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

Yago, Tadayuki; Lou, Jizhong; Wu, Tao; Yang, Jun; Miner, Jonathan J.; Coburn, Leslie; López, José A.; Crúz, Miguel A.; Dong, Jing; McIntire, Larry V.; McEver, Rodger P.; Zhu, Cheng

doi:10.1172/jci35754

Cited by 228 publications

(459 citation statements)

References 59 publications

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“…As mentioned previously, the characteristic timescale for vWF tE10 À 4 s, which implies that we expect the binding energy to be in between the lowest binding energy we have studied here of 4 k B T and the intermediate energy of 5 k B T. Along the reaction coordinate, the distance between the binding minima and the top of the barrier for the GPIba-vWF A1 pair has been experimentally measured to be B2 nm 28 . This gives a bond breakup force of the order of B10 pN that is in excellent agreement with experiments 28,29 .…”

Section: Discussionsupporting

confidence: 88%

Blood-clotting-inspired reversible polymer–colloid composite assembly in flow

et al. 2013

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Blood clotting is a process by which a haemostatic plug is assembled at the site of injury. The formation of such a plug, which is essentially a (bio)polymer-colloid composite, is believed to be driven by shear flow in its initial phase, and contrary to our intuition, its assembly is enhanced under stronger flowing conditions. Here, inspired by blood clotting, we show that polymer-colloid composite assembly in shear flow is a universal process that can be tailored to obtain different types of aggregates including loose and dense aggregates, as well as hydrodynamically induced 'log'-type aggregates. The process is highly controllable and reversible, depending mostly on the shear rate and the strength of the polymer-colloid binding potential. Our results have important implications for the assembly of polymercolloid composites, an important challenge of immense technological relevance. Furthermore, flow-driven reversible composite formation represents a new paradigm in non-equilibrium self-assembly.

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Section: Discussionsupporting

confidence: 88%

Blood-clotting-inspired reversible polymer–colloid composite assembly in flow

et al. 2013

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“…Nonequilibrium processes can be produced by mechanical perturbations such as force and flow. Indeed, a recent study has demonstrated that force slows off-rate of GPIb␣-VWF dissociation (an unusual characteristic called catch bonds), which underlies f lowenhanced platelet rolling on VWF and prevents platelet agglutination (21). GOF mutations in the A1 domain away from the binding site eliminate catch bonds, abolish the flow requirement for rolling, and cause platelet agglutination.…”

Section: Discussionmentioning

confidence: 99%

Flow induces loop-to-β-hairpin transition on the β-switch of platelet glycoprotein Ibα

Lou¹,

Zhu

2008

Proc. Natl. Acad. Sci. U.S.A.

