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Neonatal Jaundice Diagnosis and Treatment Guide

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Mahtab Alam

NEONATAL JAUNDICE IS MOST COMMON CAUSE OF MORBIDITY IN 1ST WEEK OF LIFE IT IS ALSO MOST COMMON CAUSE OF READMISSION AFTER DISCHARGE .THIS BEAUTIFUL SLIDE FOR NNJ.

Health & Medicine
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NEONATAL JAUNDICE DR MAHTAB MBBS,DCH,DNB HIMSR,NEW DELHI
INTRODUCTION MOST COMMON MORBIDITY IN 1ST WEEK OF LIFE OCCUR IN; 60% TERM,80% PRETERM MOST COMMON CAUSE OF READMIASSON AFTER DISCHARGE IN NEONATES JAUNDICE VISIBLE SKIN AND EYE >5-7MG/DL IN ADULT >2MG/DL MOST CASES JAUNDICE IS BENINGN AND NO INTERVENTION IS REQUIRED.APPROX 5-10% HAVE SINGIFICANT JAUNDICE REQUIRED TREATMENT TO LOWER S. BILIRUBIN LEVEL HIGH LEVEL CARRY RISK OF NEUROLOGICAL IMPAIRMENT SO REQUIRE T/T TO LOWER DOWN
3 BASIC MECHANISM ; 1. INCREASED PRODUCTION FROM DEGRADATION OF RED CELL 2. DECREASE CLEARENCE BY IMMATURE HEPATIC MECHANISM 3. REABSORBTION BY ENTEROHEPATIC MECHANISM
TYPE OF BILIRUBIN UNCONJUGATED BILIRUBIN CONJUGATED BILIRUBIN BIND TO ALBUMIN CONJUGATED WITH GLUCOURONIC ACID FAT SOLUBLE WATER SOLUBLE CAN CROSS BBB EXCREATED IN STOOL AND URINE TOXIN IN HIGH LEVEL TO BRAIN NOT TOXIC
PHYSIOLOGICAL VS PATHOLOGICAL JAUNDICE PHYSIOLOGICAL IMMATURITY OF NEONATES TO HANDLE INCREASED BILIRUBIN PRODUCTION, IN TERM JAUNDICE APPEAR 24-72 HR OF LIFE TSB GOES PEAK LEVEL 12-15MG/DL @ DAY 3 THAN FALL IN PT PEAK LEVEL OCCUR ON 3-7 DAYS OF AGE CAN RISE OVER 15MG/DL THAN FALL CAN TAKE WEEKS
PATHOLOGICAL JAUNDICE PRESENCE OF ONE OR MORE OF FOLLOWING CONDITION WOULD QUALIFY A NEONATES HAVE PATHOLOGICAL JAUNDICE 1. VISIBLE JAUNDICE ON DAY 1ST OF LIFE( >5) 2. PRESENCE OF JAUNDICE ARM AND LEG ON D2(121-13MG/DL) 3. YELLOW PALM AND SOLE ANYTIME 4. TSB INCREASES >.2MG/DL PER HR YA 5MG/DL IN 24 HR 5. SIGN OF ACUTE BILIRUBIN ENCEPHALOPATHY AND KERNICTERUS 6. DIRECT BILIRUBIN >1.5-2MG/DL AT ANY TIME 7. CLINICAL JAUNDICE PERSISTINGBEYOND 2WK IN TERM AND 3 WK IN PRETERM
