Von Willebrand factor

Von Willebrand factor
PDB rendering based on 1ao3.
Available structures PDB Ortholog search: PDBe, RCSB List of PDB id codes 1AO3​, 1ATZ​, 1AUQ​, 1FE8​, 1FNS​, 1IJB​, 1IJK​, 1M10​, 1OAK​, 1SQ0​, 1U0N​, 1UEX​, 2ADF​, 2MHP​, 2MHQ​, 3GXB​, 3HXO​, 3HXQ​, 3PPV​, 3PPW​, 3PPX​, 3PPY​, 3ZQK​, 4C29​, 4C2A​, 4C2B​, 4DMU​, 4NT5​
Identifiers
Symbols	VWF ; F8VWF; VWD
External IDs	OMIM: 613160 MGI: 98941 HomoloGene: 466 GeneCards: VWF Gene
Gene ontology Molecular function • glycoprotein binding • protease binding • integrin binding • protein binding • collagen binding • immunoglobulin binding • identical protein binding • protein homodimerization activity • protein N-terminus binding • chaperone binding Cellular component • extracellular region • proteinaceous extracellular matrix • endoplasmic reticulum • extracellular matrix • platelet alpha granule • platelet alpha granule lumen • Weibel-Palade body • extracellular exosome Biological process • platelet degranulation • cell adhesion • blood coagulation • blood coagulation, intrinsic pathway • hemostasis • response to wounding • platelet activation • extracellular matrix organization • cell-substrate adhesion • protein homooligomerization Sources: Amigo / QuickGO
RNA expression pattern
More reference expression data
Orthologs
Species	Human	Mouse
Entrez	7450	22371
Ensembl	ENSG00000110799	ENSMUSG00000001930
UniProt	P04275	Q8CIZ8
RefSeq (mRNA)	NM_000552	NM_011708
RefSeq (protein)	NP_000543	NP_035838
Location (UCSC)	Chr 12: 5.95 – 6.12 Mb	Chr 6: 125.55 – 125.69 Mb
PubMed search

Von Willebrand factor (vWF) (/ˌfʌnˈvɪlᵻbrɑːnt/) is a blood glycoprotein involved in hemostasis. It is deficient or defective in von Willebrand disease and is involved in a large number of other diseases, including thrombotic thrombocytopenic purpura, Heyde's syndrome, and possibly hemolytic-uremic syndrome.^[1] Increased plasma levels in a large number of cardiovascular, neoplastic, and connective tissue diseases are presumed to arise from adverse changes to the endothelium, and may contribute to an increased risk of thrombosis.

Biochemistry

Synthesis

vWF is a large multimeric glycoprotein present in blood plasma and produced constitutively as ultra-large vWF in endothelium (in the Weibel-Palade bodies), megakaryocytes (α-granules of platelets), and subendothelial connective tissue.^[1]

Structure

The basic vWF monomer is a 2050-amino acid protein. Every monomer contains a number of specific domains with a specific function; elements of note are:^[1]

• the D'/D3 domain, which binds to factor VIII, (Von Willebrand factor type D domain)
• the A1 domain, which binds to:
  • platelet GPIb-receptor
  • heparin
  • possibly collagen
• the A3 domain, which binds to collagen (Von Willebrand factor type A domain)
• the C1 domain, in which the RGD domain binds to platelet integrin α_IIbβ₃ when this is activated
• the "cysteine knot" domain (at the C-terminal end of the protein), which vWF shares with platelet-derived growth factor (PDGF), transforming growth factor-β (TGFβ) and β-human chorionic gonadotropin (βHCG, of pregnancy test fame). (Von Willebrand factor type C domain)

Monomers are subsequently N-glycosylated, arranged into dimers in the endoplasmic reticulum and into multimers in the Golgi apparatus by crosslinking of cysteine residues via disulfide bonds. With respect to the glycosylation, vWF is one of only a few proteins that carry ABO blood group system antigens.^[1]

Multimers of vWF can be extremely large, >20,000 kDa, and consist of over 80 subunits of 250 kDa each. Only the large multimers are functional. Some cleavage products that result from vWF production are also secreted but probably serve no function.^[1]

Function

Von Willebrand factor's primary function is binding to other proteins, in particular factor VIII, and it is important in platelet adhesion to wound sites.^[1] It is not an enzyme and, thus, has no catalytic activity.

vWF binds to a number of cells and molecules. The most important ones are:^[1]

• Factor VIII is bound to vWF while inactive in circulation; factor VIII degrades rapidly when not bound to vWF. Factor VIII is released from vWF by the action of thrombin.
• vWF binds to collagen, e.g., when it is exposed in endothelial cells due to damage occurring to the blood vessel.
• vWF binds to platelet gpIb when it forms a complex with gpIX and gpV; this binding occurs under all circumstances, but is most efficient under high shear stress (i.e., rapid blood flow in narrow blood vessels, see below).
• vWF binds to other platelet receptors when they are activated, e.g., by thrombin (i.e., when coagulation has been stimulated).

