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Dr VISHAL H KACHHY

  FELLOW IN NEONATAL
       MEDICINE
   SYNERGY HOSPIAL,
      AHMEDABAD
3 Month old child referred for neonatal
                  Hepatitis .
First child
Born out of non consanguineous marriage.
Birth weight was 2.1kg(Low) and on
regular follow up
O/E: failure to thrive
      Mild Fullness of Abdomen
      Liver size- Just Palpable.(May be
     considered Normal)
• RS - WNL
• CVS- WNL
INVESTIGATION

• CBC
     Hb:12.1; TC:8900 ,DC:65/35/2/2
               Platelet:3.25
• CRP-0.8 ( Neg)
• SGPT-112
• PT -17/13
• S. Bil – T- 4.2
           D-2.2
           I-2.0
DIAGNOSIS
                  Neonatal Hepatitis
               (Viral markers- Negative)

Supportive Treatment was started and advise to follow up
  after one week
One week on,jaundice- persistent; there was no
  appreciable change in SGPT and PT and now there was
  some abdominal distention due to ascites.
 Liver and Spleen was just palpable,
 CNS, CVS and RS were all normal.
FURTHER INVESTIGATION
• S. Ammonia- Raised
• Urine for Routein Biochemestry - Normal
• Total plasma galactose - Normal
The child appeared well but there was a failure
 to thrive with his weight actually showing
 progressive decreasing trend.
    Now the ascites had increased. So small
 dose of diuretics was added

      Investigation were repeated
• LFT showed hepatocellular damage, both PT
  and ammonia showed worsening trend.
  RFT, Electrolytes were normal
  Patient was sent for further opinion.
• USG Moderate ascites and mild hepato-
  spleenomegaly
• Serum albumin: ascitic fluid albumin
  gradient was less than 0.8
• Bilirubin 15 mg with 70% direct,
• SGPT - 762, ALP was 308
• PT was 27/14 sec.
• Ammonia was 131,
• Creatinine 1.4 mg.
• S.ferritin, S. alpha fetoprotein- Normal
Differential diagnosis ?

How will you proceed now
Neonatal Ascites:
                       .
• Fetal or neonatal ascites is rare and occurs in
  about 1:3000 pregnancies
Common causes include
• Metabolic diseases.
   – Lysosomal storage disorders like,
      •   Salla disease
      •   Mucolipidosis type-II
      •   Niemann-Pick type-C
      •   MPS type-VII
      •   GMI galgliosidosis
      •   Wolman’s disease
      •   Gaucher’s diseases
Neonatal Ascites(Cont):

    – Hepatorenal Tyrosinemia type-I
    – Neonatal Hemochromatosis
    – Carbohydrate Deficient Glycoprotein Syndrome.
•   Urinary ascites.
•   Biliary ascites.
•   Chylous ascites.
•   Cardiac ascites.
Ascites(Cont):
In older children, due to
     Trauma,
      Infection, particularly tuberculosis,
      Hepatocellular disease,
      Pancreatic ascites,
      Gynecologic,
      GI abnormalities,
      Neoplasia,
      and other miscellaneous causes.
Biliary Ascites:

• Rare in Neonates.
• occurs in infants younger than 3 months.
• Hepatobiliary isotope scanning demonstrates radionuclide in
  the peritoneal cavity.
• Ultrasonography is usually necessary to rule out congenital
  anomalies and obstructing lesions.
• Paracentesis reveals elevated bilirubin levels in the fluid. .
• The perforation usually seals in a few weeks in the absence
  of obstruction or else it requires surgical intervention
Chylous Ascites
• Most cases occur in infancy, with a male
  predominance,
• The diagnosis is confirmed with paracentesis;
  markedly elevated triglyceride content (>1500
  mg/dL) and a predominance of lymphocytes
  (>75%).
• After surgical causes, eg, malrotation, obstruction,
  and neoplasia) have been ruled out with
  appropriate imaging studies, more than one half of
  patients respond to conservative treatment with
  parenteral nutrition and bowel rest for 2-4 weeks.
• Idiopathic neonatal chylous ascites is associated
  with a high mortality rate.
Hepatocellular Diseases

