Independent modulation of von Willebrand factor and fibrinogen binding to the platelet membrane glycoprotein IIb/IIIa complex as demonstrated by monoclonal antibody.

Lombardo, Vincenzo; Hodson, Elisabeth M; Roberts, James R.; Kunicki, Thomas J.; Zimmerman, Theodore S.; Ruggeri, Zaverio M.

doi:10.1172/jci112193

Cited by 103 publications

(37 citation statements)

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“…The inhibition by these peptides also suggests that these adhesive proteins share a common binding site on the activated I1 bIIIa complex. However, data mentioned in this study and those recently reported by Trapani Lombardo et al [47] show that monoclonal antibodies can specifically inhibit fibronectin or vWf binding to stimulated platelets without affecting fibrinogen binding or platelet aggregation. Plow et al 1451 have recently suggested that high-affinity interactions of any of these four adhesive proteins with platelets may call for common as well as unique binding sites.…”

supporting

confidence: 55%

Identification of two distinct regions within the binding sites for fibrinogen and fibronectin on the IIb–IIIa human platelet membrane glycoprotein complex by monoclonal antibodies P2 and P4

McGregor

Bauer

et al. 1986

European Journal of Biochemistry

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The effect of two monoclonal antibodies P2 (LyP 2) or P4 (LyP 4), specific for the platelet membrane glycoprotein I1 bj1Il a complex, on binding of '251-labelled fibrinogen or '251-labelled fibronectin to thrombinstimulated platelets was studied. These monoclonal antibodies are directed against different determinants on the I1 b-IIIa complex and react only with the complex and not with the individual glycoproteins. Fibrinogen binding to thrombin-stimulated platelets was significantly inhibited by P2 but not by P4. Fibronectin binding to thrombinstimulated platelets was significantly inhibited by P4 but only poorly by P2. These results indicate the presence of specific regions on the glycoprotein I1 b-I11 a complex which act as binding sites for fibrinogen or fibronectin. glycoprotein IIb or IIIa had no effect on platelet functionsRecently a number of monoclonal antibodies have been used to investigate the role of glycoproteins IIb and IIIa in platelet function [S]. Monoclonal antibodies, directed against glycoproteins I1 b and/or Ill a, inhibit platelet aggregation and binding of '251-labelled fibrinogen either completely, partially or have no effect [9-171. The degree of inhibition caused by these monoclonal antibodies appears to be linked to the position of their determinants in relation to the fibrinogenbinding site in the Ilb-IIIa complex 19-171. Recent reports suggest that the I1 b-111 a complex contains receptor sites not only for fibrinogen but also for fibronectin, thrombospondin and von Willebrand factor (vWf) [18-211. Very little is known about the regions of the 11 b-IIIa complex that serve as binding sites for these four adhesive proteins (fibrinogen, fibronectin, thrombospondin and vWf). A tetrapeptide, Arg-Gly-Asp-Ser (RGDS), was shown to inhibit the binding of three of these proteins to stimulated platelets [22, 231. It was, therefore. suggested that fibrinogen, fibronectin and vWf interact with a common site on thrombinactivated platelets. To test this hypothesis this study has examined the binding of 1251-labelled fibrinogen or '251-labelled fibronectin to thrombin-stimulated platelets in the presence or absence ofmonoclonal antibodies P2 (LyP 2) or P4 (LyP 4). These monoclonal antibodies are directed against different [71.

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supporting

confidence: 55%

Identification of two distinct regions within the binding sites for fibrinogen and fibronectin on the IIb–IIIa human platelet membrane glycoprotein complex by monoclonal antibodies P2 and P4

McGregor

Bauer

et al. 1986

European Journal of Biochemistry

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“…Accordingly, this antibody inhibited 1251I-vWF binding to normal or afibrinogenemic platelets stimulated by ADP plus adrenaline (Table I). In previous studies we have shown that antibody UPS has no effect on the binding of fibrinogen to GPIIb/IIIa (see reference 24 for full details). Moreover, antibody UP5 has no effect on the aggregation of normal platelet-rich plasma (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…belong to three different kindreds and have been previously described in detail (19-2 1 Monoclonal antibody. The anti-GPIIb/IIIa monoclonal antibody UP5 has been recently described in detail (24). It blocks vWF binding to stimulated platelets without affecting fibrinogen binding.…”

Section: Methodsmentioning

confidence: 99%

“…It blocks vWF binding to stimulated platelets without affecting fibrinogen binding. Monovalent Fab fragment of this antibody was prepared as described (24). It was stored in 0.02 M Tris * HCI-0.…”

Section: Methodsmentioning

confidence: 99%

“…The method for preparation ofwashed platelet suspensions using the albumin density gradient technique has also been reported (24,27).…”

Section: Methodsmentioning

confidence: 99%

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von Willebrand factor interaction with the glycoprotein IIb/IIa complex. Its role in platelet function as demonstrated in patients with congenital afibrinogenemia.

Marco¹,

Girolami²,

Zimmerman³

et al. 1986

J. Clin. Invest.

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173

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We have studied three afibrinogenemic patients, who had only trace amounts of plasma and platelet fibrinogen as measured by radioimmunoassay, and demonstrate here that the residual aggregation observed in their platelet-rich plasma is dependent upon von Willebrand factor (vWF) binding to the platelet membrane glycoprotein (GP)IIb/IIIa complex. The abnormality of aggregation was more pronounced when ADP, rather than thrombin, collagen, or the combination of ADP plus adrenaline was used to stimulate platelets. With all stimuli, nevertheless, the platelet response was completely inhibited by a monoclonal antibody (LJP5) that is known to block vWF, but not fibrinogen binding to GPIIb/IIIa. Addition of purified vWF to the afibrinogenemic plasma resulted in marked increase in the rate and extent ofaggregation, particularly when platelets were stimulated with ADP. This response was also completely blocked by LJP5.Addition of fibrinogen, however, restored normal aggregation even in the presence of IPS, a finding consistent with the knowledge that antibody LJP5 has no effect on platelet aggregation mediated by fibrinogen binding to GPIIb/IIIa. Two patients gave their informed consent to receiving infusion of 1-desamino--D-arginine vasopressin (DDAVP), a vasopressin analogue known to raise the vWF levels in plasma by two-to fourfold. The bleeding time, measured before and 45 min after infusion, shortened from >24 min to 12 min and 50 s in one patient and from 16 min to 9 min and 30 s in the other. Concurrently, the rate and extent of ADP-induced platelet aggregation improved after DDAVP infusion. The pattern, however, reversed to baseline levels within 4 h. The concentration of plasma vWF increased after DDAVP infusion, but that of fibrinogen remained at trace levels. We conclude that vWF interaction with GPIIb/Il~a mediates platelet-platelet interaction and may play a role in primary hemostasis.

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Von Willebrand Factor Structure and Function

Montgomery¹,

Haberichter²

2011

Von Willebrand Disease

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Independent modulation of von Willebrand factor and fibrinogen binding to the platelet membrane glycoprotein IIb/IIIa complex as demonstrated by monoclonal antibody.

Cited by 103 publications

References 50 publications

Identification of two distinct regions within the binding sites for fibrinogen and fibronectin on the IIb–IIIa human platelet membrane glycoprotein complex by monoclonal antibodies P2 and P4

Identification of two distinct regions within the binding sites for fibrinogen and fibronectin on the IIb–IIIa human platelet membrane glycoprotein complex by monoclonal antibodies P2 and P4

von Willebrand factor interaction with the glycoprotein IIb/IIa complex. Its role in platelet function as demonstrated in patients with congenital afibrinogenemia.

Von Willebrand Factor Structure and Function

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