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Hemophilia

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Sabawoon Mirwais, M.B.B.S, M.D.[2]Vahid Eidkhani, M.D.Fahd Yunus, M.D. [3]

Synonyms and keywords: Haemophilia, hemophilia, Bleeder’s disease

Overview

Overview

Hemophilia is considered a very old disease with its history dating back to the 2nd century AD. The first modern descriptions of the condition appeared during the 19th century. Extensive work has been done over the centuries regarding the classification, inheritance pattern, and treatment of hemophilia. Hemophilia may be classified into three sub-types based on the lack of functional clotting factors: hemophilia A , hemophilia B, hemophilia C. It can also be divided into different categories based on the severity of the condition. Hemophilia can also be acquired in the setting of antibodies directed against the clotting factors. Hemophilia is a genetic bleeding disorder resulting from the insufficient levels of clotting factors in the body. The clotting factors irregularity causes a lack of clumping of blood required to form a clot to plug a site of a wound. The genes involved in the pathogenesis of hemophilia include the F8 gene in hemophilia A, F9 gene in hemophilia B, and F11 gene in C. Hemophilia predominantly affects the male population but the sub-type hemophilia C, with an autosomal inheritance pattern, can affect the males as well as females. Hemophilia A, B, and C are caused by mutations in F8, F9, and F11 genes respectively. It can also occur as a result of autoantibodies directed against the clotting factors. Hemophilia must be differentiated from other diseases leading to spontaneous bleeding and bleeding following injuries or surgery such as von Willebrand disease, hepatic failure, thrombocytopenia, vitamin K deficiency, disseminated intravascular coagulation, uremia, congenital afibrinogenemia, factor V deficiency, factor X deficiency as seen in amyloid purpura, glanzmann’s thrombasthenia, Bernard-Soulier syndrome, factor XII deficiency and C1-inhibitor (C1INH) deficiency. The prevalence of hemophilia is estimated to be 20,000 cases in the United States annually. The age-adjusted prevalence of hemophilia in six US states (Oklahoma, Massachusetts, Colorado, Georgia, Louisiana, and New York) in 1994 was 13.4 cases per 100, 000 males. The incidence of hemophilia is estimated to be 1 in 5,000 male births for hemophilia A and 1 in 30,000 births for hemophilia B. The most potent risk factor in the development of hemophilia is the family history of hemophilia. Other risk factors include male sex and malignancies. Initial screening blood investigations for any child with suspected bleeding disorder include platelet count, prothrombin time (PT), activated partial thromboplastin time (aPTT), and fibrinogen test. Chorionic villus sampling at 11-14 weeks of gestation can be performed for the genetic diagnosis of hemophilia. Hemophilia can present with a bleeding episode during the neonatal period that is difficult to manage or it can present with signs and symptoms of concealed bleeding into the joint or viscera. If left untreated, hemophilia can result in complications involving multiple organs and in severe bleeding episodes it can result in death. Hemophilia patients can lead an active and healthy life and life expectancy depends on the treatment response and the presence of comorbidities. Complications of hemophilia include AIDS, hepatitis, Vitamin D deficiency, osteoporosis, and renal pathologies. Coagulation tests and coagulation assays are the gold standard for the diagnosis of hemophilia. Prolonged activated partial thromboplastin time (aPTT), normal prothrombin time (PT), prolonged bleeding time (BT), and normal fibrinogen concentration are diagnostic of hemophilia. Coagulation tests should be followed by measuring the clotting factors level by coagulation assays. Once the coagulation discrepancy has been established, individual clotting factor assay can be performed to determine the deficient/absent clotting factor. Bethesda assay can be performed in the case of acquired hemophilia to detect and quantify antibodies directed against factor VIII. Patients with hemophilia can present with a history of excessive bleeding after minor injuries or spontaneous bleeding. They can also report family history of hemophilia. Hemophilia when mild, can be asymptomatic. Common symptoms, when present, include epistaxis, oral mucosal bleeding, joint pain and swelling, lethargy and fatigue, excessive bleeding after dental procedures, prolonged bleeding after circumcision and muscle hematoma after vaccination. Patients with hemophilia usually appear normal. Physical examination of patients with hemophilia is usually remarkable for tachycardia, pallor, bruising, abdominal pain and distension, hypotension, and muscle or joint swelling. Laboratory findings consistent with the diagnosis of hemophilia include normal prothrombin time (PT), prolonged activated partial thromboplastin time (aPTT), prolonged bleeding time (BT), and normal platelet count. There are no ECG findings associated with hemophilia. An x-ray of the joints in the case of hemophilic arthropathy may be helpful in the diagnosis of hemophilia. Pettersson scoring system, designed in 1980, is widely applied for the classification of osteochondral changes of hemophilic arthropathy in elbows, knees, and ankles. This scoring system is based on typical findings of hemophilic arthropathy on posterioranterior and lateral x-rays. Arnold-Hilgartner classification is also a plain radiograph grading system for hemophilic arthropathy. CT scan may be helpful in the diagnosis of hemophilia. Findings on CT scan suggestive of hemophilia include muscle, intracranial, and intraabdominal hematomas, hemophilic pseudotumor, intracranial hemorrhage, muscle ossification, and pseudoaneurysm following arterial trauma. MRI may be helpful in the diagnosis of hemophilia. Findings on MRI suggestive of hemophilic arthropathy include effusion, synovial hypertrophy, erosion, subchondral cyst, cartilage loss, osteonecrosis, fibrocartilage tear, ligament tear, loose body. There are no echocardiography findings associated with hemophilia. Ultrasound may be helpful in the diagnosis and follow-up of hemophilic arthropathy and in diagnosing massive intraabdominal bleeds. Findings on an ultrasound suggestive of hemophilic arthropathy inlcude soft-tissue changes, osteochondral changes, joint effusion, synovial hypertrophy, hemosiderin, and osteochondral abnormalities. There are no other imaging findings associated with hemophilia. There are no other diagnostic studies associated with hemophilia. Clotting factor replacement is the mainstay of hemophilia treatment. Plasma-derived factor concentrates and recombinant factor concentrates are the two types used in the replacement therapy. Other products used as therapy include desmopressin acetate, antifibrinolytics, and cryoprecipitate. Gene therapy has the potential to change the course of hemophilia therapy and care. Surgery is not recommended for the treatment of hemophilia. Primary prevention of hemophilia encompasses measures taken to raise awareness regarding the genetics of the disease and the genetic transmission of the condition. Having an X-linked mode of transmission, genetic counselling in female carriers and awareness are the main focus for the primary prevention of hemophilia. Effective measures for the secondary prevention of hemophilia include avoidance of invasive fetal monitoring of a hemophilic fetus, avoidance of operative vaginal delivery, administration of vitamin K injection with care, availability of the factor concentrate at the time of delivery, infusion of factor VIII or IX concentrate at least once weekly for ≥ 45 weeks per year, and the use of e-Diaries to improve record keeping of hemophilia patients’ home treatment and bleeding episodes.

Historical Perspective

Hemophilia is considered a very old disease with its history dating back to the 2nd century AD. The first modern descriptions of the condition appeared during the 19th century. Extensive work has been done over the centuries regarding the classification, inheritance pattern, and treatment of hemophilia.

