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Haemophilia B

January 01, 1970

This article is about the bleeding disorder with factor IX deficiency. For the disorder with factor VIII deficiency, see haemophilia A.

Haemophilia B, also spelled hemophilia B, is a blood clotting disorder causing easy bruising and bleeding due to an inherited mutation of the gene for factor IX, and resulting in a deficiency of factor IX. It is less common than factor VIII deficiency (haemophilia A).[3]

Haemophilia B
Other namesHemophilia B, Christmas disease
This condition is inherited in an X-linked recessive manner.
SpecialtyHaematology
SymptomsEasy bruising[1]
CausesFactor IX deficiency[1]
Diagnostic methodBleeding scores, Coagulation factor assays[2]
TreatmentFactor IX concentrate[1]

Haemophilia B was first recognized as a distinct disease entity in 1952.[4] It is also known by the eponym Christmas disease,[1] named after Stephen Christmas, the first patient described with haemophilia B. In addition, the first report of its identification was published in the Christmas edition of the British Medical Journal.[4][5]

Most individuals who have Hemophilia B and experience symptoms are men.[6] The prevalence of Hemophilia B in the population is about one in 40,000; Hemophilia B represents about 15% of patients with hemophilia.[6] Many women carriers of the disease have no symptoms.[6] However, an estimated 10-25% of women carriers have mild symptoms; in rare cases, women may have moderate or severe symptoms.[6]

Signs and symptoms edit

Symptoms include easy bruising, urinary tract bleeding (haematuria), nosebleeds (epistaxis), and bleeding into joints (haemarthrosis).[1]

Complications edit

Patients with bleeding disorders show a higher incidence of periodontal disease as well as dental caries, concerning the fear of bleeding which leads to a lack of oral hygiene and oral health care. The most prominent oral manifestation of a mild haemophilia B would be gingival bleeding during exfoliation of primary dentition, or prolonged bleeding after an invasive procedure/tooth extraction; In severe haemophilia, there may be spontaneous bleeding from the oral tissues (e.g. soft palate, tongue, buccal mucosa), lips and gingiva, with ecchymoses. In rare cases, haemarthrosis (bleeding into joint space) of the temporomandibular joint (TMJ) may be observed.[7]

Patients with haemophilia will experience many episodes of oral bleeding over their lifetime. Average 29.1 bleeding events per year are serious enough to require factor replacement in F VIII-deficient patients which 9% involved oral structures. Children with severe haemophilia have significant lower prevalence of dental caries and lower plaque scores compared with matched, healthy controls.[8]

Genetics edit

 
X chromosome

The factor IX gene is located on the X chromosome (Xq27.1-q27.2). It is an X-linked recessive trait, which explains why males are affected in greater numbers.[9][10]

In 1990, George Brownlee and Merlin Crossley showed that two sets of genetic mutations were preventing two key proteins from attaching to the DNA of people with a rare and unusual form of haemophilia B – haemophilia B Leyden – where patients experience episodes of excessive bleeding in childhood but have few bleeding problems after puberty.[10]

This lack of protein attachment to the DNA was thereby turning off the gene that produces clotting factor IX, which prevents excessive bleeding.[10]

Pathophysiology edit

 
Coagulation (FIX is on left)

Factor IX deficiency leads to an increased propensity for haemorrhage, which can be either spontaneously or in response to mild trauma.[11]

Factor IX deficiency can cause interference of the coagulation cascade, thereby causing spontaneous haemorrhage when there is trauma. Factor IX when activated activates factor X which helps fibrinogen to fibrin conversion.[11]

Factor IX becomes active eventually in coagulation by cofactor factor VIII (specifically IXa). Platelets provide a binding site for both cofactors. This complex (in the coagulation pathway) will eventually activate factor X.[12]

Diagnosis edit

The diagnosis for haemophilia B can be done via the following tests/methods:[2]

Differential diagnosis edit

The differential diagnosis for this inherited condition is the following: haemophilia A, factor XI deficiency, von Willebrand disease, fibrinogen disorders and Bernard–Soulier syndrome[10]

Treatment edit

Treatment is given intermittently, when there is significant bleeding. It includes intravenous infusion of factor IX and/or blood transfusions. NSAIDS should be avoided once the diagnosis is made since they can exacerbate a bleeding episode. Any surgical procedure should be done with concomitant tranexamic acid.[4][13]

Etranacogene dezaparvovec (Hemgenix) was approved for medical use in the United States in November 2022.[6] It is the first gene therapy approved by the US Food and Drug Administration (FDA) to treat Hemophilia B.[6]

