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We are analyzing https://link.springer.com/article/10.1007/s00401-007-0315-5.

Title:
Severe subcortical TDP-43 pathology in sporadic frontotemporal lobar degeneration with motor neuron disease | Acta Neuropathologica
Description:
Recently, TDP-43, a 43 kDa nuclear TAR DNA-binding protein, was identified as the major disease protein in frontotemporal lobar degeneration with ubiquitinated inclusions (FTLD-U), FTLD-U with motor neuron disease (FTLD–MND), and amyotrophic lateral sclerosis. To date, TDP-43 pathology in sporadic FTLD–MND has been reported only in select central nervous system areas. However, this distribution of lesions is insufficient to explain all clinical signs of FTLD–MND and the extent of TDP-43 pathology, throughout the brain, remains unknown. Therefore, as a pilot study, we performed an immunohistochemical whole brain scan of two cases diagnosed clinically as FTLD–MND and two control subjects. We found evidence of both neuronal and glial TDP-43 pathology in multiple brain areas including the nigro-striatal system, neo- and allocortical brain areas, with varying frequency, morphology, and degree, and nowhere in control tissue. The finding of a distinct cytopathological profile consisting of a cell nucleus devoid of endogenous TDP-43 staining coupled with diffuse/granular cytoplasmic staining (ā€œpre-inclusionā€) was prominent in a couple of brain areas. These pre-inclusions were not or only weakly ubiquitin-immunoreactive. While the findings of severe involvement of extracortical or extrapyramidal areas are strongly suggestive for FTLD–MND being a TDP-43 multisystem proteinopathy rather than a disease predominantly affecting the cortex and spinal cord, more detailed clinicopathological studies of larger cohorts are needed to fully elucidate the distribution and severity of pathological TDP-43 in this disease.
Website Age:
28 years and 1 months (reg. 1997-05-29).

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Custom-built

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🌠 Phenomenal Traffic: 5M - 10M visitors per month


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Keywords {šŸ”}

article, tdp, google, scholar, pubmed, frontotemporal, disease, cas, degeneration, lobar, lee, trojanowski, neuropathol, acta, pathology, motor, neuron, kwong, sclerosis, amyotrophic, lateral, neumann, vmy, dementia, sporadic, geser, inclusions, brain, neurol, mackenzie, pathological, access, privacy, cookies, content, research, brandmeir, ftldmnd, areas, kretzschmar, grossman, information, publish, search, nicholas, protein, proteinopathy, alzheimers, white, cairns,

Topics {āœ’ļø}

neurodegenerative disease research tar dna-binding protein month download article/chapter amador-ortiz motor neuron disease diffuse/granular cytoplasmic staining post-stroke emotional incontinence amyotrophic lateral sclerosis motor neuron disorders ubiquitin-positive inclusions delineated white cl iii major disease protein full article pdf frontotemporal lobar degeneration disease predominantly affecting privacy choices/manage cookies disease core center nuclear factor tdp-43 tdp-43 multisystem proteinopathy rna binding properties familial frontotemporal dementia nigro-striatal system related subjects pseudobulbar affect including ubiquitin-positive inclusions small lenticulocapsular stroke cerebral tdp-43 pathology weakly ubiquitin-immunoreactive parkinsonism–dementia complex european economic area cases diagnosed clinically cell nucleus devoid graff-radford nr leverenz jb expert technical assistance check access instant access glial tdp-43 pathology conditions privacy policy vcp gene mutations alpha-synuclein pathology cairns nj de rijik mc detailed clinicopathological studies sod1 gene mutation tdp-43-immunoreactive neuronal van swieten jc allocortical brain areas accepting optional cookies article log

