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M.Prasad Naidu
MSc Medical Biochemistry, Ph.D,.
 Proteins  most abundant org.compound
 Major part of the body dry wt (10-12Kg)
 Perform wide variety of functions. Viz
 1. Static functions ( Structural functions)
 2. Dynamic functions( Enzy, hor, receptors)
 Half of the body protein is (Collagen) is present
in supportive tissue (skeletan & connective)
while the other half is intracellur.
 Proteins are the N- containing macro molecules
 Consists of L- AAs as repeating units
 Of the 20 AAs half can be synthesized
 Essential and non-essential AAs
 Proteins on degradation release AAs
 Each AA undergoes its own metabolism
 Proteins metabolism is more appropriately learnt
as metabolism of amino acids.
 An adult has about 100 gm of Free AA which represent
the AA pool of the body.
 Glutamate and Glutamine together constitute about 50%
and EAA 10% of the body pool.
 The conc of intracellular AA is always higher than the
Extracellular AA
 AAs enter the cells againt Active transport
 The AA pool is maintained by the sources that contribute
( input) and the metabolic pathways that utilize (out put)
the amino acids.
 1. Turnover of body protein
 2. intake of dietary protein
 3. synthesis of non- EAAs
 The protein present in the body is in a dynamic state.
 About 300-400 gm of protein per day is constantly
degraded and synthesized which represent the body
protein turnover.
 There is wide variation the turnover of individual
proteins.
 Eg: plasma proteins & digestive enzymes are rapidly
degraded ( half life is hrs/days)
 Structural proteins have long half lives often months and
years.
 many factors
 1. Ubiquitin : small PP – 8,500 – tags with the
proteins and facilitates degradation.
 2. PEST Sequences: - Certain proteins with
Pro, Gln, Ser, Thr sequence are rapidly degraded.
 Regular loss of protein due to degradation of AAs.
 About 30-50 gm protein is lost every day from the body.
 This amount must be supplied daily in the diet to
maintain N Balance.
 There is no storage form of AAs unlike the
Carbohydrates and lipids (TG)
 The excess AAs – metabolised – oxidized –Energy or
glucose or fat.
 The daily protein intake by adults is 40-100gm
 10 out of 20 naturally occurring AAs can be
synthesized by the body which contributes to AA
pool.
 1. most of the body proteins (300-400g/D) degraded are
synthesized from the AA pool. ( enzymes, hormones,
immuno proteins, contractile proteins)
 Many imp N compounds ( porphyrins, purines &
pyrimidines) are produced from AA . About 30g of
protein is daily utilized for this purpose.
 Generally, about 10-15% of body energy requirements
are met from the AAs
 The AAs are converted to Car, fats. This becomes
predominant when the protein consumption is in excess
of the body requirements.
 AAs undergo common reactions
 Transamination followed by
 Deamination for the liberation of NH3
 The NH2 group of AAs is utilized for the
formation of urea (excretory end product of
protein metabolism)
 The C-skeleton of the AAs is first converted to
keto acids (by transamination) which meet one
or more of the following fates
 Utilized to generate energy
 Used for the synthesis of glucose
 Derived for the formation of fat / ketone bodies
 Involved in the production of non-EAAs
 Transfer of an amino group from an AA to a keto
acid
 This process involves the interconversion of a pair
of AAs and a pair of keto acids
 Transaminases / aminotransferases
 All transaminases require PALP
 Specific transaminases exist for each pair of amino and keto acids
 However, only two namely Asp. transaminase & Ala. transaminase
make a significant contribution for transamination
 There is no free NH3 liberated, only the transfer of NH3 group occurs
 Reversible
 Production of non-EAAs as per the requirement of the cell
 Diverts the excess of AAs towards Energy generation
 AAs undergo TAN to finally concentrate N in glutamate
 Glutamate is the only AA that undergoes OD to liberate
free NH3 for urea synthesis
 All AAs except Lys, Thr, Pro & Hy.pro participate in TAN
 TAN is not restricted to α-group only. (eg: δ-amino group
of Ornithine is transaminated.