Dental considerations edit

Surgical treatment, including a simple dental extraction, must be planned to minimize the risk of bleeding, excessive bruising, or haematoma formation. Soft vacuum-formed splints can be used to provide local protection following a dental extraction or prolonged post-extraction bleed.[14]

Research edit

In July 2022 results of a gene therapy candidate for haemophilia B called FLT180 were announced, it works using an adeno-associated virus (AAV) to restore the clotting factor IX (FIX) protein, normal levels of the protein were observed with low doses of the therapy but immunosuppression was necessitated to decrease the risk of vector-related immune responses.[15][16][17]

History edit

 
Factor IX

Stephen Christmas (12 February 1947 – 20 December 1993) was the first patient described to have Christmas disease (or Haemophilia B) in 1952 by a group of British doctors. Christmas was born to a British family in London. He was the son of film and television actor Eric Christmas.[18] He emigrated to Toronto, Ontario, Canada, with his family, and was there at the age of two years that hemophilia was diagnosed at the Hospital for Sick Children. The family returned to London in 1952 to visit their relatives, and during the trip Stephen was admitted to hospital. A sample of his blood was sent to the Oxford Haemophilia Centre in Oxford, where Rosemary Biggs and Robert Gwyn Macfarlane discovered that he was not deficient in Factor VIII, which is normally decreased in classic hemophilia, but a different protein, which received the name Christmas factor in his honour (and later Factor IX).[18] Stephen was dependent on blood and plasma transfusions, and was infected with HIV in the period during which blood was not routinely screened for this virus. He became an active worker for the Canadian Hemophilia Society and campaigned for transfusion safety ever since getting infected, but developed AIDS and died from it in 1993.[18]

In the 1950s and 1960s, with newfound technology and gradual advances in medicine, pharmaceutical scientists found a way to take the factor IX from fresh frozen plasma (FFP) and give it to those with haemophilia B. Though they found a way to treat the disease, the FFP contained only a small amount of factor IX, requiring large amounts of FFP to treat an actual bleeding episode, which resulted in the person requiring hospitalization. By the mid-1960s scientists found a way to get a larger amount of factor IX from FFP. By the late 1960s, pharmaceutical scientists found methods to separate the factor IX from plasma, which allows for neatly packaged bottles of factor IX concentrates. With the rise of factor IX concentrates it became easier for people to get treatment at home.[19] Although these advances in medicine had a significant positive impact on the treatment of haemophilia, there were many complications that came with it. By the early 1980s, scientists discovered that the medicines they had created were transferring blood-borne viruses, such as hepatitis, and HIV, the virus that causes AIDS. With the rise of these deadly viruses, scientists had to find improved methods for screening the blood products they received from donors. In 1982, scientists made a breakthrough in medicine and were able to clone factor IX gene. With this new development it decreased the risk of the many viruses. Although the new factor was created, it was not available for haemophilia B patients until 1997.[citation needed]

Society and culture edit

Main article: Haemophilia in European royalty

In 2009, an analysis of genetic markers revealed that haemophilia B was the blood disease affecting many European royal families of the United Kingdom, Germany, Russia and Spain: so-called "Royal Disease".[20][21]

