Von Willebrand Factor disease: Difference between revisions

Latest revision as of 02:53, 20 November 2020

Background

Deficiency in quantity or quality of von Willebrand Factor (vWF) increasing risk of bleeding

Classification

Type 1 (80%): mild quantitative deficiency
Type 2 (20%): qualitative deficiency (i.e. doesn't work properly)
- Type 2A: normal quantity, abnormal quality
- Type 2B: enhanced GP1b-binding, leading to platelet adhesion and clearance
- Type 2M, Type 2N
Type 3 (<1%): autosomal-recessive absolute quantitative deficiency (i.e. none made)
Acquired: vWF cleared by autoantibodies, sheared by aortic stenosis, or sequestered by thrombocytosis

Pathophysiology

vWF is long multimer that helps platelet aggregation in response to endothelial damage
vWF is released by endothelium in response to damage
vWF binds Factor VIII as well as platelets
It unravels, thereby exposing platelet binding sites

Epidemiology

Most common inherited bleeding disorder, with a prevalence of 1 in 100
Prevalence of significant bleeding is 1 in 10,000
Most are inherited in autosomal dominant pattern (including types 1 and 2B and most 2A and 2M), though type 2N and 3, and some type 2A and 2M, are autosomal recessive

Clinical Manifestations

Abnormal bleeding, usually mucocutaneous, and ranging from mild (common) to severe (rare)
Easy bruising
Heavy menstrual bleeding/menorrhagia
Postpartum bleeding
Types 2N and 3 can include joint, soft tissue, and GI bleeding
Type 3 typically presents in infancy, such as prolonged bleeding after circumcision

Investigations

CBC, PT/INR, PTT
vWD screen: Factor VIII, vWF antigen, vWF activity (either ristocetin cofactor or collagen)
Consider PFA-100 (in-vitro bleeding time) and blood type
If suspecting Type 2:
- RIPA (ristocetin-induced platelet agglutination)
- Multimer studies for high molecular weight multimers (MHWM)
- vWF genetic testing

	vWF-Ag	vWF-RCo	FVIII	RIPA	Multimers
Type 1	↓	↓	↓	↓	N
Type 2A	↓/N	↓↓	↓/N	↓↓	Lack of HMWM
Type 2B	↓/N	↓	↓/N	↑	Lack of HMWM
Type 2M	N	↓↓	N	↓↓	N
Type 2N	N	N	↓	N	N
Type 3	Absent	Absent	0.05 u/mL	Absent	Absent

Management

For Type 1 and 2A
- Desmopressin (ddAVP) 0.3mg/kg (max 20mg) IV/SC can promote release of vWF from endothelium
- Lasts 8-12h, so can repeat q12-24h as long as needed
- Monitor for tachyphylaxis after 4 doses