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Interaction of glycoprotein Ib␣ (GPIb␣) with von Willebrand factor (VWF) initiates platelet adhesion to injured vascular wall to stop bleeding. A major contact between GPIb␣ and VWF involves the ␤-switch region, which is a loop in the unliganded GPIb␣ but switches to a ␤-hairpin in the complex structure. Paradoxically, flow enhances rather than impedes GPIb␣-VWF binding. Gain-offunction mutations (e.g., M239V) in the ␤-switch reduce the flow requirement for VWF binding, whereas loss-of-function mutations (e.g., A238V) increase the flow requirement. These phenomena cannot be explained by crystal structures or energy calculations. Herein we demonstrate that the ␤-hairpin is unstable without contacting VWF, in that it switches to a loop in free molecular dynamics simulations. Simulations with a novel flow molecular dynamics algorithm show that the loop conformation is unstable in the presence of flow, as it switches to ␤-hairpin even without contacting VWF. Compared with the wild-type, it is easier for the M239V mutant but harder for the A238V mutant to switch to ␤-hairpin in the presence of flow. These results elucidate the structural basis for the two mutants and suggest a regulatory mechanism by which flow activates GPIb␣ via inducing a loop-to-␤-hairpin conformational transition on the ␤-switch, thereby promoting VWF binding. flow molecular dynamics ͉ Platelet-type von Willebrand disease ͉ von Willebrand factor ͉ conformational change ͉ mechanical sensing B inding of glycoprotein Ib␣ (GPIb␣) to von Willebrand factor (VWF) initiates a multistep platelet adhesion and signaling cascade of the hemostatic process (1, 2). Dysfunction of GPIb␣-VWF interaction may cause bleeding disorders such as von Willebrand diseases (VWD) (3). A rapid kinetic on-rate of GPIb␣-VWF binding is required for flowing platelets to tether to injured vessel wall. Counterintuitively, however, GPIb␣-VWF binding is enhanced by blood flow, despite the fact that increasing flow shortens contact time for molecular interaction (4). A minimum flow is required for platelets to tether to VWF (4, 5). The kinetic rates of GPIb␣-VWF binding and their mechanical regulation by flow can be altered by structural variations. Mutations may require higher or lower flows for platelet to tether to VWF compared with the wild-type (WT) GPIb␣ (6). The former is referred to as a gain-of-function (GOF) mutant, whereas the latter is a loss-of-function (LOF) mutant. GOF mutations G233V and M239V naturally occur in some patients with platelet-type (PT) VWD (5,7,8).GPIb␣ consists of a glycosylated N-terminal domain (GPIb␣N), a long mucin stalk, a transmembrane domain, and a cytoplasmic tail (9, 10). The binding site for VWF resides on GPIb␣N, which contains eight tandem leucine-rich repeats (Fig. 1A) (11). The monomeric subunit of VWF consists of multiple copies of A, B, C, and D type domains (12). The binding site for GPIb␣ resides on the A1 domain ( Fig. 1 B, cyan) (13). Regions of GPIb␣N at each end of the leucine-rich repeats bind, respectively, to the top and botto...

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“…Surprisingly, we find a complex mechanical regulation of adhesive bonds at the single-molecule level: tensile force prolongs the bond lifetime (that is, catch bonds). In contrast to the well-known catch bonds of bimolecular systems, such as cell adhesion receptors (integrins 28,38,39 , selectins 40,41 , glycoprotein Iba 30,42 , E-cadherin 43 and FimH 44 ), the T-cell receptor 31 and cytoskeletal linkages 45,46 , the Thy-1 catch bond is strongly correlated with a bond-stiffening phenotype, termed 'dynamic catch', which partially shifts force to the already engaged but unstretched coreceptor Syn4. Thus, the data reveal a unique, previously unreported class of receptor-ligand bonds whereby force tightens co-receptor engagement that is required for forcemediated adhesion signalling.…”

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confidence: 99%

Dynamic catch of a Thy-1–α5β1+syndecan-4 trimolecular complex

Fiore

Chen

et al. 2014

Nat Commun

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Cancer cell adhesion to the vascular endothelium is a critical step of tumour metastasis. Endothelial surface molecule Thy-1 (CD90) is implicated in the metastatic process through its interactions with integrins and syndecans. However, how Thy-1 supports cell-cell adhesion in a dynamic mechanical environment is not known. Here we show that Thy-1 supports b 1 integrin-and syndecan-4 (Syn4)-mediated contractility-dependent mechanosignalling of melanoma cells. At the single-molecule level, Thy-1 is capable of independently binding a 5 b 1 integrin and syndecan-4 (Syn4) receptors. However, in the presence of both a 5 b 1 and Syn4, the two receptors bind cooperatively to Thy-1, to form a trimolecular complex. This trimolecular complex displays a unique phenomenon we coin 'dynamic catch', characterized by abrupt bond stiffening followed by the formation of catch bonds, where force prolongs the bond lifetime. Thus, we reveal a new class of trimolecular interactions where force strengthens the synergistic binding of two co-receptors and modulates downstream mechanosignalling.

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

Cited by 228 publications

References 59 publications

Blood-clotting-inspired reversible polymer–colloid composite assembly in flow

Blood-clotting-inspired reversible polymer–colloid composite assembly in flow

Flow induces loop-to-β-hairpin transition on the β-switch of platelet glycoprotein Ibα

Dynamic catch of a Thy-1–α5β1+syndecan-4 trimolecular complex

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