CAUSES OF PATHOLOGICAL JAUNDICE HEMOLYSIS; ABO,RH,MINOR GROUP INCOMPATIBILITY,ENZYME DEF EG G6PD DEFICIT,AIHA DECREASED CONJUGATION DUE LIVER ENZYME IMMATURITY INCREASE ENTEROHEPATIC CIRCULATION SUCH AS LACK OF ADEQUATE FEEDING THAT INCLUDE INSUFFICIENT BREASTFEEDING /INFANT NOT FEED DUE TO ILLNESS,GI OBSTRUCTION EXTRAVASATED BLOOD ;CEPHALHEMATOMA,EXTENSIVE BRUISING ETC
VISUAL INSPECTION EXAMINE BABY IN BRIGHT NATURAL LIGHT /ALT IN WHITE FLUORESCENT LIGHT,WITH NO YELLOW BACKGROUND NAKED BABY….EXAMINE BLANCHED SKIN AND GUMS AND SCLERA NOTE EXTENT OF JAUNDICE (KRAMER S LAW FACE 5-7MG/DL CHEST 8-10MG/DL LOWE ABD AND THIGH 12-15MG/DL SOLES/PALMS >15MG/DL
NEONATES AT HIGHER RISK OF JAUNDICE <38 WK PREVIOUS CHILD WITH SIGNIFICANT JAUNDICE VISIBLE JAUNDICE IN FIRST 24 HR OF LIFE AGE SPECEFIC TSB LEVEL BEING ABOVE >95TH CENTILE INADEQUACY OF BREASTFEEDING COMMON CAUSE I.E BREASTFEEDING JAUNDICE
MEASUREMENT OF SERUM BILIRUBIN 1. TRANSCUTANEOUS BILIRUBINOMETRY TcB CAN USE >35 WEEK OR MORE GESTATION AFTER 24 HR OF LIFE , TcB HAS A GOOD CPRRELATION WITH TSB AT LOWER LEVEL BUT IT BECOME UNRELIABLE ONCE TSB LEVEL GOES BEYOND 14MG/DL 2. BIOCHEMICAL ; HIGH PERFORMANCE LIQUED CHROMATOGRAPHY(HPLC) GOLD STANDARD TSB ESMITATION BY VANDENBERGH REACTION 3. MICRO METHOD OF TSB ESTIMATION; BASED ON SPECTROPHOTOMETRY AND ESTIMATE TSB ON MICRO BLOOD SAMPLE
LABORATORY TESTS 1. TOTAL AND DIRECT BILIRUBIN 2. BLOOD GROUP AND RH OF MOTHER AND BABY 3. HEMATOCRIT,RETICULOCYTE COUNT AND PERIPHERAL SMEAR 4. G6PD ASSAY 5. COOMB TEST 6. SEPTIC SCREEN 7. LFT.TFT 8. TPORCH TITRE 9. LIVER SCAN WHEN CONJUGATED HYPERBILIRUBINEMIA 10.USG OF LIVER AND BILE DUCT IN CHOLESTASIS
LABORATORY DIAGNOSIS LABORATORY FEATURE RH ABO BLOOD TYPE OF MOTHER RH NEGATIVE O BLOOD TYPE IN INFANT RH POSITIVE A OR B ANEMIA MARKED MINIMAL DCT POSITIVE NEGATIVE ICT POSITIVE USUALLY POSITIVE
MANAGEMENT 1. PHOTOTHERAPY 2. IVIG 3. EXCHANGE TRANSFUSION 4. DRUGS
PHOTOTHERAPY MAINSTAY OF TREATING HYPERBINEMIA BLUE GREEN LIGHT 460-490NM ,BILIRUBIN MOLECULE ISOMERISE TO HARMLESS FORM CFL,HALOGEN BULB,HIGH INTENSITY LIGHT EMITTING DIODE(LED) AND FIBROOPTIC SOURCES. CFL MOST COMMONLY DUE LOW COST AND EASY AVABIELITY
