Pathogenic huntingtin inhibits fast axonal transport by activating JNK3 and phosphorylating kinesin

Gerardo A. Morfini; Yi Mei You; Sarah L. Pollema; Agnieszka Kaminska; Katherine Liu; Katsuji Yoshioka; Benny Björkblom; Eleanor T. Coffey; Carolina Bagnato; David Han; Chun Fang Huang; Gary Banker; Gustavo Pigino; Scott T. Brady

doi:10.1038/nn.2346

Pathogenic huntingtin inhibits fast axonal transport by activating JNK3 and phosphorylating kinesin

Gerardo A. Morfini, Yi Mei You, Sarah L. Pollema, Agnieszka Kaminska, Katherine Liu, Katsuji Yoshioka, Benny Björkblom, Eleanor T. Coffey, Carolina Bagnato, David Han, Chun Fang Huang, Gary Banker, Gustavo Pigino, Scott T. Brady

Neurology

Research output: Contribution to journal › Article › peer-review

219 Scopus citations

Abstract

Selected vulnerability of neurons in Huntington's disease suggests that alterations occur in a cellular process that is particularly critical for neuronal function. Supporting this idea, pathogenic Htt (polyQ-Htt) inhibits fast axonal transport (FAT) in various cellular and animal models of Huntington's disease (mouse and squid), but the molecular basis of this effect remains unknown. We found that polyQ-Htt inhibited FAT through a mechanism involving activation of axonal cJun N-terminal kinase (JNK). Accordingly, we observed increased activation of JNK in vivo in cellular and mouse models of Huntington's disease. Additional experiments indicated that the effects of polyQ-Htt on FAT were mediated by neuron-specific JNK3 and not by ubiquitously expressed JNK1, providing a molecular basis for neuron-specific pathology in Huntington's disease. Mass spectrometry identified a residue in the kinesin-1 motor domain that was phosphorylated by JNK3 and this modification reduced kinesin-1 binding to microtubules. These data identify JNK3 as a critical mediator of polyQ-Htt toxicity and provide a molecular basis for polyQ-Htt-induced inhibition of FAT.

Original language	English (US)
Pages (from-to)	864-871
Number of pages	8
Journal	Nature Neuroscience
Volume	12
Issue number	7
DOIs	https://doi.org/10.1038/nn.2346
State	Published - Jul 2009

ASJC Scopus subject areas

General Neuroscience

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@article{3a57514cb8fe459581bc7cec74549029,

title = "Pathogenic huntingtin inhibits fast axonal transport by activating JNK3 and phosphorylating kinesin",

abstract = "Selected vulnerability of neurons in Huntington's disease suggests that alterations occur in a cellular process that is particularly critical for neuronal function. Supporting this idea, pathogenic Htt (polyQ-Htt) inhibits fast axonal transport (FAT) in various cellular and animal models of Huntington's disease (mouse and squid), but the molecular basis of this effect remains unknown. We found that polyQ-Htt inhibited FAT through a mechanism involving activation of axonal cJun N-terminal kinase (JNK). Accordingly, we observed increased activation of JNK in vivo in cellular and mouse models of Huntington's disease. Additional experiments indicated that the effects of polyQ-Htt on FAT were mediated by neuron-specific JNK3 and not by ubiquitously expressed JNK1, providing a molecular basis for neuron-specific pathology in Huntington's disease. Mass spectrometry identified a residue in the kinesin-1 motor domain that was phosphorylated by JNK3 and this modification reduced kinesin-1 binding to microtubules. These data identify JNK3 as a critical mediator of polyQ-Htt toxicity and provide a molecular basis for polyQ-Htt-induced inhibition of FAT.",

author = "Morfini, {Gerardo A.} and You, {Yi Mei} and Pollema, {Sarah L.} and Agnieszka Kaminska and Katherine Liu and Katsuji Yoshioka and Benny Bj{\"o}rkblom and Coffey, {Eleanor T.} and Carolina Bagnato and David Han and Huang, {Chun Fang} and Gary Banker and Gustavo Pigino and Brady, {Scott T.}",

