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Urea cycle and its defects

Urea cycle and its defects . Dr.S.Chakravarty MD. Learning objectives:. Explain the fate of carbon skeleton and nitrogen group of amino acids. Explain the ways of transport of nitrogen from various parts of the body to the liver

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Urea cycle and its defects

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  1. Urea cycle and its defects Dr.S.Chakravarty MD

  2. Learning objectives: • Explain the fate of carbon skeleton and nitrogen group of amino acids. • Explain the ways of transport of nitrogen from various parts of the body to the liver • Describe the urea cycle and the enzymes involved in production of urea in the liver • Define and classify Hyperammonemias . List the enzymes deficient in various hyperammonemias and its clinical features

  3. Catabolism of Amino acids • Amino group – NH3Formation of urea • Carbon skeletons – Formation of Glucose and Ketone bodies.

  4. FATE OF THE CARBON SKELETONS Carbon skeletons are used for energy Glucogenic: TCA cycle intermediates or Pyruvate (Gluconeogenesis) Ketogenic: Acetyl CoA, Acetoacetyl CoA, or Acetoacetate

  5. DIGESTION AND ABSORPTION • PROTEINS • Gastric juice ( acidity denatures proteins ) • Intestinal enzymes hydrolyze • AMINO ACIDS • Amino acid transporters Na+Amino acid symporter (can take up di and tri peptides ) • UPTAKE DEFECTS :- 1)Hartnups disease  Long neutral amino acid transporter defect( Trp is not taken up  Pellagra like symptoms as Trp Niacin is not formed ) 2)Cystinuria Basic amino acid transporter defect that also transports cysteineUrinary stones .Cystine forms Cystine by disulfide linkage (less soluble Stones )

  6. EXCESS AMINO ACIDS ARE DEGRADED NOT STORED OVERVIEW OF AMINO ACID METABOLISM ENVIRONMENTORGANISM Bio- synthesis Protein Ingested protein 2 3 1 Recycling a AMINO ACIDS b c Degradation (required) c Purines Pyrimidines Porphyrins Nitrogen NH3 Carbon skeletons Urea (ketogenic) (glucogenic) pyruvate α-ketoglutarate succinyl-CoA fumarate oxaloacetate Used for energy acetoacetate acetyl CoA

  7. NH3 is TOXIC

  8. Why ammonia is toxic ? • Affects central nervous system • Alkalization of intracellular compartment • Disrupts oxidative phosphorylationATP depletion • Increased glutamate in Brain • Decreased Neurotransmitters – GABA – convulsions • Cerebral edema

  9. Symptoms of AMMONIA toxicity • Flapping Tremor (Asterixis) • ( Correlate flapping tremor later on with Liver failure in Clinical medicine ) • Slurred Speech • Blurred Vision • COMA  Death

  10. Metabolic fates of ammonia • Ammonotelic – Fishes • Lots of water available • Uricotelic – Reptiles and birds • Birds have to keep minimum body weight for flight • Ureotelic – Mammals

  11. Adults degrade 1-2% of body protein daily Body Proteins 80-85% Amino acids 25% Catabolism UREA

  12. Amino acids Sources of Amino Acids : Utilization of Amino acids: Synthesis of New proteins Formation of Nucleotides Formations of Porphyrins and Catecholamines Production of energy and Ammonia. • Exogenous – Diet • Endogenous – • Breakdown of muscle protein • Biosynthesis from intermediates of citric acid cycle.

  13. Fate of Amino group 1) Reutilization: Glutamate and Glutamine are involved in recycling of amino acids. ATP ADP Glutamate + Ammonia Glutamine Glutamine Synthase • They are secreted by the peripheral tissues in form of glutamine which is taken up by hepatocytes where the NH3 is re-used for amino acid and nucleotide synthesis Glutamine Glutamate + Ammonia Glutaminase

  14. 2. Formation of amino acids from carbon skeletons require ammonia • Two important reactions are involved in fixing ammonia back to amino acids: • Reductive Amination: • Amino Transferases: • All non-essential amino acids except for tyrosine and cysteineare derived and are dependent on transamination from glutamate.

  15. 1. Reductive Amination : NAD(P)H NAD(P) Alpha ketoglutarate + Ammonia Glutamate Glutamate dehydrogenase 2. Transamination reaction: Alpha keto acid-1 Amino acid-1 Transaminase Alpha keto acid-2 Amino acid-2 PLP

  16. UREA • Well balanced polarity (Quite uncharged because of amide nitrogen yet sufficiently soluble in plasma  No transporter required ) • Non-Toxic AMMONIA ASPARTATE

  17. CATABOLISM OF PROTEINS • UREA BIOSYNTHESIS IS DIVIDED INTO 4 STAGES:- • 1. TRANSAMINATION • 2. OXIDATIVE DEAMINATION • 3. AMMONIA TRANSPORT • 4. REACTIONS OF THE UREA CYCLE

  18. TRANSAMINATION • DEF:-THE TRANSFER OF THE ALPHA-AMINO GROUP FROM ONE AMINO ACID TO A KETO ACID , RESULTING IN FORMATION OF A NEW AMINO ACID AND CORRESPONDING KETO ACID . • E.G :- REACTION CATALYZED BY ALANINE AMINOTRANSFERASE ALANINE PYRUVATE (AMINO ACID ) (CORRESPONDING KETO ACID ) α-KETOGLUTARATE GLUTAMATE (KETO ACID )(NEW AMINO ACID) ALT ALL TRANSAMINASES REQUIRE PLP (VIT B6) PLP

  19. TRANSAMINATION Corresponding KA AA New AA KA

  20. USES OF TRANSAMINATION • FIRST STEP OF CATABOLISM OF PROTEINS • SYNTHESIS OF NON-ESSENTIAL AMINO ACIDS and INTERCONVERSION OF AMINO ACIDS • REGENERATION OF TCA CYCLE intermediates

  21. OVERALL FLOW OF NITROGEN IN AMINO ACID CATABOLISM

  22. Sources of ammonia in the body • Aminoacids: • Transamination • Deamination • Transulfuration • Glutaminase • Gastrointestinal tract bacteria • Degradation of Amino sugars • Monoamine Oxidase • Pyrimidine catabolism

  23. Nitrogen metabolism • Nitrogen part is toxic. Excreted in the form of either : • Ammonia – charged and alkaline. Excreted as ammonium ion in urine (3%) • Urea – Neutral molecule – Non toxic –( 80-85%) • Creatinine (3-4%) – constant in urine ( 1% of Creatine every day) • Uric acid – from Purines only !

