Thrombocytopenia in pregnancy: Difference between revisions

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== Definition ==
== Background ==


===Definition===
* Low platelet count in pregnancy, generally considered to be less than 100


*Low platelet count in pregnancy, generally considered to be less than 100
== Pathophysiology ==


===Pathophysiology===
* Most commonly, thrombocytopenia of pregnancy is caused by dilution from increased plasma volume, similar to anemia in pregnancy, and is usually more noticeable in T2 and T3


*Most commonly, thrombocytopenia of pregnancy is caused by dilution from increased plasma volume, similar to anemia in pregnancy, and is usually more noticeable in T2 and T3
== Etiology ==


===Etiology===
* Gestational thrombocytopenia of pregnancy (70%)
* Hypertensive disorders (20%)
** Preeclampsia
** HELLP
* Immune disorders (5%)
** Immune-mediated thrombocytopenia (ITP)
** CAPS
** SLE
** Thrombotic microangiopathy: aHUS/TTP
* Other (5%)
** AFLP


*[[Gestational thrombocytopenia]] of pregnancy (70%)
== Epidemiology ==
*Hypertensive disorders (20%)
**[[Preeclampsia]]
**[[HELLP]]
*Immune disorders (5%)
**[[Immune-mediated thrombocytopenia]] (ITP)
**[[CAPS]]
**[[SLE]]
**[[Thrombotic microangiopathy]]: [[aHUS]]/[[TTP]]
*Other (5%)
**[[AFLP]]


===Epidemiology===
* About 10% of pregnant women have platelets less than 150


*About 10% of pregnant women have platelets less than 150
== Investigations ==


==Clinical Manifestations==
* CBC and blood film
** Look for bicytopenia concerning for thrombotic microangiopathy
** Platelets <70 more consistent with ITP than gestational thrombocytopenia
* For ITP
** HIV, HBV, HCV
** Liver and thyroid tests
** Immunoglobulin levels
** DAT
** APLA and ANA
* Platelet antibody testing is useless


{| class="wikitable"
== Common Causes ==
!Disease

!%
{|
!Diagnostic Features
! Disease
!Lab Findings
! %
! Diagnostic Features
!Clinical Features
!Pathophys
! Lab Findings
!Comments
! Clinical Features
! Pathophys
! Comments
|-
|-
| Gestational thrombocytopenia
|[[Gestational thrombocytopenia]]
| 5-9
|5-9
| Onset 2nd-3rd trimester. Normal PLT previously. No neonatal thrombocytopenia.
|Onset 2nd-3rd trimester. Normal PLT previously. No neonatal thrombocytopenia.
| Plt >70
|Plt >70
| Typically normal
|Typically normal
| Unclear
|Unclear
| Diagnosis of exclusion. Resolves postpartum. No fetal thrombocytopenia.
|Diagnosis of exclusion. Resolves postpartum. No fetal thrombocytopenia.
|-
|-
| ITP
|[[ITP]]
| <1
|<1
| Onset any trimester. May see thrombocytopenia outside pregnancy.
|Onset any trimester. May see thrombocytopenia outside pregnancy.
| Plt <100 +/- large platelets
|Plt <100 +/- large platelets
| May have bleeding, bruising, petechiae
|May have bleeding, bruising, petechiae
| Antibody-mediated peripheral plt destruction with decrease thrombopoiesis.
|Antibody-mediated peripheral plt destruction with decrease thrombopoiesis.
| Diagnosis of exclusion. May be associated with fetal thrombocytopenia.
|Diagnosis of exclusion. May be associated with fetal thrombocytopenia.
|-
|-
| Preeclampsia
|[[Preeclampsia]]
| 5-8
|5-8
| Onset late 2nd or 3rd trimester (>20 weeks).
|Onset late 2nd or 3rd trimester (>20 weeks).
| Proteinuria >0.3 g/d
|Proteinuria >0.3 g/d
| BP ≥140/90
|BP ≥140/90
| Systemic endothelial dysfunction. Inadequate placentation.
|Systemic endothelial dysfunction. Inadequate placentation.
| May precede other manifestations of preeclampsia. Can present postpartum.
|May precede other manifestations of preeclampsia. Can present postpartum.
|-
|-
| HELLP
|[[HELLP]]
| <1
|<1
| 70% late 2nd or 3rd trimester, 30% postpartum.
|70% late 2nd or 3rd trimester, 30% postpartum.
| MAHA, high liver enzymes, high LDH.
|MAHA, high liver enzymes, high LDH.
| Signs of preeclampsia, but may be normotensive without proteinuria.
|Signs of preeclampsia, but may be normotensive without proteinuria.
| Same as preeclampsia.
|Same as preeclampsia.
| Variant of preeclampsia.
|Variant of preeclampsia.
|-
|-
| AFLP
|[[AFLP]]
| <0.01
|<0.01
| Onset in 3rd trimester.
|Onset in 3rd trimester.
| Plt >50. High liver panel, creat, WBC, urate, ammonia. High PT/PTT, decreased fibrinogen. Hypoglycemia.
|Plt >50. High liver panel, creat, WBC, urate, ammonia. High PT/PTT, decreased fibrinogen. Hypoglycemia.
| RUQ pain. Jaundice, nausea/vomiting. Hepatic encephalopathy.
|RUQ pain. Jaundice, nausea/vomiting. Hepatic encephalopathy.
| Preeclampsia spectrum.
|Preeclampsia spectrum.
| MAHA not characteristic. Conjugated bili often high. Liver dysfunction greater than HELLP/preeclampsia.
|MAHA not characteristic. Conjugated bili often high. Liver dysfunction greater than HELLP/preeclampsia.
|-
|-
| TTP/aHUS
|[[TTP]]/[[aHUS]]
| <0.01
|<0.01
| Onset any trimester, but more common during 3rd or postpartum.
|Onset any trimester, but more common during 3rd or postpartum.
| MAHA, elevated creatinine, schostocytes on blood film.
|MAHA, elevated creatinine, schostocytes on blood film.
| Fever, abdo pain, n/v, headache, vis changes, altered mental status.
|Fever, abdo pain, n/v, headache, vis changes, altered mental status.
| Congenital deficiency of ADAMTS13 (TTP) or complement dysregulation (aHUS).
|Congenital deficiency of ADAMTS13 (TTP) or complement dysregulation (aHUS).
| ADAMTS13 activity <5% in TTP. Liver panel and BP usually normal.
|ADAMTS13 activity <5% in TTP. Liver panel and BP usually normal.
|}
|}<br />