See also edit

References edit

  1. ^ a b c d e "Hemophilia B: MedlinePlus Medical Encyclopedia". medlineplus.gov. Retrieved 2016-09-21.
  2. ^ a b Konkle, Barbara A.; Josephson, Neil C.; Nakaya Fletcher, Shelley (1 January 1993). "Hemophilia B". GeneReviews. PMID 20301668. Retrieved 7 October 2016.update 2014
  3. ^ Kliegman, Robert (2011). Nelson textbook of pediatrics (19th ed.). Philadelphia: Saunders. pp. 1700–1. ISBN 978-1-4377-0755-7.
  4. ^ a b c "Haemophilia B (Factor IX Deficiency) information | Patient". Patient. 3 July 2014. Retrieved 2016-04-21.
  5. ^ Biggs R, Douglas AS, MacFarlane RG, Dacie JV, Pitney WR, Merskey C, O'Brien JR (1952). "Christmas disease: a condition previously mistaken for haemophilia". Br Med J. 2 (4799): 1378–82. doi:10.1136/bmj.2.4799.1378. PMC 2022306. PMID 12997790.
  6. ^ a b c d e f "FDA Approves First Gene Therapy to Treat Adults with Hemophilia B". U.S. Food and Drug Administration (FDA). 22 November 2022. Retrieved 22 November 2022.   This article incorporates text from this source, which is in the public domain.
  7. ^ "Hemophilia A" (PDF). College of Dental Hygienists of Ontario. September 2, 2015.
  8. ^ Glick, Michael (2015). Burket's Oral Medicine. USA: People's Medical Publishing House. pp. 473, 475, 481, 482. ISBN 978-1-60795-188-9.
  9. ^ "OMIM Entry - # 306900 - HEMOPHILIA B; HEMB". omim.org. Retrieved 2016-10-07.
  10. ^ a b c d "Hemophilia".
  11. ^ a b "Hemophilia B: Practice Essentials, Background, Pathophysiology". eMedicine. Medscape. 24 August 2016. Retrieved 7 October 2016.
  12. ^ . eMedicine. Medscape. 24 August 2016. Archived from the original on 6 October 2016. Retrieved 7 October 2016.
  13. ^ Beck, Norman (2009). Diagnostic hematology. London: Springer. p. 416. ISBN 9781848002951. Retrieved 7 October 2016.
  14. ^ Andrew Brewer, Maria Elvira Correa (May 2006). "Guildelines for Dental Treatment of Patients with Inherited Bleeding Disorders" (PDF). Treatment of Hemophilia. 40: 9 – via World Federation of Hemophilia (WFH).
  15. ^ Chowdary, Pratima; Shapiro, Susan; Makris, Mike; Evans, Gillian; Boyce, Sara; Talks, Kate; Dolan, Gerard; Reiss, Ulrike; Phillips, Mark; Riddell, Anne; Peralta, Maria R. (2022-07-21). "Phase 1–2 Trial of AAVS3 Gene Therapy in Patients with Hemophilia B". New England Journal of Medicine. 387 (3): 237–247. doi:10.1056/NEJMoa2119913. ISSN 0028-4793. PMID 35857660. S2CID 250697905.
  16. ^ "Novel gene therapy could reduce bleeding risk for haemophilia patients". ScienceDaily. Retrieved 2022-08-03.
  17. ^ "Transformational therapy cures haemophilia B". BBC News. 2022-07-21. Retrieved 2022-08-03.
  18. ^ a b c Giangrande PL (June 2003). "Six characters in search of an author: the history of the nomenclature of coagulation factors". Br. J. Haematol. 121 (5): 703–12. doi:10.1046/j.1365-2141.2003.04333.x. PMID 12780784. S2CID 22694905.
  19. ^ Schramm, Wolfgang (November 2014). "The history of haemophilia – a short review". Thrombosis Research. 134: S4–S9. doi:10.1016/j.thromres.2013.10.020. ISSN 1879-2472. PMID 24513149. – via ScienceDirect (Subscription may be required or content may be available in libraries.)
  20. ^ Michael Price (8 October 2009). "Case Closed: Famous Royals Suffered From Hemophilia". ScienceNOW Daily News. AAAS. Retrieved 9 October 2009.
  21. ^ Evgeny I. Rogaev; et al. (8 October 2009). "Genotype Analysis Identifies the Cause of the "Royal Disease"". Science. 326 (5954): 817. Bibcode:2009Sci...326..817R. doi:10.1126/science.1180660. PMID 19815722. S2CID 206522975.subscription required

Further reading edit

  • Franchini, Massimo; Frattini, Francesco; Crestani, Silvia; Sissa, Cinzia; Bonfanti, Carlo (1 January 2013). "Treatment of hemophilia B: focus on recombinant factor IX". Biologics: Targets and Therapy. 7: 33–38. doi:10.2147/BTT.S31582. ISSN 1177-5475. PMC 3575125. PMID 23430394.
  • Nathwani, Amit C.; Reiss, Ulreke M.; Tuddenham, Edward G.D.; Rosales, Cecilia; Chowdary, Pratima; McIntosh, Jenny; Della Peruta, Marco; Lheriteau, Elsa; Patel, Nishal; Raj, Deepak; Riddell, Anne; Pie, Jun; Rangarajan, Savita; Bevan, David; Recht, Michael; Shen, Yu-Min; Halka, Kathleen G.; Basner-Tschakarjan, Etiena; Mingozzi, Federico; High, Katherine A.; Allay, James; Kay, Mark A.; Ng, Catherine Y.C.; Zhou, Junfang; Cancio, Maria; Morton, Christopher L.; Gray, John T.; Srivastava, Deokumar; Nienhuis, Arthur W.; Davidoff, Andrew M. (20 November 2014). "Long-Term Safety and Efficacy of Factor IX Gene Therapy in Hemophilia B". New England Journal of Medicine. 371 (21): 1994–2004. doi:10.1056/NEJMoa1407309. ISSN 0028-4793. PMC 4278802. PMID 25409372.

