Distinct Priming Kinases Contribute to Differential Regulation of Collapsin Response Mediator Proteins by Glycogen Synthase Kinase-3 in Vivo

Cole, Adam R.; Causeret, Frédéric; Yadirgi, Gokhan; Hastie, C. James; McLauchlan, Hilary; McManus, Edward J.; Hernández, Félix; Eickholt, Britta J.; Nikolic, Margareta; Sutherland, Calum

doi:10.1074/jbc.m513344200

Cited by 203 publications

(253 citation statements)

References 37 publications

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“…1B). Interestingly, inhibitors of CDK5 (cyclin-dependent kinase-5), the presumed S522 kinase that primes other CRMP2 sites for subsequent GSK3β phosphorylation (25), did not decrease CRMP2-p-T514, suggesting that lithium decreases CRMP2-p-S522 independently of CDK5 in human neurons (SI Appendix, Fig. S9C).…”

Section: Resultsmentioning

confidence: 99%

“…However, phosphorylation of CRMP2-T514 (as well as of CRMP2-S518 and CRMP2-T509) must first be primed by phosphorylation at CRMP2-S522. Phosphorylation of CRMP2 by kinases is balanced by its dephosphorylation by phosphatases (24)(25)(26) (Fig. 1B).…”

Section: Resultsmentioning

confidence: 99%

“…It is known that phosphorylation of CRMP2 at threonine (T) 514 (CRMP2-p-T514) causes its dissociation from cytoskeletal proteins (e.g., tubulin heterodimers) (24)(25)(26). However, phosphorylation of CRMP2-T514 (as well as of CRMP2-S518 and CRMP2-T509) must first be primed by phosphorylation at CRMP2-S522.…”

Section: Resultsmentioning

confidence: 99%

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Probing the lithium-response pathway in hiPSCs implicates the phosphoregulatory set-point for a cytoskeletal modulator in bipolar pathogenesis

Tobe

Crain

Winquist

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

129

118

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The molecular pathogenesis of bipolar disorder (BPD) is poorly understood. Using human-induced pluripotent stem cells (hiPSCs) to unravel such mechanisms in polygenic diseases is generally challenging. However, hiPSCs from BPD patients responsive to lithium offered unique opportunities to discern lithium's target and hence gain molecular insight into BPD. By profiling the proteomics of BDP-hiPSCderived neurons, we found that lithium alters the phosphorylation state of collapsin response mediator protein-2 (CRMP2). Active nonphosphorylated CRMP2, which binds cytoskeleton, is present throughout the neuron; inactive phosphorylated CRMP2, which dissociates from cytoskeleton, exits dendritic spines. CRMP2 elimination yields aberrant dendritogenesis with diminished spine density and lost lithium responsiveness (LiR). The "set-point" for the ratio of pCRMP2:CRMP2 is elevated uniquely in hiPSC-derived neurons from LiR BPD patients, but not with other psychiatric (including lithium-nonresponsive BPD) and neurological disorders. Lithium (and other pathway modulators) lowers pCRMP2, increasing spine area and density. Human BPD brains show similarly elevated ratios and diminished spine densities; lithium therapy normalizes the ratios and spines. Consistent with such "spine-opathies," human LiR BPD neurons with abnormal ratios evince abnormally steep slopes for calcium flux; lithium normalizes both. Behaviorally, transgenic mice that reproduce lithium's postulated site-of-action in dephosphorylating CRMP2 emulate LiR in BPD. These data suggest that the "lithium response pathway" in BPD governs CRMP2's phosphorylation, which regulates cytoskeletal organization, particularly in spines, modulating neural networks. Aberrations in the posttranslational regulation of this developmentally critical molecule may underlie LiR BPD pathogenesis. Instructively, examining the proteomic profile in hiPSCs of a functional agent-even one whose mechanism-of-action is unknownmight reveal otherwise inscrutable intracellular pathogenic pathways. have proven valuable for studying the molecular pathology of monogenic diseases, one of the technique's greatest challenges has been to offer similar insights into the molecular pathogenesis of polygenic, multifactorial disorders for which the underlying pathophysiology is unknown. The struggle has been to go beyond phenotypic description to discerning underlying molecular mechanisms. Neuropsychiatric illnesses are a prototype for such complex conditions (1-3). They are difficult to model not only because of the likelihood of polygenic influences, but also because of the subjectivity with which these diseases must often be diagnosed, the empirical fashion with which drugs are prescribed, and the heterogeneity of patient response. Of such maladies, bipolar disorder

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

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Probing the lithium-response pathway in hiPSCs implicates the phosphoregulatory set-point for a cytoskeletal modulator in bipolar pathogenesis

