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Alzheimer's disease and amyloid
Chapter by: Frangione B; Wisniewski T; Ghiso J
in: Amyloid and amyloidosis 1993 by Kisilevsky R [Eds]
New York : Parthenon, 1993
pp. 310-315
ISBN: 1850705798
CID: 5144
Epitope map of two polyclonal antibodies that recognize amyloid lesions in patients with Alzheimer's disease
Ghiso J; Wisniewski T; Vidal R; Rostagno A; Frangione B
ORIGINAL:0006630
ISSN: 0923-7372
CID: 101632
Characterization and fibrillogenesis of a construct (C109) homologus to the carboxyl end of the amyloid precusor protein of Alzheimer's disease
Chapter by: Gardella JE; Gorgone G; Ghiso J; Castano E; Frangione B; Gorevic PD
in: Alzheimer's disease : advances in clinical and basic research by Corain B [Eds]
New York : Wiley, 1993
pp. 411-420
ISBN: 0471938408
CID: 5143
The cerebrospinal-fluid soluble form of Alzheimer's amyloid beta is complexed to SP-40,40 (apolipoprotein J), an inhibitor of the complement membrane-attack complex
Ghiso J; Matsubara E; Koudinov A; Choi-Miura NH; Tomita M; Wisniewski T; Frangione B
The amyloid fibrils deposited in Alzheimer's neuritic plaque cores and cerebral blood vessels are mainly composed of aggregated forms of a unique peptide, 39-42 amino acids long, named amyloid beta (A beta). A similar, although soluble, A beta ('sA beta') has been identified in cerebrospinal fluid, plasma and cell supernatants, indicating that it is normally produced by proteolytic processing of its precursor protein, amyloid precursor protein (APP). Using direct binding experiments we have isolated and characterized an 80 kDa circulating protein that specifically interacts with a synthetic peptide identical with A beta. The protein was unmistakably identified as SP-40,40 or ApoJ, a cytolytic inhibitor and lipid carrier, by means of amino acid sequence and immunoreactivity with specific antibodies. Immunoprecipitation with anti-SP-40,40 retrieved soluble A beta from cerebrospinal fluid, indicating that the interaction occurs in vivo
PMCID:1134315
PMID: 8328966
ISSN: 0264-6021
CID: 8397
Alzheimer's disease and Dutch variant: Opposing faces of a single coin
Chapter by: Frangione, Blas; Wisniewski, Thomas; Tagliavini, Fabrizio; Bugiani, Orso; Ghiso, Jorge
in: Alzheimer's disease : advances in clinical and basic research by Corain B [Eds]
New York : Wiley, 1993
pp. 387-396
ISBN: 0471938408
CID: 4969
Beta PP participates in PrP-amyloid plaques of Gerstmann-Straussler-Scheinker disease, Indiana kindred
Bugiani O; Giaccone G; Verga L; Pollo B; Frangione B; Farlow MR; Tagliavini F; Ghetti B
Gerstmann-Straussler-Scheinker disease in the Indiana kindred is pathologically characterized by deposits of PrP-amyloid, neurofibrillary tangles and degenerating neurites. The aim of this study was to investigate seven patients of different ages for beta PP and A beta immunoreactivities associated with PrP-amyloid deposits and degenerating neurites. In one asymptomatic individual with PrP-amyloid deposits, Alz50 and A beta immunoreactivities were absent. In six symptomatic patients, the degenerating neurites surrounding PrP-amyloid deposits were labeled by Alz50 and by antibodies to synaptophysin, ubiquitin and the N- and C-terminal domains of beta PP. In one symptomatic, senile patient, A beta immunoreactivity was present in the extracellular space, often in association with PrP-amyloid deposits. The analysis of the immunohistochemical findings suggested that in the Indiana kindred the intracellular accumulation of beta PP, synaptophysin and ubiquitinated material most probably revealed a reaction of neurites to PrP-amyloid, whereas the extracellular deposition of A beta was likely an age-related phenomenon
PMID: 8093899
ISSN: 0022-3069
CID: 9531
Gelsolin immunoreactivity in corneal amyloid, wound healing, and macular and granular dystrophies
Rodrigues MM; Rajagopalan S; Jones K; Nirankari V; Wisniewski T; Frangione B; Gorevic PD
Immunohistologic studies of tissue sections obtained from patients with type 1 or type 2 lattice corneal dystrophy, polymorphic amyloid degeneration, or gelatinous amyloid degeneration were performed by using a monoclonal antibody raised to a chymotryptic fragment inclusive of the carboxy-terminal half of plasma gelsolin, and also with a series of polyclonal antibodies specific for synthetic peptides corresponding to immunogenic epitopes of gelsolin. These epitopes are parts of sequences at the amino- and carboxy-terminal ends of gelsolin, as well as adjacent to and inclusive of the codon 187 mutant 7-11 kD fragment that has been shown to be the subunit protein of amyloid fibrils occurring systemically in patients affected by Finnish type familial amyloidosis. These antibodies were also tested on tissue sections obtained from patients with granular and macular corneal dystrophy, corneal wounds, and normal control corneas. Specificity of staining was established by absorption with gelsolin purified from plasma, or the appropriate synthetic peptide. Gelsolin immunoreactivity was detected in the conjunctival and skin amyloid in familial amyloidosis by using familial amyloid (Finnish type) antibody. In other types of corneal amyloid, including lattice dystrophy type 1, immunoreactivity with gelsolin and synthetic peptides was observed adjacent to the deposits, but rarely within them. In macular dystrophy, variable staining of the deposits could result from the association of subunit proteins with glycosaminoglycans
PMID: 7683843
ISSN: 0002-9394
CID: 9528
ALZHEIMERS AMYLOID BETA-SUBUNIT IS PRESENT IN PREAMYLOID DEPOSITS AND IN CSF [Meeting Abstract]
WISNIEWSKI, T; WEGIEL, J; WISNIEWSKI, HM; FRANGIONE, B
ISI:A1993KY35601007
ISSN: 0028-3878
CID: 97629
Ubiquitinated neurites are associated with preamyloid and cerebral amyloid beta deposits in patients with hereditary cerebral hemorrhage with amyloidosis Dutch type
Tagliavini F; Giaccone G; Bugiani O; Frangione B
Hereditary cerebral hemorrhage with amyloidosis Dutch type (HCHWA-D) is characterized clinically by recurrent strokes and pathologically by deposition of amyloid beta (A beta) in cerebral vessel walls and, to a lesser extent, in the neuropil. Distinct from Alzheimer's disease, amyloid formation in HCHWA-D is not associated with neurofibrillary changes. Since a central issue in the pathophysiology of Alzheimer's disease and related conditions is the role of A beta in the neurodegenerative process, we investigated HCHWA-D brains for the presence of neuritic abnormalities using antibodies to ubiquitin and to phosphorylated neurofilaments. The study showed that amyloid deposits in the vessel walls and in the neuropil were surrounded by abnormal ubiquitinated neurites, suggesting that A beta deposition induces neuritic changes
PMID: 8384771
ISSN: 0001-6322
CID: 9529
Sequencing of the Alzheimer's APP gene Dutch variant (APP-D) [Letter]
Vidal RG; Fernandez-Madrid I; Frangione B; Levy E
PMID: 8111419
ISSN: 1059-7794
CID: 9530