External links edit

 
Scholia has a topic profile for Haemophilia B.

January 01, 1970
haemophilia, this, article, about, bleeding, disorder, with, factor, deficiency, disorder, with, factor, viii, deficiency, haemophilia, also, spelled, hemophilia, blood, clotting, disorder, causing, easy, bruising, bleeding, inherited, mutation, gene, factor, . This article is about the bleeding disorder with factor IX deficiency For the disorder with factor VIII deficiency see haemophilia A Haemophilia B also spelled hemophilia B is a blood clotting disorder causing easy bruising and bleeding due to an inherited mutation of the gene for factor IX and resulting in a deficiency of factor IX It is less common than factor VIII deficiency haemophilia A 3 Haemophilia BOther namesHemophilia B Christmas diseaseThis condition is inherited in an X linked recessive manner SpecialtyHaematologySymptomsEasy bruising 1 CausesFactor IX deficiency 1 Diagnostic methodBleeding scores Coagulation factor assays 2 TreatmentFactor IX concentrate 1 Haemophilia B was first recognized as a distinct disease entity in 1952 4 It is also known by the eponym Christmas disease 1 named after Stephen Christmas the first patient described with haemophilia B In addition the first report of its identification was published in the Christmas edition of the British Medical Journal 4 5 Most individuals who have Hemophilia B and experience symptoms are men 6 The prevalence of Hemophilia B in the population is about one in 40 000 Hemophilia B represents about 15 of patients with hemophilia 6 Many women carriers of the disease have no symptoms 6 However an estimated 10 25 of women carriers have mild symptoms in rare cases women may have moderate or severe symptoms 6 Contents 1 Signs and symptoms 1 1 Complications 2 Genetics 3 Pathophysiology 4 Diagnosis 4 1 Differential diagnosis 5 Treatment 5 1 Dental considerations 6 Research 7 History 8 Society and culture 9 See also 10 References 11 Further reading 12 External linksSigns and symptoms editSymptoms include easy bruising urinary tract bleeding haematuria nosebleeds epistaxis and bleeding into joints haemarthrosis 1 Complications edit Patients with bleeding disorders show a higher incidence of periodontal disease as well as dental caries concerning the fear of bleeding which leads to a lack of oral hygiene and oral health care The most prominent oral manifestation of a mild haemophilia B would be gingival bleeding during exfoliation of primary dentition or prolonged bleeding after an invasive procedure tooth extraction In severe haemophilia there may be spontaneous bleeding from the oral tissues e g soft palate tongue buccal mucosa lips and gingiva with ecchymoses In rare cases haemarthrosis bleeding into joint space of the temporomandibular joint TMJ may be observed 7 Patients with haemophilia will experience many episodes of oral bleeding over their lifetime Average 29 1 bleeding events per year are serious enough to require factor replacement in F VIII deficient patients which 9 involved oral structures Children with severe haemophilia have significant lower prevalence of dental caries and lower plaque scores compared with matched healthy controls 8 Genetics edit nbsp X chromosome The factor IX gene is located on the X chromosome Xq27 1 q27 2 It is an X linked recessive trait which explains why males are affected in greater numbers 9 10 In 1990 George Brownlee and Merlin Crossley showed that two sets of genetic mutations were preventing two key proteins from attaching to the DNA of people with a rare and unusual form of haemophilia B haemophilia B Leyden where patients experience episodes of excessive bleeding in childhood but have few bleeding problems after puberty 10 This lack of protein attachment to the DNA was thereby turning off the gene that produces clotting factor IX which prevents excessive bleeding 10 Pathophysiology edit nbsp Coagulation FIX is on left Factor IX deficiency leads to an increased propensity for haemorrhage which can be either spontaneously or in response to mild trauma 11 Factor IX deficiency can cause interference of the coagulation cascade thereby causing spontaneous haemorrhage when there is trauma Factor IX when activated activates factor X which helps fibrinogen to fibrin conversion 11 Factor IX becomes active eventually in coagulation by cofactor factor VIII specifically IXa Platelets provide a binding site for both cofactors This complex in the coagulation pathway will eventually activate factor X 12 Diagnosis