Literature DB >> 17021172

Activity-independent regulation of dendrite patterning by postsynaptic density protein PSD-95.

Erik I Charych1, Barbara F Akum, Joshua S Goldberg, Rebecka J Jörnsten, Christopher Rongo, James Q Zheng, Bonnie L Firestein.   

Abstract

Dendritic morphology determines many aspects of neuronal function, including action potential propagation and information processing. However, the question remains as to how distinct neuronal dendrite branching patterns are established. Here, we report that postsynaptic density-95 (PSD-95), a protein involved in dendritic spine maturation and clustering of synaptic signaling proteins, plays a novel role in regulating dendrite outgrowth and branching, independent of its synaptic functions. In immature neurons, overexpression of PSD-95 decreases the proportion of primary dendrites that undergo additional branching, resulting in a marked reduction of secondary dendrite number. Conversely, knocking down PSD-95 protein in immature neurons increases secondary dendrite number. The effect of PSD-95 is activity-independent and is antagonized by cypin, a nonsynaptic protein that regulates PSD-95 localization. Binding of cypin to PSD-95 correlates with formation of stable dendrite branches. Finally, overexpression of PSD-95 in COS-7 cells disrupts microtubule organization, indicating that PSD-95 may modulate microtubules to regulate dendritic branching. Whereas many factors have been identified which regulate dendrite number, our findings provide direct evidence that proteins primarily involved in synaptic functions can also play developmental roles in shaping how a neuron patterns its dendrite branches.

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Year:  2006        PMID: 17021172      PMCID: PMC6674632          DOI: 10.1523/JNEUROSCI.2379-06.2006

Source DB:  PubMed          Journal:  J Neurosci        ISSN: 0270-6474            Impact factor:   6.167


  53 in total

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Journal:  Neuron       Date:  1999-07       Impact factor: 17.173

4.  Synaptic targeting of the postsynaptic density protein PSD-95 mediated by lipid and protein motifs.

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Journal:  Neuron       Date:  1999-03       Impact factor: 17.173

5.  Cation channel control of neurite morphology.

Authors:  J E Heng; D Zurakowski; C K Vorwerk; C L Grosskreutz; E B Dreyer
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6.  Cypin: a cytosolic regulator of PSD-95 postsynaptic targeting.

Authors:  B L Firestein; B L Firestein; J E Brenman; C Aoki; A M Sanchez-Perez; A E El-Husseini; D S Bredt
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8.  Microtubule binding by CRIPT and its potential role in the synaptic clustering of PSD-95.

Authors:  M Passafaro; C Sala; M Niethammer; M Sheng
Journal:  Nat Neurosci       Date:  1999-12       Impact factor: 24.884

9.  Specific coupling of NMDA receptor activation to nitric oxide neurotoxicity by PSD-95 protein.

Authors:  R Sattler; Z Xiong; W Y Lu; M Hafner; J F MacDonald; M Tymianski
Journal:  Science       Date:  1999-06-11       Impact factor: 47.728

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  67 in total

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2.  ALTERED CALCIUM CURRENTS AND AXONAL GROWTH IN Nf1 HAPLOINSUFFICIENT MICE.

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3.  RhoA regulates dendrite branching in hippocampal neurons by decreasing cypin protein levels.

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Review 5.  The yin-yang of dendrite morphology: unity of actin and microtubules.

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6.  Cranial irradiation compromises neuronal architecture in the hippocampus.

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7.  Deafferentation-induced alterations in mitral cell dendritic morphology in the adult zebrafish olfactory bulb.

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Journal:  J Bioenerg Biomembr       Date:  2018-09-13       Impact factor: 2.945

8.  Synaptic adhesion-like molecules (SALMs) promote neurite outgrowth.

Authors:  Philip Y Wang; Gail K Seabold; Robert J Wenthold
Journal:  Mol Cell Neurosci       Date:  2008-06-07       Impact factor: 4.314

9.  Maternal hypothyroxinemia impairs spatial learning and synaptic nature and function in the offspring.

Authors:  M C Opazo; A Gianini; F Pancetti; G Azkcona; L Alarcón; R Lizana; V Noches; P A Gonzalez; M P Marassi; M Porto; S Mora; D Rosenthal; E Eugenin; D Naranjo; S M Bueno; A M Kalergis; C A Riedel
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10.  Hippocampal spine-associated Rap-specific GTPase-activating protein induces enhancement of learning and memory in postnatally hypoxia-exposed mice.

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