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Dr. Shantanu
2nd Yr DNB,
DEPT OF PEDIATRICS
J.L.N.Hospital & Research centre,
Bhilai Steel Plant
WHAT   WHAT ARE THE TOPICS?




       Definition and classification

       Causes

       APPROACH TO NEONATAL THROMBOCYTOPENIAS

       NAIT

       GUIDELINE FOR PLATELET TRANSFUSION IN NICU
   Thrombocytopenia in neonates is traditionally
    difined as a platelet count <150000/mcL

 OveralI ncidence of neonatal
    thrombocytopenia is (0.7%–0.9%)

 In  Neonatal Intensive Care Unit (NICU) it is
    very high (22%–35%)
Mild- (PC = 100000 – 150000/mcl)


Moderate (PC = 50000 – 99000/mcl)


Severe (PC < 50000/mcl)
CONDITION

Fetal   Alloimmune condition

        Congenital infection (e.g., CMV,
        toxoplasma, rubella, HIV)

        Aneuploidy (e.g., trisomy 18,13, or 21,
        or triploidy)

        Autoimmune condition (e.g., ITP,
        SLE)

        Severe Rh hemolytic disease

        Congenital/inherited (e.g., Wiskott-
        Aldrich syndrome)
CONDITION

Early-onset     Placental insufficiency (e.g., PET, IUGR, diabetes)
neonatal (<72
hr)
                Perinatal asphyxia
                Perinatal infection (e.g., Escherichia coli, GBS, Haemophilus
                influenzae), DIC

                Alloimmune condition
                Autoimmune condition (e.g., ITP, SLE)

                Congenital infection (e.g., CMV, toxoplasma, rubella, HIV)


                Thrombosis (e.g., aortic, renal vein)
                Bone marrow replacement (e.g., congenital leukemia)


                Kasabach-Merritt syndrome
                Metabolic disease (e.g., proprionic and methylmalonic acidemia)


                Congenital/inherited (e.g., TAR, CAMT)
Late-onset          Late-onset sepsis
neonatal (>72 hr)
                    NEC

                    Congenital infection (e.g., CMV, toxoplasma,
                    rubella, HIV)

                    Autoimmune

                    Kasabach-Merritt syndrome

                    Metabolic disease (e.g., proprionic and
                    methylmalonic acidemia)

                    Congenital/inherited (e.g., TAR, CAMT
Early-onset thrombocytopenia (<72 hr)



                                     MILD TO                                                SEVERE
                                    MODERATE                                               PC <50000
                                   (PC 50000 -
                                     149000)



                                                                                          Next slde
         -BABY WELL
  -EVIDENCE OF PLACENTAL                                           -BABY ILL
       INSUFFICIENCY                                          - NO EVIDENCE OF
                                                                  PLACENTAL
                                                                INSUFFICIENCY

                    Pc raising
                  pc n by 10 days
                                                               Evaluate sepsis
                                                                    , dic

                      No further
                      evaluation
                                              Evidence of
                                            sepsis.DIC pc                   No evidence of
Pc not raising                                 >with Tt                  sepsis,DIC persistent
pc not n by 10                                                            thrombocytopenias
     days

                                                 No further
                                                 evaluation

    Motherwith <pc                                                        Mother with <pc
    pe s/oTAR PRUS
    trisomy13,18, 2                                                       pe s/o TAR PRUS
           1                                                              trisomy 18, 21,13
    noonan, Turnar                                                    turnar, Noonan syndrome
          syn
Severe   (PC <50000)




                     Evaluate for sepsis , DIC , NAIT




                                            Evidence of sepsis,DIC,NAIT
No sepsis,DIC, NAIT Persistent                  PC improved with Tt
     thombocytopenias




                                                 No further evaluation
        Mother <PC
       Pe s/oTAR PRUS
      trisomy 18, 21,13
       Noonan, Turnar
             syn
Mother <PC
                          Pe s/oTAR PRUS
                         trisomy 18, 21,13
                        Noonan, Turnar syn




                                             Yes to any q:
If no to all questions, consider:            confirmatory
     TORCH infections Viral                       test
  infections (HIV, enterovirus)
  Chromosomal abnormalities
  Inborn errors of metabolism
     Thrombosis (i.e., RVT)
Congenital thrombocytopenias
Late-onset
                      Thrombocytopenia




                    Evaluate for sepsis , NEC




   Evidence of                                  No Evidence of
   sepsis,NEC                                     sepsis,NEC
PC normal with Tt

                                                    • DIC
                                 Viral infection (i.e., HSV, acquired CMV)
                                  Thrombosis (especially if central line
                                                  present)
   No further                        drug-induced thrombocytopenia
   evaluation                           inborn errors of metabolism
                                              Fanconi anemia
   Immune thrombocytopenia occurs due to the passive
    transfer of antibodies from the maternal to the fetal
    circulation.