editThe diagnosis for haemophilia B can be done via the following tests methods 2 Coagulation screening test Bleeding scores Coagulation factor assays Differential diagnosis edit The differential diagnosis for this inherited condition is the following haemophilia A factor XI deficiency von Willebrand disease fibrinogen disorders and Bernard Soulier syndrome 10 Treatment editTreatment is given intermittently when there is significant bleeding It includes intravenous infusion of factor IX and or blood transfusions NSAIDS should be avoided once the diagnosis is made since they can exacerbate a bleeding episode Any surgical procedure should be done with concomitant tranexamic acid 4 13 Etranacogene dezaparvovec Hemgenix was approved for medical use in the United States in November 2022 6 It is the first gene therapy approved by the US Food and Drug Administration FDA to treat Hemophilia B 6 Dental considerations edit Surgical treatment including a simple dental extraction must be planned to minimize the risk of bleeding excessive bruising or haematoma formation Soft vacuum formed splints can be used to provide local protection following a dental extraction or prolonged post extraction bleed 14 Research editIn July 2022 results of a gene therapy candidate for haemophilia B called FLT180 were announced it works using an adeno associated virus AAV to restore the clotting factor IX FIX protein normal levels of the protein were observed with low doses of the therapy but immunosuppression was necessitated to decrease the risk of vector related immune responses 15 16 17 History edit nbsp Factor IX Stephen Christmas 12 February 1947 20 December 1993 was the first patient described to have Christmas disease or Haemophilia B in 1952 by a group of British doctors Christmas was born to a British family in London He was the son of film and television actor Eric Christmas 18 He emigrated to Toronto Ontario Canada with his family and was there at the age of two years that hemophilia was diagnosed at the Hospital for Sick Children The family returned to London in 1952 to visit their relatives and during the trip Stephen was admitted to hospital A sample of his blood was sent to the Oxford Haemophilia Centre in Oxford where Rosemary Biggs and Robert Gwyn Macfarlane discovered that he was not deficient in Factor VIII which is normally decreased in classic hemophilia but a different protein which received the name Christmas factor in his honour and later Factor IX 18 Stephen was dependent on blood and plasma transfusions and was infected with HIV in the period during which blood was not routinely screened for this virus He became an active worker for the Canadian Hemophilia Society and campaigned for transfusion safety ever since getting infected but developed AIDS and died from it in 1993 18 In the 1950s and 1960s with newfound technology and gradual advances in medicine pharmaceutical scientists found a way to take the factor IX from fresh frozen plasma FFP and give it to those with haemophilia B Though they found a way to treat the disease the FFP contained only a small amount of factor IX requiring large amounts of FFP to treat an actual bleeding episode which resulted in the person requiring hospitalization By the mid 1960s scientists found a way to get a larger amount of factor IX from FFP By the late 1960s pharmaceutical scientists found methods to separate the factor IX from plasma which allows for neatly packaged bottles of factor IX concentrates With the rise of factor IX concentrates it became easier for people to get treatment at home 19 Although these advances in medicine had a significant positive impact on the treatment of haemophilia there were many complications that came with it By the early 1980s scientists discovered that the medicines they had created were transferring blood borne viruses such as hepatitis and HIV the virus that causes AIDS With the rise of these deadly viruses scientists had to find improved methods for screening the blood products they received from donors In 1982 scientists made a breakthrough in medicine and were able to clone factor IX gene With this new development it decreased the risk of the many viruses Although the new factor was created it was not available for haemophilia B patients until 1997 citation needed Society and culture editMain article Haemophilia in European royalty In 2009 an analysis of genetic markers revealed that haemophilia B was the blood disease affecting many European royal families of the United Kingdom