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A NEW AND RAPID METHOD FOR EXTRACTION AND MICROSEQUENCING OF AMYLOID FROM FRESH-FROZEN AND FORMALIN-FIXED BRAINS [Meeting Abstract]

Coria, F; Prelli, F; Castano, EM; Larrondolillo, M; Fernandez, J; Shelanski, ML; Frangione, B
ISI:A1988N498700165
ISSN: 0022-3069
CID: 31476

HUMAN CEREBRAL AMYLOIDOSIS

Frangione, B
ISI:A1988R571900004
ISSN: 0272-4391
CID: 31655

PRIMARY IDIOPATHIC AMYLOIDOSIS-A - IMMUNOHISTOCHEMICAL AND BIOCHEMICAL-CHARACTERIZATION [Meeting Abstract]

PICKEN, MM; FRANGIONE, B; NEELAKANTAPPA, K; GALLO, G
ISI:A1988L610500834
ISSN: 0085-2538
CID: 41838

FIBRONECTIN IGG INTERACTION CHARACTERIZATION OF THE BINDING SITES IN FIBRONECTIN MOLECULE

ROSTAGNO A; FRANGIONE B; GOLD L I
BIOSIS:PREV198936092828
ISSN: 0021-9525
CID: 101626

[Amyloidosis of the central nervous system]

Castano EM; Ghiso JA; Frangione B
PMID: 3333077
ISSN: 0025-7680
CID: 57573

Constitutive secretion of cystatin C (gamma-trace) by monocytes and macrophages and its downregulation after stimulation

Warfel AH; Zucker-Franklin D; Frangione B; Ghiso J
Cystatin C (gamma-trace) was found to be a constitutively secreted protein of isolated human monocytes and mouse peritoneal macrophages, as well as the histiocytic lymphoma cell lines U937, P388D.1, and J774. This proteinase inhibitor is not uniquely secreted by monocytes/macrophages, but was also identified in the conditioned media from several primary cells, including brain cells, and diverse established cell lines. In vitro treatment of resident mouse peritoneal macrophages with either LPS or IFN-gamma caused a downregulation in cystatin C secretion. Elaboration of this protein was also diminished by macrophages that had been stimulated by thioglycollate in vivo, and treatment of these cells with LPS led to further decline. It is suggested that, under some inflammatory conditions, downregulation of cystatin C may contribute to tissue pathology
PMCID:2188799
PMID: 3119764
ISSN: 0022-1007
CID: 9437

Degradation and deposition of amyloid AA fibrils are tissue specific

Prelli F; Pras M; Frangione B
The complete amino acid sequences of two related AA proteins (Mr 9700 and 5300) derived from thyroid tissue from a patient, NOR, with the autosomal recessive disease familial Mediterranean fever were determined. Heterogeneity found at position 52 indicates these proteins are fragments of two allelic or isotypic SAA precursor molecules similarly degraded at unusual sites and deposited in the thyroid. Degradation appears to be tissue and/or enzyme(s) specific since the carboxy terminus of both fragments is Ala-Ala and is different from other AA amyloid fibrils extracted from various tissues in different patients. Electron micrographic studies reveal these fragments retain the characteristics of native amyloid fibrils under physiological conditions even after exposure to dissociating agents
PMID: 3442653
ISSN: 0006-2960
CID: 9583

Primary amyloidosis A. Immunohistochemical and biochemical characterization [Case Report]

