Purα is essential for postnatal brain development and developmentally coupled cellular proliferation as revealed by genetic inactivation in the mouse

Kamel Khalili; Luis Del Valle; Vandhana Muralidharan; William J. Gault; Nune Darbinian; Jessica Otte; Ellen Meier; Edward M. Johnson; Dianne C. Daniel; Yayoi Kinoshita; Shohreh Amini; Jennifer Gordon

doi:10.1128/MCB.23.19.6857-6875.2003

Purα is essential for postnatal brain development and developmentally coupled cellular proliferation as revealed by genetic inactivation in the mouse

Kamel Khalili, Luis Del Valle, Vandhana Muralidharan, William J. Gault, Nune Darbinian, Jessica Otte, Ellen Meier, Edward M. Johnson, Dianne C. Daniel, Yayoi Kinoshita, Shohreh Amini, Jennifer Gordon

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146 Scopus citations

Abstract

The single-stranded DNA- and RNA-binding protein, Purα, has been implicated in many biological processes, including control of transcription of multiple genes, initiation of DNA replication, and RNA transport and translation. Deletions of the PURA gene are frequent in acute myeloid leukemia. Mice with targeted disruption of the PURA gene in both alleles appear normal at birth, but at 2 weeks of age, they develop neurological problems manifest by severe tremor and spontaneous seizures and they die by 4 weeks. There are severely lower numbers of neurons in regions of the hippocampus and cerebellum of PURA^-/- mice versus those of age-matched +/+ littermates, and lamination of these regions is aberrant at time of death. Immunohistochemical analysis of MCM7, a protein marker for DNA replication, reveals a lack of proliferation of precursor cells in these regions in the PURA^-/- mice. Levels of proliferation were also absent or low in several other tissues of the PURA^-/- mice, including those of myeloid lineage, whereas those of PURA^+/- mice were intermediate. Evaluation of brain sections indicates a reduction in myelin and glial fibrillary acidic protein labeling in oligodendrocytes and astrocytes, respectively, indicating pathological development of these cells. At postnatal day 5, a critical time for cerebellar development, Purα and Cdk5 were both at peak levels in bodies and dendrites of Purkinje cells of PURA^+/+ mice, but both were absent in dendrites of PURA^-/- mice. Purα and Cdk5 can be coimmunoprecipitated from brain lysates of PURA^+/+ mice. Immunohistochemical studies reveal a dramatic reduction in the level of both phosphorylated and nonphosphorylated neurofilaments in dendrites of the Purkinje cell layer and of synapse formation in the hippocampus. Overall results are consistent with a role for Purα in developmentally timed DNA replication in specific cell types and also point to a newly emerging role in compartmentalized RNA transport and translation in neuronal dendrites.

Original language	English
Pages (from-to)	6857-6875
Number of pages	19
Journal	Molecular and Cellular Biology
Volume	23
Issue number	19
DOIs	https://doi.org/10.1128/MCB.23.19.6857-6875.2003
State	Published - Oct 2003

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10.1128/MCB.23.19.6857-6875.2003

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Khalili, K., Del Valle, L., Muralidharan, V., Gault, W. J., Darbinian, N., Otte, J., Meier, E., Johnson, E. M., Daniel, D. C., Kinoshita, Y., Amini, S., & Gordon, J. (2003). Purα is essential for postnatal brain development and developmentally coupled cellular proliferation as revealed by genetic inactivation in the mouse. Molecular and Cellular Biology, 23(19), 6857-6875. https://doi.org/10.1128/MCB.23.19.6857-6875.2003

@article{40848a8409784f22bd6141d6195d78d8,

title = "Purα is essential for postnatal brain development and developmentally coupled cellular proliferation as revealed by genetic inactivation in the mouse",

abstract = "The single-stranded DNA- and RNA-binding protein, Purα, has been implicated in many biological processes, including control of transcription of multiple genes, initiation of DNA replication, and RNA transport and translation. Deletions of the PURA gene are frequent in acute myeloid leukemia. Mice with targeted disruption of the PURA gene in both alleles appear normal at birth, but at 2 weeks of age, they develop neurological problems manifest by severe tremor and spontaneous seizures and they die by 4 weeks. There are severely lower numbers of neurons in regions of the hippocampus and cerebellum of PURA-/- mice versus those of age-matched +/+ littermates, and lamination of these regions is aberrant at time of death. Immunohistochemical analysis of MCM7, a protein marker for DNA replication, reveals a lack of proliferation of precursor cells in these regions in the PURA-/- mice. Levels of proliferation were also absent or low in several other tissues of the PURA-/- mice, including those of myeloid lineage, whereas those of PURA+/- mice were intermediate. Evaluation of brain sections indicates a reduction in myelin and glial fibrillary acidic protein labeling in oligodendrocytes and astrocytes, respectively, indicating pathological development of these cells. At postnatal day 5, a critical time for cerebellar development, Purα and Cdk5 were both at peak levels in bodies and dendrites of Purkinje cells of PURA+/+ mice, but both were absent in dendrites of PURA-/- mice. Purα and Cdk5 can be coimmunoprecipitated from brain lysates of PURA+/+ mice. Immunohistochemical studies reveal a dramatic reduction in the level of both phosphorylated and nonphosphorylated neurofilaments in dendrites of the Purkinje cell layer and of synapse formation in the hippocampus. Overall results are consistent with a role for Purα in developmentally timed DNA replication in specific cell types and also point to a newly emerging role in compartmentalized RNA transport and translation in neuronal dendrites.",