Germany Russia and Spain so called Royal Disease 20 21 See also editHaemophilia A Haemophilia C Haemophilia in European royalty von Willebrand s diseaseReferences edit a b c d e Hemophilia B MedlinePlus Medical Encyclopedia medlineplus gov Retrieved 2016 09 21 a b Konkle Barbara A Josephson Neil C Nakaya Fletcher Shelley 1 January 1993 Hemophilia B GeneReviews PMID 20301668 Retrieved 7 October 2016 update 2014 Kliegman Robert 2011 Nelson textbook of pediatrics 19th ed Philadelphia Saunders pp 1700 1 ISBN 978 1 4377 0755 7 a b c Haemophilia B Factor IX Deficiency information Patient Patient 3 July 2014 Retrieved 2016 04 21 Biggs R Douglas AS MacFarlane RG Dacie JV Pitney WR Merskey C O Brien JR 1952 Christmas disease a condition previously mistaken for haemophilia Br Med J 2 4799 1378 82 doi 10 1136 bmj 2 4799 1378 PMC 2022306 PMID 12997790 a b c d e f FDA Approves First Gene Therapy to Treat Adults with Hemophilia B U S Food and Drug Administration FDA 22 November 2022 Retrieved 22 November 2022 nbsp This article incorporates text from this source which is in the public domain Hemophilia A PDF College of Dental Hygienists of Ontario September 2 2015 Glick Michael 2015 Burket s Oral Medicine USA People s Medical Publishing House pp 473 475 481 482 ISBN 978 1 60795 188 9 OMIM Entry 306900 HEMOPHILIA B HEMB omim org Retrieved 2016 10 07 a b c d Hemophilia a b Hemophilia B Practice Essentials Background Pathophysiology eMedicine Medscape 24 August 2016 Retrieved 7 October 2016 Factor IX Deficiency Background Pathophysiology Epidemiology eMedicine Medscape 24 August 2016 Archived from the original on 6 October 2016 Retrieved 7 October 2016 Beck Norman 2009 Diagnostic hematology London Springer p 416 ISBN 9781848002951 Retrieved 7 October 2016 Andrew Brewer Maria Elvira Correa May 2006 Guildelines for Dental Treatment of Patients with Inherited Bleeding Disorders PDF Treatment of Hemophilia 40 9 via World Federation of Hemophilia WFH Chowdary Pratima Shapiro Susan Makris Mike Evans Gillian Boyce Sara Talks Kate Dolan Gerard Reiss Ulrike Phillips Mark Riddell Anne Peralta Maria R 2022 07 21 Phase 1 2 Trial of AAVS3 Gene Therapy in Patients with Hemophilia B New England Journal of Medicine 387 3 237 247 doi 10 1056 NEJMoa2119913 ISSN 0028 4793 PMID 35857660 S2CID 250697905 Novel gene therapy could reduce bleeding risk for haemophilia patients ScienceDaily Retrieved 2022 08 03 Transformational therapy cures haemophilia B BBC News 2022 07 21 Retrieved 2022 08 03 a b c Giangrande PL June 2003 Six characters in search of an author the history of the nomenclature of coagulation factors Br J Haematol 121 5 703 12 doi 10 1046 j 1365 2141 2003 04333 x PMID 12780784 S2CID 22694905 Schramm Wolfgang November 2014 The history of haemophilia a short review Thrombosis Research 134 S4 S9 doi 10 1016 j thromres 2013 10 020 ISSN 1879 2472 PMID 24513149 via ScienceDirect Subscription may be required or content may be available in libraries Michael Price 8 October 2009 Case Closed Famous Royals Suffered From Hemophilia ScienceNOW Daily News AAAS Retrieved 9 October 2009 Evgeny I Rogaev et al 8 October 2009 Genotype Analysis Identifies the Cause of the Royal Disease Science 326 5954 817 Bibcode 2009Sci 326 817R doi 10 1126 science 1180660 PMID 19815722 S2CID 206522975 subscription requiredFurther reading editFranchini Massimo Frattini Francesco Crestani Silvia Sissa Cinzia Bonfanti Carlo 1 January 2013 Treatment of hemophilia B focus on recombinant factor IX Biologics Targets and Therapy 7 33 38 doi 10 2147 BTT S31582 ISSN 1177 5475 PMC 3575125 PMID 23430394 Nathwani Amit C Reiss Ulreke M Tuddenham Edward G D Rosales Cecilia Chowdary Pratima McIntosh Jenny Della Peruta Marco Lheriteau Elsa Patel Nishal Raj Deepak Riddell Anne Pie Jun Rangarajan Savita Bevan David Recht Michael Shen Yu Min Halka Kathleen G Basner Tschakarjan Etiena Mingozzi Federico High Katherine A Allay James Kay Mark A Ng Catherine Y C Zhou Junfang Cancio Maria Morton Christopher L Gray John T Srivastava Deokumar Nienhuis Arthur W Davidoff Andrew M 20 November 2014 Long Term Safety and Efficacy of Factor IX Gene Therapy in Hemophilia B New England Journal of Medicine 371 21 1994 2004 doi 10 1056 NEJMoa1407309 ISSN 0028 4793 PMC 4278802 PMID 25409372 External links edit nbsp Scholia has a topic profile for Haemophilia B Retrieved from https en wikipedia org w index php title Haemophilia B amp oldid 1190411994, wikipedia, wiki, book, books, library,

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