• Storage disease, neonatal or viral hepatitis,
  alpha1-antitrypsin deficiency,Hemochomatosis
• Paracentesis reveals the presence of fluid with
  a serum-to-ascites albumin gradient (<1.1
  g/dL).
Peritoneal infection:

• Appendicitis is common in
 patients in developed countries,
 whereas tuberculous fluid
 collections and Salmonella
 organisms are observed in
 patients in the developing
 world.
Pancreatic Ascites
• Either from trauma or pancreatitis.
• Paracentesis reveals fluid with markedly
  elevated amylase and lipase levels
• Bowel rest and TPN are the initial therapies,
  with the administration of somatostatin
  analogs.
Iatrogenic ascites:

• Ascites may occur (particularly while the
  patient is in the neonatal intensive care unit
  [NICU]) as a result of gastric perforation from
  gastric catheters.
• Umbilical catheter perforation may result in
  the leakage of parenteral nutrition fluid
Some useful clues for diagnosis:
•       If a large bladder is present, the ascites is probably
  urinary.
•      If vomiting occurs or bowel loops are abnormal
  even though not distended, gastrointestinal causes are
  likely.
•      If there is impressive peripheral or body wall
  edema, consider infection, heart disease, liver disease,
  erythroblastosis, and other causes of hydrops fetalis
•       If hepatomegaly is present, metabolic causes of
  liver diseases are most likely.
Rapid liver failure in a neonatal jaundice is
 almost always secondary to metabolic
 disorders.
         Infection or structural diseases take a
 longer time to produce liver failure.
Common Metabolic liver
       diseases of the newborn:
• Galactosemia:
         Hyperbilirubinemia,(initially even
             unconjugated),
         Hemolytic anemia,
         Sepsis, especially with E. coli.
         Cataract (not very common in Indian neonatal
  population).
Common Metabolic liver
 diseases of the newborn(Cont)
• Hepatorenal Tyrosinemia:
    High Plasma tyrosine levels and urinary
 succinyl acetone, very high alpha fetoprotein
 and marked coagulopathy.
• Hereditary Fructose Intolerance (HFI):
 Lactic acidosis, hypoglycemia, hyperuricemia.
 Menifest after introduction of fructose;
 presence of reducing substances in the urine,
Common Metabolic liver
 diseases of the newborn(Cont)
• Glycogen Storage Diseases type-IV:
  Cirrhosis early in the disease,prominent
  hypoglycemia, and myopathy.

• Peroxisomal Disorders and Mitochondrial
  Disorders: : Developmental delay, failure to
  thrive, seizures, hypotonia.Multi System
  Disease
Common Metabolic liver diseases
    of the newborn(Cont)

 • Neonatal Hemochromatosis:
     Severe hepatocellular dysfunction,
     High ferritin and
     High transferrin saturation.
Any Lead to Diagnosis?
Storage Disease
TMS blood sent- Normal
Urine was screened for metabolic disorders.
Sialic acid level in urine was measured and it
 was 30 times the normal, suggesting sialic
 aciduria or Salla disease.
Patient was treated with diuretics and
supportive treatment for liver failure; but had
convulsions and GI bleed and died within a
fortnight.
Salla disease
• Refers to LSD first reported in a geographically
  restricted area in northern Finland.
• The enzyme defect in this condition has not been well
  documented as yet.
• Defect in gene SLC17A5 located on chromosome 6
• Increased levels of free neuraminic acid are found in
  the urine.
• Abdominal distension due to varying amounts of
  ascites and hepatosplenomegaly may be the presenting
  feature.
• The cause for ascites is obscure.
• Sialic acid storage disease
    - Autosomal Reccesive disorder that
  primarily affects the nervous system.
  - Signs and symptoms that may vary widely in
  severity.
  - Classified into one of three forms:
       * Infantile free sialic acid storage disease,
       * Salla disease, and
       *Intermediate severe Salla disease.
Infantile Free Sialic Acid Storage Disease (ISSD)


         The most severe form of this disorder. Babies
with this condition have severe developmental delay,
hypotonia, and failure to thrive coarse facial features
seizures, bone malformations, hepatosplenomegaly and
rarely cardiomegaly. Affected infants may have a
condition called hydrops fetalis
        Children with this severe form of the condition
usually live only into early childhood.
The Diagnosis can be confirmed by
• Characteristic histological findings on light
  and electron microscopy
• Characteristic cellular enzyme defects and
• Urinary excretory products in these patients.
        No spacific treatment is avilable, only
  supportive and symptomatic treatment directed
  towards complication
Salla disease

