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In Born Error of Metabolism (IEM)

In Born Error of Metabolism (IEM). Dr Mohammad Khassawneh Assistant professor of pediatrics. Introduction. When to consider it What to do quickly to determine it is present or not. How to identify?. Prospective approach for a healthy newborn

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In Born Error of Metabolism (IEM)

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  1. In Born Error of Metabolism (IEM) Dr Mohammad Khassawneh Assistant professor of pediatrics

  2. Introduction • When to consider it • What to do quickly to determine it is present or not

  3. How to identify? • Prospective approach for a healthy newborn • Reactive approach to a clinically abnormal child

  4. Common conception about IEM • Rarely a cause of disease in neonates • Hyperphenylalaninemia 1:10,000 • Galactosemia 1:50,000 • Homocystinurea 1:200,000 • Estimated overall incidence 1:2000 • Many of metabolic diseases are under diagnosed

  5. Common conceptions • It should only be considered with a family history • AR disease 2 sibs diseased 6%, 2 of 3 14%… • X-linked commonly a new mutation • Hard to differentiate from sepsis • Galctosemia and e- coli • Many diseases present different from sepsis illness

  6. Common Conception • Biochemical pathway are impossible to remember • This is true for expert • Pathways are not the important part of the evaluation • general approach is more important • It is difficult to conduct diagnostic study • Should progress from broad to specific

  7. Continue • Few metabolic diseases are treatable • Should give more consideration to treatable conditions • Genetic counseling sake • Gene therapy hold a promise

  8. Newborn Screening • Reliable screen test and low false negative • Test is simple and inexpensive • Available results soon to start effective therapy • Definite follow up test • Outcome without treatment is very bad • Effective therapy is available

  9. Clinical presentations • The “sick” newborn infant • Cardiomegaly/cardiomyopathy • Eye anomalies / Gastrointestinal abnormalities • Hair and skin abnormalities • Hematological / Hepatic dysfunction • Sepsis • Unusual odor • PKU mousy smell • Cystiurea sulfourus smell

  10. Sick newborn • Cardiorespiratory, central nervous system, poor feeding • Present in1st week of life • Lethargy and coma low tone & Seizure • Acidosis or hyperamonemia may lead to respiratory distress • Causes: • include fatty acid, carbohydrate, organic acid, respiratory chain, ammonia metabolism

  11. Example/hyperglycenemia • AR disorder • Profound hypotonia, poor feeding, hiccupping, lethargy • Coma and Seizure with myoclonic jerk • Elevated CSF/plasma glycine • EEG findings

  12. Cardiomegaly and cardiomyopathy • Beta oxidation • glycogen storage • Most common is Pompe disease (acid maltase) generalize hypotonia and FTT • Lysosomal (cytoplasmic organelles) • MPS, sphingolipid, glycoprotein • mitochondria disorders

  13. Hurler Syndrome and others • AR, alfa L-idurinidase • Coarsening of feature 6-12 monthes • Cloud cornea • Deafness • Cardiomypathy • Airway obstruction • Death by early teenage • Scheie, Hunter, Sanfilippo’s, Morquio

  14. Eye abnormalities • Cataract: galactosemia, adrenoleukodystrophy, mucopolysacharidosis • Lens dislocation: homocystinurea, marfan • Blue sclera in oseogenesis imperfecta • Cherry red spot in lysosomal disorder (farber disease)

  15. Gastrointestinal/Hair and skin • Vomiting in acidosis and urea cycle defect • Menkes disease: spares kinky scalp hair associated with hypotonia, intractable seizure and developmental delay • PKU: Fair hair and skin • Multiple carboxylase deficiency skin rash and partial allopecia

  16. Hepatic dysfunction • Enlargement (lysosomal storage disorder) • Hypoglycemia • Galactosemia • Hereditary fructose intolerance • Hepatocellular damage, like above and adrenoleukodystrophy, fatty acid oxidase def. • Cholestatic disease • Alfa 1 antitrepsine, ZZgenotype

  17. Initial laboratory screening • Blood • Cell count, electrolytes, amonia, uric acid • Blood gas, lactate and pyrovate • Glucose and ketones • Urine: • smell, pH, acetone, ketone • Reducing substances • CSF: lactate pyrovate and glucose

  18. Specialized biochemical testing • Amino acid analysis • Maple syrup apple disease with increase leuocine, valine and isoleuocine • Hyperglycinemia: increase glycine • Organic acid : propionic acidemia • Carnitine level • Chromatographic of glycolipid • Increased level of long chain fatty acid with perioxysomal disorder

  19. galactosemia • Deficiency of galactose-1 phosphate uridyl transferase • 1/50,000 • Start early after feeding • Autosomal recessive on chromosome 9p13 with male=female • Affect brain, liver, kidny and overies

  20. Galactosemia / clinical • No enzyme …accumulation of galactose1 phosphate • Liver; cirrhosis • Kidney; fancony syndrome • Brain; mental retardation • Overy; amenorrhea • Galactose to galactitol cause cataract

  21. Hepatic and GI manifestation • Lethargy irritability and vomiting • Feeding difficulty and poor weight gain • Jaundice, hypoglycemia, hepatomegally • Ascites • Hepatic cirrhosis

  22. others • Plydypsia, polyurea • Rickets • Mental retardation • Seizure • Cataract: perinuclear haziness to complete opacification • Fulminante-coli sepsis

  23. investigation • Positive clinitest and negative clinistix • Urine galactose by chromatography • Direct hyperbilirubinemia • RBC’s galactose 1 phosphate uridyl transferase activity • Increase galactose 1phosphate in RBC

  24. management • Lactose free formula • Control seizure • Consult ophthalmology • Consult endocrinology • Genetic counseling

  25. Phenylketonurea (PKU) • Phenylalanine hydroxylase deficiency • Excess phenylalanine and its metabolites • Normal at birth and months to diagnose • Vomitting sever/ misdiagnosed pyloric stenosis. • Fair skin and blue eyes • Eczema and skin rash

  26. PKU…continue • Musty or mousey smell • Microcephaly • Growth retardation • 50 point loss of IQ in the first year • Clinical feature are rarely seen Neonatal screening

  27. diagnosis • Guthrie test; bacterial inhibition , positive in 4 hr old • Preferable sample at >24-48 hr of life • Positive test should be followed by Phenylalanine and tyrosine • Increase PA, NL tyrosine, and increase PA metabolites in urine like phenylpyrovic

  28. treatment • Reduce phenylalanine and metabolites in blood. • Formula low in phenylalanine • Level between 3-15mg/dl • Remember over treatment • Lethargy anorexia anemia rash diarrhea • Treatment indefinitely • Maternal PKU. Mental retarded/ microcphaly/ cardiac defect, keep level <10mg/dl

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