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Overview

Von Willebrand’s Disease:

Historical Perspective

Von Willebrand’s Disease(vWD) was first discovered by Erik Adolf von Willebrand, a Finnish Physician, in 1926, in a Swedish-language article “Hereditär pseudohemofili” ("Hereditary pseudohemophilia") after assessing a 5 year-old Finnish Girl and 66 members of her family from 1924-1926. In 1957, decreased level of a plasma factor ‘ Factor ⅷ later called ‘Von Willebrand factor’ were first identified in the pathogenesis of Von Willebrand’s Disease. In early 1970s Ristocetin was used to diagnose vWD after inducing platelet aggregation ^[1] . Later immunoprecipitation techniques were used to understand vWD and it’s varieties.

Classification

vWD may be classified according to Hereditary and Aquired causes. vWD is sub-classified according to Hereditary in four types.

Type 1
Type 2: Type 2 is further divided into 4 subtypes: 2A, 2B, 2M, 2N
Type 3
Pseudo or platelet-type

Aquired vWD is thought to be caused by Autoantibodies. It can be subclassified into lymphoproliferative, cardiovascular, myeloproliferative, neoplastic, autoimmune disorders ^[2] .

References

↑ Favaloro EJ (July 2014). "Diagnosing von Willebrand disease: a short history of laboratory milestones and innovations, plus current status, challenges, and solutions". Semin. Thromb. Hemost. 40 (5): 551–70. doi:10.1055/s-0034-1383546. PMID 24978322.
↑ Kumar S, Pruthi RK, Nichols WL (February 2002). "Acquired von Willebrand disease". Mayo Clin. Proc. 77 (2): 181–7. doi:10.4065/77.2.181. PMID 11838652.

[pmid24978322-1] Favaloro EJ (July 2014). "Diagnosing von Willebrand disease: a short history of laboratory milestones and innovations, plus current status, challenges, and solutions". Semin. Thromb. Hemost. 40 (5): 551–70. doi:10.1055/s-0034-1383546. PMID 24978322.

[pmid11838652-2] Kumar S, Pruthi RK, Nichols WL (February 2002). "Acquired von Willebrand disease". Mayo Clin. Proc. 77 (2): 181–7. doi:10.4065/77.2.181. PMID 11838652.

[1]

[2]

@@ Line 6: / Line 6: @@
 Von Willebrand’s Disease(vWD) was first discovered by Erik Adolf von Willebrand, a Finnish Physician, in 1926, in a Swedish-language article “Hereditär pseudohemofili” ("Hereditary pseudohemophilia") after assessing a 5 year-old Finnish Girl and 66 members of her family from 1924-1926. In 1957, decreased level of a plasma factor ‘ Factor ⅷ later called ‘Von Willebrand factor’ were first identified in the pathogenesis of Von Willebrand’s Disease. In early 1970s Ristocetin was used to diagnose vWD after inducing platelet aggregation <ref name="pmid24978322">{{cite journal |vauthors=Favaloro EJ |title=Diagnosing von Willebrand disease: a short history of laboratory milestones and innovations, plus current status, challenges, and solutions |journal=Semin. Thromb. Hemost. |volume=40 |issue=5 |pages=551–70 |date=July 2014 |pmid=24978322 |doi=10.1055/s-0034-1383546 |url=}}</ref> . Later immunoprecipitation techniques were used to understand vWD and it’s varieties.
 ==Classification==
-[[vWD]] may be classified according to [[Hereditary]] and [[Aquired]] causes.[[vWD]] is sub-classified according to [[Hereditary]] in four types.
+[[vWD]] may be classified according to [[Hereditary]] and [[Aquired]] causes.
+[[vWD]] is sub-classified according to [[Hereditary]] in four types.
 *Type 1
 *Type 2: Type 2 is further divided into 4 subtypes: 2A, 2B, 2M, 2N
 *Type 3
 *Pseudo or platelet-type
+[[Aquired]]  vWD is thought to be caused by [[Autoantibodies]]. It can be subclassified into lymphoproliferative, cardiovascular, myeloproliferative, neoplastic, autoimmune disorders <ref name="pmid11838652">{{cite journal |vauthors=Kumar S, Pruthi RK, Nichols WL |title=Acquired von Willebrand disease |journal=Mayo Clin. Proc. |volume=77 |issue=2 |pages=181–7 |date=February 2002 |pmid=11838652 |doi=10.4065/77.2.181 |url=}}</ref> .
 ==References==
 {{reflist|1}}