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Salla disease

  • 1. Dr VISHAL H KACHHY FELLOW IN NEONATAL MEDICINE SYNERGY HOSPIAL, AHMEDABAD
  • 2. 3 Month old child referred for neonatal Hepatitis . First child Born out of non consanguineous marriage. Birth weight was 2.1kg(Low) and on regular follow up O/E: failure to thrive Mild Fullness of Abdomen Liver size- Just Palpable.(May be considered Normal) • RS - WNL • CVS- WNL
  • 3. INVESTIGATION • CBC Hb:12.1; TC:8900 ,DC:65/35/2/2 Platelet:3.25 • CRP-0.8 ( Neg) • SGPT-112 • PT -17/13 • S. Bil – T- 4.2 D-2.2 I-2.0
  • 4. DIAGNOSIS Neonatal Hepatitis (Viral markers- Negative) Supportive Treatment was started and advise to follow up after one week One week on,jaundice- persistent; there was no appreciable change in SGPT and PT and now there was some abdominal distention due to ascites. Liver and Spleen was just palpable, CNS, CVS and RS were all normal.
  • 5. FURTHER INVESTIGATION • S. Ammonia- Raised • Urine for Routein Biochemestry - Normal • Total plasma galactose - Normal
  • 6. The child appeared well but there was a failure to thrive with his weight actually showing progressive decreasing trend. Now the ascites had increased. So small dose of diuretics was added Investigation were repeated
  • 7. • LFT showed hepatocellular damage, both PT and ammonia showed worsening trend. RFT, Electrolytes were normal Patient was sent for further opinion.
  • 8. • USG Moderate ascites and mild hepato- spleenomegaly • Serum albumin: ascitic fluid albumin gradient was less than 0.8 • Bilirubin 15 mg with 70% direct, • SGPT - 762, ALP was 308 • PT was 27/14 sec. • Ammonia was 131, • Creatinine 1.4 mg. • S.ferritin, S. alpha fetoprotein- Normal
  • 9. Differential diagnosis ? How will you proceed now
  • 10. Neonatal Ascites: . • Fetal or neonatal ascites is rare and occurs in about 1:3000 pregnancies Common causes include • Metabolic diseases. – Lysosomal storage disorders like, • Salla disease • Mucolipidosis type-II • Niemann-Pick type-C • MPS type-VII • GMI galgliosidosis • Wolman’s disease • Gaucher’s diseases
  • 11. Neonatal Ascites(Cont): – Hepatorenal Tyrosinemia type-I – Neonatal Hemochromatosis – Carbohydrate Deficient Glycoprotein Syndrome. • Urinary ascites. • Biliary ascites. • Chylous ascites. • Cardiac ascites.
  • 12. Ascites(Cont): In older children, due to Trauma, Infection, particularly tuberculosis, Hepatocellular disease, Pancreatic ascites, Gynecologic, GI abnormalities, Neoplasia, and other miscellaneous causes.
  • 13. Biliary Ascites: • Rare in Neonates. • occurs in infants younger than 3 months. • Hepatobiliary isotope scanning demonstrates radionuclide in the peritoneal cavity. • Ultrasonography is usually necessary to rule out congenital anomalies and obstructing lesions. • Paracentesis reveals elevated bilirubin levels in the fluid. . • The perforation usually seals in a few weeks in the absence of obstruction or else it requires surgical intervention
  • 14. Chylous Ascites • Most cases occur in infancy, with a male predominance, • The diagnosis is confirmed with paracentesis; markedly elevated triglyceride content (>1500 mg/dL) and a predominance of lymphocytes (>75%). • After surgical causes, eg, malrotation, obstruction, and neoplasia) have been ruled out with appropriate imaging studies, more than one half of patients respond to conservative treatment with parenteral nutrition and bowel rest for 2-4 weeks. • Idiopathic neonatal chylous ascites is associated with a high mortality rate.
  • 15. Hepatocellular Diseases • Storage disease, neonatal or viral hepatitis, alpha1-antitrypsin deficiency,Hemochomatosis • Paracentesis reveals the presence of fluid with a serum-to-ascites albumin gradient (<1.1 g/dL).
  • 16. Peritoneal infection: • Appendicitis is common in patients in developed countries, whereas tuberculous fluid collections and Salmonella organisms are observed in patients in the developing world.
