Subscribe to RSS
DOI: 10.1055/s-0037-1614849
Parallel Reduction of Plasma Levels of High and Low Molecular Weight Kininogen in Patients with Cirrhosis
Publication History
Received
31 March 1999
Accepted after resubmission
22 July 1999
Publication Date:
09 December 2017 (online)
Summary
Little is known about the regulation of high-molecular-weight-kininogen (HK) and low-molecular-weight-kininogen (LK) or the relationship of each to the degree of liver function impairment in patients with cirrhosis. In this study, we evaluated HK and LK quantitatively by a recently described particle concentration fluorescence immunoassay (PCFIA) and qualitatively by SDS PAGE and immunoblotting analyses in plasma from 33 patients with cirrhosis presenting various degrees of impairment of liver function. Thirty-three healthy subjects served as normal controls. Patients with cirrhosis had significantly lower plasma levels of HK (median 49 μg/ml [range 22-99 μg/ml]) and LK (58 μg/ml [15-100 μg/ml]) than normal subjects (HK 83 μg/ml [65-115 μg/ml]; LK 80 μg/ml [45-120 μg/ml]) (p < 0.0001). The plasma concentrations of HK and LK were directly related to plasma levels of cholinesterase (P < 0.0001) and albumin (P < 0.0001 and P < 0.001) and inversely to the Child-Pugh score (P < 0.0001) and to prothrombin time ratio (P < 0.0001) (reflecting the clinical and laboratory abnormalities in liver disease). Similar to normal individuals, in patients with cirrhosis, plasma HK and LK levels paralleled one another, suggesting that a coordinate regulation of those proteins persists in liver disease. SDS PAGE and immunoblotting analyses of kininogens in cirrhotic plasma showed a pattern similar to that observed in normal controls for LK (a single band at 66 kDa) with some lower molecular weight forms noted in cirrhotic plasma. A slight increase of cleavage of HK (a major band at 130 kDa and a faint but increased band at 107 kDa) was evident. The increased cleavage of HK was confirmed by the lower cleaved kininogen index (CKI), as compared to normal controls. These data suggest a defect in hepatic synthesis as well as increased destructive cleavage of both kininogens in plasma from patients with cirrhosis. The decrease of important regulatory proteins like kininogens may contribute to the imbalance in coagulation and fibrinolytic systems, which frequently occurs in cirrhotic patients.
-
References
- 1 Jacobsen S, Kriz M. Some data on two purified kininogens from human plasma. Br J Pharmacol Chemother 1967; 29: 25-36.
- 2 Bhoola KD, Figueroa CD, Worthy K. Bioregulation of kinins: kallikrein, kininogen, and kininases. Pharmacol Rev 1992; 44: 1-80.
- 3 Jacobsen S. Separation of two different substrates for plasma kinin-forming enzymes. Nature 1966; 210: 98-9.
- 4 Scott CF, Silver LD, Schapira M, Colman RW. Cleavage of human high molecular weight kininogen markedly enhances its coagulant activity. Evidence that this molecule exists as a procofactor. J Clin Invest 1984; 73: 954-62.
- 5 Scott CF, Colman RW. Function and immunochemistry of prekallikrein-high molecular weight kininogen complex in plasma. J Clin Invest 1980; 65: 413-21.
- 6 Lin Y, Harris RB, Yan W, McCrae KR, Zhong H, Colman RW. High molecular weight kininogen peptides inhibit the formation of kallikrein on endothelial cell surfaces and subsequent urokinase-dependent plasmin formation. Blood 1997; 90: 690-7.
- 7 Asakura S, Hurley RW, Skorstengaard K, Ohkubo I, Mosher DF. Inhibition of cell adhesion by high molecular weight kininogen. J Cell Biol 1992; 116: 465-76.
- 8 Müller-Esterl W, Fritz H, Machleidt W, Ritonja A, Brzin J, Kotnik M, Turk V, Kellermann J, Lottspeich F. Human plasma kininogens are identical with α2-cysteine proteinase inhibitors. Evidence from immunological, enzymological and sequence data. FEBS Lett 1985; 182: 310-4.
- 9 Puri RN, Zhou F, Hu CJ, Colman RF, Colman RW. High molecular weight kininogen inhibits thrombin-induced platelet aggregation and cleavage of aggregin by inhibiting binding of thrombin to platelets. Blood 1991; 77: 500-7.
- 10 Bradford HN, DeLa Cadena RA, Kunapuli SP, Dong JF, Lopez JA, Colman RW. Human Kininogens regulate thrombin binding to platelets through the glycoprotein Ib-IX-V complex. Blood 1997; 90: 1508-15.
- 11 Kitamura N, Kitagawa H, Fukushima D, Takagaki Y, Miyata T, Nakanishi S. Structure organization of the kininogen gene and a model for its evolution. J Biol Chem 1985; 260: 8610-7.
