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Temporal-spatial expressions of p27(kip1) and its phosphorylation on Serine-10 after acute spinal cord injury in adult rat: Implications for post-traumatic glial proliferation.

Temporal-spatial expressions of p27(kip1) and its phosphorylation on Serine-10 after acute spinal cord injury in adult rat: Implications for post-traumatic glial proliferation. Research Abstract Details 

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  • Temporal-spatial expressions of p27(kip1) and its phosphorylation on Serine-10 after acute spinal cord injury in adult rat: Implications for post-traumatic glial proliferation. Abstract Text:

    aiguo shenAiguo Shen,yonghua liuYonghua Liu,jian zhaoJian Zhao,jing qinJing Qin,shuxian shiShuxian Shi,mengling chenMengling Chen,shangfeng gaoShangfeng Gao,feng xiaoFeng Xiao,qiuyan luQiuyan Lu,chun chengChun Cheng,

    p27(kip1), as a member of Cip/Kip family of cyclin-dependent kinase inhibitors, plays important roles in cell cycle regulation and neurogenesis in the developing central nervous system. Serine-10 is the major phosphorylation site of p27(kip1), and post-translational regulation of p27(kip1) by different phosphorylation events is critical for its function. To elucidate the expressions and possible functions of p27(kip1) and its phosphorylation in central nervous system lesion and repair, we performed an acute spinal cord contusion injury model in adult rats. Our work studied the temporal-spatial expression patterns of p27(kip1) and Serine-10 phosphorylated p27(kip1) (p-p27s10). Western blot analysis showed p27(kip1) level significantly decreased at day 3 after damage, while p-p27s10 was detected at a high-level at the same time reaching the uninjured level. Moreover, immunofluorescence double labeling suggested these changes were striking in microglia and astrocytes, which were largely proliferated. Immunohistochemical analysis revealed subcellular localization changes of p27(kip1) and p-p27s10 staining between nucleus and cytoplasm after injury in about 20% of total positive cells including neurons and glial cells. We also investigated the increased interactions of p27(kip1) and p-p27s10 with CRM1 3 days after injury by co-immunoprecipitation studies. Taken together, we hypothesized spinal cord injury stimulated mitogenic signals to induce a serine-threonine kinase KIS (kinase interacting stathmin) to phosphorylate p27(kip1) on Serine-10, so that p27(kip1) could bind to CRM1 and be exported from nuclei for degradation. Such an event facilitated cell cycle progression of glial cells, especially microglia and astrocytes which had a prevalent proliferation.

    Temporal-spatial expressions of p27(kip1) and its phosphorylation on Serine-10 after acute spinal cord injury in adult rat: Implications for post-traumatic glial proliferation. Publishing Authors By Initials

    a shenA Shen,y liuY Liu,j zhaoJ Zhao,j qinJ Qin,s shiS Shi,m chenM Chen,s gaoS Gao,f xiaoF Xiao,q luQ Lu,c chengC Cheng,

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    Temporal-spatial expressions of p27(kip1) and its phosphorylation on Serine-10 after acute spinal cord injury in adult rat: Implications for post-traumatic glial proliferation. Journal Published:

    PUBLICATION TYPE: Journal Article

    Journal: Neurochemistry international

    VOLUME: 52

    Page Numbers: 1266-75

    Journal Abbreviation:

    ISSN: 0197-0186

    DAY: 31

    MONTH: 01

    YEAR: 2008

    Temporal-spatial expressions of p27(kip1) and its phosphorylation on Serine-10 after acute spinal cord injury in adult rat: Implications for post-traumatic glial proliferation. Information

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    LANGUAGE: eng

    NlmUniqueID: 8006959

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    Grant and Affiliation Information for Temporal-spatial expressions of p27(kip1) and its phosphorylation on Serine-10 after acute spinal cord injury in adult rat: Implications for post-traumatic glial proliferation.

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    Country: England

    England Research PublicationEngland Research Publication

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    MEDLINETA: Neurochem Int

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