Picken MM; Pelton K; Frangione B; Gallo G
Primary 'idiopathic' amyloidosis is usually related to immunoglobulin light chain (AL) associated with immunocytic dyscrasias, while secondary 'reactive' amyloidosis (AA) is related to serum amyloid A protein (SAA) and typically occurs with chronic inflammation, malignancy, or familial Mediterranean fever. In the present study, amyloid fibril protein extracted from frozen and paraffin-embedded tissue from a patient (CAR) with primary systemic amyloidosis proved to be AA protein by immunohistochemical, immunochemical, and amino terminal sequence. Extracts from both frozen and formalin-fixed paraffin-embedded kidney and spleen yielded similar monomers and dimers of the AA protein. The additional high-molecular-weight bands and a distinct 12,000-dalton fragment in the amyloid protein extracted from the formalin-fixed paraffin-embedded lung suggest that different processing of proteins, ie, by polymerization and/or degradation, may occur in different organs
PMCID:1899827
PMID: 3425691
ISSN: 0002-9440
CID: 9584

Brain amyloid in normal aging and cerebral amyloid angiopathy is antigenically related to Alzheimer's disease beta-protein

Coria F; Castano EM; Frangione B
Amyloid deposition is a prominent feature of a number of brain disorders, in which amyloid fibrils are found within blood vessel walls, the neuropil (neuritic plaques), neurons (neurofibrillary tangles). These include Alzheimer's disease (AD), AD changes associated with Down's syndrome, neurologically asymptomatic amyloidosis, Parkinson dementia of Guam, hereditary cerebral hemorrhage with amyloidosis of Icelandic origin (HCHWA-I), hereditary cerebral hemorrhage with amyloidosis of Dutch origin (HCHWA-D), and sporadic cerebral amyloid angiopathy (SCAA). Recently it was shown that the amyloid deposits in AD, Parkinson dementia of Guam, and HCHWA-D are formed by a similar 4-kd polypeptide called beta-protein. Because the nature of the amyloid deposits in other types of cerebral amyloidosis is not known, we have conducted immunocytochemical studies on brains from autopsy cases of AD, HCHWA-D, SCAA and neurologically asymptomatic elderly individuals. Brains from two subjects without neurologic involvement were used as controls. Sections from these specimens were incubated with rabbit polyclonal antibodies against 1) a synthetic peptide of 28 residues (anti-SP28), homologous to the NH2-terminal sequence of the beta-protein, 2) the main amyloid component of the HCHWA-I, a variant of cystatin C, and 3) purified fraction of neurofibrillary tangles. In all cases, anti-SP28 antibody specifically stained amyloid deposits in leptomeningeal and cortical vessels and neuritic plaques. These findings demonstrate that the amyloid deposits of SCAA and aged brains are composed of a protein antigenically similar to AD, HCHWA-D, and Parkinson dementia of Guam beta-protein, suggesting that all of these clinically and etiologically different morbid conditions are pathogenetically related. On this basis, they can be tentatively grouped as beta-protein deposition diseases. In addition, we found that HCHWA-D and SCAA vessels were mainly affected, while in AD parenchymal involvement predominates. These differences in the localization and extent of beta-protein deposits may account from the predominance of vascular complications in HCHWA-D and SCAA and of dementia in AD
PMCID:1899825
PMID: 3322021
ISSN: 0002-9440
CID: 9585

A 25-kDa NH2-terminal fragment carries all the antibacterial activities of the human neutrophil 60-kDa bactericidal/permeability-increasing protein

Ooi CE; Weiss J; Elsbach P; Frangione B; Mannion B
We have isolated, after limited proteolysis of the bactericidal/permeability-increasing protein (BPI) of human neutrophils, a 25-kDa fragment that possesses the bactericidal and envelope-altering activities of the 60-kDa parent protein. On a molar basis, the fragment is as potent as holo-human BPI against rough Escherichia coli, is more potent than holo-BPI against more resistant smooth E. coli, and retains the specificity of BPI toward Gram-negative bacteria. NH2-terminal amino acid sequence analysis shows that the fragment is derived from the NH2 terminus of the BPI molecule. These findings suggest that all of the molecular determinants of the antibacterial properties of BPI reside within the NH2-terminal 25-kDa segment, implying a novel structural/functional organization for a cytotoxic protein
PMID: 3667613
ISSN: 0021-9258
CID: 9586