   Types:

    1) Neonatal alloimmune thrombocytopenia (NAIT)
    2) Autoimmune thrombocytopenia
   The antibody is produced in the mother against a specific
    human platelet antigen (HPA) present in the fetus but
    absent in the mother.

   The antigen is inherited from the father of the fetus.

   Early onset severe thrombocytopenia.

   The combination of severe neonatal thrombocytopenia with
    a parenchymal (rather than intraventricular) intracranial
    hemorrhage is highly suggestive of NAIT.
 Investigation   :
      1)Antigen screening (HPA 1,3,5,9,15,4)
      2)Brain imaging studies
 Management:
 1) Suspected NAIT in an unknown pregnancy
 2) Known case of NAIT
 3)Antenatal management of pregnant woman with previous
 history of NAIT
   Management of the neonate with suspected NAIT in
    an unknown pregnancy.
    1) Random-donor platelet transfusion

    2)IVIG (1g/kg/day for 2 days)

    3) Antigen-negative platelet transfusion

    4) Methylprednisolone (1 mg/kg bid for 3–5 days)

 Management of the neonate with known NAIT
   Antigen-negative platelet transfusion
 Antenatal management of pregnant women with
  previous history of NAIT
      IVIG to mother
Platelet Count   (*10000mcl)



<30                            Transfuse all
30-49                          Transfuse if:
                               • BW <1,500g and & 7 days old
                               • Clinically unstable
                               • Concurrent coagulopathy
                               • Previous significant hemorrhage
                               (i.e., grade 3 or 4 IVH)
                               • Prior to surgical procedure
                               • Postoperative period (72 hours)



50–100                         Transfuse if:
                               • Active bleeding
                               • NAIT with intracranial bleed
                               • Before or after neurosurgical
                               procedures
 Dose:   10 -15 ml/kg

 Complications:
     Transfusion-transmitted CMV infections
     Graft-versus-host disease (GVHD)
     TRALI
THANK YOU

