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Phosphoproteomics Profiling Defines a Target Landscape of the Basophilic Protein Kinases AKT, S6K, and RSK in Skeletal Myotubes. | LitMetric

AI Article Synopsis

  • - The study focuses on the role of specific protein kinases (AKT, S6K, RSK) in regulating skeletal muscle cell functions through phosphorylation-dependent signal transduction, particularly within key signaling pathways like PI3K-AKT-mTOR-S6K and RAF-MEK-ERK-RSK.
  • - Researchers conducted a detailed phosphoproteomics study to identify kinase target sites, revealing 49 previously unknown targets and showing interactions among the kinases, including feedback loops and connections to insulin and glucose metabolism.
  • - The findings highlight that these kinases influence numerous proteins essential for muscle development and function, suggesting a complex signaling network that regulates processes like RNA maturation and translation in skeletal muscle cells.

Article Abstract

Phosphorylation-dependent signal transduction plays an important role in regulating the functions and fate of skeletal muscle cells. Central players in the phospho-signaling network are the protein kinases AKT, S6K, and RSK as part of the PI3K-AKT-mTOR-S6K and RAF-MEK-ERK-RSK pathways. However, despite their functional importance, knowledge about their specific targets is incomplete because these kinases share the same basophilic substrate motif RxRxx[ST]. To address this, we performed a multifaceted quantitative phosphoproteomics study of skeletal myotubes following kinase inhibition. Our data corroborate a cross talk between AKT and RAF, a negative feedback loop of RSK on ERK, and a putative connection between RSK and PI3K signaling. Altogether, we report a kinase target landscape containing 49 so far unknown target sites. AKT, S6K, and RSK phosphorylate numerous proteins involved in muscle development, integrity, and functions, and signaling converges on factors that are central for the skeletal muscle cytoskeleton. Whereas AKT controls insulin signaling and impinges on GTPase signaling, nuclear signaling is characteristic for RSK. Our data further support a role of RSK in glucose metabolism. Shared targets have functions in RNA maturation, stability, and translation, which suggests that these basophilic kinases establish an intricate signaling network to orchestrate and regulate processes involved in translation.

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Source
http://dx.doi.org/10.1021/acs.jproteome.2c00505DOI Listing

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