Expression of terminal α2-6–linked sialic acid on von Willebrand factor specifically enhances proteolysis by ADAMTS13

McGrath, Rachel T.; McKinnon, Thomas A. J.; Byrne, Barry; O’Kennedy, Richard; Terraube, Virginie; McRae, Emily; Preston, Roger J. S.; Laffan, Michael; O’Donnell, James S.

doi:10.1182/blood-2009-09-241547

Cited by 77 publications

(95 citation statements)

References 49 publications

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“…11,14 In recent studies, we and others have clearly demonstrated the key role played by VWF glycans in regulating proteolysis by ADAMTS13. [15][16][17][18] Importantly, expression of both ABO blood group antigens and terminal sialic acid on VWF were shown to be of critical importance. 15,16,18 In this study, we have characterized terminal carbohydrate expression on platelet-VWF.…”

Section: Introductionmentioning

confidence: 99%

“…[15][16][17][18] Importantly, expression of both ABO blood group antigens and terminal sialic acid on VWF were shown to be of critical importance. 15,16,18 In this study, we have characterized terminal carbohydrate expression on platelet-VWF. Our findings demonstrate that platelet-VWF exists as a distinct natural glycoform, with a particular marked reduction in N-linked sialic acid expression compared with plasma-VWF.…”

Section: Introductionmentioning

confidence: 99%

“…Finally, platelet-VWF was purified by immunoaffinity chromatography employing the monoclonal antibody CLB-RAg20 as previously described in detail. 20 Plasma-derived VWF was purified by cryoprecipitation and 2BCL gel filtration as before, 18 followed by CLB-RAg20 immunoaffinity chromatography.…”

Section: Introductionmentioning

confidence: 99%

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Altered glycosylation of platelet-derived von Willebrand factor confers resistance to ADAMTS13 proteolysis

McGrath

Biggelaar

Byrne

et al. 2013

Blood

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Altered glycosylation of platelet-derived von Willebrand factor confers resistance to ADAMTS13 proteolysis

McGrath

Biggelaar

Byrne

et al. 2013

Blood

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“…6,7,[9][10][11] Although the O-linked glycans of VWF also demonstrate marked heterogeneity, disialyl core 1 structures account for ;70% of the total population. 8,12 Importantly, although the majority of its glycans are capped by negatively charged sialic acid, 7,13 VWF is unusual in that a minority of both N-linked and O-linked carbohydrate chains express terminal ABO(H) blood group determinants. 7,8,11 Although substantial progress has been achieved in understanding the biosynthesis, structure, and functions of VWF, the biological mechanism(s) responsible for modulating VWF clearance from the plasma remain poorly understood.…”

Section: Introductionmentioning

confidence: 99%

N-linked glycans within the A2 domain of von Willebrand factor modulate macrophage-mediated clearance

Chion

O’Sullivan

Drakeford

et al. 2016

Blood

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Key Points• The A1 domain of VWF contains a cryptic binding site that plays a key role in regulating macrophage binding and clearance.• The N-linked glycans presented at N1515 and N1574 within the A2 domain of VWF modulate macrophage-mediated clearance.Enhanced von Willebrand factor (VWF) clearance is important in the etiology of von Willebrand disease. However, the molecular mechanisms underlying VWF clearance remain poorly understood. In this study, we investigated the role of VWF domains and specific glycan moieties in regulating in vivo clearance. Our findings demonstrate that the A1 domain of VWF contains a receptor-recognition site that plays a key role in regulating the interaction of VWF with macrophages. In A1-A2-A3 and full-length VWF, this macrophage-binding site is cryptic but becomes exposed following exposure to shear or ristocetin. Previous studies have demonstrated that the N-linked glycans within the A2 domain play an important role in modulating susceptibility to ADAMTS13 proteolysis. We further demonstrate that these glycans presented at N1515 and N1574 also play a critical role in protecting VWF against macrophage binding and clearance. Indeed, loss of the N-glycan at N1515 resulted in markedly enhanced VWF clearance that was significantly faster than that observed with any previously described VWF mutations. In addition, A1-A2-A3 fragments containing the N1515Q or N1574Q substitutions also demonstrated significantly enhanced clearance. Importantly, clodronate-induced macrophage depletion significantly attenuated the increased clearance observed with N1515Q and N1574Q in both full-length VWF and A1-A2-A3.Finally, we further demonstrate that loss of these N-linked glycans does not enhance clearance in VWF in the presence of a structurally constrained A2 domain. Collectively, these novel findings support the hypothesis that conformation of the VWF A domains plays a critical role in modulating macrophage-mediated clearance of VWF in vivo. (Blood. 2016;128(15):1959-1968

