Publication | Open Access
The Function of Embryonic Stem Cell-expressed RAS (E-RAS), a Unique RAS Family Member, Correlates with Its Additional Motifs and Its Structural Properties
15
Citations
62
References
2015
Year
Adult Stem CellSignaling PathwayRas FamilyReceptor Tyrosine KinaseRemarkable Sequence DeviationsStem CellsCell SignalingStructural PropertiesMorphogenesisClassical Ras IsoformsGene ExpressionCell BiologyCell LineageDevelopmental BiologySignal TransductionAdditional MotifsTumor SuppressorSystems BiologyMedicineEmbryonic Stem Cell
E-RAS is a member of the RAS family specifically expressed in embryonic stem cells, gastric tumors, and hepatic stellate cells. Unlike classical RAS isoforms (H-, N-, and K-RAS4B), E-RAS has, in addition to striking and remarkable sequence deviations, an extended 38-amino acid-long unique N-terminal region with still unknown functions. We investigated the molecular mechanism of E-RAS regulation and function with respect to its sequence and structural features. We found that N-terminal extension of E-RAS is important for E-RAS signaling activity. E-RAS protein most remarkably revealed a different mode of effector interaction as compared with H-RAS, which correlates with deviations in the effector-binding site of E-RAS. Of all these residues, tryptophan 79 (arginine 41 in H-RAS), in the interswitch region, modulates the effector selectivity of RAS proteins from H-RAS to E-RAS features.
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