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Biochemical studies on the interaction of fibronectin with Ig
Rostagno AA; Frangione B; Gold L
We have previously biochemically characterized three separate sites on the fibronectin (Fn) molecule that interact with IgG. These studies have been extended to examine the interaction of Fn with other classes and subclasses of Ig. By ELISA, a preferential quantitative binding order of Fn to the major Ig classes and subclasses was obtained as follows: IgG greater than IgM greater than IgA, IgG1 greater than IgG3 = IgG4 greater than IgG2, and IgA1 = IgA2. Using fragments of Fn obtained by subtilisin digestion followed by IgM and IgA affinity chromatography, immunoblot analysis using monospecific antisera to separate regions of the Fn molecule, and amino acid sequence analysis, these studies indicate that polyclonal IgA and IgM interact with Fn in the same three regions and under the same ionic conditions as previously described for IgG. Site 1 is a 22-kDa fragment that commences at residue 1 of the Fn molecule. Sites 2 (16 kDa) and 3 (26-29 kDa) begin at residues 588 and 1597, respectively. Under physiological conditions a monoclonal antibody that recognizes site 1 completely inhibited the interaction of intact Fn with IgG, IgM, and IgA. Therefore, this is the only physiologically active site in the intact molecule. Aggregated but not monomeric IgG competitively inhibited the binding of Fn to IgG-coated microtiter ELISA plates; thus, this interaction can take place in a fluid-phase system. These results indicate that Fn can potentially interact with immune complexes and aggregates of all Ig in the circulation and thus may play a significant role in both their clearance and deposition in Fn-containing tissues, such as occurs in immune-complex-related disorders
PMID: 2016522
ISSN: 0022-1767
CID: 9547
Mixed cryoglobulinemia cross-reactive idiotypes: implications for the relationship of MC to rheumatic and lymphoproliferative diseases
Gorevic PD; Frangione B
PMID: 1876865
ISSN: 0037-1963
CID: 9548
Regulation and genetic control of brain amyloid. FESN Study Group
Gajdusek DC; Beyreuther K; Brown P; Cork LC; Cunningham DD; Frangione B; Gibbs CJ Jr; Goldfarb LG; Goldgaber D; Hsiao KK
PMID: 1677826
ISSN: 0165-0173
CID: 9549
NATURAL-HISTORY OF GERSTMANN-STRAUSSLER-SCHEINKER DISEASE (GSS) IN THE INDIANA KINDRED (IK) [Meeting Abstract]
GHETTI, B; FARLOW, MR; FRANGIONE, B; GIACCONE, G; TAGLIAVINI, F; BUGIANI, O
ISI:A1991FK14000094
ISSN: 0022-3069
CID: 51595
THE PLATELET - A POTENTIAL SOURCE OF AMYLOID PROTEIN IN ALZHEIMERS-DISEASE [Meeting Abstract]
GOREVIC, PD; GARDELLA, JE; NEWMAN, PJ; FRANGIONE, B
ISI:A1991FH32300343
ISSN: 0009-9279
CID: 51606
LATTICE CORNEAL-DYSTROPHY (LCD) TYPE-II - GELSOLIN GENE MUTATION CODON 187 DEMONSTRATED IN AN AMERICAN FAMILY BY PCR AMPLIFICATION AND DNA SEQUENCING [Meeting Abstract]
GOREVIO, PD; MUNOZ, PC; GORGONE, G; PURCELL, F; RODRIGUES, M; LEVY, E; FRANGIONE, B
ISI:A1991FH32300732
ISSN: 0009-9279
CID: 51610
IMMUNOHISTOCHEMICAL COMPARISON OF EXPERIMENTAL AMYLOIDOSIS IN CLASSICAL, CASEIN-INDUCED, AND ACCELERATED, AMYLOID-ENHANCING-FACTOR-(AEF)-INDUCED, MURINE MODELS [Meeting Abstract]
PICKEN, MM; FRANGIONE, B; GALLO, GR
ISI:A1991EV36600638
ISSN: 0023-6837
CID: 51740
Familial amyloidosis - Finish type - and its relationship to Lewy bodies in Parkinson's and Diffuse Lewy Body disease
Chapter by: Frangione B; Haltia M; Levy E; Ghiso J; Kiuru S; Prelli F; Wisniewski T
in: Proceedings of the XIth International Congress of Neuropathology, September 2-8, 1990, Kyoto, Japan by
[Tokyo] : Japanese Society of Neuropathology, 1991
pp. 150-156
ISBN: n/a
CID: 4980
LEWY BODIES ARE IMMUNOREACTIVE WITH ANTIBODIES RAISED TO GELSOLIN AMYLOID
WISNIEWSKI T; HALTIA M; GHISO J; FRANGIONE B
BIOSIS:PREV199141031748
ISSN: 0028-3878
CID: 97655
ALZHEIMER'S AMYLOID PRECURSOR PROTEIN CONTAINS A TETRAPEPTIDE SEQUENCE-RHIDS THAT PROMOTES CELL ADHESION [Meeting Abstract]
GHISO J; ROSTAGNO A; FRANGIONE B
BIOSIS:PREV199242104041
ISSN: 0190-5295
CID: 101623