Hemophilia: Difference between revisions

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== Background ==
==Background==
*TREAT FIRST, Diagnose second. Assume bleeding until proven otherwise.
*Two types (clinically indistinguishable):
**Hemophilia A: Factor VIII deficiency
**Hemophilia B (Christmas disease): Factor IX deficiency
*Substantial proportion (~1/3) of both types arise from spontaneous mutations
*Most common X-linked disorder<ref>[http://emedicine.medscape.com/article/779322-overview#a1 Medscape: Hemophilia A]</ref>(overwhelmingly a disease of men)
*[[ICH]] is most common cause of hemorrhagic death
*Do ''not'' give [[NSAIDs]] or IM injections
*Avoid invasive procedures (e.g. central lines, LP)


*Two types (clinically indistinguishable):
===Prehospital Care===
**Hemophilia A: Factor VIII deficiency
*Rapid transport to definitive care
**Hemophilia B: Factor IX deficiency
*Apply pressure and achieve hemostasis in active bleeding patients
*Substantial proportion of both types arise from spontaneous mutations
*Bring Factor therapy with patient and encourage use during transport
*ICH is most common cause of hemorrhagic death
*Determine history of trauma or prior complications with hemophilia
*Never give NSAIDs or IM injections
*For hemarthrosis; elevate, ice, and protect joint (crutches for knee/ankle)
*Consult hematology if pt has h/o inhibitors


== Diagnosis ==
==Clinical Features==
''Patient does not need objective exam finding to treat. Subjective complaints are a harbinger of serious issues.''
===Hemarthroses===
*Location
**Peds: Ankle 80% of the time
**Adults: Knees, then elbows, then ankles
*Leads to joint destruction and chronic arthropathy if not adequately treated
*Patients can reliably report when bleeding is occurring
*Most common bleeding complaint
===Hematomas===
*Bleeding into soft tissues or muscle
**Neck (airway compromise)
**Limbs (compartment syndromes)
**Eye ([[retrobulbar hematoma|retro-orbital hematoma]])
**Spine ([[epidural hematoma]])
**[[retroperitoneal bleed|Retroperitoneum]] (iliopsoas bleeds and massive blood loss)
*Most common initial complaint
===Mucocutaneous bleeding===
*Spontaneous bleeding uncommon from oropharynx, [[GI bleed|GI tract]], [[epistaxis]], or [[hemoptysis]]
===CNS===
*[[ICH|Intracranial bleeding]] is most common cause of hemorrhagic death
*[[Subdural hematoma]]s occur spontaneously or with minimal trauma
===[[Hematuria]]===
*Common, usually not serious, source is rarely found


*Easy bruising or bleeding out of proportion to the history of trauma
==Differential Diagnosis==
*Recurrent bleeding into joints and muscles
{{Increased bleeding DDX}}
*Hematuria
**Common but typically not severe


== Work-Up ==
==Evaluation==
===Work-Up===
*Coags
**Only helpful in making the diagnosis; once established unlikely to yield new information
**PT - normal
**PTT - abnormal (unless mild hemophilia)
**PTT s/p factor - should correct to normal
*Factor VIII assay
 
====Consider====
*[[Head CT]]
**If [[headache]], [[altered mental status]], blunt [[head trauma|head injury]]
**[[Brain MRI|MRI]] is preferred to CT if available (better visualization of posterior fossa)
*CT A/P
**Back, thigh, groin, or abdominal pain
*If [[LP]] required
**replete factor before attempting
 
===Evaluation===
*Pain in soft tissue is bleeding until proven otherwise
*Paresthesias in legs - consider retroperitoneal bleed
*Flexion contracture at the hip- iliopsoas bleed
*Easy bruising or bleeding out of proportion to the history of trauma
*Recurrent bleeding into joints and muscles
**Arthrocentesis not indicated
*Prolonged PTT; normal PT
 