  24. Inter organ exchange of amino acids

  25. The Glucose alanine cycle

  26. Kaplan lecture notes USMLE step 1

  27. Kaplan lecture notes USMLE step 1 Very important NH3 removal mechanism ( esp BRAIN)

  28. Kaplan lecture notes USMLE step 1 WHY ALANINE ? NOT GLUTAMATE DIRECTLY (ALT) (AST) 2ND NITROGEN 1ST NITROGEN

  29. Sources of ammonia in the body • Aminoacids: • Transamination • Deamination • Transulfuration • Glutaminase • Gastrointestinal tract bacteria • Degradation of Amino sugars • Monoamine Oxidase • Pyrimidine catabolism

  30. Nitrogen metabolism • Nitrogen is Excreted in the form of either : • Ammonia – charged and alkaline. Excreted as ammonium ion in urine (3%) • Urea – Neutral molecule – Non toxic –( 80-85%) • Creatinine (3-4%) – constant in urine ( 1% of Creatine every day) • Uric acid – from Purines only !

  31. Inter organ exchange of amino acids in post absorptive state (FASTING)

  32. Inter organ exchange of amino acids in absorptive state (after feeding)

  33. The Glucose alanine cycle ALT (Transamination) ALT (Transamination)

  34. UREA • Well balanced polarity (Quite non polar because of amide nitrogen yet sufficiently soluble in plasma  No transporter required ) • Non-Toxic AMMONIA ASPARTATE

  35. Urea cycle High protein Diet Ammonia + Bicarbonate + ATP NAG – N-acetyl Glutamate CPS -1 activator Carbomyl Phosphate OrnithineTranscarbomylase Ornithine Citrulline Mitochondria Cytoplasm Arginosuccinatesynthase Aspartate Oxaloacetate Arginosuccinate ArginosuccinateLyase Fumarate TCA cycle Arginase Arginine Urea

  36. Production of NAG: Acetyl Co-A + Glutamate N-acetyl Glutamate (NAG) N-acetyl glutamate synthase (NAGS) Arginine N-acetyl glutamate is the allosteric activator of Carbomyl phosphate synthase-1.

  37. Urea cycle disorders • Hyperammonemia • Encephalopathy • Respiratory alkalosis • VOMITING • AVOIDANCE OF HIGH PROTEIN FOODS • INTERMITTENT ATAXIA • LETHARGY • SEVERE MENTAL RETARDATION

  38. Symptoms of AMMONIA toxicity • Tremor • ( Correlate flapping tremor later on with Liver failure in Clinical medicine ) • Slurred Speech • Blurred Vision • COMA  Death

  39. Disorders of UREA cycle Hyperammonemia type -1 Hyperammonemia type -2 X-linked recessive Defect in OTC MC urea cycle defect Oroticaciduria present Cerebral oedema , coma and death. • Autosomal recessive • Defect in CPS- 1 • 1 in 200,000 • No oroticaciduria • Cerebral Oedema , coma and death . CAUSE OF OROTIC ACIDURIA Increased Carbamoyl phosphate  spills out from mitochondia to cytosolPyrimidine synthesis Orotic acid

  40. 3. Citrullinemia : • Defect in arginosuccinatesynthase • Citrullinuria • Autosomal recessive 4. Arginosuccinicaciduria: • Defect in arginosuccinatelyase • Arginosuccinic acid  blood, CSF, Urine 5. Hyperargininemia : • Diet without arginine • Defect in arginase enzyme

  41. Treatment of Hyperammonemia: • Limit protein intake • Decrease bacterial source of ammonia – Antibiotics (Like Neomycin, Azithromycin)and Lactulose (purgative ) • Replace intermediates of urea cycle – ArginineCitrulline, Aspartate • Remove excess ammonia – Hemodialysis, sodium benzoate, phenyl acetate Very Important Very Important

  42. Drugs • Lactulose – Acidification – conversion to NH4+ and induction of Purgation • Mainstay • Gut sterilization :-Neomycin/Azithromycinother antibiotics • Very Important • Combination of Sodium benzoate and Phenylacetate/Phenylbutyrate • Sodium benzoate + Glycine  Hippuric acid  excreted • Phenylacetate phenylacetyl glutamine  excreted. (Phenylacetate conjugates with glutamine to form phenylacetylglutamine, which is excreted by the kidneys) • Rarely used

  43. Source http://biocadmin.otago.ac.nz

  44. MCQ 1 Select the CORRECT answer . The first reaction in the degradation of the majority of common amino –acids involves participation of : • NAD + • Pyridoxal Phosphate • Thiamine Pyrophosphate(TPP) • FAD • NAD and TPP

  45. MCQ 2 • After thorough investigations a man is diagnosed with oroticaciduria. To find out the cause of oroticaciduria which of the following investigations will you prefer? • A. ALP levels • B. vitamin b12 assay • C. FIGLU excretion assay • D. Peripheral smear • E. serum bilirubin

  46. Thank you

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