J Constantinidis scite author profile

During a recent clinical and neuropathological evaluation of a large autopsy population of brains our attention was drawn to a subset of patients with Alzheimer's disease (AD) presenting with a major impairment of visuospatial skills referred to as Balint's syndrome. In this subset a shift in the distribution of certain pathological profiles had occurred in that the visual areas of the occipital and posterior parietal regions had an increased number of lesions, whereas the prefrontal cortex had fewer lesions than usually observed in AD. Previous quantitative analyses have shown that generally in AD, primary sensory cortical areas are less damaged than association areas of the frontal and temporal lobes, as demonstrated by the laminar and regional distribution of two neuropathological features of the disease, neurofibrillary tangles and neuritic (senile) plaques. The distribution of pathological lesions in the AD cases with Balint's syndrome revealed that specific visual association pathways were disrupted, which are normally spared in AD. These data suggest that in some cases of AD, the particular psychological and neurological symptomatology may be caused by the selective loss of specific corticocortical systems, as reflected in the differential distribution of the neuropathological markers of the disease.

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An immunohistochemical study of pro-somatostatin-derived peptides in the human brain

Bouras¹,

Magistretti²,

Morrison

et al. 1987

Neuroscience

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The malignancy of dementias

Todorov

Elston

et al. 1978

Annals of Neurology

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changes in acute experimental hypertension. An ultrasrructural study. Lab Invest 3615C161. 1977 16. Owman CH, Edvinsson L, Hardebo JE, et al: Immunohistochemical demonstration of actin and myosin in brain capillaries, in Ingvar DH, Lassen N A (eds): Cerebral Function, Metabolism and Circulation. Copenhagen, Munksgaard, 1977, pp 384-385 17. Petito CK, Schaefer JA, Plum F The blood-brain barrier in experimental seizures, in Pappius HM, Feindel W (eds): Dynamics of Brain Edema. Heidelberg, New York, Springer, 1976, pp 38-42 18. Pollard TD, Shelron E, Weihing RR, et al: Ultrastructural characterization of F-actin isolated from Aranthamorba ratel-Laii and identificarion of cytoplasmic filaments as F-actin by reaction with rabbit heavy meromyosin. J Mol Biol50:91-97, 1970 19. Roggendorf W, Cervos-Navarro J, Matakas F The ultrastructural criteria of intracerebrd arterioles, in Cerv6s-Navarro J, Betz E, Matakas F, et al (eds): The Cerebral Vessel Wall. New York, Raven Press, pp 23-31, 1976 20. Rohlich P, Olah I: Cross-striated fibrils in the endothelium of the rat myomeuial arterioles. Epstein L, Simon A, Meck R. Clinical neuropathologic correlates in senile and cerebral arteriosclerotic psychoses, in Hatsen P (ed): Old Age w i t h a Future. Copenhagen, Munksgaard, 1964, p 272 Katzman R: T h e prevalence and malignancy of Alzheimer's disease. Arch Neurol 33:217-218, 1976 Kay D W K Outcome and cause of Qach in mental disorders of old age: a long term follow up of functional and organic psychoses. Acta Psychiatr Scand 38:249-276, 1962 Litjrmae H, Fuld PA, Katzman R: Prevalence and malignancy of Alzheimer's disease. Arch Neurol 33:304, 1976 Peik A, Wolloch L, Rodstein M: Mortality of the aged with chronic brain syndrome. J Am Geriacr SOC 21:264-270, 1973 Todorov AB, Go RCP, Constantinidis J, et al: Specificity of the clinical diagnosis of dementia J Neurol Sci 2681-98, 1975 Wang HA, Whanger A: Brain impairment and longevity, in Palmore E, Jeffers FC (eds): Prediction of Life Span. Lexington, MA, DC Heath, 1971, pp 99-105 Brief Communication: Go et al: Life Expectancy of Patients with Dementia 561

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The dominant form of the pigmentary orthochromatic leukodystrophy

Constantinidis

Wisniewski

1991

Acta Neuropathol

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The present report documents a family with three cases in two successive generations of pigmentary orthochromatic leukodystrophy (POLD). The clinical features of these cases and histochemical and ultrastructural investigations of two of the brains from successive generations are discussed. A review of the familial cases of POLD reported in the literature is also presented. Transmission of these cases was by a dominant inheritance. Onset of the clinical symptoms occurred at 42 to 54 years of age; duration of the disease was from 2-11 years, and death occurred at 45 to 57 years of age. Clinical manifestations of all three cases were severe headaches; bilateral pyramidal, pseudobulbar, cerebellar, and frontal release signs; gait disturbances; euphoria, or apathy; epileptic seizures; and dementia. The neuropathological pattern consists of slight cerebral atrophy, brownish discoloration of the cerebral white matter with demyelination and severe gliosis, sparing the sub-cortical U fibers; presence in the macrophages of lipid pigment granules that are sudanophilic, non metachromatic, and PAS and iron positive. The electron microscopic pattern of the lipid pigment in the macrophages is that of ceroid: electron-dense, membrane-bound intracytoplasmic lysosomes with curvilinear and/or fingerprint profiles.

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