Thrombophilia: Difference between revisions

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{{SK}} Hypercoagulability, coagulability, hypercoagulable state
{{SK}} Hypercoagulability, coagulability, hypercoagulable state


==Overview==
'''Thrombophilia''' is defined as an increased risk of [[thrombosis]] in the body, due to an abnormality in the system of [[coagulation]]. Thrombophilia can be inherited or acquired. More than 50% of the cases of [[thrombosis]] are associated with an underlying thrombophilia. Thrombophilias are mostly associated with venous thromboembolism like [[deep vein thrombosis]] in lower extremities or [[pulmonary embolism]]. Relatively less is known about thrombophilias that predispose to arterial thromboembolism<ref name="pmid11309638">{{cite journal |author=Seligsohn U, Lubetsky A |title=Genetic susceptibility to venous thrombosis |journal=N. Engl. J. Med. |volume=344 |issue=16 |pages=1222–31 |year=2001 |month=April |pmid=11309638 |doi=10.1056/NEJM200104193441607 |url=}}</ref>.


==Classification==
Thrombophilia can be classified in various forms.
* The most common classification is by the nature of the thrombosis: [[artery|arterial]], [[vein|venous]] or combined.
* Crowther & Kelton (2003) propose to classify the abnormality by the molecular deficiency, type I being the (severe) deficiencies of inhibitors, and type II being the less severe elevation of coagulation factors.<ref>{{cite journal |author=Crowther MA, Kelton JG |title=Congenital thrombophilic states associated with venous thrombosis: a qualitative overview and proposed classification system |journal=Ann. Intern. Med. |volume=138 |issue=2 |pages=128-34|year=2003 |pmid=12529095 |doi= |url=http://www.annals.org/cgi/reprint/138/2/128}}</ref>
* Inherited vs. acquired
==Pathophysiology==
The Virchow's triad has been described classically as the patho-physiologic mechanism responsible for any thrombosis, which includes 3 components:
* [[Endothelial dysfunction]]
* [[Venous stasis]]
* [[Hypercoaguability]]
The mechanism of thrombophilia involves affecting the pathway of thrombosis<ref name="pmid11309638">{{cite journal |author=Seligsohn U, Lubetsky A |title=Genetic susceptibility to venous thrombosis |journal=N. Engl. J. Med. |volume=344 |issue=16 |pages=1222–31 |year=2001 |month=April |pmid=11309638 |doi=10.1056/NEJM200104193441607 |url=}}</ref>:
[[Image: Figure_thrombophilia_mechanism.jpg‎]]
Adapted from: N Engl J Med. 2001 Apr 19;344(16):1222-31.
==Epidemiology and Demographics==
===Prevalence of various inherited thrombophilias and their clinical impact===
{| border="1" cellpadding="5" cellspacing="0" align="center" class="sortable"
|-
  ! Disorder
  ! Healthy subjects/General population (%)
  ! Patients with known thrombosis (%)
  ! Estimated increase in thrombosis risk
|-
  | [[Antithrombin deficiency]]
  | 0.02
  | 1 - 4
  | 10 - 20X
|-
  | [[Dysfibrinogenemia]]
  | <1
  | <1
  | Variable
|-
  | [[Protein C deficiency]]
  | 0.2 - 0.4
  | 3 - 5
  | 10X
|-
  | [[Protein S deficiency]]
  | 0.3 - 0.13
  | 2 - 4
  | 10X
|-
  | [[Factor V Leiden]]
  | 1 - 15
  | 18 - 40
  | 5X
|-
  | G20210A [[prothrombin]] gene mutation
  | 2 - 5
  | 7 - 16
  | 3X
|-
  | [[Hyperhomocystenemia]]
  | 5
  | 10
  | 3X
|-
  | Elevated [[factor VIII]] levels
  | 11
  | 25
  | 5X
|-
|}
The table has been adapted from Best Pract Res Clin Obstet Gynaecol. 2003 Jun;17(3):397-411<ref name="pmid12787534">{{cite journal |author=Buchanan GS, Rodgers GM, Ware Branch D |title=The inherited thrombophilias: genetics, epidemiology, and laboratory evaluation |journal=Best Pract Res Clin Obstet Gynaecol |volume=17 |issue=3 |pages=397–411 |year=2003 |month=June |pmid=12787534 |doi= |url=}}</ref> and data has been obtained from references<ref name="pmid11309638">{{cite journal |author=Seligsohn U, Lubetsky A|title=Genetic susceptibility to venous thrombosis |journal=N. Engl. J. Med. |volume=344 |issue=16 |pages=1222–31 |year=2001 |month=April |pmid=11309638|doi=10.1056/NEJM200104193441607 |url=}}</ref><ref name="pmid11702218">{{cite journal |author=Franco RF, Reitsma PH |title=Genetic risk factors of venous thrombosis |journal=Hum. Genet. |volume=109 |issue=4 |pages=369–84 |year=2001 |month=October |pmid=11702218 |doi=10.1007/s004390100593 |url=}}</ref><ref name="pmid7740487">{{cite journal |author=Haverkate F, Samama M |title=Familial dysfibrinogenemia and thrombophilia. Report on a study of the SSC Subcommittee on Fibrinogen |journal=Thromb. Haemost. |volume=73 |issue=1 |pages=151–61 |year=1995 |month=January |pmid=7740487 |doi= |url=}}</ref>.
