Please use this identifier to cite or link to this item: http://223.31.159.10:8080/jspui/handle/123456789/744
Title: Regulation of neuromuscular junction organization by Rab2 and its effector ICA69 in Drosophila
Authors: Mallik, Bhagaban
Dwivedi, Manish Kumar
Mushtaq, Zeeshan
Kumari, Manisha
Verma, Praveen K.
Kumar, Vimlesh
Keywords: Neuromuscular junction
dICA69
BAR domain
α-Spectrin
dRab2
Glutamate receptors
Issue Date: 2017
Publisher: The Company of Biologists
Citation: Development, 144(11): 2032-2044
Abstract: Mechanisms underlying synaptic differentiation, which involves neuronal membrane and cytoskeletal remodeling, are not completely understood. We performed a targeted RNAi-mediated screen of Drosophila BAR-domain proteins and identified islet cell autoantigen 69 kDa (dICA69) as one of the key regulators of morphological differentiation of larval neuromuscular junction (NMJ). We show that Drosophila ICA69 colocalizes with α-Spectrin at the NMJ. The conserved N-BAR domain of dICA69 deforms liposomes in vitro Full length and ICAC but not the N-BAR domain of dICA69 induces filopodia in cultured cells. Consistent with its cytoskeleton regulatory role, dICA69 mutant show reduced α-Spectrin immunoreactivity at the larval NMJ. Manipulating levels of dICA69 or its interactor dPICK1 alters synaptic level of ionotropic glutamate receptors (iGluRs). Moreover, reducing dPICK1 or dRab2 levels phenocopies dICA69 mutation. Interestingly, dRab2 regulates not only synaptic iGluR but also dICA69 levels. Thus, our data suggest that: a) dICA69 regulates NMJ organization through a pathway that involves dPICK1 and dRab2, and b) dRab2 genetically functions upstream of dICA69 and regulates NMJ organization and targeting/retention of iGluRs by regulating dICA69 levels.
Description: Accepted date: April 19, 2017
URI: http://59.163.192.83:8080/jspui/handle/123456789/744
ISSN: 1477-9129
Appears in Collections:Institutional Publications

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