Schema {šŸ—ŗļø}

WebPage:
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         headline:Severe subcortical TDP-43 pathology in sporadic frontotemporal lobar degeneration with motor neuron disease
         description:Recently, TDP-43, a 43Ā kDa nuclear TAR DNA-binding protein, was identified as the major disease protein in frontotemporal lobar degeneration with ubiquitinated inclusions (FTLD-U), FTLD-U with motor neuron disease (FTLD–MND), and amyotrophic lateral sclerosis. To date, TDP-43 pathology in sporadic FTLD–MND has been reported only in select central nervous system areas. However, this distribution of lesions is insufficient to explain all clinical signs of FTLD–MND and the extent of TDP-43 pathology, throughout the brain, remains unknown. Therefore, as a pilot study, we performed an immunohistochemical whole brain scan of two cases diagnosed clinically as FTLD–MND and two control subjects. We found evidence of both neuronal and glial TDP-43 pathology in multiple brain areas including the nigro-striatal system, neo- and allocortical brain areas, with varying frequency, morphology, and degree, and nowhere in control tissue. The finding of a distinct cytopathological profile consisting of a cell nucleus devoid of endogenous TDP-43 staining coupled with diffuse/granular cytoplasmic staining (ā€œpre-inclusionā€) was prominent in a couple of brain areas. These pre-inclusions were not or only weakly ubiquitin-immunoreactive. While the findings of severe involvement of extracortical or extrapyramidal areas are strongly suggestive for FTLD–MND being a TDP-43 multisystem proteinopathy rather than a disease predominantly affecting the cortex and spinal cord, more detailed clinicopathological studies of larger cohorts are needed to fully elucidate the distribution and severity of pathological TDP-43 in this disease.
         datePublished:2007-11-15T00:00:00Z
         dateModified:2007-11-15T00:00:00Z
         pageStart:123
         pageEnd:131
         sameAs:https://doi.org/10.1007/s00401-007-0315-5
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            TDP-43
            Frontotemporal dementia
            Frontotemporal lobar degeneration
            Motor neuron disease
            Pathology
            Neurosciences
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      headline:Severe subcortical TDP-43 pathology in sporadic frontotemporal lobar degeneration with motor neuron disease
      description:Recently, TDP-43, a 43Ā kDa nuclear TAR DNA-binding protein, was identified as the major disease protein in frontotemporal lobar degeneration with ubiquitinated inclusions (FTLD-U), FTLD-U with motor neuron disease (FTLD–MND), and amyotrophic lateral sclerosis. To date, TDP-43 pathology in sporadic FTLD–MND has been reported only in select central nervous system areas. However, this distribution of lesions is insufficient to explain all clinical signs of FTLD–MND and the extent of TDP-43 pathology, throughout the brain, remains unknown. Therefore, as a pilot study, we performed an immunohistochemical whole brain scan of two cases diagnosed clinically as FTLD–MND and two control subjects. We found evidence of both neuronal and glial TDP-43 pathology in multiple brain areas including the nigro-striatal system, neo- and allocortical brain areas, with varying frequency, morphology, and degree, and nowhere in control tissue. The finding of a distinct cytopathological profile consisting of a cell nucleus devoid of endogenous TDP-43 staining coupled with diffuse/granular cytoplasmic staining (ā€œpre-inclusionā€) was prominent in a couple of brain areas. These pre-inclusions were not or only weakly ubiquitin-immunoreactive. While the findings of severe involvement of extracortical or extrapyramidal areas are strongly suggestive for FTLD–MND being a TDP-43 multisystem proteinopathy rather than a disease predominantly affecting the cortex and spinal cord, more detailed clinicopathological studies of larger cohorts are needed to fully elucidate the distribution and severity of pathological TDP-43 in this disease.
      datePublished:2007-11-15T00:00:00Z
      dateModified:2007-11-15T00:00:00Z
      pageStart:123
      pageEnd:131
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         TDP-43
         Frontotemporal dementia
         Frontotemporal lobar degeneration
         Motor neuron disease
         Pathology
         Neurosciences
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            name:Jiang Qian
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                     name:Center for Neurodegenerative Disease Research, Department of Pathology and Laboratory Medicine, Alzheimer’s Disease Core Center, Institute on Aging, University of Pennsylvania School of Medicine, Philadelphia, USA
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         name:Alzheimer’s Disease Center, Albany Medical Center, Albany, USA
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         name:Department of Pathology and Laboratory Medicine, Albany Medical College, Albany, USA
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         name:Center for Neurodegenerative Disease Research, Department of Pathology and Laboratory Medicine, Alzheimer’s Disease Core Center, Institute on Aging, University of Pennsylvania School of Medicine, Philadelphia, USA
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            name:University of Pennsylvania School of Medicine
            address:
               name:Center for Neurodegenerative Disease Research, Department of Pathology and Laboratory Medicine, Alzheimer’s Disease Core Center, Institute on Aging, University of Pennsylvania School of Medicine, Philadelphia, USA
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      name:Jiang Qian
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            address:
               name:Department of Pathology and Laboratory Medicine, Albany Medical College, Albany, USA
               type:PostalAddress
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      name:Virginia M.-Y. Lee
      affiliation:
            name:University of Pennsylvania School of Medicine
            address:
               name:Center for Neurodegenerative Disease Research, Department of Pathology and Laboratory Medicine, Alzheimer’s Disease Core Center, Institute on Aging, University of Pennsylvania School of Medicine, Philadelphia, USA
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               name:Center for Neurodegenerative Disease Research, Department of Pathology and Laboratory Medicine, Alzheimer’s Disease Core Center, Institute on Aging, University of Pennsylvania School of Medicine, Philadelphia, USA
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      name:Alzheimer’s Disease Center, Albany Medical Center, Albany, USA
      name:Center for Neurodegenerative Disease Research, Department of Pathology and Laboratory Medicine, Alzheimer’s Disease Core Center, Institute on Aging, University of Pennsylvania School of Medicine, Philadelphia, USA
      name:Center for Neurodegenerative Disease Research, Department of Pathology and Laboratory Medicine, Alzheimer’s Disease Core Center, Institute on Aging, University of Pennsylvania School of Medicine, Philadelphia, USA
      name:Alzheimer’s Disease Center, Albany Medical Center, Albany, USA
      name:Department of Pathology and Laboratory Medicine, Albany Medical College, Albany, USA
      name:Center for Neurodegenerative Disease Research, Department of Pathology and Laboratory Medicine, Alzheimer’s Disease Core Center, Institute on Aging, University of Pennsylvania School of Medicine, Philadelphia, USA
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