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Neonatal thrombocytopenia

  • 1. Dr. Shantanu 2nd Yr DNB, DEPT OF PEDIATRICS J.L.N.Hospital & Research centre, Bhilai Steel Plant
  • 2. WHAT WHAT ARE THE TOPICS? Definition and classification Causes APPROACH TO NEONATAL THROMBOCYTOPENIAS NAIT GUIDELINE FOR PLATELET TRANSFUSION IN NICU
  • 3. Thrombocytopenia in neonates is traditionally difined as a platelet count <150000/mcL  OveralI ncidence of neonatal thrombocytopenia is (0.7%–0.9%)  In Neonatal Intensive Care Unit (NICU) it is very high (22%–35%)
  • 4. Mild- (PC = 100000 – 150000/mcl) Moderate (PC = 50000 – 99000/mcl) Severe (PC < 50000/mcl)
  • 5. CONDITION Fetal Alloimmune condition Congenital infection (e.g., CMV, toxoplasma, rubella, HIV) Aneuploidy (e.g., trisomy 18,13, or 21, or triploidy) Autoimmune condition (e.g., ITP, SLE) Severe Rh hemolytic disease Congenital/inherited (e.g., Wiskott- Aldrich syndrome)
  • 6. CONDITION Early-onset Placental insufficiency (e.g., PET, IUGR, diabetes) neonatal (<72 hr) Perinatal asphyxia Perinatal infection (e.g., Escherichia coli, GBS, Haemophilus influenzae), DIC Alloimmune condition Autoimmune condition (e.g., ITP, SLE) Congenital infection (e.g., CMV, toxoplasma, rubella, HIV) Thrombosis (e.g., aortic, renal vein) Bone marrow replacement (e.g., congenital leukemia) Kasabach-Merritt syndrome Metabolic disease (e.g., proprionic and methylmalonic acidemia) Congenital/inherited (e.g., TAR, CAMT)
  • 7. Late-onset Late-onset sepsis neonatal (>72 hr) NEC Congenital infection (e.g., CMV, toxoplasma, rubella, HIV) Autoimmune Kasabach-Merritt syndrome Metabolic disease (e.g., proprionic and methylmalonic acidemia) Congenital/inherited (e.g., TAR, CAMT
  • 8.
  • 9. Early-onset thrombocytopenia (<72 hr) MILD TO SEVERE MODERATE PC <50000 (PC 50000 - 149000) Next slde -BABY WELL -EVIDENCE OF PLACENTAL -BABY ILL INSUFFICIENCY - NO EVIDENCE OF PLACENTAL INSUFFICIENCY Pc raising pc n by 10 days Evaluate sepsis , dic No further evaluation Evidence of sepsis.DIC pc No evidence of Pc not raising >with Tt sepsis,DIC persistent pc not n by 10 thrombocytopenias days No further evaluation Motherwith <pc Mother with <pc pe s/oTAR PRUS trisomy13,18, 2 pe s/o TAR PRUS 1 trisomy 18, 21,13 noonan, Turnar turnar, Noonan syndrome syn
  • 10. Severe (PC <50000) Evaluate for sepsis , DIC , NAIT Evidence of sepsis,DIC,NAIT No sepsis,DIC, NAIT Persistent PC improved with Tt thombocytopenias No further evaluation Mother <PC Pe s/oTAR PRUS trisomy 18, 21,13 Noonan, Turnar syn
  • 11. Mother <PC Pe s/oTAR PRUS trisomy 18, 21,13 Noonan, Turnar syn Yes to any q: If no to all questions, consider: confirmatory TORCH infections Viral test infections (HIV, enterovirus) Chromosomal abnormalities Inborn errors of metabolism Thrombosis (i.e., RVT) Congenital thrombocytopenias
  • 12.
  • 13. Late-onset Thrombocytopenia Evaluate for sepsis , NEC Evidence of No Evidence of sepsis,NEC sepsis,NEC PC normal with Tt • DIC Viral infection (i.e., HSV, acquired CMV) Thrombosis (especially if central line present) No further drug-induced thrombocytopenia evaluation inborn errors of metabolism Fanconi anemia
  • 14. Immune thrombocytopenia occurs due to the passive transfer of antibodies from the maternal to the fetal circulation.  Types: 1) Neonatal alloimmune thrombocytopenia (NAIT) 2) Autoimmune thrombocytopenia
  • 15. The antibody is produced in the mother against a specific human platelet antigen (HPA) present in the fetus but absent in the mother.  The antigen is inherited from the father of the fetus.  Early onset severe thrombocytopenia.  The combination of severe neonatal thrombocytopenia with a parenchymal (rather than intraventricular) intracranial hemorrhage is highly suggestive of NAIT.
  • 16.  Investigation : 1)Antigen screening (HPA 1,3,5,9,15,4) 2)Brain imaging studies  Management: 1) Suspected NAIT in an unknown pregnancy 2) Known case of NAIT 3)Antenatal management of pregnant woman with previous history of NAIT
  • 17. Management of the neonate with suspected NAIT in an unknown pregnancy. 1) Random-donor platelet transfusion 2)IVIG (1g/kg/day for 2 days) 3) Antigen-negative platelet transfusion 4) Methylprednisolone (1 mg/kg bid for 3–5 days)  Management of the neonate with known NAIT Antigen-negative platelet transfusion  Antenatal management of pregnant women with previous history of NAIT IVIG to mother
  • 18.
  • 19. Platelet Count (*10000mcl) <30 Transfuse all 30-49 Transfuse if: • BW <1,500g and & 7 days old • Clinically unstable • Concurrent coagulopathy • Previous significant hemorrhage (i.e., grade 3 or 4 IVH) • Prior to surgical procedure • Postoperative period (72 hours) 50–100 Transfuse if: • Active bleeding • NAIT with intracranial bleed • Before or after neurosurgical procedures
  • 20.  Dose: 10 -15 ml/kg  Complications: Transfusion-transmitted CMV infections Graft-versus-host disease (GVHD) TRALI