Tobe

Crain

Winquist

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

129

118

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“…Based upon the established important role of phosphorylation in modulating CRMP-2's activity and interaction with partners proteins, we hypothesized that phosphorylation may also affect its modulation of CaV2.2. Here, we focused solely on evaluating the effect of Cdk5-phosphoryalted CRMP-2 on CaV2.2 because (i) Cdk5 is an obligatory priming kinase [28], (ii) Cdk5-phosphorylated CRMP-2 (at Ser-522) has reduced interaction with partner proteins tubulin and numb [24], (iii) Cdk5-phosphorylated CRMP-2 leads to altered neuronal functionality manifested as a halt in neurite growth [29], and (iv) the Cdk5-phosphorylation site is near the CBD3 binding site on CRMP-2 that is important for its interaction with CaV2.2. Our results show that mutation of the Cdk5-phosphorylation site, but not the RhoK phosphorylation site, regulates CRMP-2-mediated enhancement of Ca 2+ influx.…”

Section: Introductionmentioning

confidence: 99%

Cdk5‐mediated phosphorylation of CRMP‐2 enhances its interaction with CaV2.2

et al. 2012

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Edited by Maurice Montal Keywords:CaV2.2 CRMP-2 Interaction Cdk5 RhoK Phosphorylation a b s t r a c tThe axon/dendrite specification collapsin response mediator protein-2 (CRMP-2) bidirectionally regulates N-type voltage-gated Ca 2+ channels (CaV2.2). But how cyclin dependent kinase 5 (Cdk5)-mediated phosphorylation of CRMP-2 affects its interaction/regulation with CaV2.2 is unknown. CRMP-2-mediated enhancement of currents via CaV2.2 was not observed with a Cdk5 phospho-null CRMP-2-S522A mutant or in cells expressing an inactive Cdk5. Concomitant knockdown of endogenous CRMP2 and overexpression of CRMP2-S522A mutant refractory to knockdown phenocopied the reduction in Ca 2+ influx while the Rho kinase CRMP2-T555A mutant was ineffective. Cdk5-phosphorylated CRMP-2 had increased association with CaV2.2. These results identify an important role for Cdk5 in CRMP2-mediated CaV2.2 regulation. Structured summary of protein interactions:Gsk3b phosphorylates Crmp2by phosphatase assay (View interaction) Crmp2 physically interacts with Cav2.2 by anti tag coimmunoprecipitation (View interaction)

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“…CRMP2 regulates multiple processes in neurons and was initially discovered to regulate mechanisms of neuronal polarity (9,10). CRMP2 phosphorylation by cyclin-dependent kinase 5 (Cdk5) (11), glycogen synthase kinase 3β (10), Rho-associated protein kinase (12), or the Src-family kinases Fyn (13) and Yes (14) drives its diverse cellular functions, including neurite outgrowth, endocytosis, and ion-channel trafficking (8,(15)(16)(17). Studies of CRMP2 trafficking functions have revealed that CRMP2 facilitates endocytosis of L1-cell adhesion molecule by interacting with the endocytic protein Numb (18) that recruits epidermal growth factor receptor pathway substrate 15 (Eps15), an initiator of clathrin-mediated endocytosis (19).…”

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confidence: 99%

Hierarchical CRMP2 posttranslational modifications control NaV1.7 function

Dustrude

Moutal

Yang

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

103

252

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Voltage-gated sodium channels are crucial determinants of neuronal excitability and signaling. Trafficking of the voltage-gated sodium channel NaV1.7 is dysregulated in neuropathic pain. We identify a trafficking program for NaV1.7 driven by hierarchical interactions with posttranslationally modified versions of the binding partner collapsin response mediator protein 2 (CRMP2). The binding described between CRMP2 and NaV1.7 was enhanced by conjugation of CRMP2 with small ubiquitin-like modifier (SUMO) and further controlled by the phosphorylation status of CRMP2. We determined that CRMP2 SUMOylation is enhanced by prior phosphorylation by cyclin-dependent kinase 5 and antagonized by Fyn phosphorylation. As a consequence of CRMP2 loss of SUMOylation and binding to NaV1.7, the channel displays decreased membrane localization and current density, and reduces neuronal excitability. Preventing CRMP2 SUMOylation with a SUMO-impaired CRMP2-K374A mutant triggered NaV1.7 internalization in a clathrindependent manner involving the E3 ubiquitin ligase Nedd4-2 (neural precursor cell expressed developmentally down-regulated protein 4) and endocytosis adaptor proteins Numb and epidermal growth factor receptor pathway substrate 15. Collectively, our work shows that diverse modifications of CRMP2 cross-talk to control NaV1.7 activity and illustrate a general principle for regulation of NaV1.7.NaV1.7 sodium channel | trafficking | CRMP2 | SUMOylation | phosphorylation

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Distinct Priming Kinases Contribute to Differential Regulation of Collapsin Response Mediator Proteins by Glycogen Synthase Kinase-3 in Vivo

Cited by 203 publications

References 37 publications

Probing the lithium-response pathway in hiPSCs implicates the phosphoregulatory set-point for a cytoskeletal modulator in bipolar pathogenesis

Probing the lithium-response pathway in hiPSCs implicates the phosphoregulatory set-point for a cytoskeletal modulator in bipolar pathogenesis

Cdk5‐mediated phosphorylation of CRMP‐2 enhances its interaction with CaV2.2

Hierarchical CRMP2 posttranslational modifications control NaV1.7 function

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