LED HAS ADVANTAGE OF LONG LIFE (50,000 HR) AND CAPABLE OF DELIVER HIGHER IRRADIANCE THAN CFL LAMPS EXPOSE MAXIMAL SURFACE AREA OF BABY ( AVOIAD BLOCKING OF LIGHT BY ANY EQUIPMENT,LARGE DIAPER OR EYE PATCHES,CAP,HAT ,TAPE MAKE SURE LIGHT FALL ON BABY PERPENDICULARLY IF THE BABY IN INCUBATOR MINIMUM INTERRUPTION OF PT DURING FEEDING SESSION OR PROCEDURE KEEP THE DISTANCE BABY AND LIGHT 30-45CM
PRINCIPLE OF PHOTOTHERAPY NATIVE BILIRUBIN (WATER INSOLUBLE) PHOTO ISOMER OF BILIRUBIN (WATER SOLUBLE) STRUCTURAL ISOMERISM I.E LUMIRUBIN URINE 2. CONFIGURATIONAL PHOTO ISOMERISM Z..E 3. PHOTO OXIDATION OF BILIRUBIN INTO WATER SOLUBLE AND LESS LIPOPHILIC COLORLESS FORM OF BILIRUBIN
PHOTOTHERAPY TECHNIQUE • PERFORM HAND WASH • PLACE BABY NAKED IN CRADLE OR INCUBATOR • FIX EYE SHADES • KEEP BABY ATLEAST 45 CM FROM LIGHT • START PHOTOTHERAPY • FREQUENT EXTRA FEED 2 HRLY • TURN BABY AFTER EACH FEED • TEMP RECORD 2-4 HRLY • WEIGHT RECORD DAILY • MONITOR URINE FREQUENTLY • MONITOR BILIRUBIN LEVEL
SE OF PHOTOTHERAPY 1. INCREASED INSENSABLE WATER LOSS 2. LOOSE STOOL 3. SKIN RASH 4. BRONZE BABY SYNDROME 5. HYPERTHERMIA 6. HYPOCALCEMIA
MONITORING AND STOPPING PHOTOTHERAPY MONITOR TEMP OF BABY EVERY 2-4 HR,MEASURE TSB EVERY 12-24HR DISCONTINUE PT ONCE 2 VALUE 12 HR APART FALL BELOW CURRENT AGE SPECIFIC CUT OFFS MONITOR REBOUND BILIRUBIN RISE WITHIN 24 HR AFTER STOPPING PT ROLE OF SUNLIGHT NOT HELP IN TREATMENT A/W RISK OF SUNBURN AND THEREFORE SHOULD BE AVOIDED
EXCHANGE TRANSFUSION DVET SHOULD BE PERFORM IF TSB LEVEL REACH TO AGE SPECEFIC CUT-OFF VALUE FOR EXCHANGE TRANSFUSION OR INFANT SHOW SIGN OF ENCEPHALOPATHY IRRESPECTIVE OF TSB LEVEL INDICATION @ BIRTH----- CORD TSB IS ≥ 5 OR CORD HB≤ 10G/DL DONE BY PULL AND PUSH TECHNIQUE VIA UMBILICUS UMBILICAL CATHETOR VOLUME OF BLOOD 2X VOLUME OF BLOOD OF BABY 160-180ML/KG TO PREPARE BLOOD FOR DVET 2/3 OF PRBC AND 1/3 OF P PLASMA
