Cysteine proteinase-1 and cut protein isoform control dendritic innervation of two distinct sensory fields by a single neuron

Gray R. Lyons; Ryan O. Andersen; Khadar Abdi; Won Seok Song; Chay T. Kuo

doi:10.1016/j.celrep.2014.02.003

Cysteine proteinase-1 and cut protein isoform control dendritic innervation of two distinct sensory fields by a single neuron

Gray R. Lyons, Ryan O. Andersen, Khadar Abdi, Won Seok Song, Chay T. Kuo

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

6 Scopus citations

Abstract

Dendrites often exhibit structural changes in response to local inputs. Although mechanisms that pattern and maintain dendritic arbors are becoming clearer, processes regulating regrowth, during context-dependent plasticity or after injury, remain poorly understood. We found that a class of Drosophila sensory neurons, through complete pruning and regeneration, can elaborate two distinct dendritic trees, innervating independent sensory fields. An expression screen identified Cysteine proteinase-1 (Cp1) as a critical regulator of this process. Unlike known ecdysone effectors, Cp1-mutant ddaC neurons pruned larval dendrites normally but failed to regrow adult dendrites. Cp1 expression was upregulated/concentrated in the nucleus during metamorphosis, controlling production of a truncated Cut homeodomain transcription factor. This truncated Cut, but not the full-length protein, allowed Cp1-mutant ddaC neurons to regenerate higher-order adult dendrites. These results identify a molecular pathway needed for dendrite regrowth after pruning, which allows the same neuron to innervate distinct sensory fields.

Original language	English (US)
Pages (from-to)	783-791
Number of pages	9
Journal	Cell Reports
Volume	6
Issue number	5
DOIs	https://doi.org/10.1016/j.celrep.2014.02.003
State	Published - 2014
Externally published	Yes

ASJC Scopus subject areas

Biochemistry, Genetics and Molecular Biology(all)

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10.1016/j.celrep.2014.02.003

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@article{ae7f40a85f7b47b0befea6e4828bca65,

title = "Cysteine proteinase-1 and cut protein isoform control dendritic innervation of two distinct sensory fields by a single neuron",

abstract = "Dendrites often exhibit structural changes in response to local inputs. Although mechanisms that pattern and maintain dendritic arbors are becoming clearer, processes regulating regrowth, during context-dependent plasticity or after injury, remain poorly understood. We found that a class of Drosophila sensory neurons, through complete pruning and regeneration, can elaborate two distinct dendritic trees, innervating independent sensory fields. An expression screen identified Cysteine proteinase-1 (Cp1) as a critical regulator of this process. Unlike known ecdysone effectors, Cp1-mutant ddaC neurons pruned larval dendrites normally but failed to regrow adult dendrites. Cp1 expression was upregulated/concentrated in the nucleus during metamorphosis, controlling production of a truncated Cut homeodomain transcription factor. This truncated Cut, but not the full-length protein, allowed Cp1-mutant ddaC neurons to regenerate higher-order adult dendrites. These results identify a molecular pathway needed for dendrite regrowth after pruning, which allows the same neuron to innervate distinct sensory fields.",

author = "Lyons, {Gray R.} and Andersen, {Ryan O.} and Khadar Abdi and Song, {Won Seok} and Kuo, {Chay T.}",

note = "Funding Information: We thank A. Spradling (Carnegie), L. Cooley (Yale), E. Gavis (Princeton), W. Grueber (Columbia), and D. Kiehart for generously providing fly stocks; Developmental Studies Hybridoma Bank for Cut antibody; E. Spana for transgene injections; C. Nicchitta, S. Soderling, and D. Tracey for discussions; and R. Yang, P. Volkan, A. West, and B. Hogan for comments on the manuscript. R.O.A. was a Ruth K. Broad Postdoctoral Fellow. This work was supported by the Alfred P. Sloan Foundation and George & Jean Brumley, Jr. Endowment (to C.T.K.). ",

year = "2014",

doi = "10.1016/j.celrep.2014.02.003",

language = "English (US)",

volume = "6",

pages = "783--791",

journal = "Cell Reports",

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T1 - Cysteine proteinase-1 and cut protein isoform control dendritic innervation of two distinct sensory fields by a single neuron

AU - Lyons, Gray R.

AU - Andersen, Ryan O.

AU - Abdi, Khadar

AU - Song, Won Seok

AU - Kuo, Chay T.

N1 - Funding Information: We thank A. Spradling (Carnegie), L. Cooley (Yale), E. Gavis (Princeton), W. Grueber (Columbia), and D. Kiehart for generously providing fly stocks; Developmental Studies Hybridoma Bank for Cut antibody; E. Spana for transgene injections; C. Nicchitta, S. Soderling, and D. Tracey for discussions; and R. Yang, P. Volkan, A. West, and B. Hogan for comments on the manuscript. R.O.A. was a Ruth K. Broad Postdoctoral Fellow. This work was supported by the Alfred P. Sloan Foundation and George & Jean Brumley, Jr. Endowment (to C.T.K.).

PY - 2014

Y1 - 2014

N2 - Dendrites often exhibit structural changes in response to local inputs. Although mechanisms that pattern and maintain dendritic arbors are becoming clearer, processes regulating regrowth, during context-dependent plasticity or after injury, remain poorly understood. We found that a class of Drosophila sensory neurons, through complete pruning and regeneration, can elaborate two distinct dendritic trees, innervating independent sensory fields. An expression screen identified Cysteine proteinase-1 (Cp1) as a critical regulator of this process. Unlike known ecdysone effectors, Cp1-mutant ddaC neurons pruned larval dendrites normally but failed to regrow adult dendrites. Cp1 expression was upregulated/concentrated in the nucleus during metamorphosis, controlling production of a truncated Cut homeodomain transcription factor. This truncated Cut, but not the full-length protein, allowed Cp1-mutant ddaC neurons to regenerate higher-order adult dendrites. These results identify a molecular pathway needed for dendrite regrowth after pruning, which allows the same neuron to innervate distinct sensory fields.

AB - Dendrites often exhibit structural changes in response to local inputs. Although mechanisms that pattern and maintain dendritic arbors are becoming clearer, processes regulating regrowth, during context-dependent plasticity or after injury, remain poorly understood. We found that a class of Drosophila sensory neurons, through complete pruning and regeneration, can elaborate two distinct dendritic trees, innervating independent sensory fields. An expression screen identified Cysteine proteinase-1 (Cp1) as a critical regulator of this process. Unlike known ecdysone effectors, Cp1-mutant ddaC neurons pruned larval dendrites normally but failed to regrow adult dendrites. Cp1 expression was upregulated/concentrated in the nucleus during metamorphosis, controlling production of a truncated Cut homeodomain transcription factor. This truncated Cut, but not the full-length protein, allowed Cp1-mutant ddaC neurons to regenerate higher-order adult dendrites. These results identify a molecular pathway needed for dendrite regrowth after pruning, which allows the same neuron to innervate distinct sensory fields.

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Cysteine proteinase-1 and cut protein isoform control dendritic innervation of two distinct sensory fields by a single neuron

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