Neonatal Jaundice and Hematology

Neonatal Jaundice and Hematology Raegan Wetzel, M.D. Oct 5, 2010

Causes of Anemia • Accelerated Loss • Hemorrhage, Twin-twin transfusion, early umbilical cord clamping, fetal-maternal transfusion • Accelerated Destruction • Immune hemolytic anemia, hemoglobinopathies, enzyme defects, membrane defects, mechanical destruction, infection, vit E deficiency • Diminished Production • Anemia of prematurity, Fanconi/Diamond-Blackfan anemia, parvovirus, iron deficiency

Case 1 • You are called to an emergent C/S for twins now with decelerations. You are unable to get much history from L&D except that they are 33 4/7 weeks, twin A with EFW 1700 g and twin B at 1200 g. • At delivery, Twin A is a female who appears LGA with ruddy appearance. Twin B also female appears smaller with pallor and poor perfusion. • What is the diagnosis ?

Twin to Twin Transfusion • Who is at risk and why ? • Monozygotic/monochornic twins • 13-33% of twin pregnancies • Donor • Anemia • Recipient • Hyperbili, Hyperviscosity

Blood Loss • Fetal-placental • Infant position after delivery • Cord abnormalities • Velamentous insertion, short cords, chord rupture with precipitous delivery or entanglement, nuchal/knot • Placental abnormalities • Abruption or previa • Fetal-maternal • What should you order ? • Kleihauer-Betke

Case 2 • Ex 27 week preemie, now 5 weeks old “feeding and growing” is noted to have poor weight gain, increased A/B’s, and new flow murmur. • Lab results reveal: normocytic normochromic anemia (hct 25%) with normal WBC and platelet indices. • What do you think the diagnosis is ?

Anemia of Prematurity • Why does it happen ? • Blood loss • Shortened RBC lifespan • Preterm 40-60 days • Inadequate RBC production • Suboptimal erythropoiesis in response to hypoxia • Switch from hepatic to renal O2 sensor not till term

Do term infants get anemic ? • YES • Physiologic anemia of infancy happens later in term infants. True or False ? • True • Term: • 8-12 weeks, Hemoglobin 9-11 g/dL • Preterm: • 3-6 weeks, Hemoglobin 7-9 g/dL

Transfusion Guidlines

Decreased RBC Production • Nutritional • Iron Deficiency • Bone Marrow Suppression • Rubella • Parvovirus • Aplastic/Hypoplastic Anemia • Diamond Blackfan Anemia • Fanconi Anemia

Case 3 • You are notified by the state lab that a newborn has Hemoglobin Barts. What does this mean ? • Does this relate to Beta or Alpha Thalassemia ?

Alpha Thalassemia • % Hgb Bart’s = number of alpha globin genes that are deleted • Silent Carrier – 1 abnormal gene • Alpha thal trait – 2 abnormal genes • Hb H disease – 3 abnormal genes • Moderate anemia • Thal Major - 4 abnormal genes • Hydrops fetalis • Transfusion dependent

Beta Thalassemia • 2 genes of beta-globin production • Silent Carrier: Normal smear and electrophoresis • B-thal trait: Frequently misdiagnosed as iron deficiency anemia, mild anemia • Thal intermedia: Able to maintain Hgb > 7 without transfusion • Thal major: Require regular transfusions

Case 4 • 3 day old term female presents to your office for first check up. Mom had prenatal care and decided to have the baby at home with a midwife. Uncomplicated pregnancy and delivery. Mom doesn’t believe in immunizations and didn’t want her baby to get any medicines at birth. • Baby has been having some mild bleeding around her gums with feeding and mom noticed a small amount of blood in the diaper this morning.

What is her diagnosis ? • Hemorrhagic Disease of the Newborn • How could this have been avoided ? • 0.5 to 1 mg IM of vitamin K

Hemorrhagic Disease of the Newborn Why are Newborns deficient in Vit K ? • Placental transfer is poor • Breast milk is a poor source • GI tract is sterile at birth • What lab values are associated ? • Platelet Count • Normal • Fibrinogen • Normal • PT • prolonged

3 Types of HD of N • Early Disease • 1st 24 hours • Maternal use of anticoagulant/anticonvulsant • Severe bleeding/intracranial hemorrhage • Classic Disease • 1-7 days • Cutaneous, GI or circumcision site bleeding • Late-onset • Beyond 1 week • Associated with exclusively breast-fed