====Factor VIII assay====
''Consider before treatment (for heme to follow)''
*Normal: 50-150%
*Mild: >5% (usually an insult causes bleeding)
*Moderate: 1-5% (usually an insult causes bleeding)
*Severe: <1% (spontaneous bleeding not uncommon, multiple bleeding episodes/month)


*Coags
==Treatment<ref>Bitting RL, Bent S, Li Y, Kohlwes J. The prognosis and treatment of acquired hemophilia: a systematic review and meta-analysis. Blood Coagul Fibrinolysis. Oct 2009;20(7):517-23</ref>==
**Only helpful for making the dx; once established unlikely to yield new information
*Always inquire whether patient has known inhibitors - may be refractory to conventional treatment
**PT - normal
**If so, obtain hematology consult before treatment
**PTT - abnormal (unless mild hemophilia)
**If no known inhibitors, and patient not improving after replacement, order mixing study
*Head CT
***PTT will not correct if inhibitors present
**If c/o HA, AMS, sig. flunt head injury
*CT A/P
**Back, thigh, groin, or abd pain


== Treatment ==
===Indications for Factor Replacement===
* Suspected bleeding into muscles or joints
* Trauma to [[head trauma|head]] or [[neck trauma|neck]]
* Any new or concerning [[headache]] (spontaneous or traumatic)
* [[Trauma]] with potential for internal bleeding
* Prior to any planned invasive procedure or surgery
* [[GI bleed|Gastrointestinal]] bleeding
* Acute [[fractures]], [[joint dislocations|dislocations]] and sprains


*FFP if dx is unknown (contains VIII and IX)
===Factor Replacement===
**Each bag raises factor levels by 3-5%
*Major bleeding (GI, CNS, large muscle, trauma) requires factor replacement level 80-100%
*Factor replacement if dx is known
*Moderate bleeding (soft tissue, small muscle, joint) requires 30-50%
**Factor VIII required = (Target FVIII – Baseline FVIII)/2 x wt in kg
*Diagnosis unknown
***If baseline is unknown assume zero
**Give [[FFP]] (contains VIII and IX)  
***After the initial correction maintain via half the initial dose q 8-12hr
**Each bag raises factor levels by 3-5%  
**Factor IX required = (Target FIX – Baseline FIX) x wt in kg
*Severe mechanism of injury (head, neck trauma), even without evidence of bleeding
***Half this dose should be readministered in 24 hr
**Hemophilia is factor deficiency, not platelet deficiency/malfunction so initial hemostasis may be achieved but clot stabilization will not persist
**Major bleeding (CNS, GI, neck, throat, large muscle, severe injury)
**Delayed bleeding is a serious risk, so factor replacement must occur immediately
***Requires factor levels between 80-100% are necessary
====Hemophilia A====
**Less severe bleeding (soft tissue, muscle, joints)
*'''Dose of Factor VIII = weight (kg) x % increased desired x 0.5'''
***Requires factor levels between 30-50%
**After initial correction give half this dose q8-12hr  
**Mild bleeding (hemophilia A)
**1 IU/kg will increase the plasma concentration by 2%
***May only require desmopressin (increases vWF which carries VIII in the plasma)
**For severe bleeding, desired factor level is 80-100%.
***0.3mcg/kg IV over 15-30min
**For less severe bleeding, the desired factor level is 30-50%
*[[Desmopressin]]
**May be sufficient in patients with mild bleeding
**0.3mcg/kg IV over 15-30min
====Hemophilia B====
*'''Dose of Factor IX = weight (kg) x % increase desired'''
**After initial correction give half this dose 24 hr later
**1 IU/kg will increase the plasma concentration by 1%
**For severe bleeding, desired factor level is 80-100%.
**For less severe bleeding, the desired factor level is 30-50%


=== Treatment for Specific Conditions ===
;Use the percentage as integer, not percentage (e.g. for 25% multiply by "25" not "0.25")


