4.2 Article

The intralaminar nuclei assigned to the medial pain system and other components of this system are early and progressively affected by the Alzheimer's disease-related cytoskeletal pathology

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JOURNAL OF CHEMICAL NEUROANATOMY
卷 23, 期 4, 页码 279-290

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DOI: 10.1016/S0891-0618(02)00007-8

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Alzheimer's disease; beta-amyloid; cytoskeletal pathology; medial pain system; tau protein

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The intralaminar nuclei of the human thalamus are integrated into the ascending reticular activating system and into limbic, oculomotor and somatomotor loops. In addition, some of them also represent important components of the medial pain system. We examined the occurrence and severity of the Alzheimer's disease (AD)-related cytoskeletal pathology and beta-amyloidosis in the seven intralaminar nuclei (central lateral nucleus, CL, central medial nucleus, CEM, centromedian nucleus, CM; cucullar nucleus, CU; paracentral nucleus, PC parafascicular nucleus, PF: subparafascicular nucleus, SPF) in 27 autopsy cases a( different stages of the cortical neurofibrillary pathology (cortical NFT/NT-stages I-VI) and beta-amyloidosis (cortical phases 1-4). The CEM. CL, PF, and SPF are slightly affected at stage II (corresponding to preclinical AD). They are markedly involved at stages III and IV (i.e. incipient AD) and severely affected at stages V and VI (i.e. clinical AD). In the PC and CU, the cytoskeletal pathology is mild at stage III, marked at stage IV. and severe at stages V-VI, whereas the CM is only mildly affected Lit stages IV VI, In all of the intralaminar nuclei, deposits of the protein beta-amyloid occur for the first time during the Final phase of cortical beta-amyloidosis. Functionally, the cytoskeletal pathology encountered in the intralaminar nuclei may contribute to the memory and affective symptoms. attention deficits, and dysfunctions related to horizontal saccades and smooth pursuits seen in AD patients. Equally important. however, are the findings that the cytoskeletal pathology developing within the intralaminar nuclei assigned to the medial pain system (CEM, CL, CU, PC, PF) as well as within other components of this system begins already during the preclinical or incipient phases of AD. Given this fact, the question arises as to whether non-discriminative aspects mediated by the medial pain system could be employed to identify individuals in the very earliest stages of AD. (C) 2002 Elsevier Science B,V. All rights reserved.

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