==Causes==
===Inherited===
Common types:
* G1691A mutation in factor V gene ([[Factor V Leiden|Factor V, Leiden type]]; 5% of the population are [[heterozygous]] for FVL)
* [[Prothrombin]] (factor II) mutation (G20210A, 5'UTR)
* Homozygous C677T mutation in the [[MTHFR]] gene
Rare forms:
* [[Plasminogen]] and [[fibrinolysis]] disorders
* [[Paroxysmal nocturnal hemoglobinuria]]
* [[Protein C deficiency]]
* [[Protein S deficiency]]
* [[Antithrombin|Antithrombin III]] deficiency
* [[Dysfibrinogenemia]]
* Homozygous [[homocystinuria]]
* Increased levels of factor VIII, factor IX, factor XI, or [[fibrinogen]].
===Acquired===
* [[Antiphospholipid antibodies]]
** [[anti-cardiolipin antibodies]] and/or
** [[lupus anticoagulant]]s
* [[Kidney|Renal disease]] (renal loss of antithrombin)
* High [[homocysteine]] levels due to vitamin deficiency (vitamins B6, B12 and folic acid).
* Immobility
* [[Pregnancy]] and [[puerperium]]
* [[Oral contraceptive pills]]
* [[Malignancy]]
* [[Obesity]]
* African American race
* [[Hormone replacement therapy]]
* Surgery and trauma
* Older age
* [[Myeloproliferative disorders]]
* Previous thrombosis
==Differential Diagnosis of Thrombophilia==
(By organ system)
{|style="width:75%; height:100px" border="1"
|style="height:100px"; style="width:25%" border="1" bgcolor="LightSteelBlue" | '''Cardiovascular'''
|style="height:100px"; style="width:75%" border="1" bgcolor="Beige" | • [[Cerebral vein thrombosis]] • [[Acute myocardial infarction]] • [[Deep vein thrombophlebitis]] • [[Portal vein thrombosis]] • [[Pelvic thrombophlebitis]]
|-
|-bgcolor="LightSteelBlue"
| '''Drug Side Effect'''
|bgcolor="Beige"| • [[Asparaginase]] • [[Bevacizumab]] • [[Combined oral contraceptive pill]] • [[Cyproterone]] • [[Diethylstilboestrol]] • [[Drospirenone]] • [[Eltrombopag]] • [[Erythropoietin]] • [[Ethinylestradiol]] • [[Fosfestrol]] • [[Granulocyte-macrophage colony stimulating factor]] • [[Heparin]] • [[Hormone replacement therapy]] • [[Lenalidomide]] • [[Peginesatide]] • [[Polyestradiol]] • [[Raloxifene]] • [[Strontium ranelate]] • [[Tamoxifen]] • [[Tobacco smoking]] • [[Tranexamic acid]] • [[Vorinostat]]
|-
|-bgcolor="LightSteelBlue"
| '''Endocrine'''
|bgcolor="Beige"| • [[Hyperosmolar non-ketotic diabetic coma]]
|-bgcolor="LightSteelBlue"
| '''Gastroenterologic'''
|bgcolor="Beige"| • Acute [[pancreatitis]] • [[Portal hypertension]]
|-
|-bgcolor="LightSteelBlue"
| '''Genetic'''
|bgcolor="Beige"| [[Congenital Dysfibrinogenemia]] • [[Factor II mutation]] • [[Hereditary thrombophlebitis]] • [[Antithrombin III deficiency]] • [[Factor V Leiden mutation]] • [[Protein C deficiency]] • [[Protein S deficiency]] • [[Klippel-Trenaunay syndrome]] • [[Klinefelter syndrome]] • [[Sickle cell disease]] • [[Carbohydrate-deficient glycoprotein syndrome type 1b]] • [[Factor XII deficiency]] • [[Haemoglobin SC disease]] • [[Hyperprothrombinemia 20210G-A]] • [[Plasminogen deficiency]] • [[Activated protein C resistance]] • [[CD59 antigen deficiency]] • [[Cystathionine beta-synthase deficiency]]
|-
|-bgcolor="LightSteelBlue"
| '''Hematologic'''
