Your search keyword '"Han YN"' showing total 3 results

1. Flaujeac factor deficiency. Reconstitution with highly purified bovine high molecular weight-kininogen and delineation of a new permeability-enhancing peptide released by plasma kallikrein from bovine high molecular weight-kininogen.

Author

Matheson RT, Miller DR, Lacombe MJ, Han YN, Iwanaga S, Kato H, and wuepper KD

Subjects

Animals, Blood Coagulation Tests, Bradykinin pharmacology, Cattle, Chlorpheniramine pharmacology, Drug Synergism, Fibrinolysis, Kininogens blood, Molecular Weight, Blood Coagulation Disorders drug therapy, Capillary Permeability drug effects, Kallikreins blood, Kininogens administration & dosage, Peptide Fragments administration & dosage

Abstract

Flaujeac trait is the functional deficiency of a plasma protein of the intrinsic coagulation, kinin-forming, and plasma fibrinolytic pathways. The Flaujeac factor in man has been isolated and tentatively identified as a kininogen of high molecular weight (HMW). Highly purified bovine HMW-kininogen, but not bovine low molecular weight kininogen, repaired Flaujeac factor deficiency. The two subspecies of this molecule, HMW-kininogen a and HMW-kininogen b, also corrected Flaujeac factor deficiency. When bovine HMW-kininogen was incubated with bovine plasma kallikrein, kinin-free HMW-kininogen, bradykinin, and a glycopeptide fragment (peptide 1-2; 12,584 daltons) were rapidly released. None of these fragmentation products corrected Flaujeac factor deficiency alone or in mixtures. The function of HMW-kininogen appeared to depend upon the structural integrity of the native molecule. When injected in concentrations of 2 pmol-8 nmol/0.1 ml, peptide 1-2 caused increased vascular permeability in rabbits, rats, or guinea pigs. The enhanced permeability was maximal within 1-2 min and terminated in 5-10 min, differing from that of bradykinin or histamine. Injected together in equimolar amounts, peptide 1-2 and bradykinin produced a synergistic permeability response which was immediate in onset as well as prolonged in duration. Peptide 1-2 is a rapidly acting, highly basic glyco-peptide which mediates increased vascular permeability in a complementary and synergistic manner with bradykinin.

Published

1976

2. Relation between structure and correcting activity of bovine high molecular weight kininogen upon the clotting time of Fitzgerald-trait plasma.

Author

Scicli AG, Waldmann R, Guimaraes JA, Scicli G, Carretero OA, Kato H, Han YN, and Iwanaga S

Subjects

Animals, Cattle, Humans, Kallikreins pharmacology, Molecular Weight, Peptide Fragments pharmacology, Structure-Activity Relationship, Blood Coagulation drug effects, Blood Coagulation Disorders blood, Kininogens pharmacology

Abstract

Bovine high molecular weight kininogen (bHMWK) partially corrects the activated plasma thromboplastin time (aPTT) of Fitzgerald trait plasma which is congenitally deficient in HMWK. The relationship between the structure and activity of HMWK was clarified by studying the effects of different fragments of bHMWK on the aPTT of Fitzgerald-trait plasma. The peptides studied were lys-bradykinin-free HMWK, bradykinin-fragment 1-2-free HMWK, heavy chain, fragment 1-2-light chain, and light chain. All fragments were tested in equimolar concentrations. Bradykinin-fragment 1-2-free HMWK, heavy chain, and light chain have little or no correcting activity upon Fitzgerald-trait plasma aPTr. Fragment 1-2 light chain has the same correcting activity as intact bHMWK, while that of lys-bradykinin-free HMWK appears to be higher. Both fragment 1-2 and fragment 2 inhibit the clotting time of normal human plasma. When compared on a molar basis, fragment 2 is a more active inhibitor than fragment 1-2. When the effects of bovine plasma kallikrein upon bHMWK and hHMWK were studied, it was found that it released kinins from both kininogens. However, while the correcting activity of bHMWK was completely destroyed after 60 min of incubation, that of hHMWK was fully retained. These data suggest that: (a) the active part of bHMWK is comprised of the fragment 1-2 light chain portion; (b) fragment 1-2 or fragment 2 is the binding site to negatively charged surfaces, while the light chain interacts with other components of the surface-mediated reactions; and (c) bovine plasma kallikrein releases kinins, but probably does not cause the release of fragment 1-2 from human HMWK.

Published

1979

3. Effect of bovine high molecular weight kininogen and its fragments on Fitzgerald trait plasma.

Author

Waldmann R, Scicli AG, McGregor RK, Carretero OA, Abraham JP, Kato H, Han YN, and Iwanaga S

Subjects

Animals, Blood Coagulation drug effects, Cattle blood, Factor XII, Fibrinolysis drug effects, Histidine pharmacology, Humans, Prekallikrein, Thromboplastin analysis, Time Factors, Blood Coagulation Disorders blood, Kininogens pharmacology, Molecular Weight, Peptide Fragments pharmacology

Published

1976