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637


Inhibition of Alzheimer's amyloidosis by peptides that prevent beta-sheet conformation

Soto C; Kindy MS; Baumann M; Frangione B
Amyloid beta-peptide (A beta) is a major fibrillar component of neuritic plaques in Alzheimer's disease (AD) brains and is related to the pathogenesis of the disease. We hypothesized that amyloid formation could be inhibited by peptides homologous to A beta (position 17-21) with a similar degree of hydrophobicity, but with a very low propensity to adopt a beta-sheet conformation by incorporating proline residues (anti-beta-sheet peptides or beta-sheet inhibitors). An 11-residue peptide with these characteristics binds to A beta, inhibits A beta fibril formation and partially disaggregates preformed fibrils in vitro. Shorter anti-beta-sheet peptides and analogs containing D-amino acids are also able to inhibit A beta fibrillogenesis. The latter are more resistant to proteolytic degradation and may serve as a starting point to design more efficient peptides derivatives to inhibit amyloidogenesis in vivo
PMID: 8831674
ISSN: 0006-291x
CID: 7092

Apolipoprotein E, TTR and Alzheimer's disease - General discussion .3 [Editorial]

Pepys; Frangione; Goldgaber; Kelly; Arvinte; Masters; Benson; Saraiva; Sipe; Costa
ISI:A1996BG31D00014
ISSN: 0300-5208
CID: 52801

Proteinase K (PK) resistant prion protein (PrP) isoforms in Gerstmann-Straussler-Scheinker disease (GSS) F198S [Meeting Abstract]

Piccardo, P; Seiler, C; Dlouhy, S; Young, K; Farlow, M; Prelli, F; Frangione, B; Bugiani, O; Tagliavini, F; Ghetti, B
ISI:A1996UK93300137
ISSN: 0022-3069
CID: 52925

Meningocerebrovascular amyloidosis associated with a novel transthyretin mis-sense mutation at codon 18 (TTRD 18G) [see comments] [Comment]

Vidal R; Garzuly F; Budka H; Lalowski M; Linke RP; Brittig F; Frangione B; Wisniewski T
We describe a novel transthyretin mutation at codon 18 where Asp is replaced by Gly (D18G) in a Hungarian kindred. This mutation is associated with meningocerebrovascular amyloidosis, producing dementia, ataxia, and spasticity. Fifty different transthyretin mutations are related to amyloid deposition, typically producing a peripheral neuropathy or cardiac dysfunction. These symptoms are absent in this family. Up to now, amyloid-beta (A beta), cystatin C, and prion proteins have been known to be deposited as amyloid in the brain, leading to stroke or dementia. With this report we establish that transthyretin amyloid deposition can also produce central nervous system dysfunction as the major clinical symptom
PMCID:1861701
PMID: 8579098
ISSN: 0002-9440
CID: 6970

HB-GAM is a cytokine present in Alzheimer's and Down's syndrome lesions

Wisniewski T; Lalowski M; Baumann M; Rauvala H; Raulo E; Nolo R; Frangione B
The distribution of heparin binding growth associated molecule (HB-GAM) in the cerebral amyloidoses of Alzheimer's disease (AD) and Down's syndrome (DS), conditions characterized by the deposition of amyloid beta (A beta), was investigated immunohistochemically. Antibodies to HB-GAM, a cytokine which plays an important role in brain development and maturation, showed strong immunoreactivity with senile plaques in both AD and DS. Anti-HB-GAM reacted with pre-amyloid lesions, but only when markers of dystrophic neurites were present. The presence of HB-GAM in AD brains, but not in control brains, was confirmed by Western blotting. We suggest that the presence of HB-GAM in A beta lesions is a marker of neuronal injury
PMID: 8730853
ISSN: 0959-4965
CID: 6974