|bgcolor="Beige"|  • [[Polycythemia vera]] • [[Essential thrombocythemia]] • [[Myeloproliferative disease]] • [[Hyperviscosity]] syndrome • [[Paroxysmal Nocturnal Hemoglobinuria]] • [[Thrombocytosis]] • Raised homocysteine levels
|-
|-bgcolor="LightSteelBlue"
| '''Iatrogenic'''
|bgcolor="Beige"| • Surgical complication
|-
|-bgcolor="LightSteelBlue"
| '''Infectious Disease'''
|bgcolor="Beige"| • [[Intraperitoneal abscess]] • [[Acute peritonitis]] • [[Visceral abscess]] • [[Diverticulitis]] • [[Intravenous catheter infection]]
|-
|-bgcolor="LightSteelBlue"
| '''Musculoskeletal / Ortho'''
|bgcolor="Beige"| • Orthopedic surgeries • Abdominal surgery
|-
|-bgcolor="LightSteelBlue"
| '''Nutritional / Metabolic'''
|bgcolor="Beige"| • [[Cystathionuria]] • [[Homocystinuria]] • [[Methyltetrahydrofolate reductase deficiency]] • [[Metabolic Syndrome]] • [[Insulin resistance]] • [[Folic acid deficiency]] • [[Obesity]]
|-
|-bgcolor="LightSteelBlue"
| '''Obstetric/Gynecologic'''
|bgcolor="Beige"| • [[Pregnancy]] • [[Puerperium period]] • [[Ovarian hyperstimulation syndrome]]
|-
|-bgcolor="LightSteelBlue"
| '''Oncologic'''
|bgcolor="Beige"|  • [[Malignancy]] • [[Peritoneal metastasis]] • [[Adenocarcinoma of cecum]] • [[Adenocarcinoma of colon]] • Occult malignancy • [[Leukemia]] • [[Pancreatic cancer]] • [[Glucagonoma]]
|-
|-bgcolor="LightSteelBlue"
| '''Renal / Electrolyte'''
|bgcolor="Beige"| • [[Chronic renal failure]] • [[Paroxysmal Nocturnal Hemoglobinuria]] • [[Nephrotic syndrome]]
|-
|-bgcolor="LightSteelBlue"
| '''Rheum / Immune / Allergy'''
|bgcolor="Beige"|  • [[Antiphospholipid Syndrome]] • [[Circulating anticoagulant]] • [[Heparin induced thrombocytopenia]] • [[Inflammatory bowel disease]] • [[Crohn's disease]]• [[Behcet disease]] • [[Hughes-Stovin syndrome]] • [[Polyarteritis Nodosa]] • [[SLE]]
|-
|-bgcolor="LightSteelBlue"
| '''Trauma'''
|bgcolor="Beige"|  • [[Trauma]] • [[Abdominal trauma]]
|-
|-bgcolor="LightSteelBlue"
| '''Miscellaneous'''
|bgcolor="Beige"| • [[Paraneoplastic syndrome]] • [[Hypereosinophilic syndrome]] • [[Immobility]]
|-
|}
==Laboratory testing==
===Indications for screening===
Routine screening is not indicated in those individuals with an obvious acquired cause. For example, if the thrombosis is due to immobilisation after recent [[orthopedic surgery]], it is unlikely that an underlying cause is found. Comprehensive testing in any patient should include complete assessment of risk factors and its effect on long-term therapy. Some of the indications of further testing may include<ref name="pmid19289024">{{cite journal |author=Foy P, Moll S |title=Thrombophilia: 2009 update |journal=Curr Treat Options Cardiovasc Med |volume=11 |issue=2 |pages=114–28 |year=2009 |month=April |pmid=19289024 |doi= |url=}}</ref><ref name="pmid11309638">{{cite journal |author=Seligsohn U, Lubetsky A |title=Genetic susceptibility to venous thrombosis |journal=N. Engl. J. Med. |volume=344 |issue=16 |pages=1222–31 |year=2001 |month=April |pmid=11309638 |doi=10.1056/NEJM200104193441607 |url=}}</ref>:
* Unexplained venous thromboembolism at an age of less than 50 years
* Recurrent spontaneous thrombosis
* Unusual sites like portal, splenic, mesenteric, hepatic or renal veins