== Investigations ==

*CBC and blood film
**Look for bicytopenia concerning for thrombotic microangiopathy
**Platelets &lt;70 more consistent with ITP than gestational thrombocytopenia
*For ITP
**HIV, HBV, HCV
**Liver and thyroid tests
**Immunoglobulin levels
**DAT
**APLA and ANA
*Platelet antibody testing is useless


== Management ==
==Management==


* Depends on etiology
*Depends on etiology
* Gestational thrombocytopenia
*Gestational thrombocytopenia
** No specific management
**No specific management
*[[Immune-mediated thrombocytopenia#Management|ITP]]
* ITP
** No need to treat until 36 weeks if platelets over 30
**No need to treat until 36 weeks if platelets over 30
** If platelets &lt; 30 or bleeding
**If platelets &lt; 30 or bleeding
*** Prednisone 0.25-1mg/kg) or IVIg (1g/kg ideally body weight, max 60mg)
***[[Prednisone]] (0.25-1 mg/kg) or [[IVIg]] (1 g/kg ideally body weight, max 60mg)
** Monitor newborn for post-partum thrombocytopenia
**Monitor newborn for post-partum thrombocytopenia


== Prognosis ==
==Prognosis==


* In ITP, 25% of neonates will have thrombocytopenia and 10% will need treatment
*In [[ITP]], 25% of neonates will have thrombocytopenia and 10% will need treatment


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

Latest revision as of 13:07, 2 August 2020

Background

Definition

  • Low platelet count in pregnancy, generally considered to be less than 100

Pathophysiology

  • Most commonly, thrombocytopenia of pregnancy is caused by dilution from increased plasma volume, similar to anemia in pregnancy, and is usually more noticeable in T2 and T3

Etiology

Epidemiology

  • About 10% of pregnant women have platelets less than 150

Clinical Manifestations

Disease % Diagnostic Features Lab Findings Clinical Features Pathophys Comments
Gestational thrombocytopenia 5-9 Onset 2nd-3rd trimester. Normal PLT previously. No neonatal thrombocytopenia. Plt >70 Typically normal Unclear Diagnosis of exclusion. Resolves postpartum. No fetal thrombocytopenia.
ITP <1 Onset any trimester. May see thrombocytopenia outside pregnancy. Plt <100 +/- large platelets May have bleeding, bruising, petechiae Antibody-mediated peripheral plt destruction with decrease thrombopoiesis. Diagnosis of exclusion. May be associated with fetal thrombocytopenia.
Preeclampsia 5-8 Onset late 2nd or 3rd trimester (>20 weeks). Proteinuria >0.3 g/d BP ≥140/90 Systemic endothelial dysfunction. Inadequate placentation. May precede other manifestations of preeclampsia. Can present postpartum.
HELLP <1 70% late 2nd or 3rd trimester, 30% postpartum. MAHA, high liver enzymes, high LDH. Signs of preeclampsia, but may be normotensive without proteinuria. Same as preeclampsia. Variant of preeclampsia.
AFLP <0.01 Onset in 3rd trimester. Plt >50. High liver panel, creat, WBC, urate, ammonia. High PT/PTT, decreased fibrinogen. Hypoglycemia. RUQ pain. Jaundice, nausea/vomiting. Hepatic encephalopathy. Preeclampsia spectrum. MAHA not characteristic. Conjugated bili often high. Liver dysfunction greater than HELLP/preeclampsia.
TTP/aHUS <0.01 Onset any trimester, but more common during 3rd or postpartum. MAHA, elevated creatinine, schostocytes on blood film. Fever, abdo pain, n/v, headache, vis changes, altered mental status. Congenital deficiency of ADAMTS13 (TTP) or complement dysregulation (aHUS). ADAMTS13 activity <5% in TTP. Liver panel and BP usually normal.


Investigations

  • CBC and blood film
    • Look for bicytopenia concerning for thrombotic microangiopathy
    • Platelets <70 more consistent with ITP than gestational thrombocytopenia
  • For ITP
    • HIV, HBV, HCV
    • Liver and thyroid tests
    • Immunoglobulin levels
    • DAT
    • APLA and ANA
  • Platelet antibody testing is useless

Management

  • Depends on etiology
  • Gestational thrombocytopenia
    • No specific management
  • ITP
    • No need to treat until 36 weeks if platelets over 30
    • If platelets < 30 or bleeding
      • Prednisone (0.25-1 mg/kg) or IVIg (1 g/kg ideally body weight, max 60mg)
    • Monitor newborn for post-partum thrombocytopenia

Prognosis

  • In ITP, 25% of neonates will have thrombocytopenia and 10% will need treatment
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