- 12 Lottspeich F, Kellermann A, Henschen A, Rauth G, Müller-Esterl W. Human low molecular mass kininogen. Amino acid sequence of the light chain; homology with other protein sequences. Eur J Biochem 1984; 142: 227-32.
- 13 Gerok W, Gross V. Secretory proteins; synthesis, secretion, and function. In: Oxford Textbook of Clinical Hepatology. McIntyre N, Benhamou JP, Bircher J, Rizzetto M, Rodes J. Eds. Oxford Medical Publications; 1991: 174-98.
- 14 Cordova C, Violi F, Alessandri C, Ferro D, Saliola M, Balsano F. Hageman factor, high molecular weight kininogen, and prekallikrein in chronic liver disease. J Clin Pathol 1986; 39: 1003-5.
- 15 Saito H. Contact factors in health and disease. Sem Thromb Hemost 1987; 13: 36-49.
- 16 Scott CF, Shull B, Müller-Esterl W, Colman RW. Rapid direct determination of low and high molecular weight kininogen in human plasma by particle concentration fluorescence immunoassay (PCFIA). Thromb Haemost 1997; 77: 109-18.
- 17 Berrettini M, Lämmle B, White T, Curd J, Griffin JH. Detection of the in vivo cleavage of high molecular weight kininogen in human plasma by immunoblotting with monoclonal antibodies. Blood 1986; 68: 455-62.
- 18 Pugh RNH, Murray-Lyon IM, Dawson JL, Pietroni MC, Williams R. Transection of the oesophagus for bleeding oesophageal varices. Br J Surg 1973; 60: 646-9.
- 19 Kaufmann J, Haasemann M, Modrow S, Müller-Esterl W. Structural dissection of the multi-domain kininogens. Fine mapping of target epitopes of antibodies interfering with their functional properties. J Biol Chem 1993; 268: 9079-91.
- 20 Pincus MR, Zimmerman HJ, Henry JB. Clinical enzymology. In: Clinical diagnosis and management by laboratory methods. Henry JB. ed. Philadelphia: WB Saunders Company; 1991: 250-84.
- 21 Jaffe EH, Hoyer LW, Nachman RL. Synthesis of von Willebrand Factor by cultured endothelial cells. Proc Natl Acad Sci 1973; 71: 1906-11.
- 22 Maisonneuve P, Sultan Y. Modification of Factor VIII complex properties in patients with liver disease. J Clin Pathol 1977; 30: 221-7.
- 23 Pixley RA, Zellis S, Bankes P, DeLa Cadena RA, Page JD, Scott CF, Kappelmayer J, Wyshock EG, Kelly JJ, Colman RW. Prognostic value of assessing contact system activation and factor V in systemic inflammatory response syndrome. Crit Care Med 1995; 23: 41-51.
- 24 DeLa Cadena R, Suffredini AF, Page JD. Activation of the kallikrein-kinin system after endotoxin administration to normal human volunteers. Blood 1993; 8: 3313-7.
- 25 Lumsden AB, Henderson JM, Kutner MH. Endotoxin levels measured by chromogenic assay in portal, hepatic and peripheral venous blood in patients with cirrhosis. Hepatology 1988; 8: 232-6.
- 26 Kleniewski J, Blankenship DT, Cardin AD, Donaldson VH. Mechanism of enhanced kinin release from high molecular weight kininogen by plasma kallikrein after its exposure to plasmin. J Lab Clin Med 1992; 120: 129-39.
- 27 Agostoni A, Gardinali M, Frangi D, Cafaro C, Conciato L, Sponzilli C, Salvioni A, Cugno M, Cicardi M. Activation of complement and kinin systems after thrombolytic therapy in patients with acute myocardial infarction. A comparison between streptokinase and recombinant tissue-type plasminogen activator. Circulation 1994; 90: 2666-70.
- 28 Cugno M, Salerno F, Mandelli M, Lorenzano E, Paonessa R, Agostoni A. Cleavage of high molecular weight kininogen in ascites and plasma of patients with cirrhosis. Thromb Res 1995; 78: 277-82.
- 29 Cumming AD, Nimmo GR, Craig KJ, McGilchrist A, Hayes PC. Vasoactive effects of aprotinin. Agents actions suppl 1992; 38: 211-8.
- 30 Loureiro-Silva MR, Molina HM, Borges DR. The portal hypertensive response to bradykinin is mediated by the B2-type receptor and modulated by nitric oxide. Int Hepatol Commun 1995; 4: 175-80.
- 31 Wirth KJ, Bickel M, Hropot M, Günzler V, Heitsch H, Ruppert D, Schölkens BA. The bradykinin B2 receptor antagonist Icatibant (HOE 140) corrects avid Na+ retention in rats with CCl4-induced liver cirrhosis: possible role of enhanced microvascular leakage. Eur J Pharmacol 1997; 337: 45-53.