* Family history in first-degree relatives
* Recurrent pregnancy losses<ref>Dawood, F., Farquharson, R., Quenby, S.''Recurrent miscarriage.'' Current Obstetrics & Gynaecology, 2004; 14:247-253.</ref>
* Recurrence of venous thromboembolism while adequately anticoagulated
* Warfarin-induced skin necrosis
* Unexplained arterial thromboembolism in a younger patient without significant arteriosclerosis risk factors and no cardioembolic source
===Timing===
The timing of tests is very important as it influences the levels of various thrombogenic factors in the body.
* Testing at the time of acute venous thrombosis is not indicated or during ongoing anti-coagulation.
* Best time to test is 4 weeks after completion of anticoagulation.
* Avoid intercurrent severe illness
* Pregnancy, oral contraceptives, hormone replacement therapy and cancer chemotherapy may also affect some tests.
* Factor V Leiden and Prothrombin mutation can be done in patients on anticoagulants and even in acute phase, as these are PCR tests. However, other tests can be done only at a later stage to rule out two disorders.
===Type of tests===
Tests for thrombophilia are categorized according to their priority, as discussed below:
'''1. General tests:''' These include [[prothrombin time]], INR, and [[partial thromboplastin time]].
'''2. High priority tests:''' 
* Activated protein C resistance
* Factor V Leiden (Homozygosity or heterozygosity)
* Prothrombin gene mutation (G20210A)
* Homocysteine levels
* Factor VIII
* Lupus anticoagulant
'''3. Intermediate priority'''
* Protein C activity
* Protein S activity
* Antithrombin activity
* Anticardiolipin antibodies
'''4. Low priority'''
* Thrombin time
* Fibrinogen levels
* Factor IX activity
* Factor X activity
* [[MTHR]] gene
* '''High priority and intermediate priority tests''' should be performed in those with an unprovoked thrombotic event and have a recurrent event, cerebral-or visceral thrombosis, stillbirth, three or more unexplained spontaneous abortions, family history of venous thrombosis, or are younger than 45 years.
* '''High priority tests''' only should be conducted in those who have a first unprovoked event, age > 45 years, event provoked by pregnancy/puerperium/use of oral contraceptives or hormone-replacement therapy, proximal-vein thrombosis, pulmonary embolism, or both provoked by surgery, trauma, or immobilization.
* It is recommended that all these patients be treated with anticoagulation for at least 6 months, unless contraindicated.
==Treatment==
The treatment algorithm for various thrombophilias is presented below:
[[Image: Figure_Thrombophilia_treatment.jpg]]
The figure has been adapted from Seligsohn ''et al''. N Engl J Med. 2001 Apr 19;344(16):1222-31.<ref name="pmid11309638">{{cite journal |author=Seligsohn U, Lubetsky A |title=Genetic susceptibility to venous thrombosis |journal=N. Engl. J. Med. |volume=344 |issue=16 |pages=1222–31 |year=2001 |month=April |pmid=11309638 |doi=10.1056/NEJM200104193441607 |url=}}</ref>
==References==
{{Reflist|2}}


[[Category:Hematology]]
[[Category:Hematology]]

Revision as of 13:25, 21 September 2012