Classification

Hemophilia may be classified into three sub-types based on the lack of functional clotting factors: hemophilia A , hemophilia B, hemophilia C. It can also be divided into different categories based on the severity of the condition. Hemophilia can also be acquired in the setting of antibodies directed against the clotting factors.

Pathophysiology

Hemophilia is a genetic bleeding disorder resulting from the insufficient levels of clotting factors in the body. The clotting factors irregularity causes a lack of clumping of blood required to form a clot to plug a site of a wound. The genes involved in the pathogenesis of hemophilia include the F8 gene in hemophilia A, F9 gene in hemophilia B, and F11 gene in C. Hemophilia predominantly affects the male population but the sub-type hemophilia C, with an autosomal inheritance pattern, can affect the males as well as females.

Causes

Hemophilia A, B, and C are caused by mutations in F8, F9, and F11 genes respectively. It can also occur as a result of autoantibodies directed against the clotting factors.

Differentiating Hemophilia from other diseases

Hemophilia must be differentiated from other diseases leading to spontaneous bleeding and bleeding following injuries or surgery such as von Willebrand disease, hepatic failure, thrombocytopenia, vitamin K deficiency, disseminated intravascular coagulation, uremia, congenital afibrinogenemia, factor V deficiency, factor X deficiency as seen in amyloid purpura, glanzmann’s thrombasthenia, Bernard-Soulier syndrome, factor XII deficiency and C1-inhibitor (C1INH) deficiency.

Epidemiology and Demographics

The prevalence of hemophilia is estimated to be 20,000 cases in the United States annually. The age-adjusted prevalence of hemophilia in six US states (Oklahoma, Massachusetts, Colorado, Georgia, Louisiana, and New York) in 1994 was 13.4 cases per 100, 000 males. The incidence of hemophilia is estimated to be 1 in 5,000 male births for hemophilia A and 1 in 30,000 births for hemophilia B.

Risk Factors

The most potent risk factor in the development of hemophilia is the family history of hemophilia. Other risk factors include male sex and malignancies.

Screening

Initial screening blood investigations for any child with suspected bleeding disorder include platelet count, prothrombin time (PT), activated partial thromboplastin time (aPTT), and fibrinogen test. Chorionic villus sampling at 11-14 weeks of gestation can be performed for the genetic diagnosis of hemophilia.

Natural History, Complications and Prognosis

Hemophilia can present with a bleeding episode during the neonatal period that is difficult to manage or it can present with signs and symptoms of concealed bleeding into the joint or viscera. If left untreated, hemophilia can result in complications involving multiple organs and in severe bleeding episodes it can result in death. Hemophilia patients can lead an active and healthy life and life expectancy depends on the treatment response and the presence of comorbidities. Complications of hemophilia include AIDS, hepatitis, Vitamin D deficiency, osteoporosis, and renal pathologies.

Diagnosis

Diagnostic Study of Choice

Coagulation tests and coagulation assays are the gold standard for the diagnosis of hemophilia. Prolonged activated partial thromboplastin time (aPTT), normal prothrombin time (PT), prolonged bleeding time (BT), and normal fibrinogen concentration are diagnostic of hemophilia. Coagulation tests should be followed by measuring the clotting factors level by coagulation assays. Once the coagulation discrepancy has been established, individual clotting factor assay can be performed to determine the deficient/absent clotting factor. Bethesda assay can be performed in the case of acquired hemophilia to detect and quantify antibodies directed against factor VIII.

History and Symptoms

Patients with hemophilia can present with a history of excessive bleeding after minor injuries or spontaneous bleeding. They can also report family history of hemophilia. Hemophilia when mild, can be asymptomatic. Common symptoms, when present, include epistaxis, oral mucosal bleeding, joint pain and swelling, lethargy and fatigue, excessive bleeding after dental procedures, prolonged bleeding after circumcision and muscle hematoma after vaccination.

Physical Examination

Patients with hemophilia usually appear normal. Physical examination of patients with hemophilia is usually remarkable for tachycardia, pallor, bruising, abdominal pain and distension, hypotension, and muscle or joint swelling.

Laboratory Findings

Laboratory findings consistent with the diagnosis of hemophilia include normal prothrombin time (PT), prolonged activated partial thromboplastin time (aPTT), prolonged bleeding time (BT), and normal platelet count.

Electrocardiogram

There are no ECG findings associated with hemophilia.

X-ray

An x-ray of the joints in the case of hemophilic arthropathy may be helpful in the diagnosis of hemophilia. Pettersson scoring system, designed in 1980, is widely applied for the classification of osteochondral changes of hemophilic arthropathy in elbows, knees, and ankles. This scoring system is based on typical findings of hemophilic arthropathy on posterioranterior and lateral x-rays. Arnold-Hilgartner classification is also a plain radiograph grading system for hemophilic arthropathy.

CT scan

CT scan may be helpful in the diagnosis of hemophilia. Findings on CT scan suggestive of hemophilia include muscle, intracranial, and intraabdominal hematomas, hemophilic pseudotumor, intracranial hemorrhage, muscle ossification, and pseudoaneurysm following arterial trauma.

MRI

MRI may be helpful in the diagnosis of hemophilia. Findings on MRI suggestive of hemophilic arthropathy include effusion, synovial hypertrophy, erosion, subchondral cyst, cartilage loss, osteonecrosis, fibrocartilage tear, ligament tear, loose body.

Echocardiography/Ultrasound

There are no echocardiography findings associated with hemophilia. Ultrasound may be helpful in the diagnosis and follow-up of hemophilic arthropathy and in diagnosing massive intraabdominal bleeds. Findings on an ultrasound suggestive of hemophilic arthropathy inlcude soft-tissue changes, osteochondral changes, joint effusion, synovial hypertrophy, hemosiderin, and osteochondral abnormalities.

Other Imaging Findings

There are no other imaging findings associated with hemophilia.

Other Diagnostic Studies

There are no other diagnostic studies associated with hemophilia.

Treatment

Medical Therapy

Clotting factor replacement is the mainstay of hemophilia treatment. Plasma-derived factor concentrates and recombinant factor concentrates are the two types used in the replacement therapy. Other products used as therapy include desmopressin acetate, antifibrinolytics, and cryoprecipitate. Gene therapy has the potential to change the course of hemophilia therapy and care.

Surgery

Surgical intervention is not recommended for the management of hemophilia.

Primary Prevention

Primary prevention of hemophilia encompasses measures taken to raise awareness regarding the genetics of the disease and the genetic transmission of the condition. Having an X-linked mode of transmission, genetic counselling in female carriers and awareness are the main focus for the primary prevention of hemophilia.

Secondary Prevention

Effective measures for the secondary prevention of hemophilia include avoidance of invasive fetal monitoring of a hemophilic fetus, avoidance of operative vaginal delivery, administration of vitamin K injection with care, availability of the factor concentrate at the time of delivery, infusion of factor VIII or IX concentrate at least once weekly for ≥ 45 weeks per year, and the use of e-Diaries to improve record keeping of hemophilia patients’ home treatment and bleeding episodes.

