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Usage Information

Flaujeac trait. Deficiency of human plasma kininogen.
K D Wuepper, … , D R Miller, M J Lacombe
K D Wuepper, … , D R Miller, M J Lacombe
Published December 1, 1975
Citation Information: J Clin Invest. 1975;56(6):1663-1672. https://doi.org/10.1172/JCI108248.
View: Text | PDF
Research Article

Flaujeac trait. Deficiency of human plasma kininogen.

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Abstract

Flaujeac trait plasma resembled Hageman trait or Fletcher trait, in that the intrinsic coagulation pathway, plasma fibinolytic pathway, kinin-forming system, permeability factor of dilution (PF/dil) phenomenon were abnormal. The defect in each assay was reconstituted by afactor separable from Hageman factor or Fletcher factor. This substance was an alpha-globulin with an approximate mol wt of 170,000. Flaujeac plasma did not release a kinin upon incubation with kallikrein and was deficient in total kininogen antigen. Antiserum to kininogen inhibited the activity of the factor in solution. Flaufeac factor was identified as a kininogen of high molecular weight (HMW-kininogen). The mean total kininogen antigen in four children of the proposita was 51% (range 34-62%) of normal. A functional coagulation assay of HMW-kininogen in the children was 34% (range 23-55%). The results were consistent with autosomal recessive inheritance. The plasma pathways of intrinsic coagulation, fibrinolysis, kinin formation, and PF/dil generation are dependent upon HMW-kininogen. We believe this is the first demonstration of biological function for a kininogen apart from its role as a substrate for kallikreins.

Authors

K D Wuepper, D R Miller, M J Lacombe

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Usage data is cumulative from July 2024 through July 2025.

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