Case 5 • Term male infant noted to be bleeding from the umbilical stump in WBN. Physical exam otherwise unremarkable. • Family history of maternal uncle with frequent nose bleeds. • Labs: • Platelet count : 200 • PTT : prolonged • PT : normal • Bleeding time normal • Fibrinogen level : normal • Factor IX and VII : pending

Hemophilia A and B • X linked disorder • Hemophilia A (factor VIII) : 5x more common • Hemophilia B (factor IX) : milder • Bleeding less common in newborn period • Common bleeding sites ? • Circumcision, umbilical bleeding, subdural > IVH

How is this different than Von Willebrand’s disease ? • V W is most common heritable bleeding disorder • V W is autosomal dominant • V W will have prolonged bleeding time • What test should you order for diagnosis ? • von Willebrand factor activity (ristocetin cofactor • von Willebrand factor antigen

Case 6 • Newborn male in WBN noted to be oozing from umbilical stump. Physical exam significant for petechiae. Infant born to a primagravida with no prenatal problems. Maternal CBC is normal. • Laboratory on baby: • Platelet count 20 • Normal PT,PTT • Normal fibrinogen

What is the diagnosis ? • Neonatal Alloimmune Thrombocytopenia • What is the pathophysiology ? • Placental transfer of maternal antibodies against paternally inherited antigens on fetal platelets. • HPA-1a (78%) and HPA-5b alloantigens • Can the disease occur in the first pregnancy ? • Yes • Antigenic determinants expressed on placental endothelium • Extended window of time for sensitization

BlueBerry Muffin Rash Petechiae

Bilirubin Metabolism

Case 7 • 72 hr old infant who was delivered after an uncomplicated pregnancy @ 39 WGA appears clinically jaundiced at discharge. Baby is bottle feeding, no family history of jaundice and MBT O+. You get the following lab values: • Total bilirubin 11mg/dl • Direct fraction 0.8 mg/dl • Infant Hct 52% • IBT O+ • Does this seem physiologic or pathologic ? • Physiologic

Physiologic Elevation is universal and transient Mechanisms: Increased RBC destruction Decreased uptake and conjugation Ineffective excretion Pathologic Jaundice that varies significantly from physiologic expectations in: Time of appearance Duration Pattern of serially determined concentrations Pathologic Vs. PhysiologicWhat’s the difference ?

Pathologic Jaundice • Occurs in the first ____ hrs of life • 24 hrs of life • Rate of bilirubin rise > ____ mg/dl/day • > 5mg/dl/day • Clinical jaundice > ____ days in duration • > 1 week duration • Direct bilirubin > _____ • > 2mg/dl or > 15% of total

Term Infant Peak day 3-5 Peak Level 8-13 mg/dl Decline day 5-10 Preterm Infant Peak day 5-7 Peak level 12-15 mg/dl Decline day 7-15 Natural History

Case 8 • Term AGA male born to a 35 yo G3P3 without any prenatal/neonatal complications, presents for 2 week check. Mom is exclusively breastfeeding without any difficulty and infant is gaining weight. He looks a little jaundiced. • Lab results: • H/H and platelet count WNL • Total Bilirubin 19mg/dl • Direct Bilirubin 0.8 mg/dl

Breast Milk Jaundice • 10-30 % of breast fed infants • After first 5 days • Peaks at 2 weeks • Gradual decline over months • Cause ? • Progesterone Metabolite • Fatty acids

Breastfeeding Failure Jaundice • First few days of life • First time moms • Poor enteral intake → delayed meconium→ increased enterohepatic uptake of bilirubin • Prevention: • Lactation consultant • At least 8-12 feeds/day • Avoid supplements

Why would these neonates be at risk for hyperbili ?

Case 9 • 2 week old infant here for routine check. Uncomplicated delivery and WBN stay. Vit K given at birth, discharged at 72 hrs, breastfeeding well. Feeding every 3 hrs, stooling 6 x/day and voiding 9x/day. Exam significant for clinical jaundice. • What labs would you order ? • What maternal blood type would you be concerned about ?