OTHER IVIG REDUCE HEMOLYSIS SO REDUCE JAUNDICE IN ABO/RH INCMPATABILITY REDUCE SIGNIFICANTLY NEED OF EXCHANGE TRANSFUSION NOW IVIG HAS REPLACED EXCHANGE TRANSFUSION AS THE SECOND LINE OF TREATMENT IN INFANT WITH ISOIMMUNE JAUNDICE DOSE 1G/KG/DOSE IV IV HYDRATION; IN SEVERE HYPERBILIRUBINEMIA AND EVIDENCE OF DEHYDRATION EG WT LOSS AN EXTRA FLUID 50ML/KG N/3 OVER 8 HR DECREASE NEED OF ET PHENOBARBITAL (LUMINAL)/CLOFIBRATE OR STEROIDS NO PROVEN EVIDENCE OF BENEFIT SO SHOULD NOT BE EMPLOYED
THANK YOU HIMSR SOURCE NELSON CLOHERTY AIIMS NEONATALOGY PROTOCOL

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Neonatal Jaundice Diagnosis and Treatment Guide

  • 2. INTRODUCTION MOST COMMON MORBIDITY IN 1ST WEEK OF LIFE OCCUR IN; 60% TERM,80% PRETERM MOST COMMON CAUSE OF READMIASSON AFTER DISCHARGE IN NEONATES JAUNDICE VISIBLE SKIN AND EYE >5-7MG/DL IN ADULT >2MG/DL MOST CASES JAUNDICE IS BENINGN AND NO INTERVENTION IS REQUIRED.APPROX 5-10% HAVE SINGIFICANT JAUNDICE REQUIRED TREATMENT TO LOWER S. BILIRUBIN LEVEL HIGH LEVEL CARRY RISK OF NEUROLOGICAL IMPAIRMENT SO REQUIRE T/T TO LOWER DOWN
  • 3. 3 BASIC MECHANISM ; 1. INCREASED PRODUCTION FROM DEGRADATION OF RED CELL 2. DECREASE CLEARENCE BY IMMATURE HEPATIC MECHANISM 3. REABSORBTION BY ENTEROHEPATIC MECHANISM
  • 4.
  • 5.
  • 6. TYPE OF BILIRUBIN UNCONJUGATED BILIRUBIN CONJUGATED BILIRUBIN BIND TO ALBUMIN CONJUGATED WITH GLUCOURONIC ACID FAT SOLUBLE WATER SOLUBLE CAN CROSS BBB EXCREATED IN STOOL AND URINE TOXIN IN HIGH LEVEL TO BRAIN NOT TOXIC
  • 7. PHYSIOLOGICAL VS PATHOLOGICAL JAUNDICE PHYSIOLOGICAL IMMATURITY OF NEONATES TO HANDLE INCREASED BILIRUBIN PRODUCTION, IN TERM JAUNDICE APPEAR 24-72 HR OF LIFE TSB GOES PEAK LEVEL 12-15MG/DL @ DAY 3 THAN FALL IN PT PEAK LEVEL OCCUR ON 3-7 DAYS OF AGE CAN RISE OVER 15MG/DL THAN FALL CAN TAKE WEEKS
  • 8. PATHOLOGICAL JAUNDICE PRESENCE OF ONE OR MORE OF FOLLOWING CONDITION WOULD QUALIFY A NEONATES HAVE PATHOLOGICAL JAUNDICE 1. VISIBLE JAUNDICE ON DAY 1ST OF LIFE( >5) 2. PRESENCE OF JAUNDICE ARM AND LEG ON D2(121-13MG/DL) 3. YELLOW PALM AND SOLE ANYTIME 4. TSB INCREASES >.2MG/DL PER HR YA 5MG/DL IN 24 HR 5. SIGN OF ACUTE BILIRUBIN ENCEPHALOPATHY AND KERNICTERUS 6. DIRECT BILIRUBIN >1.5-2MG/DL AT ANY TIME 7. CLINICAL JAUNDICE PERSISTINGBEYOND 2WK IN TERM AND 3 WK IN PRETERM
