Establishing a Pathological Diagnosis in Degenerative Dementias

While clinicopathological studies have confirmed that Alzheimer's disease (AD) is the most common neurodegenerative cause of dementia, these same studies have also revealed that other degenerative pathologies account for a significant proportion of patients with cognitive decline. Because pathological assessment of non‐Alzheimer neurodegenerative diseases now demands routine use of a costly panel of immunohistochemical techniques a scheme for staged examination of brain tissue has been developed. This scheme is weighted to initially screen out cases of Alzheimer's disease, dementia with Lewy bodies and vascular dementia using conventional staining methods and established diagnostic protocols, bringing in immunochemical techniques to discriminate between non‐Alzheimer degenerative dementias. Diagnosis of pathologies causing the clinical syndrome of frontotemporal dementia can be ascertained using conventional staining supplemented by immunochemical detection of ubiquitin, tau protein and α B crystallin. The diagnosis of prion disease is reliably confirmed by immunohistochemical detection of prion protein. This morphological assessment complements emerging genetic insights into many of these neurodegenerative diseases.

[1]  W. Schlote,et al.  Tissue Handling in Suspected Creutzfeldt‐Jakob Disease (CJD) and Other Human Spongiform Encephalopathies (Prion Diseases) , 1995, Brain pathology.

[2]  D. Dickson Pick's Disease: A Modern Approach , 1998, Brain pathology.

[3]  S. Coker The diagnosis of childhood neurodegenerative disorders presenting as dementia in adults , 1991, Neurology.

[4]  J. Lowe,et al.  Motor neurone disease-inclusion dementia. , 1996, Neurodegeneration : a journal for neurodegenerative disorders, neuroprotection, and neuroregeneration.

[5]  D. Mann,et al.  τ Ubiquitin, and αB-Crystallin Immunohistochemistry Define the Principal Causes of Degenerative Frontotemporal Dementia , 1995 .

[6]  B. Ghetti,et al.  Frontotemporal Dementia and Parkinsonism Linked to Chromosome 17: A New Group of Tauopathies , 1998, Brain pathology.

[7]  K. Jellinger,et al.  Senile Dementia with Tangles (Tangle Predominant Form of Senile Dementia) , 1998, Brain pathology.

[8]  E. Perry,et al.  Dementia with Lewy Bodies. A Distinct Non‐Alzheimer Dementia Syndrome? , 1998, Brain pathology.

[9]  A. Probst,et al.  Frontal lobe degeneration: novel ubiquitin‐immunoreactive neurites within frontotemporal cortex , 1995, Neuropathology and applied neurobiology.

[10]  G. C. Román,et al.  Vascular dementia , 1993, Neurology.

[11]  E. Wagner,et al.  Do Surgical Brain Lesions Present as Isolated Dementia? A Population‐Based Study , 1995, Journal of the American Geriatrics Society.

[12]  John Q. Trojanowski,et al.  Consensus Recommendations for the Postmortem Diagnosis of Alzheimer’s Disease , 1997, Neurobiology of Aging.

[13]  L. Thal,et al.  Hippocampal Sclerosis Contributes to Dementia in the Elderly , 1997, Neurology.

[14]  D. Mann,et al.  Dementia of Frontal Type and Dementias with Subcortical Gliosis , 1998, Brain pathology.

[15]  P. Lantos,et al.  Accumulation of tubular structures in oligodendroglial and neuronal cells as the basic alteration in multiple system atrophy , 1992, Journal of the Neurological Sciences.

[16]  J. Lowe Degenerative Non‐Alzheimer Dementias , 1997 .

[17]  D. Mann,et al.  Tau, ubiquitin, and alpha B-crystallin immunohistochemistry define the principal causes of degenerative frontotemporal dementia. , 1995, Archives of neurology.

[18]  P. Lantos,et al.  Prion protein immunocytochemistry – UK five centre consensus report , 1997, Neuropathology and applied neurobiology.

[19]  K. Jellinger Dementia with Grains (Argyrophilic Grain Disease) , 1998, Brain pathology.

[20]  A. Lang,et al.  Corticobasal Ganglionic Degeneration and Progressive Supranuclear Palsy Presenting with Cognitive Decline , 1998, Brain pathology.

[21]  S. Mirra,et al.  Making the diagnosis of Alzheimer's disease. A primer for practicing pathologists. , 1993, Archives of pathology & laboratory medicine.

[22]  A. Heyman,et al.  The Consortium to Establish a Registry for Alzheimer's Disease (CERAD) , 1993, Neurology.