{| border="1" cellpadding="2"
===Desired Level Repletion<ref>DiMichele D. Hemophilia 1996. New approach to an old disease. Pediatr Clin North Am. 1996 Jun;43(3): 709-36.</ref>===
{| {{table}}
| align="center" style="background:#f0f0f0;"|'''Site of Bleed'''
| align="center" style="background:#f0f0f0;"|'''Hemostatic Level'''
| align="center" style="background:#f0f0f0;"|'''Hemophilia A'''
| align="center" style="background:#f0f0f0;"|'''Hemophilia B'''
|-
|-
! align="left" | TYPE OF BLEEDING
| Joint ||80% acutely, then 40% every other day until resolved ||40 units/kg initially and then 20 units/kg every other day until healed ||80 units/kg initially and then 40 units/kg every other day or third day as needed
! align="left" | INITIAL DOSAGE
! align="left" | DURATION
! align="left" | COMMENT
|-
|-
| colspan="4" align="left" | '''Skin'''
| Muscles ||40-50% ||20-40 units/kg per day until healed ||40-60 units/kg then 20-30 every other day as needed
|-
|-
| align="left" | Abrasion
| Oral ||100% ||50 units/kg ||100 units/kg
| align="left" | None
| align="left" | None
| align="left" | Treat with local pressure and topical thrombin
|-
|-
| align="left" | Laceration
| Nose ||Initially 80-100%, then 30% until healing ||40-50 units/kg, then 30-40 units per day ||80-100 units/kg then 35-40 units every day
| align="left" | Usually none; if necessary, treat as minor
| align="left" | None
| align="left" | Local pressure and anesthetic with epinephrine may benefit; watch 4 hours after suturing; reexamine in 24 hours
|-
|-
| align="left" | Superficial
| align="left" | <br/>
| align="left" | <br/>
| align="left" | <br/>
|-
|-
| align="left" | Deep
| Gastrointestinal ||Initially 100%, then 50% until healing ||50 units/kg, then 30-40 units/ kg per day ||100 units/kg then 30-40 units every day
| align="left" | Minor bleeding (12.5 mg/kg)
| align="left" | Single-dose coverage
| align="left" | May need hospitalization for observation; repeat may be necessary for suture removal
|-
|-
| align="left" | Nasal epistaxis
| Genitourinary ||Initially 100%, then 30% until healing ||50 units/kg then 30-40 units/ kg/day ||100 units/kg then 30-40 units every day
| align="left" | <br/>
| align="left" | <br/>
| align="left" | <br/>
|-
|-
| align="left" | Spontaneous
| Central Nervous System ||Initially 100%, then 50-100% for 14 days ||50 units/kg then 25 units/kg every 12 hours ||100 units/kg then 50 units/kg every day
| align="left" | Usually none; may need to be treated as mild bleeding
| align="left" | None
| align="left" | Uncommon; consider platelet inhibition; treat in usual manner
|-
|-
| align="left" | Traumatic
| Surgery/trauma ||Initially 100%, then 80-100% until wound healing begins, then 30% until suture removed ||50 units/kg then 40-50 units every 12 hours adjusted according to healing ||100 units/kg then 50 units every day adjusted according to healing
| align="left" | Moderate bleeding (25 mg/kg)
| align="left" | Up to 5–7 days
| align="left" | Trauma-related bleeding can be significant
|-
|-
| colspan="4" align="left" | '''Oral'''
|-
| align="left" | Mucosa or tongue bites
| align="left" | Usually none; treat as minor if persists
| align="left" | Single dose
| align="left" | Commonly seen
|-
| align="left" | Traumatic (laceration) or dental extraction
| align="left" | Moderate (25 U/kg) to severe (50 U/kg)
| align="left" | Single dose; may need more
| align="left" | Saliva rich in fibrin lytic activity; oral ε-aminocaproic acid (Amicar) may be given at 100 mg every 6 hr for 7 days to block fibrinolysis; check contraindications; hospitalize patients with severe bleeding
|-
| align="left" | '''Soft tissue/muscle hematomas'''
| align="left" | Moderate (25 U/kg) to severe (50 U/kg)
| align="left" | 2–5 days
| align="left" | May be complicated by local pressure on nerves or vessels (e.g., iliopsoas, forearm, calf)
|-
| colspan="4" align="left" | '''Hemarthrosis'''
|-
| align="left" | Early
| align="left" | Mild (12.5 U/kg)
| align="left" | Single dose
| align="left" | Treat as earliest symptom (pain); knee, elbow, ankle more common
|-
| align="left" | Late or unresponsive cases of early hemarthrosis
| align="left" | Mild to moderate (25 U/kg)
| align="left" | 3–4 days
| align="left" | Arthrocentesis rarely necessary and only with 50% level coverage; immobilization is critical point of therapy
|-
| align="left" | '''Hematuria'''
| align="left" | Mild (12.5 U/kg)
| align="left" | 2–3 days
| align="left" | Urokinase, the fibrinolytic enzyme, is in urine; with persistent hematuria an organic cause should be ruled out
|-
| align="left" | Major bleeding
| align="left" | Major bleeding (50 U/kg)
| align="left" | 7–10 days or 3–5 days after bleeding ceases
| align="left" | In head trauma, therapy should be given prophylactically; early CT scan of head recommended for all
|}
|}
*For isolated oral mucosal bleeding consider antifibrinolytic agents (e.g. - [[TXA]])


