Exploring Obscurin and SPEG Kinase Biology

Author:

Fleming Jennifer R.ORCID,Rani Alankrita,Kraft Jamie,Zenker Sanja,Börgeson Emma,Lange StephanORCID

Abstract

Three members of the obscurin protein family that contain tandem kinase domains with important signaling functions for cardiac and striated muscles are the giant protein obscurin, its obscurin-associated kinase splice isoform, and the striated muscle enriched protein kinase (SPEG). While there is increasing evidence for the specific roles that each individual kinase domain plays in cross-striated muscles, their biology and regulation remains enigmatic. Our present study focuses on kinase domain 1 and the adjacent low sequence complexity inter-kinase domain linker in obscurin and SPEG. Using Phos-tag gels, we show that the linker in obscurin contains several phosphorylation sites, while the same region in SPEG remained unphosphorylated. Our homology modeling, mutational analysis and molecular docking demonstrate that kinase 1 in obscurin harbors all key amino acids important for its catalytic function and that actions of this domain result in autophosphorylation of the protein. Our bioinformatics analyses also assign a list of putative substrates for kinase domain 1 in obscurin and SPEG, based on the known and our newly proposed phosphorylation sites in muscle proteins, including obscurin itself.

Funder

National Heart, Lung, and Blood Institute

Hjärt-Lungfonden

Knut och Alice Wallenbergs Stiftelse

Wallenberg Centre for Molecular and Translational Medicine

Vetenskapsrådet

Svenska Sällskapet för Medicinsk Forskning

European Research Council

Publisher

MDPI AG

Subject

General Medicine

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