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637


Characterization of renal amyloid derived from the variable region of the lambda light chain subgroup II [Case Report]

Picken MM; Gallo G; Buxbaum J; Frangione B
Amyloid fibrils were extracted from the kidney of a patient (CHE) shown to have tetramers and dimers of a monoclonal lambda light chain in his serum, and whose bone marrow cells in short-term culture synthesized these forms and a smaller lambda fragment of approximately 10,000 to 12,000 daltons. Biochemical and serologic analysis of a fraction of a size (obtained from amyloid fibrils extracted from the kidney) similar to that synthesized by the bone marrow cells revealed a light chain fragment corresponding to the amino terminal end of the variable region of the lambda light chain subgroup II. The presence of similarly sized short fragments of lambda light chain in both the synthesized and deposited protein suggests that aberrant synthesis and/or proteolytic degradation may play a pathogenetic role in the process of amyloidogenesis.
PMCID:1888179
PMID: 3089021
ISSN: 0002-9440
CID: 9600

Novel human light chain V kappa segment: serologic and structural analyses of the kappa III-like Bence Jones protein and IgG kappa light chain REE

Prelli F; Tummolo D; Solomon A; Frangione B
Immunochemical and sequence analyses of kappa light chain REE (Bence Jones protein REE and the light chain isolated from IgG kappa myeloma protein REE) revealed antigenic and structural features not previously described for human kappa-chains. Although closely related to proteins of the V kappa III subgroup, light chain REE is readily distinguished from light chains classified serologically as members of the kappa IIIa or kappa IIIb sub-subgroups. Light chains REE (Bence Jones protein REE and light chain REE) are identical in sequence and differ from kappa III proteins by at least 10 uncommon amino acid substitutions in the first three framework regions. Further, kappa-chain REE is unique by virtue of a four-residue deletion in the third complementarity-determining region. The deletion encompasses the three carboxyl-terminal residues in the V kappa-encoded segment and the first residue at the site of V-J recombination. Urine specimens from patient REE also contained a light chain fragment that lacked the first (amino-terminal) 85 residues of the native light chain but otherwise was identical in sequence to the light chain REE. The extensive amino acid differences and unique length of the V kappa segment in light chain REE indicate that this kappa-chain is the product of an unusual V kappa III gene or, alternatively, represents a rarely expressed and novel human V kappa gene.
PMID: 2422275
ISSN: 0022-1767
CID: 9601

Nucleotide sequence of the small double-stranded RNA segment of bacteriophage phi 6: novel mechanism of natural translational control

McGraw T; Mindich L; Frangione B
The lipid-containing bacteriophage phi 6 has a genome composed of three segments of double-stranded RNA. We determined the nucleotide sequence of a cDNA copy of the smallest RNA segment. The coding sequences of the four proteins on this segment were identified. These sequences were clustered. Three of the genes had overlapping initiation-termination codons. All noncoding sequences were at the ends of the molecule. The genes of the small double-stranded RNA segment comprised two translational polarity groups. We propose that the translational coupling is the result of an inability of ribosomes to bind independently to two of the four genes. Translation of these genes occurred when ribosomes were delivered to them by translation of an upstream gene.
PMCID:252886
PMID: 3754015
ISSN: 0022-538x
CID: 9602

HEREDITARY CEREBRAL ANGIOPATHY WITH AMYLOIDOSIS - AMYLOID FIBERS CONTAIN A VARIANT OF CYSTATIN-C, AN INHIBITOR OF LYSOSOMAL PROTEASE CYSTEINE [Meeting Abstract]

GHISO, J; ESTEL, BP; JENSSON, O; FRANGIONE, B
ISI:A1986E878600146
ISSN: 0025-7680
CID: 41331

FIBRONECTIN-COMPONENT-P INTERACTION OF AMYLOID TISSUE - CLASSIFICATION OF THE BONDING SITE IN THE FIBRONECTIN MOLECULE [Meeting Abstract]

ROSTAGNO, AA; FRANGIONE, B; PEARLSTEIN, E; GARCIAPARDO, A
ISI:A1986E878600147
ISSN: 0025-7680
CID: 41332

DIALYSIS-RELATED AMYLOIDOSIS - POLYMERIZATION OF BETA-2 MICROGLOBULIN IN TISSUE [Meeting Abstract]

GOREVIC, PD; MUNOZ, PC; CASEY, TT; DIRAIMONDO, CR; STONE, WJ; PRELLI, F; POULIK, MD; FRANGIONE, B
ISI:A1986C539801312
ISSN: 0009-9279
CID: 41398

ANTIGENIC AND SEQUENCE IDENTITY OF FIBRIL SUBUNIT PROTEINS IN SENILE SYSTEMIC AMYLOIDOSIS (SSA) AND ONE FORM OF FAMILIAL AMYLOIDOTIC POLYNEUROPATHY (FAP) - IMPLICATIONS FOR PATHOGENESIS [Meeting Abstract]

GOREVIC, PD; MUNOZ, PC; PRELLI, F; PRAS, M; FRANGIONE, B
ISI:A1986C539801313
ISSN: 0009-9279
CID: 41399

HEREDITARY CEREBRAL AMYLOID ANGIOPATHY - THE AMYLOID FIBRILS CONTAIN A PROTEIN WHICH IS A VARIANT OF CYSTATIN-C, AN INHIBITOR OF LYSOSOMAL CYSTEINE PROTEINASES [Meeting Abstract]

GHISO, J; JENSSON, O; FRANGIONE, B
ISI:A1986C539802249
ISSN: 0009-9279
CID: 41409

BICLONAL BENIGN IGMK GAMMOPATHY ONE-COMPONENT OF WHICH REACTS SPECIFICALLY TO THE GALACTAN OF HELIX-POMATIA [Meeting Abstract]

MERLINI, GP; BELLOTTI, V; MASTANDUNO, M; OSSERMAN, EF; LIAO, J; KABAT, EA; GONI, F; FRANGIONE, B
ISI:A1986C539802364
ISSN: 0009-9279
CID: 41410

HEREDITARY CYSTATIN C (GAMMA-TRACE) AMYLOID ANGIOPATHY OF THE CENTRAL-NERVOUS-SYSTEM CAUSING CEREBRAL-HEMORRHAGE [Meeting Abstract]

JENSSON, O; GUDMUNDSSON, G; ARNASON, A; THORSTEINSSON, L; BLONDAL, H; GRUBB, A; LOFBERG, H; FRANGIONE, B
ISI:A1986A916100016
ISSN: 0001-6314
CID: 41457