Literature DB >> 22661706

Headless Myo10 is a negative regulator of full-length Myo10 and inhibits axon outgrowth in cortical neurons.

Alexander N Raines1, Sarbajeet Nagdas, Michael L Kerber, Richard E Cheney.   

Abstract

Myo10 is an unconventional myosin that localizes to and induces filopodia, structures that are critical for growing axons. In addition to the ~240-kDa full-length Myo10, brain expresses a ~165 kDa isoform that lacks a functional motor domain and is known as headless Myo10. We and others have hypothesized that headless Myo10 acts as an endogenous dominant negative of full-length Myo10, but this hypothesis has not been tested, and the function of headless Myo10 remains unknown. We find that cortical neurons express both headless and full-length Myo10 and report the first isoform-specific localization of Myo10 in brain, which shows enrichment of headless Myo10 in regions of proliferating and migrating cells, including the embryonic ventricular zone and the postnatal rostral migratory stream. We also find that headless and full-length Myo10 are expressed in embryonic and neuronal stem cells. To directly test the function of headless and full-length Myo10, we used RNAi specific to each isoform in mouse cortical neuron cultures. Knockdown of full-length Myo10 reduces axon outgrowth, whereas knockdown of headless Myo10 increases axon outgrowth. To test whether headless Myo10 antagonizes full-length Myo10, we coexpressed both isoforms in COS-7 cells, which revealed that headless Myo10 suppresses the filopodia-inducing activity of full-length Myo10. Together, these results demonstrate that headless Myo10 can function as a negative regulator of full-length Myo10 and that the two isoforms of Myo10 have opposing roles in axon outgrowth.

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Year:  2012        PMID: 22661706      PMCID: PMC3408153          DOI: 10.1074/jbc.M112.369173

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  57 in total

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10.  beta1 integrin maintains integrity of the embryonic neocortical stem cell niche.

Authors:  Karine Loulier; Justin D Lathia; Veronique Marthiens; Jenne Relucio; Mohamed R Mughal; Sung-Chun Tang; Turhan Coksaygan; Peter E Hall; Srinivasulu Chigurupati; Bruce Patton; Holly Colognato; Mahendra S Rao; Mark P Mattson; Tarik F Haydar; Charles Ffrench-Constant
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  15 in total

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Journal:  Cytoskeleton (Hoboken)       Date:  2016-06-22

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Authors:  Wan-Hsin Lin; Joshua T Hurley; Alexander N Raines; Richard E Cheney; Donna J Webb
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Review 5.  Peering into tunneling nanotubes-The path forward.

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6.  IL2RG, identified as overexpressed by RNA-seq profiling of pancreatic intraepithelial neoplasia, mediates pancreatic cancer growth.

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7.  Myosin-X knockout is semi-lethal and demonstrates that myosin-X functions in neural tube closure, pigmentation, hyaloid vasculature regression, and filopodia formation.

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Authors:  Mingming Lai; Ye Guo; Jun Ma; Huali Yu; Dongdong Zhao; Wenqiang Fan; Xingda Ju; Muhammad A Sheikh; Yousra S Malik; Wencheng Xiong; Weixiang Guo; Xiaojuan Zhu
Journal:  Front Cell Neurosci       Date:  2015-08-18       Impact factor: 5.505

9.  RNA-sequencing of a mouse-model of spinal muscular atrophy reveals tissue-wide changes in splicing of U12-dependent introns.

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10.  Myosin X is required for efficient melanoblast migration and melanoma initiation and metastasis.

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