Nna1 mediates purkinje cell dendritic development via lysyl oxidase propeptide and NF-κB signaling

Jianxue Li; Xuesong Gu; Yinghua Ma; Monica L. Calicchio; Dong Kong; Yang D. Teng; Lili Yu; Andrew M. Crain; Timothy K. Vartanian; Renata Pasqualini; Wadih Arap; Towia A. Libermann; Evan Y. Snyder; Richard L. Sidman

doi:10.1016/j.neuron.2010.08.013

Nna1 mediates purkinje cell dendritic development via lysyl oxidase propeptide and NF-κB signaling

Jianxue Li, Xuesong Gu, Yinghua Ma, Monica L. Calicchio, Dong Kong, Yang D. Teng, Lili Yu, Andrew M. Crain, Timothy K. Vartanian, Renata Pasqualini, Wadih Arap, Towia A. Libermann, Evan Y. Snyder, Richard L. Sidman

Genitourinary Medical Oncology

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

61 Scopus citations

Abstract

The molecular pathways controlling cerebellar Purkinje cell dendrite formation and maturation are poorly understood. The Purkinje cell degeneration (pcd) mutant mouse is characterized by mutations in Nna1, a gene discovered in an axonal regenerative context, but whose actual function in development and disease is unknown. We found abnormal development of Purkinje cell dendrites in postnatal pcd^Sid mice and linked this deficit to a deletion mutation in exon 7 of Nna1. With single cell gene profiling and virus-based gene transfer, we analyzed a molecular pathway downstream to Nna1 underlying abnormal Purkinje cell dendritogenesis in pcd^Sid mice. We discovered that mutant Nna1 dramatically increases intranuclear localization of lysyl oxidase propeptide, which interferes with NF-κB RelA signaling and microtubule-associated protein regulation of microtubule stability, leading to underdevelopment of Purkinje cell dendrites. These findings provide insight into Nna1's role in neuronal development and why its absence renders Purkinje cells more vulnerable.

Original language	English (US)
Pages (from-to)	45-60
Number of pages	16
Journal	Neuron
Volume	68
Issue number	1
DOIs	https://doi.org/10.1016/j.neuron.2010.08.013
State	Published - Oct 6 2010

ASJC Scopus subject areas

General Neuroscience

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10.1016/j.neuron.2010.08.013

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@article{81715a746f7446c892ff23b89d5d3cb6,

title = "Nna1 mediates purkinje cell dendritic development via lysyl oxidase propeptide and NF-κB signaling",

abstract = "The molecular pathways controlling cerebellar Purkinje cell dendrite formation and maturation are poorly understood. The Purkinje cell degeneration (pcd) mutant mouse is characterized by mutations in Nna1, a gene discovered in an axonal regenerative context, but whose actual function in development and disease is unknown. We found abnormal development of Purkinje cell dendrites in postnatal pcdSid mice and linked this deficit to a deletion mutation in exon 7 of Nna1. With single cell gene profiling and virus-based gene transfer, we analyzed a molecular pathway downstream to Nna1 underlying abnormal Purkinje cell dendritogenesis in pcdSid mice. We discovered that mutant Nna1 dramatically increases intranuclear localization of lysyl oxidase propeptide, which interferes with NF-κB RelA signaling and microtubule-associated protein regulation of microtubule stability, leading to underdevelopment of Purkinje cell dendrites. These findings provide insight into Nna1's role in neuronal development and why its absence renders Purkinje cells more vulnerable.",

author = "Jianxue Li and Xuesong Gu and Yinghua Ma and Calicchio, {Monica L.} and Dong Kong and Teng, {Yang D.} and Lili Yu and Crain, {Andrew M.} and Vartanian, {Timothy K.} and Renata Pasqualini and Wadih Arap and Libermann, {Towia A.} and Snyder, {Evan Y.} and Sidman, {Richard L.}",

note = "Funding Information: We thank Kangni Zheng for assistance with cDNA sequencing, Marie G. Joseph with Affymetrix microarray, Veronica J. Peschansky with Neurolucida software, Scott B. Berger with lentiviral particle concentration, and Quanli Yang with statistic analysis. We also thank Professor Philip Leder and Janet Borden of the Harvard Medical School Department of Genetics for sharing the ataxic mice. This work was supported in part by NIH R33 CA103056 and the Nancy Lurie Marks Family Foundation (R.L.S.), and the William Randolph Hearst Fund (J.L.). ",