  • 9. CAUSES OF PATHOLOGICAL JAUNDICE HEMOLYSIS; ABO,RH,MINOR GROUP INCOMPATIBILITY,ENZYME DEF EG G6PD DEFICIT,AIHA DECREASED CONJUGATION DUE LIVER ENZYME IMMATURITY INCREASE ENTEROHEPATIC CIRCULATION SUCH AS LACK OF ADEQUATE FEEDING THAT INCLUDE INSUFFICIENT BREASTFEEDING /INFANT NOT FEED DUE TO ILLNESS,GI OBSTRUCTION EXTRAVASATED BLOOD ;CEPHALHEMATOMA,EXTENSIVE BRUISING ETC
  • 10. VISUAL INSPECTION EXAMINE BABY IN BRIGHT NATURAL LIGHT /ALT IN WHITE FLUORESCENT LIGHT,WITH NO YELLOW BACKGROUND NAKED BABY….EXAMINE BLANCHED SKIN AND GUMS AND SCLERA NOTE EXTENT OF JAUNDICE (KRAMER S LAW FACE 5-7MG/DL CHEST 8-10MG/DL LOWE ABD AND THIGH 12-15MG/DL SOLES/PALMS >15MG/DL
  • 11. NEONATES AT HIGHER RISK OF JAUNDICE <38 WK PREVIOUS CHILD WITH SIGNIFICANT JAUNDICE VISIBLE JAUNDICE IN FIRST 24 HR OF LIFE AGE SPECEFIC TSB LEVEL BEING ABOVE >95TH CENTILE INADEQUACY OF BREASTFEEDING COMMON CAUSE I.E BREASTFEEDING JAUNDICE
  • 12. MEASUREMENT OF SERUM BILIRUBIN 1. TRANSCUTANEOUS BILIRUBINOMETRY TcB CAN USE >35 WEEK OR MORE GESTATION AFTER 24 HR OF LIFE , TcB HAS A GOOD CPRRELATION WITH TSB AT LOWER LEVEL BUT IT BECOME UNRELIABLE ONCE TSB LEVEL GOES BEYOND 14MG/DL 2. BIOCHEMICAL ; HIGH PERFORMANCE LIQUED CHROMATOGRAPHY(HPLC) GOLD STANDARD TSB ESMITATION BY VANDENBERGH REACTION 3. MICRO METHOD OF TSB ESTIMATION; BASED ON SPECTROPHOTOMETRY AND ESTIMATE TSB ON MICRO BLOOD SAMPLE
  • 13.
  • 14. LABORATORY TESTS 1. TOTAL AND DIRECT BILIRUBIN 2. BLOOD GROUP AND RH OF MOTHER AND BABY 3. HEMATOCRIT,RETICULOCYTE COUNT AND PERIPHERAL SMEAR 4. G6PD ASSAY 5. COOMB TEST 6. SEPTIC SCREEN 7. LFT.TFT 8. TPORCH TITRE 9. LIVER SCAN WHEN CONJUGATED HYPERBILIRUBINEMIA 10.USG OF LIVER AND BILE DUCT IN CHOLESTASIS
  • 15. LABORATORY DIAGNOSIS LABORATORY FEATURE RH ABO BLOOD TYPE OF MOTHER RH NEGATIVE O BLOOD TYPE IN INFANT RH POSITIVE A OR B ANEMIA MARKED MINIMAL DCT POSITIVE NEGATIVE ICT POSITIVE USUALLY POSITIVE
  • 16. MANAGEMENT 1. PHOTOTHERAPY 2. IVIG 3. EXCHANGE TRANSFUSION 4. DRUGS
  • 17.
  • 18.
  • 19.