References

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Historical Perspective

Historical Perspective

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1];Associate Editor(s)-in-Chief: Sabawoon Mirwais, M.B.B.S, M.D.[2]

Overview

Hemophilia is considered a very old disease with its history dating back to the 2nd century AD. The first modern descriptions of the condition appeared during the 19th century. Extensive work has been done over the centuries regarding the classification, inheritance pattern, and treatment of hemophilia.

Historical Perspective

Discovery

  • References to a condition associated with bleeding and suggestive of hemophilia date back to the 2nd century AD.[1][2]
  • Ancient religious script compilations, such as The Babylonian Tarmud, have also mentioned the condition along with relative fatal bleeding episode prevention.[2][3]
  • Abu Qasim Khalaf Ibn Abbas Al Zahrawi, a pioneer of modern surgery, known in the West as Albucasis or Zahravius, described suspected hemophilia cases in the 10th century.
  • G. W. Consbruch of Bielefeld, Germany, described a bleeding disease very similar to hemophilia in 1793.
  • Dr John Conrad Otto, an American physician, takes the credit for the first modern description of hemophilia in 1803. He described a bleeding disorder, transmitted via unaffected females and affecting only males. His work was published under the title “An account of an hemorrhagic disposition existing in certain families”.[4]
  • In 1813, John F. Hay published his first analysis of a hemophilia family tree in the New England Journal of Medicine.[3]
  • Christian Friedrich Nasse, a German physician and psychiatrist, described the genetics of hemophilia in 1820 and his work resulted in Nasse’s law, which states that hemophilia is transmitted entirely by unaffected females to their sons.[5]
  • A German physician, Johann Lukas Schönlein and his student Friedrich Hopff, documented the word “hemophilia” for the first time in 1828 and the condition was described in his dissertation with the title “About hemophilia or the hereditary predisposition to fatal bleeding”.[6]
  • Nasse’s law prompted further scientific debate leading to publications by J. Grandidier in 1855, John Wickham Legg in 1872, and Hermann Immermann in 1879.[3]
  • The analysis of a hemophilia family tree by John F. Hay was followed by the analyses from Sir William Osler in 1885, Kathleen P. Pratt in 1908, F. Koller and his group in 1954, and Victor A. Mckusick and Samuel I. Rapaport in 1962.
  • William Bulloch and Paul Gordon Fildes published a detailed description of the early history of hemophilia in 1912 under the title “Treasury of human inheritance“.[7]

Discovery of the Antihemophilic Globulin

  • A. E. Wright was the first who documented the prolonged clotting time of hemophilic blood in a capillary tube in 1893.[8]
  • In 1908, P. Morawitz and J. Lossen proposed a deficiency in thrombokinase associated with hemophilia and disproved the association with calcium deficiency.[8]
  • In 1911, T. Addis investigated several blood and tissue factors and concluded that the hemophilic blood has defective prothrombin.[9]
  • In 1931, P. Govaerts and A. Gatia proposed that the platelets from hemophilic blood behaved normally when shifted to normal plasma. This finding hinted towards a deficiency in the plasma.[3]
  • In 1934, S. Van Creveld demonstrated that a “dispersed protein” fraction obtained from the serum decreased the clotting time of hemophilic blood.[10]
  • In 1936, A.J. Patek and F.H.L. Taylor proposed in their publication in Science that in normal blood and in citrated normal plasma rendered free from platelets by Berkefeld filtration, a substance was identified which, in small quantities, reduced the clotting time of hemophilic blood. Between 1936 and 1946, this research group published multiple papers supporting their original hypothesis[11][12]
  • A.J. Quick, M. Stanley-Brown, F.W. Bancroft solved the question of whether prothrombin or one of its derivatives is the deficient factor in hemophilia. They concluded that the hemophilic blood has a normal prothrombin content.[13]
  • In 1939, Brinkhous et al. confirmed A.J. Quick’s findings and showed that the hemophilic blood has a delayed prothrombin conversion rate.[14]
  • In 1947, A.j. Quick and K.M. Brinkhous independently demonstrated that the antihemophilic globulin and platelets react together in a fashion to generate thromboplastin. They also proposed that a deficiency in antihemophilic globulin caused defective coagulation due to defects in the generation of thromboplastin.[15][14]

Landmark Events in the Development of Treatment Strategies

Transfusion Medicine

Evolution of the Treatment Strategies
Year Therapy
1840
1911
1916
1934
1935
1936
1946
  • “Antihemophilic globulin” introduced as a term[27][28]
1953
1958
1965

Clotting Factor Concentrates and its Evolution to Modern Treatment
Year Therapy
1981
1990
1992
  • The first recombinant factor VIII product is introduced and registered
2004 – current
  • Developmental breakthroughs in the recombinant factor VIII products

Famous Cases

Hemophilia has been called “the disease of the kings” or “the royal disease” as several members of the European royal family have been affected by it.[31] The following are a few famous cases of hemophilia:

  • The Queen of England, Queen Victoria (1837–1901), was a carrier of hemophilia and she passed it onto her son, Leopold, who died of a brain hemorrhage when he was 31.[31]
  • The disease spread to other royal families in Germany, Russia and Spain through Queen Victoria’s two daughters.
  • The best known case of “the royal disease” was Tsarevich Alexei, son of the Russian Czar Nicholas II.

