Idins220 will not seem to possess any sort of enzymatic activity, such effects ought to

Idins220 will not seem to possess any sort of enzymatic activity, such effects ought to necessarily be indirect, most likely by way of the assembly of multi-protein complexes where the modifying enzyme and its target protein are brought in close proximity by implies on the Kidins220 scaffold. This can be certainly a topic worth pursuing, because it may give a sturdy contribution to our understanding from the mechanisms by which Kidins220 regulates numerous aspects of synaptic plasticity. A additional layer of complexity is offered by the recent identification of many various Kidins220 isoforms, which show age- and tissue-specific distribution (Schmieg et al., 2015). Such variants determine the intracellular localization with the Kidins220 protein itself and of its molecular partners, as shown for the TrkA receptor (Schmieg et al., 2015). Nonetheless, this field of investigation is comparatively new and lots of in the already identified interactions may well turn out to become isoform-specific.Frontiers in Cellular Neuroscience | www.frontiersin.orgMarch 2016 | Volume 10 | ArticleScholz-Starke and CescaKidins220ARMS in Neuronal PhysiologyTABLE two | Kidins220 interacting partners, and post-translational modifications (PTMs) triggered by the interactions. Interacting partner Binding site on Kidins220 Binding internet site on interacting companion Not the C-terminus Reciprocal PTMs ReferenceAMPAR-GluATransmembrane domains- and 2-syntrophin B cell antige n receptor (BCR) B-Raf Caveolin-1 CrkLPDZ-binding motif n.d. n.d. n.d. Proline-rich domain (residues 1089093) n.d.EphAPDZ domain n.d. n.d. n.d. SH3 domain (constitutive binding); SH2 domain (by binding phospho- Tyr1096 ) n.d.Kidins220 negatively regulates GluA1 phosphorylation at Ser831 and Ser845 n.d. n.d. n.d. n.d. n.d.Ar alo et al. (2010)Luo et al. (2005) Fiala et al. (2015) Deswal et al. (2013) Jean-Mairet et al. (2011) Ar alo et al. (2004, 2006)ICAM-3 IKK Kinesin 1 MAP1a, MAP1b, MAPn.d. n.d. KIM motif Residues 760n.d. n.d. KLC residues 8396 MAP1a LC2, MAP1b LCNa+ channels, Voltage-gated NMDA receptor subunits NR2A, NR2B, NR1 Olfactomedin 1 (Olfm1) p75NTR PDZ-GEF1 Pdzrn3 Protein Kinase D (PKD)n.d. n.d.n.d. n.d.n.d. Residues 1512762 Indirect binding through S-SCAM PDZ-binding motif n.d.n.d. Juxtamembrane area (residues 30015) n.d. Initially PDZ domain (residues 24939) n.d.Kidins220 and -syntrophin induce EphA4 Tyr phosphorylation; EphA4 induces Kidins220 Tyr phosphorylation n.d. n.d. n.d. Kidins220 induces phosphorylation of MAP1b HC, too as an increase in its total levels n.d. NMDAR overactivation reduces Kidins220 levels n.d. n.d. n.d. n.d. PKD phosphorylates Kidins220 on Ser919 upon phorbol ester therapy n.d. n.d. Kidins220 induces Ser phosphorylation of statmins n.d. n.d. n.d. n.d. n.d. n.d.Luo et al. (2005)Jean-Mairet et al. (2011) Singh et al. (2015) Bracale et al. (2007) Higuero et al. (2010)Cesca et al. (2015) L ez-Men dez et al. (2009)Nakaya et al. (2013) Kong et al. (2001) and Chang et al. (2004) Hisata et al. (2007) Andreazzoli et al. (2012) Iglesias et al. (2000)Septin five Sortin nexin 27 (SNX27) Statmins (SCG10, SCLIP)Residues 1603715 PDZ-binding motif Carbutamide site Ankyrin repeatsN-terminal region (residues 12513) PDZ domain n.d.Park et al. (2010) Steinberg et al. (2013) Higuero et al. (2010)S-SCAM Acs pubs hsp Inhibitors Reagents T-cell receptor (TCR) Trio TrkA, TrkB, TrkC Tubulin-III, acetylated and tyrosinated -tubulin VEGFR2, VEGFR3 n.d., not determined.PDZ-binding motif n.d. Ankyrin repeats Transmembrane domain n.d. n.d.PDZ4 domain n.d. N-terminus (spectrin re.