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doi = "10.1016/j.neuron.2010.08.013",

language = "English (US)",

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T1 - Nna1 mediates purkinje cell dendritic development via lysyl oxidase propeptide and NF-κB signaling

AU - Li, Jianxue

AU - Gu, Xuesong

AU - Ma, Yinghua

AU - Calicchio, Monica L.

AU - Kong, Dong

AU - Teng, Yang D.

AU - Yu, Lili

AU - Crain, Andrew M.

AU - Vartanian, Timothy K.

AU - Pasqualini, Renata

AU - Arap, Wadih

AU - Libermann, Towia A.

AU - Snyder, Evan Y.

AU - Sidman, Richard L.

N1 - Funding Information: We thank Kangni Zheng for assistance with cDNA sequencing, Marie G. Joseph with Affymetrix microarray, Veronica J. Peschansky with Neurolucida software, Scott B. Berger with lentiviral particle concentration, and Quanli Yang with statistic analysis. We also thank Professor Philip Leder and Janet Borden of the Harvard Medical School Department of Genetics for sharing the ataxic mice. This work was supported in part by NIH R33 CA103056 and the Nancy Lurie Marks Family Foundation (R.L.S.), and the William Randolph Hearst Fund (J.L.).

PY - 2010/10/6

Y1 - 2010/10/6

N2 - The molecular pathways controlling cerebellar Purkinje cell dendrite formation and maturation are poorly understood. The Purkinje cell degeneration (pcd) mutant mouse is characterized by mutations in Nna1, a gene discovered in an axonal regenerative context, but whose actual function in development and disease is unknown. We found abnormal development of Purkinje cell dendrites in postnatal pcdSid mice and linked this deficit to a deletion mutation in exon 7 of Nna1. With single cell gene profiling and virus-based gene transfer, we analyzed a molecular pathway downstream to Nna1 underlying abnormal Purkinje cell dendritogenesis in pcdSid mice. We discovered that mutant Nna1 dramatically increases intranuclear localization of lysyl oxidase propeptide, which interferes with NF-κB RelA signaling and microtubule-associated protein regulation of microtubule stability, leading to underdevelopment of Purkinje cell dendrites. These findings provide insight into Nna1's role in neuronal development and why its absence renders Purkinje cells more vulnerable.

AB - The molecular pathways controlling cerebellar Purkinje cell dendrite formation and maturation are poorly understood. The Purkinje cell degeneration (pcd) mutant mouse is characterized by mutations in Nna1, a gene discovered in an axonal regenerative context, but whose actual function in development and disease is unknown. We found abnormal development of Purkinje cell dendrites in postnatal pcdSid mice and linked this deficit to a deletion mutation in exon 7 of Nna1. With single cell gene profiling and virus-based gene transfer, we analyzed a molecular pathway downstream to Nna1 underlying abnormal Purkinje cell dendritogenesis in pcdSid mice. We discovered that mutant Nna1 dramatically increases intranuclear localization of lysyl oxidase propeptide, which interferes with NF-κB RelA signaling and microtubule-associated protein regulation of microtubule stability, leading to underdevelopment of Purkinje cell dendrites. These findings provide insight into Nna1's role in neuronal development and why its absence renders Purkinje cells more vulnerable.

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Nna1 mediates purkinje cell dendritic development via lysyl oxidase propeptide and NF-κB signaling

Abstract

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