References

  1. Brinkhous, K. M. (1975). Handbook of hemophilia. Amsterdam New York: Excerpta Medica Sole distributors for the U.S.A. and Canada, American Elsevier Pub. Co. ISBN 9789021920962.
  2. 2.0 2.1 Rosendaal FR, Smit C, Briët E (February 1991). “Hemophilia treatment in historical perspective: a review of medical and social developments”. Ann. Hematol. 62 (1): 5–15. PMID 1903310.
  3. 3.0 3.1 3.2 3.3 Ingram, G. I. C. (1997). “The history of haemophilia*,†”. Haemophilia. 3 (S1): 5–15. doi:10.1111/j.1365-2516.1997.tb00168.x. ISSN 1351-8216.
  4. Otto JC (July 1996). “An account of an hemorrhagic disposition existing in certain families”. Clin. Orthop. Relat. Res. (328): 4–6. PMID 8653976.
  5. Brinkhous, K. M. (1975). Handbook of hemophilia. Amsterdam New York: Excerpta Medica Sole distributors for the U.S.A. and Canada, American Elsevier Pub. Co. ISBN 9789021920962.
  6. Krieger, Marie (1920). Über die Atrophie der Menschlichen Organe bei Inanition. Berlin, Heidelberg: Springer Berlin Heidelberg Imprint Springer. ISBN 3662229374.
  7. Francis, Sir, Bulloch, William (1909). Treasury of human inheritance. London: Cambridge University Press.
  8. 8.0 8.1 Wright AE (July 1893). “On a Method of Determining the Condition of Blood Coagulability for Clinical and Experimental Purposes, and on the Effect of the Administration of Calcium Salts in Haemophilia and Actual or Threatened Haemorrhage: [Preliminary Communication]”. Br Med J. 2 (1700): 223–5. PMC 2422001. PMID 20754381.
  9. 9.0 9.1 Addis, T. (1911). “The pathogenesis of hereditary hæmophilia”. The Journal of Pathology and Bacteriology. 15 (4): 427–452. doi:10.1002/path.1700150402. ISSN 0368-3494.
  10. 10.0 10.1 10.2 Creveld, S.; Jordan, F. L. J.; Punt, K. (2009). “Deficiency ot Anti-Hemophilic Factor in a Woman, Combined with a Disturbance in Vascular Function.1”. Acta Medica Scandinavica. 151 (5): 381–389. doi:10.1111/j.0954-6820.1955.tb10306.x. ISSN 0001-6101.
  11. “Commentary on and reprint of Patek AJ Jr, Taylor FHL, Hemophilia. II. Some properties of substances obtained from human plasma effective in accelerating coagulation of hemophiliac blood, in Journal of Clinical Investigation (1937) 16:113–124”. 2000: 573–585. doi:10.1016/B978-012448510-5.50144-8.
  12. Hynes HE, Owen CA, Bowie EJ, Thompson JH (March 1969). “Development of the present concept of hemophilia”. Mayo Clin. Proc. 44 (3): 193–206. PMID 4887314.
  13. Pisciotta AV (August 1980). “Concepts of haemostasis and thrombosis: A study of the coagulation defect in hemophilia and in jaundice (Quick, Stanley-Brown and Bancroft 1935). Armand J. Quick (1894-1978)–a short biography”. Thromb. Haemost. 44 (1): 1–5. PMID 6999657.
  14. 14.0 14.1 Brinkhous, K. M. (1947). “Clotting Defect in Hemophilia: Deficiency in a Plasma Factor Required for Platelet Utilization”. Experimental Biology and Medicine. 66 (1): 117–120. doi:10.3181/00379727-66-16003. ISSN 1535-3702.
  15. QUICK AJ (September 1947). “Studies on the enigma of the hemostatic dysfunction of hemophilia”. Am. J. Med. Sci. 214 (3): 272–80. PMID 20263163.
  16. 16.0 16.1 Lane, Samuel (1840). “HÆMORRHAGIC DIATHESIS”. The Lancet. 35 (896): 185–188. doi:10.1016/S0140-6736(00)40031-0. ISSN 0140-6736.
  17. Bergmann, E. v. (2013). Die Schicksale der Transfusion im Letzten Decennium : Rede, Gehalten zur Feier des Stiftungstages der Militärärztlichen Bildungsanstalten am 2. August 1883. Berlin: Springer Berlin Heidelberg. ISBN 9783642619298.
  18. Ringer, Sydney (1882). “Regarding the Action of Hydrate of Soda, Hydrate of Ammonia, and Hydrate of Potash on the Ventricle of the Frog’s Heart”. The Journal of Physiology. 3 (3–4): 195–202. doi:10.1113/jphysiol.1882.sp000095. ISSN 0022-3751.
  19. Tan, SY; Graham, C (2013). “Karl Landsteiner (1868–1943): Originator of ABO blood classification”. Singapore Medical Journal. 54 (5): 243–244. doi:10.11622/smedj.2013099. ISSN 0037-5675.
  20. “Commentary on and reprint of Landsteiner K, Ueber Agglutinationserscheinungen normalen menschlichen Blute [On the agglutination of normal human blood], in Wiener Klinische Wochenschrift (1901) 14:1132–1134”. 2000: 769–775. doi:10.1016/B978-012448510-5.50165-5.
  21. Eckhardt, Christian (1988). Transfusionsmedizin : Grundlagen · Therapie · Methodik. Berlin, Heidelberg: Springer Berlin Heidelberg Imprint Springer. ISBN 9783662106020.
  22. Ottenberg, Reuben; Kaliski, David (2009). “Die Gefahren der Transfusionen und deren Verhütung”. DMW – Deutsche Medizinische Wochenschrift. 39 (46): 2243–2247. doi:10.1055/s-0028-1128886. ISSN 0012-0472.
  23. 23.0 23.1 Addis, T. (1916). “The effect of intravenous injections of fresh human serum and of phosphated blood, on the coagulation time of the blood in hereditary hemophila”. Experimental Biology and Medicine. 14 (1): 19–23. doi:10.3181/00379727-14-14. ISSN 1535-3702.
  24. 24.0 24.1 Bendien, W. M. (1937). “INVESTIGATIONS ON HEMOPHILIA”. Archives of Pediatrics & Adolescent Medicine. 54 (4): 713. doi:10.1001/archpedi.1937.01980040017002. ISSN 1072-4710.
  25. Macfarlane, R.G.; Barnett, Burgess (1934). “THE HÆMOSTATIC POSSIBILITIES OF SNAKE-VENOM”. The Lancet. 224 (5801): 985–987. doi:10.1016/S0140-6736(00)43846-8. ISSN 0140-6736.
  26. “Commentary on and reprint of Patek AJ Jr, Taylor FHL, Hemophilia. II. Some properties of substances obtained from human plasma effective in accelerating coagulation of hemophiliac blood, in Journal of Clinical Investigation (1937) 16:113–124”. 2000: 573–585. doi:10.1016/B978-012448510-5.50144-8.
  27. Minot GR, Davidson CS, Lewis JH, Tagnon HJ, Taylor FH (September 1945). “THE COAGULATION DEFECT IN HEMOPHILIA: THE EFFECT, IN HEMOPHILIA, OF THE PARENTERAL ADMINISTRATION OF A FRACTION OF THE PLASMA GLOBULINS RICH IN FIBRINOGEN”. J. Clin. Invest. 24 (5): 704–7. doi:10.1172/JCI101654. PMC 435506. PMID 16695264.
  28. Taylor FH, Davidson CS, Tagnon HJ, Adams MA, Macdonald AH, Minot GR (September 1945). “STUDIES IN BLOOD COAGULATION: THE COAGULATION PROPERTIES OF CERTAIN GLOBULIN FRACTIONS OF NORMAL HUMAN PLASMA IN VITRO”. J. Clin. Invest. 24 (5): 698–703. doi:10.1172/JCI101653. PMC 435505. PMID 16695263.
  29. Nilsson, I. M.; Berntorp, E.; Löfqvist, T.; Pettersson, H. (1992). “Twenty-five years’ experience of prophylactic treatment in severe haemophilia A and B”. Journal of Internal Medicine. 232 (1): 25–32. doi:10.1111/j.1365-2796.1992.tb00546.x. ISSN 0954-6820.
  30. Pool, Judith Graham; Shannon, Angela E. (1965). “Production of High-Potency Concentrates of Antihemophilic Globulin in a Closed-Bag System”. New England Journal of Medicine. 273 (27): 1443–1447. doi:10.1056/NEJM196512302732701. ISSN 0028-4793.
  31. 31.0 31.1 Ingram, G I (1976). “The history of haemophilia”. Journal of Clinical Pathology. 29 (6): 469–479. doi:10.1136/jcp.29.6.469. ISSN 0021-9746.

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Classification

Classification

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1];Associate Editor(s)-in-Chief: Sabawoon Mirwais, M.B.B.S, M.D.[2]Simrat Sarai, M.D. [3]

Overview

Hemophilia may be classified into three sub-types based on the lack of functional clotting factors: hemophilia A , hemophilia B, hemophilia C. It can also be divided into different categories based on the severity of the condition. Hemophilia can also be acquired in the setting of antibodies directed against the clotting factors.