=== &nbsp;Dosage of Factor VIII (Antihemophilic Factor) ===
===Inhibitors to Factors===
 
*Antibody inhibitors to factor therapy more common in Factor concentrates and rare in recombinant factor therapy<ref>Franchini M. et al. Systematic review of the role of FVIII concentrates in inhibitor development in previously untreated patients with severe hemophilia: A 2013 Update. Semin Thromb Hemost. 2013 Oct;39(7):752-66</ref>
{| border="1" cellpadding="2"
*Treatment should be in consultation with hematologist
|-
*In major bleeding, rVII has been suggested as potential salvage therapy for patients with inhibitors to recombinant factor<ref>O'Connell N, Mc Mahon C, Smith J, Khair K, Hann I, Liesner R, et al. Recombinant factor VIIa in the management of surgery and acute bleeding episodes in children with haemophilia and high responding inhibitors. Br J Haematol. Mar 2002;116(3):632-5</ref>
! align="left" | BLEEDING RISK
====Treatment Options====
! align="left" | DESIRED FACTOR VIII LEVEL (%)
*Activated Prothrombin Complex Concentrate Dosing: 75 units/kg
! align="left" | INITIAL DOSE (U/KG)
*FEIBA (Immuno)
|-
*Recombinant Activate VII Dosing: 90ug/kg every 2-3 hours
| align="left" | Mild
*Several studies suggest treatment with higher dosing of Recombinant Activate VII initially<ref>Shwartz K, Rubinstein M.  Hemophilia And Von Willebrand Disease in Children:  Emergency Department Evaluation and Management.  Pediatric Emergency Medicine Practice. Sept. 2015; (cited 2015 Sept 7th).  Available from:  https://www.ebmedicine.net/topics.php?paction=showTopic&topic_id=465&inittopicdload=1</ref>
| align="left" | 5–10
**270 mcg/kg dosing
| align="left" | 12.5
**Separate further dosing by at least 6 hours
|-
| align="left" | Moderate
| align="left" | 20–30
| align="left" | 25
|-
| align="left" | Severe
| align="left" | 50 or greater
| align="left" | 50
|}


{| width="100%"
==Disposition==
|-
===Admit===
| align="left" |
*Patients requiring  multiple factor replacement doses
== Source ==
*Bleeding in head, neck, pharynx, retropharynx, or retroperitoneum
*Potential for compartment syndrome
===Discharge===
*If close follow-up and mild hemarthrosis
*If no bleeding and prophylaxis given
*Coordinate follow-up with patient's hematologist or primary care provider


Tintinalli, Rosens
==See Also==
*[[Coagulopathy (Main)]]
*[[Von Willebrand Disease (vWD)]]


|}
==References==
<references/>


<br/>[[Category:Heme/Onc]] <br/><br/>
[[Category:Heme/Onc]]