vWF plays a major role in blood coagulation. Therefore, vWF deficiency or dysfunction (von Willebrand disease) leads to a bleeding tendency, which is most apparent in tissues having high blood flow shear in narrow vessels. From studies it appears that vWF uncoils under these circumstances, decelerating passing platelets.^[1] Calcium enhances the refolding rate of vWF A2 domain, allowing the protein to act as a shear force sensor.^[2]

Catabolism

The biological breakdown (catabolism) of vWF is largely mediated by the enzyme ADAMTS13 (acronym of "a disintegrin-like and metalloprotease with thrombospondin type 1 motif no. 13"). It is a metalloproteinase that cleaves vWF between tyrosine at position 842 and methionine at position 843 (or 1605–1606 of the gene) in the A2 domain. This breaks down the multimers into smaller units, which are degraded by other peptidases.^[3]

Role in disease

Hereditary or acquired defects of vWF lead to von Willebrand disease (vWD), a bleeding diathesis of the skin and mucous membranes, causing nosebleeds, menorrhagia, and gastrointestinal bleeding. The point at which the mutation occurs determines the severity of the bleeding diathesis. There are three types (I, II and III), and type II is further divided in several subtypes. Treatment depends on the nature of the abnormality and the severity of the symptoms.^[4] Most cases of vWD are hereditary, but abnormalities of vWF may be acquired; aortic valve stenosis, for instance, has been linked to vWD type IIA, causing gastrointestinal bleeding - an association known as Heyde's syndrome.^[5]

In thrombotic thrombocytopenic purpura (TTP) and hemolytic uremic syndrome (HUS), ADAMTS13 either is deficient or has been inhibited by antibodies directed at the enzyme. This leads to decreased breakdown of the ultra-large multimers of vWF and microangiopathic hemolytic anemia with deposition of fibrin and platelets in small vessels, and capillary necrosis. In TTP, the organ most obviously affected is the brain; in HUS, the kidney.^[6]

Higher levels of vWF are more common among people that have had ischemic stroke (from blood-clotting) for the first time. Occurrence is not affected by ADAMTS13, and the only significant genetic factor is the person's blood group.High plasma vWF levels were found to be an independent predictor of major bleeding in anticoagulated atrial fibrillation patients.^[7]

History

vWF is named after Dr. Erik von Willebrand (1870–1949), a Finnish doctor who in 1924 first described a hereditary bleeding disorder in families from the Åland islands, who had a tendency for cutaneous and mucosal bleeding, including menorrhagia. Although von Willebrand could not identify the definite cause, he distinguished von Willebrand disease (vWD) from hemophilia and other forms of bleeding diathesis.^[8]

In the 1950s, vWD was shown to be caused by a plasma factor deficiency (instead of being caused by platelet disorders), and, in the 1970s, the vWF protein was purified.^[1]

Interactions

Von Willebrand factor has been shown to interact with Collagen, type I, alpha 1.^[9]

Recently, It has been reported that the cooperation and interactions within the Von Willebrand factors enhances the adsorption probability in the primary hameostasis. Such cooperation is proven by calculating the adsorption probability of flowing vWF once it crosses another adsorbed one. Such cooperation is held within a wide range of shear rates.^[10]

See also

• Von Willebrand disease
• Bernard-Soulier syndrome

References

External links

• GeneReviews/NCBI/NIH/UW entry on von Willebrand Factor Deficiency. Includes: Type 1 von Willebrand Disease, Type 2A von Willebrand Disease, Type 2B von Willebrand Disease, Type 2M von Willebrand Disease, Type 2N von Willebrand Disease, Type 3 von Willebrand Disease

PDB gallery 1ao3: A3 DOMAIN OF VON WILLEBRAND FACTOR  1atz: HUMAN VON WILLEBRAND FACTOR A3 DOMAIN  1auq: A1 DOMAIN OF VON WILLEBRAND FACTOR  1fe8: CRYSTAL STRUCTURE OF THE VON WILLEBRAND FACTOR A3 DOMAIN IN COMPLEX WITH A FAB FRAGMENT OF IGG RU5 THAT INHIBITS COLLAGEN BINDING  1fns: CRYSTAL STRUCTURE OF THE VON WILLEBRAND FACTOR (VWF) A1 DOMAIN I546V MUTANT IN COMPLEX WITH THE FUNCTION BLOCKING FAB NMC4  1ijb: The von Willebrand Factor mutant (I546V) A1 domain  1ijk: The von Willebrand Factor mutant (I546V) A1 domain-botrocetin Complex  1m10: Crystal structure of the complex of Glycoprotein Ib alpha and the von Willebrand Factor A1 Domain  1oak: CRYSTAL STRUCTURE OF THE VON WILLEBRAND FACTOR (VWF) A1 DOMAIN IN COMPLEX WITH THE FUNCTION BLOCKING NMC-4 FAB  1sq0: Crystal Structure of the Complex of the Wild-type Von Willebrand Factor A1 domain and Glycoprotein Ib alpha at 2.6 Angstrom Resolution  1u0n: The ternary von Willebrand Factor A1-glycoprotein Ibalpha-botrocetin complex  1uex: Crystal structure of von Willebrand Factor A1 domain complexed with snake venom bitiscetin  2adf: Crystal Structure and Paratope Determination of 82D6A3, an Antithrombotic Antibody Directed Against the von Willebrand factor A3-Domain