Binding of ADAMTS13 to von Willebrand Factor

Majerus, Elaine M.; Anderson, Patricia J.; Sadler, J. Evan

doi:10.1074/jbc.m502529200

Cited by 110 publications

(119 citation statements)

References 37 publications

Supporting

Mentioning

109

Contrasting

Unclassified

Order By: Relevance

“…ADAMTS13 binds with high affinity and cleaves either multimeric VWF or GST-VWF73, provided the spacer domain is present (12,23). Therefore, the structural requirements for ADAMTS13 to cleave small substrates like VWF73 are similar to those for cleaving multimeric VWF, which implies that interactions limited to the A2 domain are sufficient to determine the substrate specificity of ADAMTS13.…”

Section: Discussionmentioning

confidence: 84%

See 1 more Smart Citation

Exosite interactions contribute to tension-induced cleavage of von Willebrand factor by the antithrombotic ADAMTS13 metalloprotease

Gao

Anderson

Majerus

et al. 2006

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

Self Cite

109

134

View full text Add to dashboard Cite

Von Willebrand factor (VWF) is a multimeric protein that mediates platelet adhesion at sites of vascular injury, and ADAMTS13 (a disintegrin and metalloprotease with thrombospondin)is a multidomain metalloprotease that limits platelet adhesion by a feedback mechanism in which fluid shear stress induces proteolysis of VWF and prevents disseminated microvascular thrombosis. Cleavage of the Tyr 1605 -Met 1606 scissile bond in the VWF A2 domain depends on a Glu 1660 -Arg 1668 segment in the same domain and on the noncatalytic spacer domain of ADAMTS13, suggesting that extensive enzyme-substrate interactions facilitate substrate recognition. Based on mutagenesis and kinetic analysis, we find that the ADAMTS13 spacer domain binds to an exosite near the C terminus of the VWF A2 domain. Deleting the spacer domain from ADAMTS13 or deleting the exosite from the VWF substrate reduced the rate of cleavage Ϸ20-fold. A cleavage product containing the exosite was a hyperbolic mixed-type inhibitor of ADAMTS13 proteolysis of either VWF multimers or model peptide substrates but only if the ADAMTS13 enzyme contained the spacer domain. The specificity of this unique mechanism depends on tension-induced unfolding of the VWF A2 domain, which exposes the scissile bond and exosite for interaction with complementary sites on ADAMTS13.enzyme kinetics ͉ thrombotic thrombocytopenic purpura ͉ fluid shear stress

show abstract

Section: Discussionmentioning

confidence: 84%

“…Nevertheless, VWF is the only known substrate of ADAMTS13 in plasma, even though ADAMTS13 is constitutively active (11). Furthermore, VWF is resistant to AD-AMTS13 until it is subjected to high fluid shear stress (7), adsorbed onto a surface (12), or treated with chaotropic agents such as urea (8) or guanidine hydrochloride (7).…”

mentioning

confidence: 99%

Exosite interactions contribute to tension-induced cleavage of von Willebrand factor by the antithrombotic ADAMTS13 metalloprotease

Gao

Anderson

Majerus

et al. 2006

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

Self Cite

109

134

View full text Add to dashboard Cite

show abstract

“…The less severe truncation (stl pa49 ) would remove only the C-terminal spacer. The identical null phenotypes that are associated with both of these truncation alleles affirm the importance of the C-terminal spacer region, which mediates substrate specificity in other ADAMTS proteins (Flannery et al 2002;Zheng et al 2003;Majerus et al 2005). Finally, stl a16 was found to be the most polymorphic strain, and in this mutant we found several missense mutations.…”

Section: Resultsmentioning

confidence: 76%

“…First, several ADAMTSs undergo processing at the C terminus for regulated proteolytic activity, and the C-terminal spacer region has been shown to be important for substrate binding and the specificity of the enzyme's biological activity Majerus et al 2005). ADAMTS4 is cleaved extracellularly, thereby greatly increasing its aggrecanase activity (Flannery et al 2002;Gao et al 2002Gao et al , 2004, and ADAMTS1 loses a portion of its C terminus, thereby losing affinity for heparin (Rodriguez-Manzaneque et al 2000).…”

Section: Discussionmentioning

confidence: 99%

stall Encodes an ADAMTS Metalloprotease and Interacts Genetically With Delta in Drosophila Ovarian Follicle Formation