  • 17. Pancreatic Ascites • Either from trauma or pancreatitis. • Paracentesis reveals fluid with markedly elevated amylase and lipase levels • Bowel rest and TPN are the initial therapies, with the administration of somatostatin analogs.
  • 18. Iatrogenic ascites: • Ascites may occur (particularly while the patient is in the neonatal intensive care unit [NICU]) as a result of gastric perforation from gastric catheters. • Umbilical catheter perforation may result in the leakage of parenteral nutrition fluid
  • 19. Some useful clues for diagnosis: • If a large bladder is present, the ascites is probably urinary. • If vomiting occurs or bowel loops are abnormal even though not distended, gastrointestinal causes are likely. • If there is impressive peripheral or body wall edema, consider infection, heart disease, liver disease, erythroblastosis, and other causes of hydrops fetalis • If hepatomegaly is present, metabolic causes of liver diseases are most likely.
  • 20. Rapid liver failure in a neonatal jaundice is almost always secondary to metabolic disorders. Infection or structural diseases take a longer time to produce liver failure.
  • 21. Common Metabolic liver diseases of the newborn: • Galactosemia: Hyperbilirubinemia,(initially even unconjugated), Hemolytic anemia, Sepsis, especially with E. coli. Cataract (not very common in Indian neonatal population).
  • 22. Common Metabolic liver diseases of the newborn(Cont) • Hepatorenal Tyrosinemia: High Plasma tyrosine levels and urinary succinyl acetone, very high alpha fetoprotein and marked coagulopathy. • Hereditary Fructose Intolerance (HFI): Lactic acidosis, hypoglycemia, hyperuricemia. Menifest after introduction of fructose; presence of reducing substances in the urine,
  • 23. Common Metabolic liver diseases of the newborn(Cont) • Glycogen Storage Diseases type-IV: Cirrhosis early in the disease,prominent hypoglycemia, and myopathy. • Peroxisomal Disorders and Mitochondrial Disorders: : Developmental delay, failure to thrive, seizures, hypotonia.Multi System Disease
  • 24. Common Metabolic liver diseases of the newborn(Cont) • Neonatal Hemochromatosis: Severe hepatocellular dysfunction, High ferritin and High transferrin saturation.
  • 25. Any Lead to Diagnosis?
  • 26. Storage Disease TMS blood sent- Normal Urine was screened for metabolic disorders. Sialic acid level in urine was measured and it was 30 times the normal, suggesting sialic aciduria or Salla disease.
  • 27. Patient was treated with diuretics and supportive treatment for liver failure; but had convulsions and GI bleed and died within a fortnight.
  • 28. Salla disease • Refers to LSD first reported in a geographically restricted area in northern Finland. • The enzyme defect in this condition has not been well documented as yet. • Defect in gene SLC17A5 located on chromosome 6 • Increased levels of free neuraminic acid are found in the urine. • Abdominal distension due to varying amounts of ascites and hepatosplenomegaly may be the presenting feature. • The cause for ascites is obscure.
  • 29. • Sialic acid storage disease - Autosomal Reccesive disorder that primarily affects the nervous system. - Signs and symptoms that may vary widely in severity. - Classified into one of three forms: * Infantile free sialic acid storage disease, * Salla disease, and *Intermediate severe Salla disease.
  • 30. Infantile Free Sialic Acid Storage Disease (ISSD) The most severe form of this disorder. Babies with this condition have severe developmental delay, hypotonia, and failure to thrive coarse facial features seizures, bone malformations, hepatosplenomegaly and rarely cardiomegaly. Affected infants may have a condition called hydrops fetalis Children with this severe form of the condition usually live only into early childhood.
  • 31. The Diagnosis can be confirmed by • Characteristic histological findings on light and electron microscopy • Characteristic cellular enzyme defects and • Urinary excretory products in these patients. No spacific treatment is avilable, only supportive and symptomatic treatment directed towards complication