author = "Kamel Khalili and {Del Valle}, Luis and Vandhana Muralidharan and Gault, {William J.} and Nune Darbinian and Jessica Otte and Ellen Meier and Johnson, {Edward M.} and Daniel, {Dianne C.} and Yayoi Kinoshita and Shohreh Amini and Jennifer Gordon",

year = "2003",

month = oct,

doi = "10.1128/MCB.23.19.6857-6875.2003",

language = "English",

volume = "23",

pages = "6857--6875",

journal = "Molecular and Cellular Biology",

issn = "0270-7306",

publisher = "American Society for Microbiology",

number = "19",

}

Khalili, K, Del Valle, L, Muralidharan, V, Gault, WJ, Darbinian, N, Otte, J, Meier, E, Johnson, EM, Daniel, DC , Kinoshita, Y, Amini, S & Gordon, J 2003, 'Purα is essential for postnatal brain development and developmentally coupled cellular proliferation as revealed by genetic inactivation in the mouse', Molecular and Cellular Biology, vol. 23, no. 19, pp. 6857-6875. https://doi.org/10.1128/MCB.23.19.6857-6875.2003

TY - JOUR

T1 - Purα is essential for postnatal brain development and developmentally coupled cellular proliferation as revealed by genetic inactivation in the mouse

AU - Khalili, Kamel

AU - Del Valle, Luis

AU - Muralidharan, Vandhana

AU - Gault, William J.

AU - Darbinian, Nune

AU - Otte, Jessica

AU - Meier, Ellen

AU - Johnson, Edward M.

AU - Daniel, Dianne C.

AU - Kinoshita, Yayoi

AU - Amini, Shohreh

AU - Gordon, Jennifer

PY - 2003/10

Y1 - 2003/10

N2 - The single-stranded DNA- and RNA-binding protein, Purα, has been implicated in many biological processes, including control of transcription of multiple genes, initiation of DNA replication, and RNA transport and translation. Deletions of the PURA gene are frequent in acute myeloid leukemia. Mice with targeted disruption of the PURA gene in both alleles appear normal at birth, but at 2 weeks of age, they develop neurological problems manifest by severe tremor and spontaneous seizures and they die by 4 weeks. There are severely lower numbers of neurons in regions of the hippocampus and cerebellum of PURA-/- mice versus those of age-matched +/+ littermates, and lamination of these regions is aberrant at time of death. Immunohistochemical analysis of MCM7, a protein marker for DNA replication, reveals a lack of proliferation of precursor cells in these regions in the PURA-/- mice. Levels of proliferation were also absent or low in several other tissues of the PURA-/- mice, including those of myeloid lineage, whereas those of PURA+/- mice were intermediate. Evaluation of brain sections indicates a reduction in myelin and glial fibrillary acidic protein labeling in oligodendrocytes and astrocytes, respectively, indicating pathological development of these cells. At postnatal day 5, a critical time for cerebellar development, Purα and Cdk5 were both at peak levels in bodies and dendrites of Purkinje cells of PURA+/+ mice, but both were absent in dendrites of PURA-/- mice. Purα and Cdk5 can be coimmunoprecipitated from brain lysates of PURA+/+ mice. Immunohistochemical studies reveal a dramatic reduction in the level of both phosphorylated and nonphosphorylated neurofilaments in dendrites of the Purkinje cell layer and of synapse formation in the hippocampus. Overall results are consistent with a role for Purα in developmentally timed DNA replication in specific cell types and also point to a newly emerging role in compartmentalized RNA transport and translation in neuronal dendrites.

AB - The single-stranded DNA- and RNA-binding protein, Purα, has been implicated in many biological processes, including control of transcription of multiple genes, initiation of DNA replication, and RNA transport and translation. Deletions of the PURA gene are frequent in acute myeloid leukemia. Mice with targeted disruption of the PURA gene in both alleles appear normal at birth, but at 2 weeks of age, they develop neurological problems manifest by severe tremor and spontaneous seizures and they die by 4 weeks. There are severely lower numbers of neurons in regions of the hippocampus and cerebellum of PURA-/- mice versus those of age-matched +/+ littermates, and lamination of these regions is aberrant at time of death. Immunohistochemical analysis of MCM7, a protein marker for DNA replication, reveals a lack of proliferation of precursor cells in these regions in the PURA-/- mice. Levels of proliferation were also absent or low in several other tissues of the PURA-/- mice, including those of myeloid lineage, whereas those of PURA+/- mice were intermediate. Evaluation of brain sections indicates a reduction in myelin and glial fibrillary acidic protein labeling in oligodendrocytes and astrocytes, respectively, indicating pathological development of these cells. At postnatal day 5, a critical time for cerebellar development, Purα and Cdk5 were both at peak levels in bodies and dendrites of Purkinje cells of PURA+/+ mice, but both were absent in dendrites of PURA-/- mice. Purα and Cdk5 can be coimmunoprecipitated from brain lysates of PURA+/+ mice. Immunohistochemical studies reveal a dramatic reduction in the level of both phosphorylated and nonphosphorylated neurofilaments in dendrites of the Purkinje cell layer and of synapse formation in the hippocampus. Overall results are consistent with a role for Purα in developmentally timed DNA replication in specific cell types and also point to a newly emerging role in compartmentalized RNA transport and translation in neuronal dendrites.

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U2 - 10.1128/MCB.23.19.6857-6875.2003

DO - 10.1128/MCB.23.19.6857-6875.2003

M3 - Article

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AN - SCOPUS:0141557777

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JO - Molecular and Cellular Biology

JF - Molecular and Cellular Biology

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Purα is essential for postnatal brain development and developmentally coupled cellular proliferation as revealed by genetic inactivation in the mouse

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