Shielding of the A1 Domain by the D′D3 Domains of von Willebrand Factor Modulates Its Interaction with Platelet Glycoprotein Ib-IX-V

Ulrichts, Hans; Udvardy, M.; Lenting, Peter J.; Pareyn, Inge; Vandeputte, Nele; Vanhoorelbeke, Karen; Deckmyn, Hans

doi:10.1074/jbc.m513314200

Cited by 121 publications

(115 citation statements)

References 41 publications

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“…The DЈA3 fragment was chosen because it does not form multimers; therefore, it can be used for kinetic studies in which spatial separation of the A1 domains is essential, while still encompassing the OLGs and structural elements that have been suggested to influence accessibility of the A1 domain. 31,32 We first confirmed that all the DЈA3 mutants bound to the flow slides to a similar extent as wtDЈA3. Immobilized proteins were recovered from the slides and analyzed by SDS-PAGE followed by Western blotting and immunostaining with both polyclonal anti-VWF antibody ( Figure 2C) and anti-c-myc tag antibodies ( Figure 2D).…”

Section: Vwf Olgs Modulate Platelet Translocation Over Vwfsupporting

confidence: 67%

O-linked glycosylation of von Willebrand factor modulates the interaction with platelet receptor glycoprotein Ib under static and shear stress conditions

Nowak

Canis

Riddell

et al. 2012

Blood

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AbstractWe have examined the effect of the O-linked glycan (OLG) structures of VWF on its interaction with the platelet receptor glycoprotein Ibα. The 10 OLGs were mutated individually and as clusters (Clus) on either and both sides of the A1 domain: Clus1 (N-terminal side), Clus2 (C-terminal side), and double cluster (DC), in both full-length-VWF and in a VWF construct spanning D′ to A3 domains. Mutations did not alter VWF secretion by HEK293T cells, multimeric structure, or static collagen binding. The T1255A, Clus1, and DC variants caused increased ristocetin-mediated GPIbα binding to VWF. Platelet translocation rate on OLG mutants was increased because of reduced numbers of GPIbα binding sites but without effect on bond lifetime. In contrast, OLG mutants mediated increased platelet capture on collagen under high shear stress that was associated with increased adhesion of these variants to the collagen under flow. These findings suggest that removal of OLGs increases the flexibility of the hinge linker region between the D3 and A1 domain, facilitating VWF unfolding by shear stress, thereby enhancing its ability to bind collagen and capture platelets. These data demonstrate an important functional role of VWF OLGs under shear stress conditions.

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Section: Vwf Olgs Modulate Platelet Translocation Over Vwfsupporting

confidence: 67%

O-linked glycosylation of von Willebrand factor modulates the interaction with platelet receptor glycoprotein Ib under static and shear stress conditions

Nowak

Canis

Riddell

et al. 2012

Blood

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“…The primary structure of the mature vWF protein describes the A1 domain as being flanked by the DЈD3 domains in the N-terminal region, and those domains have been described to be involved in the mechanism that inhibits the vWF-GPIb␣ interaction by shielding the A1 domain (22). However, the binding site for GPIb␣ in the A1 domain remained cryptic in our A1A2A3 protein, which excludes the DЈD3 domains (4).…”

mentioning

confidence: 61%

N-terminal Flanking Region of A1 Domain in von Willebrand Factor Stabilizes Structure of A1A2A3 Complex and Modulates Platelet Activation under Shear Stress

Auton

Sowa

Behymer

et al. 2012

Journal of Biological Chemistry

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“…These contacts may allow the D3 and/or other domains to regulate the forced dissociation of A1 from GPIbα in a manner similar to that of the salt bridges between D1269 and R1306/R1450. This may explain why deleting the D′D3 region augments binding to GPIbα and adding an isolated D′D3 region inhibits GPIbα binding to vWF lacking this region (48). Deleting the D′D3 region (residues 764-1259) may affect the D1269:R1306/R1450 salt bridges, causing a gain-of-function phenotype like that of R1450E A1.…”

Section: Figurementioning

confidence: 99%

Platelet glycoprotein Ibα forms catch bonds with human WT vWF but not with type 2B von Willebrand disease vWF

Yago¹,

Lou²,

Wu³

et al. 2008

J. Clin. Invest.

234

421

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Arterial blood flow enhances glycoprotein Ibα (GPIbα) binding to vWF, which initiates platelet adhesion to injured vessels. Mutations in the vWF A1 domain that cause type 2B von Willebrand disease (vWD) reduce the flow requirement for adhesion. Here we show that increasing force on GPIbα/vWF bonds first prolonged ("catch") and then shortened ("slip") bond lifetimes. Two type 2B vWD A1 domain mutants, R1306Q and R1450E, converted catch bonds to slip bonds by prolonging bond lifetimes at low forces. Steered molecular dynamics simulations of GPIbα dissociating from the A1 domain suggested mechanisms for catch bonds and their conversion by the A1 domain mutations. Catch bonds caused platelets and GPIbα-coated microspheres to roll more slowly on WT vWF and WT A1 domains as flow increased from suboptimal levels, explaining flowenhanced rolling. Longer bond lifetimes at low forces eliminated the flow requirement for rolling on R1306Q and R1450E mutant A1 domains. Flowing platelets agglutinated with microspheres bearing R1306Q or R1450E mutant A1 domains, but not WT A1 domains. Therefore, catch bonds may prevent vWF multimers from agglutinating platelets. A disintegrin and metalloproteinase with a thrombospondin type 1 motif-13 (ADAMTS-13) reduced platelet agglutination with microspheres bearing a tridomain A1A2A3 vWF fragment with the R1450E mutation in a shear-dependent manner. We conclude that in type 2B vWD, prolonged lifetimes of vWF bonds with GPIbα on circulating platelets may allow ADAMTS-13 to deplete large vWF multimers, causing bleeding.

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Shielding of the A1 Domain by the D′D3 Domains of von Willebrand Factor Modulates Its Interaction with Platelet Glycoprotein Ib-IX-V

Cited by 121 publications

References 41 publications

O-linked glycosylation of von Willebrand factor modulates the interaction with platelet receptor glycoprotein Ib under static and shear stress conditions

O-linked glycosylation of von Willebrand factor modulates the interaction with platelet receptor glycoprotein Ib under static and shear stress conditions

N-terminal Flanking Region of A1 Domain in von Willebrand Factor Stabilizes Structure of A1A2A3 Complex and Modulates Platelet Activation under Shear Stress

Platelet glycoprotein Ibα forms catch bonds with human WT vWF but not with type 2B von Willebrand disease vWF

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