Immortalized retinal neurons derived from SV40 T-antigen-induced tumors in transgenic mice

Joseph P. Hammang; E. Edward Baetge; Richard R. Behringer; Ralph L. Brinster; Richard D. Palmiter; Albee Messing

doi:10.1016/0896-6273(90)90204-S

Immortalized retinal neurons derived from SV40 T-antigen-induced tumors in transgenic mice

Joseph P. Hammang, E. Edward Baetge, Richard R. Behringer, Ralph L. Brinster, Richard D. Palmiter, Albee Messing

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

71 Scopus citations

Abstract

Immortalized retinal neurons have been established in tissue culture from retinal tumors arising in transgenic mice. The mice carry the SV40 Tantigen under the control of 5′ flanking sequences from the human phenylethanolamine N-methyltransferase (PNMT) gene in order to target oncogene expression to adrenergic cell types. The retinal cultures contain a proliferating population of Tantigen-positive cells with a neuronal morphology that includes formation of extensive neuritic processes. We identified the cells as amacrine-derived neurons by immunofluorescence using the cell-specific monoclonal antibodies VC1.1 and HPC-1. The cells also express all three neurofilament subunits and GAP-43. These results indicate that CNS neurons can be transformed in transgenic animals to generate cultured cells with many properties of mature neurons.

Original language	English (US)
Pages (from-to)	775-782
Number of pages	8
Journal	Neuron
Volume	4
Issue number	5
DOIs	https://doi.org/10.1016/0896-6273(90)90204-S
State	Published - May 1990
Externally published	Yes

ASJC Scopus subject areas

General Neuroscience

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10.1016/0896-6273(90)90204-S

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@article{eb8b2c98630945a8bca3db011384c8e8,

title = "Immortalized retinal neurons derived from SV40 T-antigen-induced tumors in transgenic mice",

abstract = "Immortalized retinal neurons have been established in tissue culture from retinal tumors arising in transgenic mice. The mice carry the SV40 Tantigen under the control of 5′ flanking sequences from the human phenylethanolamine N-methyltransferase (PNMT) gene in order to target oncogene expression to adrenergic cell types. The retinal cultures contain a proliferating population of Tantigen-positive cells with a neuronal morphology that includes formation of extensive neuritic processes. We identified the cells as amacrine-derived neurons by immunofluorescence using the cell-specific monoclonal antibodies VC1.1 and HPC-1. The cells also express all three neurofilament subunits and GAP-43. These results indicate that CNS neurons can be transformed in transgenic animals to generate cultured cells with many properties of mature neurons.",

author = "Hammang, {Joseph P.} and Baetge, {E. Edward} and Behringer, {Richard R.} and Brinster, {Ralph L.} and Palmiter, {Richard D.} and Albee Messing",

note = "Funding Information: We thank C. Barnstable for the gift of the VC1.1 and HPC-I antibodies, V. Lee for the gift of neurofilament-and vimentin-specific antibodies, and D. Schreyer for the gift of GAP45specific antibody. We thank B. Bavister for assistance with time-lapse cinematography and C. Cepko and T. Reh for comments on the manuscript. This work was supported by grants from the National Institutes of Health and the March of Dimes. A. M. is a recipient of a Shaw Scholars Award from the Milwaukee Foundation and a Teacher-Investigator Development Award from the NINDS.",

year = "1990",

month = may,

doi = "10.1016/0896-6273(90)90204-S",

language = "English (US)",

volume = "4",

pages = "775--782",

journal = "Neuron",

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AU - Hammang, Joseph P.

AU - Baetge, E. Edward

AU - Behringer, Richard R.

AU - Brinster, Ralph L.

AU - Palmiter, Richard D.

AU - Messing, Albee

N1 - Funding Information: We thank C. Barnstable for the gift of the VC1.1 and HPC-I antibodies, V. Lee for the gift of neurofilament-and vimentin-specific antibodies, and D. Schreyer for the gift of GAP45specific antibody. We thank B. Bavister for assistance with time-lapse cinematography and C. Cepko and T. Reh for comments on the manuscript. This work was supported by grants from the National Institutes of Health and the March of Dimes. A. M. is a recipient of a Shaw Scholars Award from the Milwaukee Foundation and a Teacher-Investigator Development Award from the NINDS.

PY - 1990/5

Y1 - 1990/5

N2 - Immortalized retinal neurons have been established in tissue culture from retinal tumors arising in transgenic mice. The mice carry the SV40 Tantigen under the control of 5′ flanking sequences from the human phenylethanolamine N-methyltransferase (PNMT) gene in order to target oncogene expression to adrenergic cell types. The retinal cultures contain a proliferating population of Tantigen-positive cells with a neuronal morphology that includes formation of extensive neuritic processes. We identified the cells as amacrine-derived neurons by immunofluorescence using the cell-specific monoclonal antibodies VC1.1 and HPC-1. The cells also express all three neurofilament subunits and GAP-43. These results indicate that CNS neurons can be transformed in transgenic animals to generate cultured cells with many properties of mature neurons.

AB - Immortalized retinal neurons have been established in tissue culture from retinal tumors arising in transgenic mice. The mice carry the SV40 Tantigen under the control of 5′ flanking sequences from the human phenylethanolamine N-methyltransferase (PNMT) gene in order to target oncogene expression to adrenergic cell types. The retinal cultures contain a proliferating population of Tantigen-positive cells with a neuronal morphology that includes formation of extensive neuritic processes. We identified the cells as amacrine-derived neurons by immunofluorescence using the cell-specific monoclonal antibodies VC1.1 and HPC-1. The cells also express all three neurofilament subunits and GAP-43. These results indicate that CNS neurons can be transformed in transgenic animals to generate cultured cells with many properties of mature neurons.

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Immortalized retinal neurons derived from SV40 T-antigen-induced tumors in transgenic mice

Abstract

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