ATPase (ATP1A1), Tec kinase and lipids such as phosphatidylinositol and phosphatidylserine. Further, we showed that the short “b” isoform of FGF12, which binds ATP1A1 and phosphatidylserine less efficiently, is not secreted from cells. We also indicated regions in the FGF12a protein sequence that are crucial for its secretion, including N-terminal fragment and specific residues, and proposed that liquid-liquid phase separation may be important in this process. Our results strongly suggest that the mechanism of this process is very similar for all unconventionally secreted FGF proteins.

Funder

Narodowe Centrum Nauki

Publisher

Springer Science and Business Media LLC

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