note = "Funding Information: We would like to thank M. MacDonald and M. DiFiglia for knock-in mice and huntingtin constructs, respectively, and B. Wang for excellent technical assistance. This work was supported by a 2007/2008 Marine Biological Laboratory summer",

year = "2009",

month = jul,

doi = "10.1038/nn.2346",

language = "English (US)",

volume = "12",

pages = "864--871",

journal = "Nature Neuroscience",

issn = "1097-6256",

publisher = "Nature Publishing Group",

number = "7",

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T1 - Pathogenic huntingtin inhibits fast axonal transport by activating JNK3 and phosphorylating kinesin

AU - Morfini, Gerardo A.

AU - You, Yi Mei

AU - Pollema, Sarah L.

AU - Kaminska, Agnieszka

AU - Liu, Katherine

AU - Yoshioka, Katsuji

AU - Björkblom, Benny

AU - Coffey, Eleanor T.

AU - Bagnato, Carolina

AU - Han, David

AU - Huang, Chun Fang

AU - Banker, Gary

AU - Pigino, Gustavo

AU - Brady, Scott T.

N1 - Funding Information: We would like to thank M. MacDonald and M. DiFiglia for knock-in mice and huntingtin constructs, respectively, and B. Wang for excellent technical assistance. This work was supported by a 2007/2008 Marine Biological Laboratory summer

PY - 2009/7

Y1 - 2009/7

N2 - Selected vulnerability of neurons in Huntington's disease suggests that alterations occur in a cellular process that is particularly critical for neuronal function. Supporting this idea, pathogenic Htt (polyQ-Htt) inhibits fast axonal transport (FAT) in various cellular and animal models of Huntington's disease (mouse and squid), but the molecular basis of this effect remains unknown. We found that polyQ-Htt inhibited FAT through a mechanism involving activation of axonal cJun N-terminal kinase (JNK). Accordingly, we observed increased activation of JNK in vivo in cellular and mouse models of Huntington's disease. Additional experiments indicated that the effects of polyQ-Htt on FAT were mediated by neuron-specific JNK3 and not by ubiquitously expressed JNK1, providing a molecular basis for neuron-specific pathology in Huntington's disease. Mass spectrometry identified a residue in the kinesin-1 motor domain that was phosphorylated by JNK3 and this modification reduced kinesin-1 binding to microtubules. These data identify JNK3 as a critical mediator of polyQ-Htt toxicity and provide a molecular basis for polyQ-Htt-induced inhibition of FAT.

AB - Selected vulnerability of neurons in Huntington's disease suggests that alterations occur in a cellular process that is particularly critical for neuronal function. Supporting this idea, pathogenic Htt (polyQ-Htt) inhibits fast axonal transport (FAT) in various cellular and animal models of Huntington's disease (mouse and squid), but the molecular basis of this effect remains unknown. We found that polyQ-Htt inhibited FAT through a mechanism involving activation of axonal cJun N-terminal kinase (JNK). Accordingly, we observed increased activation of JNK in vivo in cellular and mouse models of Huntington's disease. Additional experiments indicated that the effects of polyQ-Htt on FAT were mediated by neuron-specific JNK3 and not by ubiquitously expressed JNK1, providing a molecular basis for neuron-specific pathology in Huntington's disease. Mass spectrometry identified a residue in the kinesin-1 motor domain that was phosphorylated by JNK3 and this modification reduced kinesin-1 binding to microtubules. These data identify JNK3 as a critical mediator of polyQ-Htt toxicity and provide a molecular basis for polyQ-Htt-induced inhibition of FAT.

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Pathogenic huntingtin inhibits fast axonal transport by activating JNK3 and phosphorylating kinesin

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