Bleeding Disorders - Krafts Flashcards

Question 1

Q

What are the three hereditary bleeding disorders that we need to know?

Answer

A

von Willebrand disease
Hemophilia A and B
Hereditary platelet disorders

Question 2

Q

What are the three acquired bleeding disorders that we need to know?

Answer

A

DIC
ITP
TTP/HUS

Question 3

Q

What is the difference between platelet bleeding and factor bleeding?

Answer

A

Platelet bleeding
- spontaneous
- superficial (skin & mucous membranes)
  - dental procedures
  - heavy menses
- petechiae
Factor bleeding
- preceded by trauma
- deep (muscles and joint spaces)
- big bleeds

Question 4

Q

What is the difference between petechiae and purpura?

Answer

A

Petechiae
- small red spots
Purpura
- coalescence of petechiae

Question 5

Q

What characterizes Von Willebrand Disease?

Answer

A

Most common hereditary bleeding disorder
Autosomal dominant
vW factor decreased (or abnormal)
Variable severity

Question 6

Q

What is von Willebrand Factor?

Answer

A

Huge multimeric protein
Made by megakaryocytes and endothelial cells
Glues platelets down to subendothelium
- attaches to collagen proteins
Carries factor VIII (cofactor that works with IX)
Decreased or abnormal in vW disease

Question 7

Q

What are the three types of Von Willebrand Disease?

Answer

A

Type I
- decreased vWF
- 70% of cases
Type 2
- abnormal vWF (doesn’t work properly)
- 25% of cases
Type 3
- no vWF
- 5% of cases

Question 8

Q

What are the symptoms of Von Willebrand Disease?

Answer

A

Mucosal bleeding in most patients
Deep joint bleeding in severe cases

Question 9

Q

What are the labratory test findings in Von Willebrand Disease?

Answer

A

Bleeding time: prolonged
- platelets cannot adhere to subendothelium
PTT: prolonged
- measures intrinsic pathway (no VIII)
- (“corrects” with mixing study)
INR: normal
- measures extrinsic pathway
vWF level decreased (normal in type 2)
Platelet aggregation studies abnormal

Question 10

Q

What membrane glycoprotein binds vWF?

Question 11

Q

When diagnosing Von Willebrand Disease, what is the result when Ristocetin is added to serum in platelet aggregation studies?

Answer

A

Nothing, flat line

Question 12

Q

What is the treatment for Von Willebrand Disease?

Answer

A

DDAVP
- raises VIII and vWF levels
- only works if pt is able to make factors (Type 1)
Cryoprecipitate
- contains vWF and VIII
- try not to give because of potential for rejections (immune antibodies)
Factor VIII

Question 13

Q

What is the incidence of Von Willebrand Disease?

Answer

A

1 in 100

(relatively common, but most people do not know they have it)

Question 14

Q

What characterizes Hemophilia A?

Answer

A

Most common factor deficiency
X-linked recessive in most cases
- hereditary cases manifest mostly in males
- 30% are random mutations
Factor VIII level decreased
Variable amount of “factor” bleeding

Question 15

Q

What are the symptoms of Hemophilia A?

Answer

A

Severity depends on amount of VIII
Typical “factor” bleeding
- deep joint bleeding
- usually preceding trauma
- prolonged bleeding after dental work
Rarely, mucosal hemorrhage

Question 16

Q

What is hemophilic arthropathy?

Answer

A

Bleeding into the joint cause malformation/erosion/deformity
- bring in macrophages to get rid of blood

Question 17

Q

What are laboratory test findings in Hemophilia A?

Answer

A

INR, TT, platelet count, bleeding time: normal
- can perform initial platelet plug okay
- so they stop bleeding at normal rate
- but unable to form fibrin plug, so rebleed
PTT: prolonged
- measures intrinsic pathway
- (“corrects” with mixing study)
Factor VIII assays: abnormal
DNA studies: abnormal

Question 18

Q

What is the treatment of Hemophilia A?

Answer

A

DDAVP
- will need additional supplementation with blood product or
Factor VIII
- pt can make antibodies against it
- will need larger amounts every time

Question 19

Q

What characterizes Hemophilia B?

Answer

A

Factor IX level decreased
Much less common than hemophilia A
Same inheritance pattern
Same clinical and laboratory findings

Question 20

Q

What happens in XI deficiency?

Answer

A

bleeding only after trauma

(begining of intrinsic pathway)

Question 21

Q

What happens in XIII deficiency?

Answer

A

Severe neonatal bleeding

(unable to cross-link fibrin)

Question 22

Q

What are the four Hereditary platelet disorders that we need to know?

Answer

A

Bernard-Soulier Syndrome
Glanzmann Thrombasthenia
Gray Platelet Syndrome
Delta Granule Deficiency

Question 23

Q

What characterizes Bernard-Soulier Syndrome?

Answer

A

Abnormal GP Ib
Abnormal adhesion of platelets
Big platelets
Severe bleeding

Question 24

Q

What characterizes Glanzmann Thrombasthenia?

Answer

A

No GP IIb-IIIa
- can adhere to subendothelium
No aggregation
Severe bleeding

Question 25

Q

What characterizes Gray Platelet Syndrome?

Answer

A

No alpha granules
- can see with naked eye
Big, empty platelets
- can see absence of granules with naked eye
Mild bleeding

Question 26

Q

What characterizes Delta Granule Deficiency?

Answer

A

No delta granules
- can’t see with naked eye, need to look under microscope
Can be part of Chediak-Higashi syndrome

Question 27

Q

What characterizes Disseminated Intravascular Coagulation?

