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Section 8. Amino Acid Metabolism Urea cycle 11/18/05 Substrates for the Urea Cycle -amino acid -keto acid -ketoglutarate glutamate NADH H2N-CO-OPO32- NAD+ • Above, amino groups are transferred to glutamate, from which ammonium is produced, and then used to make carbamoyl phosphate. • Below, amino groups are transferred to produce aspartate. -amino acid -ketoglutarate -keto acid glutamate 1 aspartate oxaloacetate Urea Cycle Fig. 23.16 2 • Aspartate and carbamoyl phosphate each deliver an amino group to the cycle. • Notice that the carbamoyl phosphate production and condensation occur in the mitochondrial matrix. NH4+ from Oxidative Deamination of Glutamate O O + NH3 H CH2 CH2 O O glutamate NAD+ NADH + H+ O O O CH2 CH2 glutamate dehydrogenase O + NH4+ O -ketoglutarate • Hexameric glutamate dehydrogenase is is controlled allosterically. – High energy levels inhibit (ATP and GTP). – Low energy levels activate (ADP and GDP). • NADP+ can replace NAD+. • NH4+ , which is toxic to humans, is produced in the mitochondria and used to make carbamoyl phosphate. 3 Carbamoyl Phosphate Synthesis (p. 645) • Carbamoyl phosphate synthetase is in mitochondrial matrix. • NH4+ is source of NH3. • The hydrolysis of two ATP make this reaction essentially irreversible. 4 • N-acetyl glutamate is an allosteric activator. (see S08L05) O H O N CH 2 CH 2 Pi + O O P O O H2N CH 2 H carbamoyl phosphate O O H + H 3N CH 2 + ATP + NH 3 O O aspartate O O 4 NH 2 citrulline 1 + NH 3 + CH 2 ornithine UREA CYCLE CH 2 CH 2 + H NH 3 O 2 ~ P used 2 Pi + H NH 3 O O H2N H 2N H NH2 UREA H2O N CH 2 CH 2 H O 5 AMP + PPi + 3 O O H N N + H CH 2 CH 2 CH 2 O O CH 2 H (1-3 in cytosol, 4 in mitochondial matrix) O O H 2N NH 2 CH 2 + NH 3 O argininosuccinate 2 O H O H O O fumarate arginine 1. ARGININOSUCCINATE SYNTHASE 2. ARGININOSUCCINASE 3. ARGINASE 4. ORNITHINE TRANSCARBAMOYLASE Connection to Krebs Cycle + ATP -keto acid aspartate citrulline -amino acid 1 UREA CYCLE Oxaloacetate argininosuccinate + AMP + PPi NADH 2 Pi NAD+ 2 arginine Malate fumarate H20 6 • Fumarate is oxidized to oxaloacetate by Krebs cycle enzymes, producing NADH. • Oxaloacetate accepts an amino group instead of being condensed with acetyl CoA. amino acid -keto acid -ketoglutate glutamate * NH4+ + CO 2 Amino Acids to Urea + 2 ATP + H2O 2 ADP + Pi + H+ + carbamoyl phosphate ornithine + citrulline UREA CYCLE ATP -keto acid aspartate amino acid argininosuccinate Oxaloacetate + AMP + PPi H2N O UREA 2 Pi NH2 Malate arginine H2O fumarate *Glutamate Dehydrogenase is the control site: ADP (+), 7 GDP (+), ATP (-), GTP (-) and NADH (-). Control at other sites by glucagon (+), cortisol (+), insulin (-), growth hormone (-). Summary of Reactions and Energetics - 1 H20 + aa + NAD+ -keto acid + NH4+ + NADH + H+ and H20 + fumarate + aa + NAD+ aspartate + -keto acid + NADH + H+ then aspartate + NH4+ + HCO3- + 3 ATP urea + fumarate + 2 H20 + 2 ADP + AMP + 4 Pi + H+ Four high energy phosphate bond equivalents are used for these reactions (- 4 ~P). Two NADH are produced. 8 Summary of Reactions and Energetics - 2 Now consider NADH oxidation: 2 H+ + 2 NADH + O2 2 NAD+ + 2 H20 (+5 ~P) The net reaction is then 2 aa + HCO3- + O2 2 -keto acid + urea + H+ + 2 H20 (+1~P) 9 Hyperammonemia • Normal blood [NH4+] is 10-40 mM. • Deficiencies of carbamoyl phosphate synthetase or of any enzyme in the urea cycle cause high [NH4+]. • Affects CNS and can lead to irreversible brain damage. • Treatment strategies depend on which enzyme is deficient. 10 • Low dietary protein reduces need for urea cycle. H O NH 3 • High dietary arginine + ATP provides a path for CH carbamoyl phosphate O O and aspartate aspartate nitrogens to produce argininosuccinate, O O which is excreted. HN CH 2 H O O O P O O H2N Argininosuccinase Deficiency N CH 2 CH 2 NH 2 H 3N H 4 + NH 3 O O citrulline 1 + ornithine + 2 UREA CYCLE CH 2 CH 2 + H NH 3 O + O H2N NH2 UREA H2O H N CH2 CH2 11 + AMP + PPi 2 Pi + NH 3 O O NH2 CH2 + H NH3 O H N N H CH 2 CH 2 CH 2 O O CH 2 H H2N 3 O O H 2 CH 2 carbamoyl phosphate O + argininosuccinate 2 (excreted) O H O H O O fumarate O arginine (excess supplied) Carbamoyl Phosphate Synthetase Deficiency Fig. 23.20 12 • Hippurate and phenylacetylglutamine are excreted. • Amino groups to glycine and glutamine by transamination. Ketogenic and Glucogenic Amino Acids Fig. 23.21 • After removal of the amino group, the keto acids are used to make 13 Krebs cycle intermediates, pyruvate, acetyl CoA and acetoacetyl CoA. Nitrogen for Oral Bacteria H2NCONH2 + H+ + H2O urease 2 NH4+ + HCO3- • Urea is a major source of nitrogen for oral bacteria. • It diffuses through most membranes and is in saliva. • Bacterial urease produces NH4+. • Glutamate dehydrogenase incorporates NH4+ into -keto acids to obtain amino acids for bacterial growth. 14 Nitrogen for Bacterial Amino Acid Synthesis NADPH + H+ -ketoglutarate + NH4+ glutamate glutamate dehydrogenase ATP glutamate + NH4+ NADP+ + H20 ADP + Pi glutamine glutamine synthase NADPH + H+ -ketoglutarate + glutamine NADP+ 2 glutamate glutamate synthase • When [NH4+] is limiting, it does not bind glutamate dehydrogenase, 15 and the lower two reactions are used. Engineered Oral Bacteria to Fight Caries? • Streptococcus Salivarius urease activity affects oral microbial ecology. • It produces NH3, which in addition to promoting growth, neutralizes acids produces by other bacteria. • S. Salivarius urease gene was introduced into Streptococcus mutans GS5. It was expressed and during glucose metabolism reduced pH decrease and duration. • 16 (Clancy & Burne,1997 FEMS Microbiol Lett 151:205) Web links Nitrogen Fixation. A summary of the topic. Nitrogen Cycle. The biological big picture. Amino Acid Metabolism. Reviews reactions. Next topic: Porphyrins, heme, bile pigments