• Title of article

    Mitotic phosphoepitopes precede paired helical filaments in Alzheimer’s disease

  • Author/Authors

    I. Vincent، نويسنده , , J. -H. Zheng، نويسنده , , D. W. Dickson، نويسنده , , Y. Kress، نويسنده , , P. Davies، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 1998
  • Pages
    10
  • From page
    287
  • To page
    296
  • Abstract
    We have shown previously that the TG-3 and MPM-2 antibodies recognize phosphoepitopes common to mitosis and degenerating neurons of Alzheimer’s disease(AD) brain. Here, we have evaluated their occurrence in human brain biopsy tissue, and confirm that they are absent in mature neurons of adult brain, but reappear during neurodegeneration in AD. The TG-3 epitope appears ahead of the MPM-2 epitope and is distributed throughout the neuronal soma. Tau is the major TG-3 antigen in AD brain. The initial localization of MPM-2 immunoreactivity in primary dendrites, it’s robust occurrence in granulovacuolar bodies, and the increased immunoreactivity with 300–350-kDa proteins, suggest MAP1B as a candidate MPM-2 antigen in AD. Production of mitotic phosphepitopes in more than one type of human neurodegenerative lesion implicates mitotic kinases as common mediators of neuronal death. Because mitotic phosphoepitopes appear before paired helical filaments, it is suggested that mitotic kinase activation triggers neurofibrillary tangle formation. Future studies will need to focus on factors influencing mitotic kinase activity, a point with potential for early diagnosis and disease abrogation.
  • Keywords
    Cell cycle proteins , mitosis , Paired helical filaments , Neurofibrillary tangles , Neurodegeneration , Alzheimer’s disease , Granulovacuolar degeneration , Neuronal death , MPM-2 , Tau phosphorylation , Mitotic cdc2 , Cyclin B kinase , TG-3
  • Journal title
    Neurobiology of Aging
  • Serial Year
    1998
  • Journal title
    Neurobiology of Aging
  • Record number

    819770