Answer

A

Lots of underlying disorders
- more of a symptom
Something triggers coagulation cascade
- causes thrombosis
- main problem
Platelets and factors get used up
- causes bleeding
Microangiopathic hemolytic anemia
- fibrin strands bust apart RBCs

Question 28

Q

What are the causes of DIC?

Answer

A

Dumpers (dump pro-coagulation factors into blood)
- obstetric complications
  - amniotic fluid backwashes into blood
- adenocarcinoma (initiates coag cascade)
- acute promyelocytic leukemia
Rippers (anything that damages endothelium)
- bacterial sepsis
- trauma
- burns
- vasculitis

Question 29

Q

What are the main four things that cause DIC?

Answer

A

Malignancy
OB complications
Sepsis
Trauma

Question 30

Q

What are the general symptoms of DIC?

Answer

A

Insidious or fulminant
- usually pt is sick and then DIC strikes
Multi-system disease
Thrombosis and/or bleeding

Question 31

Q

What are the laboratory test findings in DIC?

Answer

A

INR, PTT, TT prolonged
- not a problem with platelets
FDPs: increased
- not super helpful
Fibrinogen: decreased

Question 32

Q

What is the treatment for DIC?

Answer

A

Treat underlying disorder
Support with blood products

Question 33

Q

What characterizes Idiopathic Thrombocytopenic Purpura?

Answer

A

Antiplatelet antibodies
Acute vs. chronic
Diagnosis of exclusion
Steroids or splenectomy

Question 34

Q

What is the pathogenesis of ITP?

Answer

A

Autoantibodies to GP IIb-IIIa or Ib on platelets
Binds to platelets
- prevents them from working
Splenic macrophages eat platelets

Question 35

Q

What characterizes the chronic form of ITP?

Answer

A

Chronic:
- Adult women
- Primary or secondary
- Insidious: nosebleeds, easy bruising
- Danger: bleeding into brain

Question 36

Q

What characterizes the acute form of ITP?

Answer

A

Children
Abrupt, follows viral illness
Usually self-limiting
May become chronic

Question 37

Q

What are the laboratory test findings in ITP?

Answer

A

Signs of platelet destruction:
- thrombocytopenia
- normal/increased megakaryocytes
- big platelets
INR/PTT normal
No specific diagnostic test for ITP

Question 38

Q

What are some of the other causes of Thrombocytopenia?

Answer

A

Aplastic anemia
Bone marrow replacement
Big spleen
Consumptive processes (DIC, TTP, HUS)
Drugs

Question 39

Q

What is the treatment for ITP?

Answer

A

Glucocorticoids
Intravenous immunoglobulin
Splenectomy

Question 40

Q

What are the similarities in all Thrombotic Microangiopathies?

Answer

A

All have thrombi, thrombocytopenia, and MAHA
Include TTP and HUS
Can be hard to distinguish TTP from HUS
- coags are normal
Something triggers platelet activation
- clots are formed from platelets
Different from DIC!

Question 41

Q

What characterizes Thrombotic Thrombocytopenic Purpura?

Answer

A

Sx Pentad:
- MAHA
- thrombocytopenia
- fever
- neurologic defects
- renal failure
Deficiency of ADAMTS13
Big vWF multimers trap platelets
- vWF doesn’t get chopped up properly
Tx: Plasmapheresis or plasma infusions

Question 42

Q

What is the pathogenesis of TTP?

Answer

A

Just-released vWF is unusually large (UL)
UL vWF causes platelet aggregation
ADAMTS13 cleaves UL vWF into less active pieces
- enzyme that cleaves vWF
TTP is due to ADAMTS13 deficiency

Question 43

Q

What are the clinical findings in TTP?

Answer

A

Hematuria, jaundice
- MAHA (microangiopathic hemolytic anemia)
Bleeding, bruising
- thrombocytopenia
Fever
- probably a cytokine thing
Bizarre behavior
- neurologic deficits
- little thrombi shower the brain
Decreased urine output
- due to renal failure
- little thrombi in the kidneys

Question 44

Q

What is the treatment of TTP?

Answer

A

Acquired TTP: plasmapheresis
Hereditary TTP: plasma infusions

Question 45

Q

What characterizes Hemolytic Uremic Syndrome?

Answer

A

MAHA and thrombocytopenia
Epidemic (E.coli) vs. non-epidemic
Toxin released by E.coli damages endothelium
Treat supportively

Question 46

Q

What is the pathogenesis of Epidemic HUS?

Answer

A

E.coli O157:H7 (raw hamburger)
Makes nasty toxin
Injures endothelial cells
- activates platelets

Question 47

Q

What is the pathogenesis of Non-epidemic HUS?

Answer

A

Defect in complement factor H
- protects our cells from complement busting cells open
- activates platelets
Inherited or acquired
- not very common
How does this activate platelets?

Question 48

Q

What are the clinical findings in Epidemic HUS?

Answer

A

Children, elderly
Bloody diarrhea, then renal failure
- thrombi in kidneys
Fatal in 5% of cases

Question 49

Q

What are the clinical findings in Non-Epidemic HUS?

Answer

A

Renal failure
Relapsing-remitting course
Fatal in 50% of cases

Question 50

Q

What is the treatment of Epidemic HUS?

Answer

A

Supportive care
Dialysis if not making urine
NOT antibiotics
- may kill bacteria and increase toxin release!

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Bleeding Disorders - Krafts Flashcards

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