@@ Line 1: / Line 1: @@
-== Definition ==
+==Background==
-* Deficiency in quantity or quality of von Willebrand Factor (vWF) increasing risk of bleeding
+*Deficiency in quantity or quality of von Willebrand Factor (vWF) increasing risk of bleeding
+===Classification===
-== Type ==
-* Type 1 (80%): mild quantitative deficiency
+*Type 1 (80%): mild quantitative deficiency
-* Type 2 (20%): qualitative deficiency (i.e. doesn't work properly)
+*Type 2 (20%): qualitative deficiency (i.e. doesn't work properly)
-** Type 2A: normal quantity, abnormal quality
+**Type 2A: normal quantity, abnormal quality
-** Type 2B: enhanced GP1b-binding, leading to platelet adhesion and clearance
+**Type 2B: enhanced GP1b-binding, leading to platelet adhesion and clearance
-** Type 2M, Type 2N
+**Type 2M, Type 2N
-* Type 3 (&lt;1%): autosomal-recessive absolute quantitative deficiency (i.e. none made)
+*Type 3 (&lt;1%): autosomal-recessive absolute quantitative deficiency (i.e. none made)
-* Acquired: vWF cleared by autoantibodies, sheared by aortic stenosis, or sequestered by thrombocytosis
+*Acquired: vWF cleared by autoantibodies, sheared by aortic stenosis, or sequestered by thrombocytosis
+===Pathophysiology===
-== Physiology ==
-* vWF is long multimer that helps platelet aggregation in response to endothelial damage
+*vWF is long multimer that helps platelet aggregation in response to endothelial damage
-* vWF is released by endothelium in response to damage
+*vWF is released by endothelium in response to damage
-* vWF binds Factor VIII as well as platelets
+*vWF binds Factor VIII as well as platelets
-* It unravels, thereby exposing platelet binding sites
+*It unravels, thereby exposing platelet binding sites
-== Epidemiology ==
+===Epidemiology===
-* Most common bleeding disorder with a prevalence of 1 in 100
+*Most common inherited bleeding disorder, with a prevalence of 1 in 100
-* Prevalence of significant bleeding is 1 in 10,000
+*Prevalence of significant bleeding is 1 in 10,000
+*Most are inherited in autosomal dominant pattern (including types 1 and 2B and most 2A and 2M), though type 2N and 3, and some type 2A and 2M, are autosomal recessive
-== Clinical Manifestations ==
+==Clinical Manifestations==
+*Abnormal bleeding, usually mucocutaneous, and ranging from mild (common) to severe (rare)
-== Investigations ==
+*Easy bruising
+*Heavy menstrual bleeding/menorrhagia
+*[[Postpartum bleeding]]
+*Types 2N and 3 can include joint, soft tissue, and GI bleeding
+*Type 3 typically presents in infancy, such as prolonged bleeding after circumcision
+==Investigations==
-* CBC, PT/INR, PTT
-* vWD screen: Factor VIII, vWF antigen, vWF activity (either ristocetin or collagen)
-* Consider PFA-100 (in-vitro bleeding time) and blood type
-* If suspecting Type 2:
-** RIPA (ristocetin-induced platelet agglutination)
-** Multimer studies for high molecular weight multimers (MHWM)
-** vWF genetic testing
+*CBC, PT/INR, PTT
-{|
+*vWD screen: Factor VIII, vWF antigen, vWF activity (either ristocetin cofactor or collagen)
+*Consider PFA-100 (in-vitro bleeding time) and blood type
+*If suspecting Type 2:
+**RIPA (ristocetin-induced platelet agglutination)
+**Multimer studies for high molecular weight multimers (MHWM)
+**vWF genetic testing
+{| class="wikitable"
 !
-!align="center"| '''vWF-Ag'''
+! align="center" |'''vWF-Ag'''
-!align="center"| '''vWF-RCo'''
+! align="center" |'''vWF-RCo'''
-!align="center"| '''FVIII'''
+! align="center" |'''FVIII'''
-!align="center"| '''RIPA'''
+! align="center" |'''RIPA'''
-!align="center"| '''Multimers'''
+! align="center" |'''Multimers'''
 |-
-| '''Type 1'''
+|'''Type 1'''
-|align="center"| ↓
+| align="center" |↓
-|align="center"| ↓
+| align="center" |↓
-|align="center"| ↓
+| align="center" |↓
-|align="center"| ↓
+| align="center" |↓
-|align="center"| N
+| align="center" |N
 |-
-| '''Type 2A'''
+|'''Type 2A'''
-|align="center"| ↓/N
+| align="center" |↓/N
-|align="center"| ↓↓
+| align="center" |↓↓
-|align="center"| ↓/N
+| align="center" |↓/N
-|align="center"| ↓↓
+| align="center" |↓↓
-|align="center"| Lack of HMWM
+| align="center" |Lack of HMWM
 |-
-| '''Type 2B'''
+|'''Type 2B'''
-|align="center"| ↓/N
+| align="center" |↓/N
-|align="center"| ↓
+| align="center" |↓
-|align="center"| ↓/N
+| align="center" |↓/N
-|align="center"| ↑
+| align="center" |↑
-|align="center"| Lack of HMWM
+| align="center" |Lack of HMWM
 |-
-| '''Type 2M'''
+|'''Type 2M'''
-|align="center"| N
+| align="center" |N
-|align="center"| ↓↓
+| align="center" |↓↓
-|align="center"| N
+| align="center" |N
-|align="center"| ↓↓
+| align="center" |↓↓
-|align="center"| N
+| align="center" |N
 |-
-| '''Type 2N'''
+|'''Type 2N'''
-|align="center"| N
+| align="center" |N
-|align="center"| N
+| align="center" |N
-|align="center"| ↓
+| align="center" |↓
-|align="center"| N
+| align="center" |N
-|align="center"| N
+| align="center" |N
 |-
-| '''Type 3'''
+|'''Type 3'''
-|align="center"| Absent
+| align="center" |Absent
-|align="center"| Absent
+| align="center" |Absent
-|align="center"| 0.05 u/mL
+| align="center" |0.05 u/mL
-|align="center"| Absent
+| align="center" |Absent
-|align="center"| Absent
+| align="center" |Absent
 |}
-== Management ==
+==Management==
-* For Type 1 and 2A
+*For Type 1 and 2A
-** Desmopressin (ddAVP) 0.3mg/kg (max 20mg) IV/SC can promote release of vWF from endothelium
+**[[Desmopressin]] (ddAVP) 0.3mg/kg (max 20mg) IV/SC can promote release of vWF from endothelium
-** Lasts 8-12h, so can repeat q12-24h as long as needed
+**Lasts 8-12h, so can repeat q12-24h as long as needed
-** Monitor for tachyphylaxis after 4 doses
+**Monitor for tachyphylaxis after 4 doses
 {{DISPLAYTITLE:von Willebrand Factor disease}}