 Serum transaminases are important for diagnostic and
prognostic purposes
 SGPT or ALT is elevated in all liver diseases
 SGOT or AST is increased in myocardial infarction
 Occurs in 2 stages.
 1. Transfer of the NH2 group to the coenzyme
PLP ( bound to the coenzyme) to form
Pyridoxamine Phosphate.
 2. The NH2 group of Pyridoxamine PO4 is then
transferred to a keto acid to produce a new AA
and the enzyme with PLP is regenerated.
 All the transaminases require PLP , a derivative of Vit B6
 The – CHO group of PLP is linked with έ-NH2 group of
Lys, at the active site of the enzyme forming a Schiff’s
base (imine linkage)
 When an AA comes in contact with the enzyme, it
displaces lys and a new Schiff base linkage is formed.
 The AA-PLP-Schiff base tightly binds with the enzyme
by non covalent forces.
 Snell & Braustein proposed Ping-Pong Bi Bi mechanism
involving a series of intermediates ( aldimines &
ketimines) in transamination reaction.
 The removal of amino group from the AAs as NH3
 Transamination involves only shuffling of NH3 groups
among the AAs
 Deamination results in the liberation of NH3 for urea
synthesis
 Simultaneously, the C-skeleton of AAs is converted to
keto acids
 2 types (Oxidative & Non oxidative)
 Transamination & Deamination occurs simultaneously,
often involving glutamate as the central molecule
(Transdeamination)
 Liberation of free NH3 from the AAs coupled with
oxidation
 Liver & kidney
 Purpose of OD: to provide NH3 for urea synthesis
& α-ketoacids for a variety of reactions, including
Energy generation
 In the process of Transamination, the NH3 groups of most of the AAs
are transferred to α-KG to produce glutamate
 Thus , glutamate serves as a collection centre for amino groups in
the biological system
 Glutamate rapidly undergoes oxi.deamination by GDH to liberate
NH3
 GDH is unique in that it can use utilize either NAD+ or NADP+
 Conversion of glutamate to α-KG occurs through the formation of α-
iminoglutarate
 GDH catalyzed reaction is imp as it reversibly links up glutamate
metabolism with TCA cycle through α-KG
 GDH is involved in both catabolic & anabolic reactions.
 Zn containing mitochondrial enzyme
 Complex enzyme containing 6 identical units with a
mol.wt of 56000 each.
 GDH is controlled by allosteric regulation
 GTP , ATP, steroid & Thyroid hormones are inhibitors of
GDH
 GDP and ADP are activators
 After ingestion of protein meal, liver glutamate level is ↑.
 It is converted to α-KG with liberation of NH3
 Further , when cellular E levels are ↓low, the
degradation of glutamate is ↑ to provide α-KG which
enters TCA cycle to liberate Energy
 L- AAoxidase & D-AAoxidase are flavo proteins,
possessing FMN and FAD respectively.
 They act on corresponding AAs to produce α-Ketoacids
& NH3
 In this reaction, O2 is reduced to H2O2, which is later
decomposed by catalase
 The activity of L-AAoxidase is much low while D-
AAoxidase is high in tissues (liver & kidneys)
 L-AAoxidase does n’t act on Gly & dicarboxylicacids
 D-AAs are found in plants & mos
 Absent in mammalian proteins
 But D-AAs are regularly taken in diet and are
metabolized
 D-AAoxidase converts them into α-ketoacids by od.
 The α-ketoacids so produced undergo TAN to be
converted to L-AAs
 Ketoacids may be oxidized to generate energy or serve
as precursor for glucose & fat synthesis
 Thus D-AAoxidase is imp as it initiates the first step for
the conversion of unnatural D-AAs to L-AAs in the body.
 Some of the AAs can be deaminated to liberate NH3 without
undergoing oxidation
 A) Aminoacid dehydrases:
 Ser,Thr,Homoserine α-ketoacids
 Catalyzed by PLP dependent dehydrases (dehydratases)
 B)Aminoacid desulfhydrases:
 Cys, homocysteine  pyruvate
 Deamination coupled with desulfhydration
 C) Deamination of histidine:
 Histidine  urocanate
 histidase

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Amino Acids metabolism

  • 1. M.Prasad Naidu MSc Medical Biochemistry, Ph.D,.
