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Amyloids, genes and chaperones
Chapter by: Frangione B; Wisniewski T; Castano E; Ghiso J
in: Research advances in Alzheimer's disease and related disorders by Iqbal, Khalid [Eds]
New York : Wiley, 1995
pp. 563-568
ISBN: 0471952362
CID: 4974
Gerstmann-Straussler-Scheinker disease and the Indiana kindred
Ghetti B; Dlouhy SR; Giaccone G; Bugiani O; Frangione B; Farlow MR; Tagliavini F
Gerstmann-Straussler-Scheinker disease is an autosomal dominant disorder with a wide spectrum of clinical presentations including ataxia, spastic paraparesis, extrapyramidal signs, and dementia. The patients present with symptoms in the third to sixth decade of life and the mean duration of illness is five years. Mutations at codons 102, 105, 117, 145, 198 and 217 of the open reading frame of the prion protein gene have been associated with GSS disease. As a result of the mutations, a substitution at the corresponding residues of the prion protein occurs, or as in the case of the STOP mutation at codon 145, a truncated protein is produced. Neuropathologically, the common denominator is a cerebral prion protein amyloidosis; however, there is significant variability in the pattern of amyloid deposition in regions of the central nervous system among reported families. Amyloidosis coexists with severe spongiform degeneration in patients with the mutation at codon 102, and with neurofibrillary degeneration in the patients with mutation at codons 145, 198 and 217. The development of a transmissible spongiform encephalopathy in animals inoculated with brain tissue from affected subjects with mutation at codon 102 suggests that in some forms of genetically-determined Gerstmann-Straussler-Scheinker disease, and particularly those characterized by severe spongiosis, amyloidogenesis and production of an infectious 'agent' occur concomitantly via mechanisms that are only partially understood
PMID: 7767492
ISSN: 1015-6305
CID: 9520
Early onset Alzheimer's disease in a South American pedigree from Argentina
Mangone CA; Castano EM; Levy E; Abiusi G; Wisniewski T; Marques MR; Faccio E; Gorelick PB; Frangione B; Sica RE
We report the clinical, SPET, immunohistochemical and DNA features of an early-onset familial Alzheimer's disease (FAD) in an Argentine pedigree of South American indian ethnic background. Pedigree spans 5 generations comprising more than 110 biological relatives. Clinical data supported the diagnosis of early onset FAD (mean age at onset 38.9 years) in 10 family members, including 3 with pathological confirmation (mean age at death 48.5). The pattern of transmission suggested autosomal dominant inheritance. Prominent features were mood changes, early language impairment, myoclonus, seizures and cerebellar signs. SPET displayed bilateral frontal, temporo-parietal and cerebellar hypoperfusion in early stages and in an asymptomatic member at risk, suggesting that SPET may have predictive value in this family. Immunohistochemistry showed beta amyloid deposits within neuritic plaques and vessel walls and no anti-PrP immunoreactivity. DNA analysis showed no abnormalities in the beta amyloid precursor protein gene. The identification of additional genetic defects in well characterized independent FAD pedigrees will contribute to the understanding of the pathogenesis of Alzheimer's disease
PMID: 7732777
ISSN: 0001-6314
CID: 9521
COLLOID INCLUSIONS OF PARKINSONS-DISEASE - FURTHER IMMUNOHISTOCHEMICAL CHARACTERIZATION WITH SPECIAL REFERENCE TO LEWY BODIES [Meeting Abstract]
OGBURN, J; SAMBAMURTI, K; WISNIEWSKI, T; FRANGIONE, B; DUDLEY, A; PAPPOLLA, M
ISI:A1995QX38500151
ISSN: 0022-3069
CID: 87308
PRION PROTEIN AMYLOID ANGIOPATHY AND ALZHEIMER NEUROFIBRILLARY TANGLES IN PRNP STOP CODON-145 [Meeting Abstract]
GHETTI, B; PICCARDO, P; ICHIMIYA, Y; GOEDERT, M; KITAMOTO, T; TATEISHI, J; SPILLANTINI, MG; FRANGIONE, B; BUGIANI, O; GIACCONE, G; PRELLI, F; DLOUHY, SR; TAGLIAVINI, F
ISI:A1995QX38500032