Latest revision as of 03:35, 9 February 2021

Background

  • TREAT FIRST, Diagnose second. Assume bleeding until proven otherwise.
  • Two types (clinically indistinguishable):
    • Hemophilia A: Factor VIII deficiency
    • Hemophilia B (Christmas disease): Factor IX deficiency
  • Substantial proportion (~1/3) of both types arise from spontaneous mutations
  • Most common X-linked disorder[1](overwhelmingly a disease of men)
  • ICH is most common cause of hemorrhagic death
  • Do not give NSAIDs or IM injections
  • Avoid invasive procedures (e.g. central lines, LP)

Prehospital Care

  • Rapid transport to definitive care
  • Apply pressure and achieve hemostasis in active bleeding patients
  • Bring Factor therapy with patient and encourage use during transport
  • Determine history of trauma or prior complications with hemophilia
  • For hemarthrosis; elevate, ice, and protect joint (crutches for knee/ankle)

Clinical Features

Patient does not need objective exam finding to treat. Subjective complaints are a harbinger of serious issues.

Hemarthroses

  • Location
    • Peds: Ankle 80% of the time
    • Adults: Knees, then elbows, then ankles
  • Leads to joint destruction and chronic arthropathy if not adequately treated
  • Patients can reliably report when bleeding is occurring
  • Most common bleeding complaint

Hematomas

Mucocutaneous bleeding

CNS

Hematuria

  • Common, usually not serious, source is rarely found

Differential Diagnosis

Coagulopathy

Platelet Related

Factor Related

Evaluation

Work-Up

  • Coags
    • Only helpful in making the diagnosis; once established unlikely to yield new information
    • PT - normal
    • PTT - abnormal (unless mild hemophilia)
    • PTT s/p factor - should correct to normal
  • Factor VIII assay

Consider

Evaluation

  • Pain in soft tissue is bleeding until proven otherwise
  • Paresthesias in legs - consider retroperitoneal bleed
  • Flexion contracture at the hip- iliopsoas bleed
  • Easy bruising or bleeding out of proportion to the history of trauma
  • Recurrent bleeding into joints and muscles
    • Arthrocentesis not indicated
  • Prolonged PTT; normal PT

Factor VIII assay

Consider before treatment (for heme to follow)

  • Normal: 50-150%
  • Mild: >5% (usually an insult causes bleeding)
  • Moderate: 1-5% (usually an insult causes bleeding)
  • Severe: <1% (spontaneous bleeding not uncommon, multiple bleeding episodes/month)

Treatment[2]

  • Always inquire whether patient has known inhibitors - may be refractory to conventional treatment
    • If so, obtain hematology consult before treatment
    • If no known inhibitors, and patient not improving after replacement, order mixing study
      • PTT will not correct if inhibitors present

Indications for Factor Replacement

Factor Replacement

  • Major bleeding (GI, CNS, large muscle, trauma) requires factor replacement level 80-100%
  • Moderate bleeding (soft tissue, small muscle, joint) requires 30-50%
  • Diagnosis unknown
    • Give FFP (contains VIII and IX)
    • Each bag raises factor levels by 3-5%
  • Severe mechanism of injury (head, neck trauma), even without evidence of bleeding
    • Hemophilia is factor deficiency, not platelet deficiency/malfunction so initial hemostasis may be achieved but clot stabilization will not persist
    • Delayed bleeding is a serious risk, so factor replacement must occur immediately

Hemophilia A

  • Dose of Factor VIII = weight (kg) x % increased desired x 0.5
    • After initial correction give half this dose q8-12hr
    • 1 IU/kg will increase the plasma concentration by 2%
    • For severe bleeding, desired factor level is 80-100%.
    • For less severe bleeding, the desired factor level is 30-50%
  • Desmopressin
    • May be sufficient in patients with mild bleeding
    • 0.3mcg/kg IV over 15-30min