Classification

  • Hemophilia may be classified into:

1. Hemophilia A: A recessive X-linked genetic disorder involving a lack of functional clotting factor VIII and representing approximately 80% of hemophilia cases.[1]
2. Hemophilia B: A recessive X-linked genetic disorder involving a lack of functional clotting factor IX and comprising approximately 20% of hemophilia cases.[1]
3. Hemophilia C: An autosomal genetic disorder involving a lack of functional clotting factor XI. This condition is not completely recessive, as heterozygous individuals also show increased bleeding.[2]
4. Acquired Hemophilia: An acquired condition resulting from autoantibodies directed against the clotting factors. This usually occurs in the setting of a malignancy.[3]

Classification Based on Severity
Severity Levels of Factor VIII

or IX in the blood

Normal (as in a person who does not have hemophilia) 50% to 100%
Mild Greater than 5% but less than 50%
Moderate 1% to 5%
Severe Less than 1%
Adapted from CDC Hemophilia Diagnosis> “CDC Hemophilia Diagnosis”.

References

  1. 1.0 1.1 Santagostino E, Fasulo MR (October 2013). “Hemophilia a and hemophilia B: different types of diseases?”. Semin. Thromb. Hemost. 39 (7): 697–701. doi:10.1055/s-0033-1353996. PMID 24014073.
  2. Shearin-Patterson T, Davidson E (April 2013). “Hemophilia C”. JAAPA. 26 (4): 50. PMID 23610841.
  3. Napolitano M, Siragusa S, Mancuso S, Kessler CM (January 2018). “Acquired haemophilia in cancer: A systematic and critical literature review”. Haemophilia. 24 (1): 43–56. doi:10.1111/hae.13355. PMID 28960809.
  4. “CDC Hemophilia classification”.

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Pathophysiology

Pathophysiology


Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1];Associate Editor(s)-in-Chief: Sabawoon Mirwais, M.B.B.S, M.D.[2]Fahd Yunus, M.D. [3]

Overview

Hemophilia is a genetic bleeding disorder resulting from the insufficient levels of clotting factors in the body. The clotting factors irregularity causes a lack of clumping of blood required to form a clot to plug a site of a wound. The genes involved in the pathogenesis of hemophilia include the F8 gene in hemophilia A, F9 gene in hemophilia B, and F11 gene in C. Hemophilia predominantly affects the male population but the sub-type hemophilia C, with an autosomal inheritance pattern, can affect the males as well as females.

Pathophysiology

Physiology

The normal physiology of hemostasis can be summarized as follows:

1. Primary hemostasis

2. Secondary hemostasis

3. Fibrinolysis

Cell-Based Model of Coagulation

a. Initiation

b. Amplification

c. Propagation

Pathogenesis

  • Mild (factor level > 0.05–0.40 IU/mL)
  • Moderate (factor level = 0.01–0.05 IU/mL)
  • Severe (factor level < 0.01 IU/mL)

Hemophilia A

  1. Classic mutations in the F8 gene that cause structural changes in the FVIII molecule or even produce a truncated protein lacking essential functional domains.[18][19]
  2. Mutations in proteins that interact intracellularly in the correct folding and trafficking of the FVIII protein or mutations in extracellular plasma proteins such as von Willebrand factor (VWF).[20][21][22][23]
  3. The third category encompasses patients who have the clinical disease but have no mutations in the F8 gene or in any of the known interacting partners.[16]

Hemophilia B

Hemophilia C

Genetics

Hemophilia A

Hemophilia B

Hemophilia C

Associated Conditions

  • Hemophilia can be associated with the following conditions:

Gross Pathology

On gross pathology, hemophilia is characterized by the following findings:

Microscopic Pathology

On microscopic histopathological analysis, hemophilia can be characterized by the following findings:

References

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  6. Favaloro, Emmanuel (2017). Hemostasis and thrombosis : methods and protocols. New York: Humana Press Springer. ISBN 9781493971961.
  7. Favaloro, Emmanuel (2017). Hemostasis and thrombosis : methods and protocols. New York: Humana Press Springer. ISBN 9781493971961.
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Template:WH Template:WS

Differentiating Hemophilia from other Diseases

Differentiating Hemophilia from other Diseases

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Sabawoon Mirwais, M.B.B.S, M.D.[2]Simrat Sarai, M.D. [3]Vahid Eidkhani, M.D.Fahd Yunus, M.D. [4]

Overview

Hemophilia must be differentiated from other diseases leading to spontaneous bleeding and bleeding following injuries or surgery such as von Willebrand disease, hepatic failure, thrombocytopenia, vitamin K deficiency, disseminated intravascular coagulation, uremia, congenital afibrinogenemia, factor V deficiency, factor X deficiency as seen in amyloid purpura, glanzmann’s thrombasthenia, Bernard-Soulier syndrome, factor XII deficiency and C1-inhibitor (C1INH) deficiency.

Differentiating Hemophilia from other Diseases

Hemophilia must be differentiated from other diseases leading to spontaneous bleeding and bleeding following injuries or surgery such as:

The most important differential diagnoses are enlisted in the table below:[24][25][26][27][28][29][30]

Diseases Clinical Manifestations Para-clinical Findings Additional Findings
Symptoms Physical Examination
Lab Findings
Joint Bleeding Gastrointestinal Bleeding Genitourinary Bleeding Skin Bruises Skeletal Deformity Muscle Hematoma CBC PT PTT BT Factor VIII Factor IX Fibrinogen U/A:RBC S/E:RBC
Hemophilia A + + + + + + N N N N N + + -/+Family history
Hemophilia B + + + + + + N N N N N + + -/+Family history
von Willebrand disease -/+ -/+ -/+ -/+ -/+ -/+ N N ↑/N ↓/N N N -/+ -/+ -/+Family history
Vitamin K deficiency -/+ + -/+ + -/+ N ↑/N N N N + + Mostly in infants/GI disorders
Warfarin Toxicity -/+ + -/+ + -/+ N ↑/N N N N + + +Drug history
Platelets disorders -/+ -/+ + ↓Plt N N N N N -/+ -/+ Cause-based specific findings
Liver Failure + + -/+ -/+ ↓Plt/N ↑/N ↑/N ↑/N -/+ + Neurological findings/Ascites

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  24. Hathaway WE (1993)Vitamin K deficiency. Southeast Asian J Trop Med Public Health 24 Suppl 1 ():5-9. PMID: 7886607
  25. Santagostino E, Fasulo MR (2013) Hemophilia a and hemophilia B: different types of diseases? Semin Thromb Hemost 39 (7):697-701. DOI:10.1055/s-0033-1353996 PMID: 24014073
  26. Israels SJ (2015). “Laboratory testing for platelet function disorders”. Int J Lab Hematol. 37 Suppl 1: 18–24. doi:10.1111/ijlh.12346. PMID 25976956.
  27. Lechner K, Niessner H, Thaler E (1977) Coagulation abnormalities in liver disease. Semin Thromb Hemost 4 (1):40-56. PMID: 199944
  28. Buga-Corbu I, Arion C (2014) Up to date concepts about Von Willebrand disease and the diagnose of this hemostatic disorder. J Med Life 7 (3):327-34. PMID: 25408749
  29. Giangrande P (2005) Haemophilia B: Christmas disease. Expert Opin Pharmacother 6 (9):1517-24. DOI:10.1517/14656566.6.9.1517 PMID: 16086639
  30. Deaton JG, Bhimji SS. Toxicity, Warfarin. [Updated 2017 May 23]. In: StatPearls [Internet]. Treasure Island (FL): StatPearls Publishing; 2018 Jan-.Available from: https://www.ncbi.nlm.nih.gov/books/NBK431112/