  • 2.  Proteins  most abundant org.compound  Major part of the body dry wt (10-12Kg)  Perform wide variety of functions. Viz  1. Static functions ( Structural functions)  2. Dynamic functions( Enzy, hor, receptors)  Half of the body protein is (Collagen) is present in supportive tissue (skeletan & connective) while the other half is intracellur.
  • 3.  Proteins are the N- containing macro molecules  Consists of L- AAs as repeating units  Of the 20 AAs half can be synthesized  Essential and non-essential AAs  Proteins on degradation release AAs  Each AA undergoes its own metabolism  Proteins metabolism is more appropriately learnt as metabolism of amino acids.
  • 4.  An adult has about 100 gm of Free AA which represent the AA pool of the body.  Glutamate and Glutamine together constitute about 50% and EAA 10% of the body pool.  The conc of intracellular AA is always higher than the Extracellular AA  AAs enter the cells againt Active transport  The AA pool is maintained by the sources that contribute ( input) and the metabolic pathways that utilize (out put) the amino acids.
  • 5.  1. Turnover of body protein  2. intake of dietary protein  3. synthesis of non- EAAs
  • 6.  The protein present in the body is in a dynamic state.  About 300-400 gm of protein per day is constantly degraded and synthesized which represent the body protein turnover.  There is wide variation the turnover of individual proteins.  Eg: plasma proteins & digestive enzymes are rapidly degraded ( half life is hrs/days)  Structural proteins have long half lives often months and years.
  • 7.  many factors  1. Ubiquitin : small PP – 8,500 – tags with the proteins and facilitates degradation.  2. PEST Sequences: - Certain proteins with Pro, Gln, Ser, Thr sequence are rapidly degraded.
  • 8.  Regular loss of protein due to degradation of AAs.  About 30-50 gm protein is lost every day from the body.  This amount must be supplied daily in the diet to maintain N Balance.  There is no storage form of AAs unlike the Carbohydrates and lipids (TG)  The excess AAs – metabolised – oxidized –Energy or glucose or fat.  The daily protein intake by adults is 40-100gm
  • 9.  10 out of 20 naturally occurring AAs can be synthesized by the body which contributes to AA pool.
  • 10.  1. most of the body proteins (300-400g/D) degraded are synthesized from the AA pool. ( enzymes, hormones, immuno proteins, contractile proteins)  Many imp N compounds ( porphyrins, purines & pyrimidines) are produced from AA . About 30g of protein is daily utilized for this purpose.  Generally, about 10-15% of body energy requirements are met from the AAs  The AAs are converted to Car, fats. This becomes predominant when the protein consumption is in excess of the body requirements.
  • 11.  AAs undergo common reactions  Transamination followed by  Deamination for the liberation of NH3  The NH2 group of AAs is utilized for the formation of urea (excretory end product of protein metabolism)  The C-skeleton of the AAs is first converted to keto acids (by transamination) which meet one or more of the following fates
  • 12.  Utilized to generate energy  Used for the synthesis of glucose  Derived for the formation of fat / ketone bodies  Involved in the production of non-EAAs
  • 13.  Transfer of an amino group from an AA to a keto acid  This process involves the interconversion of a pair of AAs and a pair of keto acids  Transaminases / aminotransferases
  • 14.  All transaminases require PALP  Specific transaminases exist for each pair of amino and keto acids  However, only two namely Asp. transaminase & Ala. transaminase make a significant contribution for transamination  There is no free NH3 liberated, only the transfer of NH3 group occurs  Reversible  Production of non-EAAs as per the requirement of the cell  Diverts the excess of AAs towards Energy generation
  • 15.  AAs undergo TAN to finally concentrate N in glutamate  Glutamate is the only AA that undergoes OD to liberate free NH3 for urea synthesis  All AAs except Lys, Thr, Pro & Hy.pro participate in TAN  TAN is not restricted to α-group only. (eg: δ-amino group of Ornithine is transaminated.  Serum transaminases are important for diagnostic and prognostic purposes  SGPT or ALT is elevated in all liver diseases  SGOT or AST is increased in myocardial infarction
  • 16.  Occurs in 2 stages.  1. Transfer of the NH2 group to the coenzyme PLP ( bound to the coenzyme) to form Pyridoxamine Phosphate.  2. The NH2 group of Pyridoxamine PO4 is then transferred to a keto acid to produce a new AA and the enzyme with PLP is regenerated.