Labs: • WBC 9 x 10 3/mm3, Hct 26%, Plt 175k/mm3 • Retic 7% • Total Bilirubin 19mg/dl, direct 0.6mg/dl • History from the well baby chart • Maternal Blood Type O+ • Infant Blood Type A + • DAT +

Maternal IgG (via placenta) mediated Maternal Coombs (indirect) + Hemolysis of fetal cells Hyperbilirubinemia, anemia Hydrops Fetalis Rh Alloimmunization Rhesus D most common and most severe Rhogam @ 28 wks and within 72 hrs of delivery Severity increases ABO Incompatibility Mild to severe Anti-A Anti-B Can occur in 1st pregnancy Immune Mediated Hemolytic Disease

Case 10 • 4 day old infant presents to office with jaundice. Term male, uncomplicated delivery to a G1 with blood type B+ Prenatal labs unremarkable. Breast feeding well. Jaundiced yesterday with level of 17, home phototherapy initiated and follow up today with bilirubin of 22. • PE significant for jaundice and palpable spleen.

Labs • Initial Hct 47, now 28 • Reticulocyte count 4% • Infant blood type B+, coombs – • Blood smear What specific test will be positive ? Osmotic Fragility Test

Hereditary Spherocytosis • Autosomal Dominant • Northern European descent • Anemia • Jaundice • Splenomegaly

Other Heritable Hemolytic Diseases • Pyruvate Kinase Deficiency • Inherited as …….. • Auto recessive • G6PD deficiency • Most common in people of what descent ? • Mediterranean, tropical African, and Asian • Inherited as …….. • X linked

Case 11 • 7 day old, full term male comes to office with lethargy. Unremarkable prenatal/nursery course. Exclusively breastfeeding. No stool x 2 days and mom has to wake him up for feeds. • Physical exam: lethargic, jaundiced, large head and widely open fontanelles, low tone

Congenital Hypothyroidism • Incidence 1:4000 • Usually asymptomatic at birth • Conjugating enzyme deficiency lasts weeks to months • L-thyroxine treatment by 2 weeks • Prompt treatment corrects the bilirubin

Case 12 • Ex 30 week EGA preemie, now 3 weeks old. Delivered for maternal pre-e, otherwise unremarkable pregnancy with negative maternal labs. Now on RA but with frequent feeding intolerance and multiple periods of NPO. Currently on 5 q3 enteral feeds and had been on TPN since birth. Total bili today 11 mg/dl with a direct component of 5.6mg/dl • What are some general causes ? • What labs might help narrow your differential ?

Hepatocellular Hepatitis TPN induced Alpha-1 antitrypsin Galacotsemia Cystic Fibrosis Biliary Tree Abnormalities Extra-hepatic BiliaryAtresia Paucity of bile ducts Choledochal cyst Bile Plug Causes of Direct Hyperbilirubinemia

What tests will be helpful ? • Radiology: • Abdominal ultrasound • HIDA scan • Newborn screen: • CF results • GALT enzyme activity • Infant Labs: • Hepatitis panel • ALT,AST, GGT • Urine for reducing substances

ManagementWhen to start Phototherapy

ManagementWhen to consider Exchange

Why do we treat ? • To prevent …… • Kernicterus • Which is deposition of unconjugated bilirubin in the ……….. Basal Ganglia

Phototherapy • Photoisomerizes unconjugated bilirubin into more H2O soluble form • Excreted rapidly by liver and kidney • Does not need glucuronidation

Exchange Transfusion • Double volume exchange • Replaces 85% of circulating RBC • Two neonatal blood volumes • 160ml/kg • Aliquots = 10% of total blood volume

THANK YOU

Neonatal Jaundice and Hematology

Neonatal Jaundice and Hematology

Presentation Transcript

NEONATAL JAUNDICE

NEONATAL JAUNDICE

Neonatology Neonatal Jaundice

NEONATAL JAUNDICE

NEONATAL JAUNDICE

Neonatal jaundice

Neonatal Jaundice Hyperbilirubinemia

Neonatal Jaundice

Neonatal Jaundice

Neonatal Jaundice

Jaundice – neonatal, prolonged and beyond

Neonatal Jaundice

Neonatal Jaundice

NEONATAL JAUNDICE

Neonatal Jaundice

NEONATAL JAUNDICE IN MALAYSIA

Neonatal Jaundice SGD

Neonatal Jaundice

Neonatal jaundice (N.Hyperbilirubinemia)

NEONATAL JAUNDICE

Neonatal Jaundice - Introduction and Management