  • 20. PHOTOTHERAPY MAINSTAY OF TREATING HYPERBINEMIA BLUE GREEN LIGHT 460-490NM ,BILIRUBIN MOLECULE ISOMERISE TO HARMLESS FORM CFL,HALOGEN BULB,HIGH INTENSITY LIGHT EMITTING DIODE(LED) AND FIBROOPTIC SOURCES. CFL MOST COMMONLY DUE LOW COST AND EASY AVABIELITY
  • 21. LED HAS ADVANTAGE OF LONG LIFE (50,000 HR) AND CAPABLE OF DELIVER HIGHER IRRADIANCE THAN CFL LAMPS EXPOSE MAXIMAL SURFACE AREA OF BABY ( AVOIAD BLOCKING OF LIGHT BY ANY EQUIPMENT,LARGE DIAPER OR EYE PATCHES,CAP,HAT ,TAPE MAKE SURE LIGHT FALL ON BABY PERPENDICULARLY IF THE BABY IN INCUBATOR MINIMUM INTERRUPTION OF PT DURING FEEDING SESSION OR PROCEDURE KEEP THE DISTANCE BABY AND LIGHT 30-45CM
  • 22. PRINCIPLE OF PHOTOTHERAPY NATIVE BILIRUBIN (WATER INSOLUBLE) PHOTO ISOMER OF BILIRUBIN (WATER SOLUBLE) STRUCTURAL ISOMERISM I.E LUMIRUBIN URINE 2. CONFIGURATIONAL PHOTO ISOMERISM Z..E 3. PHOTO OXIDATION OF BILIRUBIN INTO WATER SOLUBLE AND LESS LIPOPHILIC COLORLESS FORM OF BILIRUBIN
  • 23. PHOTOTHERAPY TECHNIQUE • PERFORM HAND WASH • PLACE BABY NAKED IN CRADLE OR INCUBATOR • FIX EYE SHADES • KEEP BABY ATLEAST 45 CM FROM LIGHT • START PHOTOTHERAPY • FREQUENT EXTRA FEED 2 HRLY • TURN BABY AFTER EACH FEED • TEMP RECORD 2-4 HRLY • WEIGHT RECORD DAILY • MONITOR URINE FREQUENTLY • MONITOR BILIRUBIN LEVEL
  • 24. SE OF PHOTOTHERAPY 1. INCREASED INSENSABLE WATER LOSS 2. LOOSE STOOL 3. SKIN RASH 4. BRONZE BABY SYNDROME 5. HYPERTHERMIA 6. HYPOCALCEMIA
  • 25. MONITORING AND STOPPING PHOTOTHERAPY MONITOR TEMP OF BABY EVERY 2-4 HR,MEASURE TSB EVERY 12-24HR DISCONTINUE PT ONCE 2 VALUE 12 HR APART FALL BELOW CURRENT AGE SPECIFIC CUT OFFS MONITOR REBOUND BILIRUBIN RISE WITHIN 24 HR AFTER STOPPING PT ROLE OF SUNLIGHT NOT HELP IN TREATMENT A/W RISK OF SUNBURN AND THEREFORE SHOULD BE AVOIDED
  • 26. EXCHANGE TRANSFUSION DVET SHOULD BE PERFORM IF TSB LEVEL REACH TO AGE SPECEFIC CUT-OFF VALUE FOR EXCHANGE TRANSFUSION OR INFANT SHOW SIGN OF ENCEPHALOPATHY IRRESPECTIVE OF TSB LEVEL INDICATION @ BIRTH----- CORD TSB IS ≥ 5 OR CORD HB≤ 10G/DL DONE BY PULL AND PUSH TECHNIQUE VIA UMBILICUS UMBILICAL CATHETOR VOLUME OF BLOOD 2X VOLUME OF BLOOD OF BABY 160-180ML/KG TO PREPARE BLOOD FOR DVET 2/3 OF PRBC AND 1/3 OF P PLASMA
  • 27.
  • 28. OTHER IVIG REDUCE HEMOLYSIS SO REDUCE JAUNDICE IN ABO/RH INCMPATABILITY REDUCE SIGNIFICANTLY NEED OF EXCHANGE TRANSFUSION NOW IVIG HAS REPLACED EXCHANGE TRANSFUSION AS THE SECOND LINE OF TREATMENT IN INFANT WITH ISOIMMUNE JAUNDICE DOSE 1G/KG/DOSE IV IV HYDRATION; IN SEVERE HYPERBILIRUBINEMIA AND EVIDENCE OF DEHYDRATION EG WT LOSS AN EXTRA FLUID 50ML/KG N/3 OVER 8 HR DECREASE NEED OF ET PHENOBARBITAL (LUMINAL)/CLOFIBRATE OR STEROIDS NO PROVEN EVIDENCE OF BENEFIT SO SHOULD NOT BE EMPLOYED
  • 29. THANK YOU HIMSR SOURCE NELSON CLOHERTY AIIMS NEONATALOGY PROTOCOL