  • 17.  All the transaminases require PLP , a derivative of Vit B6  The – CHO group of PLP is linked with έ-NH2 group of Lys, at the active site of the enzyme forming a Schiff’s base (imine linkage)  When an AA comes in contact with the enzyme, it displaces lys and a new Schiff base linkage is formed.  The AA-PLP-Schiff base tightly binds with the enzyme by non covalent forces.  Snell & Braustein proposed Ping-Pong Bi Bi mechanism involving a series of intermediates ( aldimines & ketimines) in transamination reaction.
  • 18.  The removal of amino group from the AAs as NH3  Transamination involves only shuffling of NH3 groups among the AAs  Deamination results in the liberation of NH3 for urea synthesis  Simultaneously, the C-skeleton of AAs is converted to keto acids  2 types (Oxidative & Non oxidative)  Transamination & Deamination occurs simultaneously, often involving glutamate as the central molecule (Transdeamination)
  • 19.  Liberation of free NH3 from the AAs coupled with oxidation  Liver & kidney  Purpose of OD: to provide NH3 for urea synthesis & α-ketoacids for a variety of reactions, including Energy generation
  • 20.  In the process of Transamination, the NH3 groups of most of the AAs are transferred to α-KG to produce glutamate  Thus , glutamate serves as a collection centre for amino groups in the biological system  Glutamate rapidly undergoes oxi.deamination by GDH to liberate NH3  GDH is unique in that it can use utilize either NAD+ or NADP+  Conversion of glutamate to α-KG occurs through the formation of α- iminoglutarate  GDH catalyzed reaction is imp as it reversibly links up glutamate metabolism with TCA cycle through α-KG  GDH is involved in both catabolic & anabolic reactions.
  • 21.  Zn containing mitochondrial enzyme  Complex enzyme containing 6 identical units with a mol.wt of 56000 each.  GDH is controlled by allosteric regulation  GTP , ATP, steroid & Thyroid hormones are inhibitors of GDH  GDP and ADP are activators  After ingestion of protein meal, liver glutamate level is ↑.  It is converted to α-KG with liberation of NH3  Further , when cellular E levels are ↓low, the degradation of glutamate is ↑ to provide α-KG which enters TCA cycle to liberate Energy
  • 22.  L- AAoxidase & D-AAoxidase are flavo proteins, possessing FMN and FAD respectively.  They act on corresponding AAs to produce α-Ketoacids & NH3  In this reaction, O2 is reduced to H2O2, which is later decomposed by catalase  The activity of L-AAoxidase is much low while D- AAoxidase is high in tissues (liver & kidneys)  L-AAoxidase does n’t act on Gly & dicarboxylicacids
  • 23.  D-AAs are found in plants & mos  Absent in mammalian proteins  But D-AAs are regularly taken in diet and are metabolized  D-AAoxidase converts them into α-ketoacids by od.  The α-ketoacids so produced undergo TAN to be converted to L-AAs  Ketoacids may be oxidized to generate energy or serve as precursor for glucose & fat synthesis  Thus D-AAoxidase is imp as it initiates the first step for the conversion of unnatural D-AAs to L-AAs in the body.
  • 24.  Some of the AAs can be deaminated to liberate NH3 without undergoing oxidation  A) Aminoacid dehydrases:  Ser,Thr,Homoserine α-ketoacids  Catalyzed by PLP dependent dehydrases (dehydratases)  B)Aminoacid desulfhydrases:  Cys, homocysteine  pyruvate  Deamination coupled with desulfhydration  C) Deamination of histidine:  Histidine  urocanate  histidase