ISSN: 0022-3069
CID: 87303
THE AMINO-TERMINAL FRAGMENT OF THE AMYLOID BETA-PEPTIDE MODULATES AMYLOID FORMATION [Meeting Abstract]
FRANGIONE, B; INESTROSA, NC; CASTANO, EM; SOTOJARA, C
ISI:A1995QT86500291
ISSN: 0730-2312
CID: 87309
Tau protein directly interacts with the amyloid beta-protein precursor: implications for Alzheimer's disease
Smith MA; Siedlak SL; Richey PL; Mulvihill P; Ghiso J; Frangione B; Tagliavini F; Giaccone G; Bugiani O; Praprotnik D; et al
The simultaneous presence of intracellular neurofibrillary tangles (NFT) and extracellular senile plaques in Alzheimer's disease (AD) suggests that the two lesions could be synergistically interrelated. However, although the main protein components of NFT and senile plaques, tau (tau) and amyloid beta-protein, respectively, are well characterized, the molecular mechanisms responsible for their deposition in lesions are unknown. We demonstrate, using four independent techniques, that tau directly interacts with a conformation-dependent domain of the amyloid beta-protein precursor (beta PP) encompassing residues beta PP714-723. The putative tau-binding domain includes beta PP717 mutation sites that are associated with familial forms of AD. Our findings strongly suggest that NFT and senile plaques, often thought of as independent structures, may play a role in each other's formation during the pathogenesis of AD
PMID: 7585068
ISSN: 1078-8956
CID: 9398
Diffuse senile plaques: amorphous or fibrous? [Comment]
Bugiani O; Tagliavini F; Giaccone G; Verga L; el-Hachimi K; Foncin JF; Frangione B
PMCID:1869186
PMID: 7887458
ISSN: 0002-9440
CID: 9517
The alpha-helical to beta-strand transition in the amino-terminal fragment of the amyloid beta-peptide modulates amyloid formation
Soto C; Castano EM; Frangione B; Inestrosa NC
Amyloid-beta peptide (A beta) consists of a hydrophobic C-terminal domain (residues 29-42) that adopts beta-strand conformation and an N-terminal domain (amino acids 10-24) whose sequence permits the existence of a dynamic equilibrium between an alpha-helix and a beta-strand. In this paper we analyzed the effect of the alternate N-terminal conformations on amyloid fibril formation through the study of the analogous A beta peptides containing single amino acidic substitutions. The single mutation of valine 18 to alanine induces a significant increment of the alpha-helical content of A beta, determined by Fourier transform infrared spectroscopy and circular dichroism and dramatically diminishes fibrillogenesis, measured by turbidity, thioflavine T binding, Congo red staining, and electron microscopic examination. In hereditary Dutch cerebral hemorrhage with amyloidosis (a variant of Alzheimer's disease), the substitution of glutamine for glutamic acid at position 22 decreased the propensity of the A beta N-terminal domain to adopt an alpha-helical structure, with a concomitant increase in amyloid formation. We propose that A beta exists in an equilibrium between two species: one 'able' and another 'unable' to form amyloid, depending on the secondary structure adopted by the N-terminal domain. Thus, manipulation of the A beta secondary structure with therapeutical compounds that promote the alpha-helical conformation may provides a tool to control the amyloid deposition observed in Alzheimer's disease patients
PMID: 7852387
ISSN: 0021-9258
CID: 9518
Amyloidosis
Ghiso, Jorge; Vidal, Ruben; Gallo, Gloria; Fragione, Blas
Amiloidose e um termo generico que descreve amplo espectro de doencas caracterizadas pela deposicao de proteinas fibrilares insoluveis em diversos orgaos. As fibrilas depositadas compoem-se predominantemente de proteinas de baixo peso molecular que sao normalmente soluveis sob condicoes fisiologicas. Todos os tipos de amiloide compartilham propriedades fisicas, estruturais e tintoriais comuns: conformacao em placa beta, alto grau de insolubilidade e aparencia fibrilar a microscopia eletronica...
ORIGINAL:0006463
ISSN: 0482-5004
CID: 90048