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Epidemiology and Demographics

Epidemiology and Demographics

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Sabawoon Mirwais, M.B.B.S, M.D.[2]

Overview

The prevalence of hemophilia is estimated to be 20,000 cases in the United States annually. The age-adjusted prevalence of hemophilia in six US states (Oklahoma, Massachusetts, Colorado, Georgia, Louisiana, and New York) in 1994 was 13.4 cases per 100, 000 males. The incidence of hemophilia is estimated to be 1 in 5,000 male births for hemophilia A and 1 in 30,000 births for hemophilia B.

Epidemiology and Demographics

Incidence

Prevalence

  • The age-adjusted prevalence of hemophilia in six US states (Oklahoma, Massachusetts, Colorado, Georgia, Louisiana, and New York) in 1994 was 13.4 cases per 100, 000 males.[1]
  • The prevalence of hemophilia in Swedish population was 13.7 per 100, 000 males in 1980.[1][5]
  • The prevalence of hemophilia in other countries identified through contact with specialized hemophilia treatment centers range from 9.7 to 20.5 per 100, 000 males.[1][6][7][8][9][10]

Mortality rate

  • In the United Kingdom, during 1977-1999, the all-cause mortality rate in severe hemophilia was higher than the corresponding age- and calendar year–specific all-cause mortality rate in the general male population by a factor of 2.69, while for patients with moderate/mild hemophilia it was increased by a factor of 1.19.[11]
  • The overall life expectancy of the patients with hemophilia did not notably change between 1972 and 2001.[12]
  • AIDS is the main cause of death (26%) and 22% of the deaths are because of hepatitis C.[12]

Age

Race

Gender

References

  1. 1.0 1.1 1.2 1.3 1.4 1.5 1.6 1.7 1.8 Soucie JM, Evatt B, Jackson D (December 1998). “Occurrence of hemophilia in the United States. The Hemophilia Surveillance System Project Investigators”. Am. J. Hematol. 59 (4): 288–94. PMID 9840909.
  2. https://www.nhlbi.nih.gov/health-topics/hemophilia
  3. https://www.nhlbi.nih.gov/health-topics/hemophilia
  4. “CDC Hemophilia Epidemiology and demographics”.
  5. Larsson SA, Nilsson IM, Blombäck M (1982). “Current status of Swedish hemophiliacs. I. A demographic survey”. Acta Med Scand. 212 (4): 195–200. PMID 7148514.
  6. Rosendaal FR, Varekamp I, Smit C, Bröcker-Vriends AH, van Dijck H, Vandenbroucke JP, Hermans J, Suurmeijer TP, Briët E (January 1989). “Mortality and causes of death in Dutch haemophiliacs, 1973-86”. Br. J. Haematol. 71 (1): 71–6. PMID 2917132.
  7. Walker I (1991). “Survey of the Canadian hemophilia population”. Can J Public Health. 82 (2): 127–9. PMID 2049704.
  8. Rizza CR, Spooner RJ (March 1983). “Treatment of haemophilia and related disorders in Britain and Northern Ireland during 1976-80: report on behalf of the directors of haemophilia centres in the United Kingdom”. Br Med J (Clin Res Ed). 286 (6369): 929–33. PMID 6403138.
  9. Koumbarelis E, Rosendaal FR, Gialeraki A, Karafoulidou A, Noteboom WM, Loizou C, Panayotopoulou C, Markakis C, Mandalaki T (December 1994). “Epidemiology of haemophilia in Greece: an overview”. Thromb. Haemost. 72 (6): 808–13. PMID 7740446.
  10. Ghirardini A, Schinaia N, Chiarotti F, De Biasi R, Rodeghiero F, Binkin N (November 1994). “Epidemiology of hemophilia and of HIV infection in Italy. GICC. Gruppo Italiano Coagulopatie Congenite”. J Clin Epidemiol. 47 (11): 1297–306. PMID 7722566.
  11. Darby SC, Kan SW, Spooner RJ, Giangrande PL, Hill FG, Hay CR, Lee CA, Ludlam CA, Williams M (August 2007). “Mortality rates, life expectancy, and causes of death in people with hemophilia A or B in the United Kingdom who were not infected with HIV”. Blood. 110 (3): 815–25. doi:10.1182/blood-2006-10-050435. PMID 17446349.
  12. 12.0 12.1 Plug I, Van Der Bom JG, Peters M, Mauser-Bunschoten EP, De Goede-Bolder A, Heijnen L, Smit C, Willemse J, Rosendaal FR (March 2006). “Mortality and causes of death in patients with hemophilia, 1992-2001: a prospective cohort study”. J. Thromb. Haemost. 4 (3): 510–6. doi:10.1111/j.1538-7836.2006.01808.x. PMID 16460432.
  13. http://www.wfh.org
  14. Berg LP, Varon D, Martinowitz U, Wieland K, Kakkar VV, Cooper DN (February 1994). “Combined factor VIII/factor XI deficiency may cause intra-familial clinical variability in haemophilia A among Ashkenazi Jews”. Blood Coagul. Fibrinolysis. 5 (1): 59–62. PMID 8180339.
  15. Pruthi RK (November 2005). “Hemophilia: a practical approach to genetic testing”. Mayo Clin. Proc. 80 (11): 1485–99. doi:10.4065/80.11.1485. PMID 16295028.
  16. Wheeler AP, Gailani D (July 2016). “Why factor XI deficiency is a clinical concern”. Expert Rev Hematol. 9 (7): 629–37. doi:10.1080/17474086.2016.1191944. PMC 4950943. PMID 27216469.
  17. Kadir RA, Economides DL, Lee CA (January 1999). “Factor XI deficiency in women”. Am. J. Hematol. 60 (1): 48–54. PMID 9883805.

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Risk Factors

Risk Factors

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Sabawoon Mirwais, M.B.B.S, M.D.[2]Simrat Sarai, M.D. [3]Fahd Yunus, M.D. [4]Vahid Eidkhani, M.D.

Overview

The most potent risk factor in the development of hemophilia is the family history of hemophilia. Other risk factors include male sex and malignancies.