Hemophilia B

  • Dose of Factor IX = weight (kg) x % increase desired
    • After initial correction give half this dose 24 hr later
    • 1 IU/kg will increase the plasma concentration by 1%
    • For severe bleeding, desired factor level is 80-100%.
    • For less severe bleeding, the desired factor level is 30-50%
Use the percentage as integer, not percentage (e.g. for 25% multiply by "25" not "0.25")

Desired Level Repletion[3]

Site of Bleed Hemostatic Level Hemophilia A Hemophilia B
Joint 80% acutely, then 40% every other day until resolved 40 units/kg initially and then 20 units/kg every other day until healed 80 units/kg initially and then 40 units/kg every other day or third day as needed
Muscles 40-50% 20-40 units/kg per day until healed 40-60 units/kg then 20-30 every other day as needed
Oral 100% 50 units/kg 100 units/kg
Nose Initially 80-100%, then 30% until healing 40-50 units/kg, then 30-40 units per day 80-100 units/kg then 35-40 units every day
Gastrointestinal Initially 100%, then 50% until healing 50 units/kg, then 30-40 units/ kg per day 100 units/kg then 30-40 units every day
Genitourinary Initially 100%, then 30% until healing 50 units/kg then 30-40 units/ kg/day 100 units/kg then 30-40 units every day
Central Nervous System Initially 100%, then 50-100% for 14 days 50 units/kg then 25 units/kg every 12 hours 100 units/kg then 50 units/kg every day
Surgery/trauma Initially 100%, then 80-100% until wound healing begins, then 30% until suture removed 50 units/kg then 40-50 units every 12 hours adjusted according to healing 100 units/kg then 50 units every day adjusted according to healing
  • For isolated oral mucosal bleeding consider antifibrinolytic agents (e.g. - TXA)

Inhibitors to Factors

  • Antibody inhibitors to factor therapy more common in Factor concentrates and rare in recombinant factor therapy[4]
  • Treatment should be in consultation with hematologist
  • In major bleeding, rVII has been suggested as potential salvage therapy for patients with inhibitors to recombinant factor[5]

Treatment Options

  • Activated Prothrombin Complex Concentrate Dosing: 75 units/kg
  • FEIBA (Immuno)
  • Recombinant Activate VII Dosing: 90ug/kg every 2-3 hours
  • Several studies suggest treatment with higher dosing of Recombinant Activate VII initially[6]
    • 270 mcg/kg dosing
    • Separate further dosing by at least 6 hours

Disposition

Admit

  • Patients requiring multiple factor replacement doses
  • Bleeding in head, neck, pharynx, retropharynx, or retroperitoneum
  • Potential for compartment syndrome

Discharge

  • If close follow-up and mild hemarthrosis
  • If no bleeding and prophylaxis given
  • Coordinate follow-up with patient's hematologist or primary care provider

See Also

References

  1. Medscape: Hemophilia A
  2. Bitting RL, Bent S, Li Y, Kohlwes J. The prognosis and treatment of acquired hemophilia: a systematic review and meta-analysis. Blood Coagul Fibrinolysis. Oct 2009;20(7):517-23
  3. DiMichele D. Hemophilia 1996. New approach to an old disease. Pediatr Clin North Am. 1996 Jun;43(3): 709-36.
  4. Franchini M. et al. Systematic review of the role of FVIII concentrates in inhibitor development in previously untreated patients with severe hemophilia: A 2013 Update. Semin Thromb Hemost. 2013 Oct;39(7):752-66
  5. O'Connell N, Mc Mahon C, Smith J, Khair K, Hann I, Liesner R, et al. Recombinant factor VIIa in the management of surgery and acute bleeding episodes in children with haemophilia and high responding inhibitors. Br J Haematol. Mar 2002;116(3):632-5
  6. Shwartz K, Rubinstein M. Hemophilia And Von Willebrand Disease in Children: Emergency Department Evaluation and Management. Pediatric Emergency Medicine Practice. Sept. 2015; (cited 2015 Sept 7th). Available from: https://www.ebmedicine.net/topics.php?paction=showTopic&topic_id=465&inittopicdload=1
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