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“…Recent studies have clarified this association and verified that B and A1 blood groups are at higher risk than O and A2 blood groups, with the relative risk of approximately 2 (38,39). It is assumed that an ABO blood group could contribute to thrombosis risk through modifications of von Willebrand factor (VWF) and factor VIII (FVIII) levels in plasma (40,41). On the other hand, several studies have revealed that ABO blood groups remain significantly associated with elevated prothrombotic risk, even after adjustment for FVIII or VWF levels (41,42).…”

Section: Other Genetic Risk Factorsmentioning

confidence: 99%

Molecular Basis of Thrombophilia / MOLEKULARNE OSNOVE TROMBOFILIJE

Đorđević¹

2014

Journal of Medical Biochemistry

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SummaryThrombophilia is a multifactorial disorder, involving both genetic and acquired risk factors that affect the balance between procoagulant and anticoagulant factors and lead to increased thrombotic tendency. The severe forms of thrombophilia are caused by a deficiency of natural anticoagulants: antithrombin, protein C and protein S. The advances in DNA technology played an important role in the identification of the exact nature of these deficiencies and opened up new possibilities in genetic research and molecular diagnostics of thrombophilia. The major breakthrough came with the discovery of activated protein C resistance and the Factor V Leiden gene mutation. Shortly afterwards, a variant in the 3' untranslated region of the Factor II gene (FII G20210A) associated with an increased concentration of Factor II in plasma was described. These two gene variants represent the most common thrombophilic genetic risk factors. Recently, a novel prothrombin mutation (c.1787G>T) was identified in a Japanese family with juvenile thrombosis. This mutation leads to impaired inhibition of mutant thrombin by antithrombin, proposing a new mechanism of thrombophilia named resistance to antithrombin. In the last decade, se veral prothrombotic genetic risk factors have been described, including gene variants associated with defects of natural coagulation inhibitors, increased levels of coagulation factors or their impaired inhibition and defects of the fibrinolytic system. However, most of them are not of diagnostic value, due to their minor or unknown impact on the thrombotic risk. Large-scale DNA analysis systems are now becoming available, opening a new era in the genetic studies of the molecular basis of thrombophilia. Keywords: thrombophilia, genetic risk factors, gene variants Kratak sadr`ajTrombofilija nastaje kao rezultat kompleksne interakcije izme|u negeneti~kih i geneti~kih faktora rizika koji hemostaznu ravnote`u pomeraju u smeru hiperkoagulacije i dovode do pojave tromboze. Veoma zna~ajan faktor rizika za nastanak trombofilije je deficijencija inhibitora koagulacije: antitrombina, proteina C ili proteina S. Veliki korak u razu mevanju geneti~ke osnove i molekularne dijagnostike trombofilije napravljen je otkri}em rezistencije na aktivirani protein C i faktor V Leiden mutacije. Ubrzo je otkrivena i varijanta u 3'-nekodiraju}em regionu gena za faktor II (FII G20210A), za koju je pokazano da dovodi do povi{ene koncentracije protrombina u plazmi. Ove dve genske varijante su naju~estaliji geneti~ki faktori rizika za nastanak trombofilije. Nedavno je opisana nova mutacija u genu za protrombin (c.1787G >T) za koju je pokazano da dovodi do rezistencije na anti trombin, odnosno do smanjene mogu}nosti inaktivacije mu tira nog trombina od strane antitrombina, {to predstavlja novi mehanizam za nastanak trombofilije. U toku poslednjih decenija, opisan je veliki broj geneti~kih faktora rizika za nastanak trombofilije, uklju~uju}i one koji dovode do: nedos tatka inhibitora koagulacije, pove}anog nivoa ili smanjene inaktivacij...

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Expression of terminal α2-6–linked sialic acid on von Willebrand factor specifically enhances proteolysis by ADAMTS13

Cited by 77 publications

References 49 publications

Altered glycosylation of platelet-derived von Willebrand factor confers resistance to ADAMTS13 proteolysis

Altered glycosylation of platelet-derived von Willebrand factor confers resistance to ADAMTS13 proteolysis

N-linked glycans within the A2 domain of von Willebrand factor modulate macrophage-mediated clearance

Molecular Basis of Thrombophilia / MOLEKULARNE OSNOVE TROMBOFILIJE

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