2009

View full text Add to dashboard Cite

Ovarian follicle formation in Drosophila melanogaster requires stall (stl) gene function, both within and outside the ovary, for follicle individualization, stalk cell intercalation, and oocyte localization. We have identified the stl transcript as CG3622 and confirmed the presence of three alternatively spliced isoforms, contrary to current genome annotation. Here we show that the gene is expressed in both ovarian and brain tissues, which is consistent with previous evidence of an ovary nonautonomous function. On the basis of amino acid sequence, stl encodes a metalloprotease similar to the ''a disintegrin and metalloprotease with thrombospondin'' (ADAMTS) family. Although stl mutant ovaries fail to maintain the branched structure of the fusome and periodically show improperly localized oocytes, stl mutants do not alter oocyte determination. Within the ovary, stl is expressed in pupal basal stalks and in adult somatic cells of the posterior germarium and the follicular poles. Genetically, stl exhibits a strong mutant interaction with Delta (Dl), and Dl mutant ovaries show altered stl expression patterns. Additionally, a previously described genetic interactor, daughterless, also modulates stl expression in the somatic ovary and may do so directly in its capacity as a basic helix-loop-helix (bHLH) transcription factor. We propose a complex model of long-range extraovarian signaling through secretion or extracellular domain shedding, together with local intraovarian protein modification, to explain the dual sites of Stl metalloprotease function in oogenesis.

show abstract

“…de la molécule de VWF native [12]. Ainsi, seul le dépliement du VWF induit soit par les forces de cisaillement élevées du flux sanguin dans les microvaisseaux in vivo, soit par des agents dénaturants (urée, hydrochlorure de guanidine), ou son immobilisation sur une surface plastique [13] in vitro, permet l'exposition de ce pont peptidique et le rend donc accessible au clivage par ADAMTS13. De plus, cet accès est facilité par la liaison du VWF à certains ligands comme la P-sélectine (qui intervient dans la fixation du VWF à la surface des cellules endothéliales à la phase initiale de sa sécrétion dans le plasma [14]) ou la glycoprotéine Ib plaquettaire (qui permet la liaison du VWF aux plaquettes au sein du clou plaquettaire formé pour réparer une brèche vasculaire [15]).…”

Section: Exploration Biologique D'adamts13unclassified

ADAMTS13, la protéase spécifique du clivage du facteur von Willebrand

Veyradier

Coppo²

2011

Med Sci (Paris)

View full text Add to dashboard Cite

> ADAMTS13 (A disintegrin and metalloprotease with thrombospondin type 1 repeats) est la protéase spécifique du facteur von Willebrand (VWF). En cas de brèche vasculaire, le VWF permet, grâce à sa structure multimérique, l'adhésion des plaquettes au sous-endothélium et l'agrégation des plaquettes entre elles dans la microcirculation, où les forces de cisaillement sont élevées. ADAMTS13 régule l'activité du VWF en réduisant la taille de ses multimères. Un déficit fonctionnel sévère en ADAMTS13 est observé dans la majorité des cas de purpura thrombotique thrombocytopénique (PTT), une microangiopathie thrombotique défi-nie par la formation spontanée, dans la microcirculation sanguine, de thrombus plaquettaires responsables d'une anémie hémolytique mécani-que, d'une thrombopénie de consommation et de signes d'ischémie multiviscérale. Il s'agit d'une maladie rare (4 cas/10 6 habitants/an) mais gravissime en l'absence de traitement immédiat et spécifique (plasmathérapie). Dans 90 % des cas, le PTT est acquis et dû à la présence d'autoanticorps anti-ADAMTS13. Dans les autres cas, il s'agit d'un déficit constitutionnel, de transmission autosomique récessive, appelé syndrome d'Upshaw-Schulman. Une meilleure caractéri-sation structurale et fonctionnelle d'ADAMTS13 combinée aux études cliniques menées chez les patients atteints de PTT est cruciale pour évaluer la pertinence d'une forme purifiée plasmatique ou recombinante à visée thérapeutique.

show abstract

Binding of ADAMTS13 to von Willebrand Factor

Cited by 110 publications

References 37 publications

Exosite interactions contribute to tension-induced cleavage of von Willebrand factor by the antithrombotic ADAMTS13 metalloprotease

Exosite interactions contribute to tension-induced cleavage of von Willebrand factor by the antithrombotic ADAMTS13 metalloprotease

stall Encodes an ADAMTS Metalloprotease and Interacts Genetically With Delta in Drosophila Ovarian Follicle Formation

ADAMTS13, la protéase spécifique du clivage du facteur von Willebrand

Contact Info

Product

Resources

About