Prion protein hereditary amyloidosis: Parenchymal and vascular

Ghetti, B; Piccardo, P; Frangione, B; Bugiani, O; Giaccone, G; Young, K; Prelli, F; Farlow, MR; Dlouhy, SR; Tagliavini, F
Prion protein (PrP) amyloidosis is a feature of Gerstmann-Straussler-Scheinker disease (GSS) and prion protein cerebral amyloid angiopathy (PrP-CAA). GSS and PrP-CAA are associated with point mutations of the prion protein gene (PRNP); there is a broad spectrum of clinical presentations and the main signs are ataxia, spastic paraparesis, extrapyramidal signs and dementia. In GSS, parenchymal amyloid may be associated with spongiform changes or neurofibrillary lesions; in PrP-CAA, vascular amyloid is associated with neurofibrillary lesions. In the two diseases, a major component of the amyloid fibrils is a 7 kDa peptide, approximately spanning residues 81-150 of PrP
ISI:A1996UQ75600005
ISSN: 1044-5773
CID: 52879

Fate of cerebrospinal fluid-borne amyloid beta-peptide: rapid clearance into blood and appreciable accumulation by cerebral arteries

Ghersi-Egea JF; Gorevic PD; Ghiso J; Frangione B; Patlak CS; Fenstermacher JD
In Alzheimer's disease, the neuritic or senile amyloid plaques in hippocampus and association cortex, the diffuse plaques in brain areas such as the cerebellum and sensorimotor cortex, and the amyloid deposits in the walls of pial and parenchymal blood vessels are mainly composed of amyloid beta-peptides. In the present study, either soluble 40-residue amyloid beta-peptide radiolabeled with 125I (I-sAbeta) or [14C]polyethylene glycol ([14C]PEG, a reference material) was briefly infused into one lateral ventricle of normal rats. By 3.5 min, 30% of the I-sAbeta was cleared from ventricular CSF into blood; another 30% was removed over the next 6.5 min. No [14C]PEG was lost from the CSF-brain system during the first 5 min, and only 20% was cleared by 10 min. Much of the I-sAbeta that reached the subarachnoid space was retained by pial arteries and arterioles. Virtually no I-sAbeta was found in brain. The clearance of amyloid beta-peptides from the CSF-brain system, reported herein for normal rats, may be reduced in Alzheimer's disease, thus contributing to amyloid deposition in cerebral tissue and blood vessels
PMID: 8764620
ISSN: 0022-3042
CID: 9392

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

Non-Alzheimer's disease amyloidoses of the nervous system

Castano EM; Frangione B
Amyloidosis and prionosis are disorders of protein conformation. The general mechanisms involved in amyloidogenesis are reviewed here. Recent progress in the molecular pathogenesis of cerebral amyloids is illustrated by three genetic disorders: hereditary amyloid angiopathies of Icelandic and Dutch origins and Gerstmann-Straussler-Scheinker disease
PMID: 7582043
ISSN: 1350-7540
CID: 9515

Hereditary cerebral haemorrhage with amyloidosis, Dutch type (HCHWA-D): clinicopathological studies

Wattendorff AR; Frangione B; Luyendijk W; Bots GT
Clinical and neuropathological findings are reported in 63 patients with hereditary cerebral haemorrhage with amyloid angiopathy. Patients had mostly recurrent strokes, and at least 80% of these were haemorrhages. Almost a third of the patients died within a year of their first and only recorded haemorrhage, half of them within two weeks. This angiopathy was restricted to the cerebral and cerebellar cortex and its covering leptomeninges. As the most important consequence, haemorrhagic infarcts and haemorrhages occurred in the subcortical white matter--that is, the region most vulnerable to impaired cortical circulation. Further development of these subcortical lesions gives rise to the fatal haemorrhages seen at necropsy. In so far as dementia occurs this is likely to result from multiple microinfarcts or haemorrhages. In most cases preamyloid lesions or diffuse plaques and early plaques were seen. No other type of plaque or neurofibrillary degeneration was found. The plaques occur in conjunction with the angiopathy, but may not occur even when the angiopathy is severe. In one patient plaques were totally absent. Angiopathy and plaques may be the result of the same mutation, the expression of which is governed by tissue factors or phenotypic differences between individual subjects
PMCID:1073548
PMID: 7608669
ISSN: 0022-3050
CID: 9516