Risk Factors

Common Risk Factors[1][2][3][4]

Risk Factors for Acquired Hemophilia[5][6][7][8]

References

  1. Mannucci PM, Tuddenham EG (June 2001). “The hemophilias–from royal genes to gene therapy”. N. Engl. J. Med. 344 (23): 1773–9. doi:10.1056/NEJM200106073442307. PMID 11396445.
  2. Ingram, G I (1976). “The history of haemophilia”. Journal of Clinical Pathology. 29 (6): 469–479. doi:10.1136/jcp.29.6.469. ISSN 0021-9746.
  3. How Hemophilia is Inherited | Hemophilia | NCBDDD | CDC. Available at http://www.cdc.gov/ncbddd/hemophilia/inheritance-pattern.html. Accessed on Sept 20, 2016
  4. Di Michele DM, Gibb C, Lefkowitz JM, Ni Q, Gerber LM, Ganguly A (March 2014). “Severe and moderate haemophilia A and B in US females”. Haemophilia. 20 (2): e136–43. doi:10.1111/hae.12364. PMID 24533955.
  5. Napolitano M, Siragusa S, Mancuso S, Kessler CM (January 2018). “Acquired haemophilia in cancer: A systematic and critical literature review”. Haemophilia. 24 (1): 43–56. doi:10.1111/hae.13355. PMID 28960809.
  6. Knoebl P, Marco P, Baudo F, Collins P, Huth-Kühne A, Nemes L; et al. (2012). “Demographic and clinical data in acquired hemophilia A: results from the European Acquired Haemophilia Registry (EACH2)”. J Thromb Haemost. 10 (4): 622–31. doi:10.1111/j.1538-7836.2012.04654.x. PMID 22321904.
  7. Kruse-Jarres R, Kempton CL, Baudo F, Collins PW, Knoebl P, Leissinger CA; et al. (2017). “Acquired hemophilia A: Updated review of evidence and treatment guidance”. Am J Hematol. 92 (7): 695–705. doi:10.1002/ajh.24777. PMID 28470674.
  8. Collins P, Baudo F, Huth-Kühne A, Ingerslev J, Kessler CM, Castellano ME et al. (2010) Consensus recommendations for the diagnosis and treatment of acquired hemophilia A. BMC Res Notes 3 ():161. DOI:10.1186/1756-0500-3-161 PMID: 20529258

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Screening

Screening

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Sabawoon Mirwais, M.B.B.S, M.D.[2]

Overview

Initial screening blood investigations for any child with suspected bleeding disorder include platelet count, prothrombin time (PT), activated partial thromboplastin time (aPTT), and fibrinogen test. Chorionic villus sampling at 11-14 weeks of gestation can be performed for the genetic diagnosis of hemophilia.

Screening

References

  1. 1.0 1.1 Sachdeva A, Gunasekaran V, Ramya HN, Dass J, Kotwal J, Seth T, Das S, Garg K, Kalra M, Sirisha RS, Prakash A (July 2018). “Consensus Statement of the Indian Academy of Pediatrics in Diagnosis and Management of Hemophilia”. Indian Pediatr. 55 (7): 582–590. PMID 30129541.
  2. Kamal AH, Tefferi A, Pruthi RK (July 2007). “How to interpret and pursue an abnormal prothrombin time, activated partial thromboplastin time, and bleeding time in adults”. Mayo Clin. Proc. 82 (7): 864–73. doi:10.4065/82.7.864. PMID 17605969.
  3. https://www.cdc.gov/ncbddd/hemophilia/diagnosis.html
  4. Qian L, Ge H, Hu P, Zhu N, Chen J, Shen J, Zhang Y (January 2019). “Pregnancy-related acquired hemophilia A initially manifesting as pleural hemorrhage: A case report”. Medicine (Baltimore). 98 (3): e14119. doi:10.1097/MD.0000000000014119. PMID 30653138.
  5. Duncan E, Collecutt M, Street A (2013). “Nijmegen-Bethesda assay to measure factor VIII inhibitors”. Methods Mol. Biol. 992: 321–33. doi:10.1007/978-1-62703-339-8_24. PMID 23546724.

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Natural History, Complications and Prognosis

Natural History, Complications and Prognosis

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Sabawoon Mirwais, M.B.B.S, M.D.[2]

Overview

Hemophilia can present with a bleeding episode during the neonatal period that is difficult to manage or it can present with signs and symptoms of concealed bleeding into the joint or viscera. If left untreated, hemophilia can result in complications involving multiple organs and in severe bleeding episodes it can result in death. Hemophilia patients can lead an active and healthy life and life expectancy depends on the treatment response and the presence of comorbidities. Complications of hemophilia include AIDS, hepatitis, Vitamin D deficiency, osteoporosis, and renal pathologies.

Natural History, Complications, and Prognosis

Natural History

Complications

Common complications of hemophilia include:

Prognosis

References

  1. 1.0 1.1 Mense L, Ferretti E, Ramphal R, Daboval T (September 2018). “A Newborn with Simmering Bleeding after Circumcision”. Cureus. 10 (9): e3324. doi:10.7759/cureus.3324. PMC 6248866. PMID 30473957.
  2. 2.0 2.1 2.2 2.3 2.4 2.5 Mannucci PM, Tuddenham EG (June 2001). “The hemophilias–from royal genes to gene therapy”. N. Engl. J. Med. 344 (23): 1773–9. doi:10.1056/NEJM200106073442307. PMID 11396445.
  3. Bolton-Maggs, Paula HB; Pasi, K John (2003). “Haemophilias A and B”. The Lancet. 361 (9371): 1801–1809. doi:10.1016/S0140-6736(03)13405-8. ISSN 0140-6736.
  4. Roosendaal G, Lafeber FP (July 2006). “Pathogenesis of haemophilic arthropathy”. Haemophilia. 12 Suppl 3: 117–21. doi:10.1111/j.1365-2516.2006.01268.x. PMID 16684006.
  5. 5.0 5.1 Berntorp E, Shapiro AD (April 2012). “Modern haemophilia care”. Lancet. 379 (9824): 1447–56. doi:10.1016/S0140-6736(11)61139-2. PMID 22456059.
  6. 6.0 6.1 Kasper CK (March 2004). “AIDS, hepatitis and hemophilia”. J. Thromb. Haemost. 2 (3): 516–8. PMID 15009473.
  7. Magallón Martínez M, Ortega F, Pinilla J (1992). “AIDS and hemophilia: experience in the La Paz Hemophilia Center”. Haemostasis. 22 (5): 281–92. doi:10.1159/000216336. PMID 1362177.
  8. 8.0 8.1 Makris M, Konkle BA (March 2017). “Hepatitis C in haemophilia: time for treatment for all”. Haemophilia. 23 (2): 180–181. doi:10.1111/hae.13183. PMID 28300362.
  9. Goodman, Catherine (2015). Pathology : implications for the physical therapist. St. Louis, Missouri: Elsevier Saunders. ISBN 9781455745913.
  10. Murphy N, O’Mahony B, Flanagan P, Noone D, White B, Bergin C, Norris S, Thornton L (September 2017). “Progression of hepatitis C in the haemophiliac population in Ireland, after 30 years of infection in the pre-DAA treatment era”. Haemophilia. 23 (5): 712–720. doi:10.1111/hae.13244. PMID 28752601.
  11. 11.0 11.1 Goedert JJ, Eyster ME, Lederman MM, Mandalaki T, De Moerloose P, White GC, Angiolillo AL, Luban NL, Sherman KE, Manco-Johnson M, Preiss L, Leissinger C, Kessler CM, Cohen AR, DiMichele D, Hilgartner MW, Aledort LM, Kroner BL, Rosenberg PS, Hatzakis A (September 2002). “End-stage liver disease in persons with hemophilia and transfusion-associated infections”. Blood. 100 (5): 1584–9. PMID 12176875.
  12. 12.0 12.1 Moreira A, Das H (2018). “Acute Life-Threatening Hemorrhage in Neonates With Severe Hemophilia A: A Report of 3 Cases”. J Investig Med High Impact Case Rep. 6: 2324709618800349. doi:10.1177/2324709618800349. PMC 6144491. PMID 30246038.
  13. Loomans JI, Eckhardt CL, Reitter-Pfoertner SE, Holmström M, van Gorkom BL, Leebeek F, Santoro C, Haya S, Meijer K, Nijziel MR, van der Bom JG, Fijnvandraat K (June 2017). “Mortality caused by intracranial bleeding in non-severe hemophilia A patients”. J. Thromb. Haemost. 15 (6): 1115–1122. doi:10.1111/jth.13693. PMID 28374963. Vancouver style error: initials (help)
  14. Pulles AE, Mastbergen SC, Schutgens RE, Lafeber FP, van Vulpen LF (January 2017). “Pathophysiology of hemophilic arthropathy and potential targets for therapy”. Pharmacol. Res. 115: 192–199. doi:10.1016/j.phrs.2016.11.032. PMID 27890816.
  15. Eldash HH, Atwa ZT, Saad MA (January 2017). “Vitamin D deficiency and osteoporosis in hemophilic children: an intermingled comorbidity”. Blood Coagul. Fibrinolysis. 28 (1): 14–18. doi:10.1097/MBC.0000000000000519. PMID 26825623.
  16. Albayrak C, Albayrak D (April 2015). “Vitamin D levels in children with severe hemophilia A: an underappreciated deficiency”. Blood Coagul. Fibrinolysis. 26 (3): 285–9. doi:10.1097/MBC.0000000000000237. PMID 25485786.
  17. 17.0 17.1 Kadir RA, Economides DL, Lee CA (January 1999). “Factor XI deficiency in women”. Am. J. Hematol. 60 (1): 48–54. PMID 9883805.
  18. Tabriznia-Tabrizi S, Gholampour M, Mansouritorghabeh H (September 2016). “A close insight to factor VIII inhibitor in the congenital hemophilia A”. Expert Rev Hematol. 9 (9): 903–13. doi:10.1080/17474086.2016.1208554. PMID 27367203.
  19. Ashrani AA, Key NS, Soucie JM, Duffy N, Forsyth A, Geraghty S (May 2008). “Septic arthritis in males with haemophilia”. Haemophilia. 14 (3): 494–503. doi:10.1111/j.1365-2516.2008.01662.x. PMC 3951979. PMID 18298584.
  20. Olivier M, Madruga M, Carlan SJ, Ge L (2018). “Hemophilia A Complicated by Ulcerative Colitis”. Case Rep Gastrointest Med. 2018: 2342618. doi:10.1155/2018/2342618. PMC 6142740. PMID 30298109.
  21. LEATHERDALE RA (April 1960). “Respiratory obstruction in haemophilic patients”. Br Med J. 1 (5182): 1316–20. PMC 1967523. PMID 14414970.
  22. 22.0 22.1 Sharma R, Dash SK, Chawla R, Kansal S, Agrawal DK, Dua H (November 2013). “Acquired hemophilia complicated by cardiorenal syndrome type 3”. Indian J Crit Care Med. 17 (6): 378–81. doi:10.4103/0972-5229.123456. PMC 3902575. PMID 24501492.
  23. Rawat J, Singh S, Chaubey D (August 2017). “Spontaneous bladder rupture: unusual presentation in a haemophilic child”. BMJ Case Rep. 2017. doi:10.1136/bcr-2017-220943. PMID 28784897.
  24. Frioui S, Jemni S (2015). “[A rare muscular complication of hemophilia: Myositis ossificans]”. Pan Afr Med J (in French). 22: 149. doi:10.11604/pamj.2015.22.149.7909. PMC 4742018. PMID 26889330.
  25. Freeman A (February 2015). “Acquired haemophilia A presenting at a District General Hospital”. BMJ Case Rep. 2015. doi:10.1136/bcr-2014-208001. PMC 4336866. PMID 25691577.
  26. 26.0 26.1 Franchini M, Mannucci PM (July 2013). “Hemophilia A in the third millennium”. Blood Rev. 27 (4): 179–84. doi:10.1016/j.blre.2013.06.002. PMID 23815950.
  27. Franchini M, Mannucci PM (December 2017). “Management of Hemophilia in Older Patients”. Drugs Aging. 34 (12): 881–889. doi:10.1007/s40266-017-0500-8. PMID 29159733.
  28. Plug I, Van Der Bom JG, Peters M, Mauser-Bunschoten EP, De Goede-Bolder A, Heijnen L, Smit C, Willemse J, Rosendaal FR (March 2006). “Mortality and causes of death in patients with hemophilia, 1992-2001: a prospective cohort study”. J. Thromb. Haemost. 4 (3): 510–6. doi:10.1111/j.1538-7836.2006.01808.x. PMID 16460432.
  29. Rosendaal, F. R.; Varekamp, I.; Smit, C.; Bröcker-Vriends, A. H. J. T.; van Dijck, H.; Vandenbroucke, J. P.; Hermans, J.; Suurmeijer, T. P. B. M.; Briët, E. (1989). “Mortality and causes of death in Dutch haemophiliacs, 1973–86”. British Journal of Haematology. 71 (1): 71–76. doi:10.1111/j.1365-2141.1989.tb06277.x. ISSN 0007-1048.
  30. Tuinenburg A, Mauser-Bunschoten EP, Verhaar MC, Biesma DH, Schutgens RE (February 2009). “Cardiovascular disease in patients with hemophilia”. J. Thromb. Haemost. 7 (2): 247–54. doi:10.1111/j.1538-7836.2008.03201.x. PMID 18983484.
  31. Soucie JM, Nuss R, Evatt B, Abdelhak A, Cowan L, Hill H, Kolakoski M, Wilber N (July 2000). “Mortality among males with hemophilia: relations with source of medical care. The Hemophilia Surveillance System Project Investigators”. Blood. 96 (2): 437–42. PMID 10887103.
  32. Angelini D, Sood SL (2015). “Managing older patients with hemophilia”. Hematology Am Soc Hematol Educ Program. 2015: 41–7. doi:10.1182/asheducation-2015.1.41. PMID 26637699.
  33. Franchini M, Mannucci PM (October 2011). “Inhibitors of propagation of coagulation (factors VIII, IX and XI): a review of current therapeutic practice”. Br J Clin Pharmacol. 72 (4): 553–62. doi:10.1111/j.1365-2125.2010.03899.x. PMC 3195733. PMID 21204915.

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Diagnosis

Diagnosis

History and Symptoms | Physical Examination | Laboratory Findings | CT | MRI | Echocardiography or Ultrasound | Other Imaging Findings | Other Diagnostic Studies

Treatment

Treatment

Medical Therapy | Secondary Prevention | Cost-Effectiveness of Therapy | Future or Investigational Therapies

Case Studies

Case Studies

Case #1



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