Reference Report

Reference
Citation	Ramachandran, P., Barria, R., Ashley, J., Budnik, V. (2009). A critical step for postsynaptic F-actin organization: Regulation of Baz/Par-3 localization by aPKC and PTEN. Dev. Neurobiol. 69(9): 583--602. (Export to RIS)
FlyBase ID	FBrf0208224
Publication Type	Research paper
PubMed ID	19472188
PubMed Abstract	Actin remodeling has emerged as a critical process during synapse development and plasticity. Thus, understanding the regulatory mechanisms controlling actin organization at synapses is exceedingly important. Here, we used the highly plastic Drosophila neuromuscular junction (NMJ) to understand mechanisms of actin remodeling at postsynaptic sites. Previous studies have suggested that the actin-binding proteins Spectrin and Coracle play a critical role in NMJ development and the anchoring of glutamate receptors most likely through actin regulation. Here, we show that an additional determinant of actin organization at the postsynaptic region is the PDZ protein Baz/Par-3. Decreasing Baz levels in postsynaptic muscles has dramatic consequences for the size of F-actin and spectrin domains at the postsynaptic region. In turn, proper localization of Baz at this site depends on both phosphorylation and dephosphorylation events. Baz phosphorylation by its binding partner, atypical protein kinase C (aPKC), is required for normal Baz targeting to the postsynaptic region. However, the retention of Baz at this site depends on its dephosphorylation mediated by the lipid and protein phosphatase PTEN. Misregulation of the phosphorylation state of Baz by genetic alterations in PTEN or aPKC activity has detrimental consequences for postsynaptic F-actin and spectrin localization, synaptic growth, and receptor localization. Our results provide a novel mechanism of postsynaptic actin regulation through Baz, governed by the antagonistic actions of aPKC and PTEN. Given the conservation of these proteins from worms to mammals, these results are likely to provide new insight into actin organization pathways. (c) 2009 Wiley Periodicals, Inc. Develop Neurobiol 2009.
DOI	10.1002/dneu.20728
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Language of Publication	English
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Publication Type	Journal
Abbreviation	Dev. Neurobiol.
Title	Developmental Neurobiology
Publication Year	2007--
ISBN/ISSN	1932-8451 1932-846X
Data from Reference
Alleles (13)
	aPKC^{dsRNA.cRa.Scer\UAS} aPKC^M.Scer\UAS baz^815-8 baz^{dsRNA.cRa.Scer\UAS} baz^GD1384 baz^{Scer\UAS.P\T.T:Avic\GFP} Pten^dj189 Pten^{dsRNA.Exel.Scer\UAS} Scer\GAL4^BG487 Scer\GAL4^C57 w^+mC β-Spec^{dsRNA.Scer\UAS} β-Spec^em6
Constructs (7)
	P{GD1384} P{UAS-aPKC.RNAi.R} P{UAS-baz.RNAi.R} P{UASp-baz.GFP} P{UAS-PKM} P{UAS-Pten.dsRNA.Exel} P{UAS-β-Spec.dsRNA}
Genes (12)
	aPKC baz dlg1 GluRIIA GluRIIB GluRIIC Pten Scer\GAL4 scrib w α-Spec β-Spec
Insertions (2)
	P{GAL4}BG487 P{GawB}C57
Natural transposons (1)
	P-element