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General Amino Acid Metabolism
Digestion & Absorption
• The main role of amino acids is in the synthesis of structural and
functional proteins.
• A 70 kg man has an average protein turnover rate of 400 g per day (same
amount synthesized and same amount broken down).
• The nonessential amino acids are either derived from the diet or
synthesized in the body.
• The essential amino acids are obtained from the diet.
• Even if one amino acid is deficient, protein synthesis cannot take place.
• The body amino acid pool is always in a dynamic steady state.
• In an adult, the rate of synthesis of proteins balances the rate of
degradation, so that nitrogen balance is maintained proteins are generally
not used for providing energy
Introduction:
Overview of metabolism of amino acids
• Proteolytic enzymes are secreted as inactive zymogens.
• These are then converted to their active form in the
intestinal lumen.
• This would prevent auto-digestion of the secretory
acini.
• Premature activation of trypsinogen results in acute
pancreatitis.
• It is a life-threatening condition.
Introduction:
Proteolytic enzymes
• The proteolytic enzymes include:
1. Endopeptidases: They act on peptide bonds inside the
protein molecule, so that the protein becomes successively
smaller and smaller units.
• This group includes Pepsin, Trypsin, Chymotrypsin and Elastase.
2. Exopeptidases: Which act only on the peptide bond located at
at the ends of the polypeptide chain.
• This group includes:
a. Carboxypeptidase, which acts only on the peptide bond at
the carboxy terminal end of the chain.
b. Aminopeptidase, which acts only on the peptide bond at the
amino terminal end of the chain.
Action of proteases. The enzyme
hydrolyses the peptide bond at the site of
arrow
Digestion of Proteins to Amino Acids
• Stomach : HCl and Pepsin
• Pancreas : Trypsin, Chymotrypsin, Elastase
• Intestine: Carboxypeptidase, Amino peptidase, Dipeptidase
GASTRIC DIGESTION OF PROTEINS
• In the stomach, hydrochloric acid is secreted.
• It makes the pH optimum for the action of pepsin and also
activates pepsin.
• The acid also denatures the proteins.
Rennin
• Rennin otherwise called Chymosin, is active in infants and is
involved in the curdling of milk.
• It is absent in adults.
• Milk protein, casein is converted to paracasein by the action
of rennin.
• This denatured protein is easily digested further by pepsin.
Pepsin
• It is secreted by the chief cells of stomach as inactive
pepsinogen.
• The conversion of pepsinogen to pepsin is brought about by
removal of 44 amino acids from the N-terminal end, by the
hydrochloric acid.
• The optimum pH for activity of pepsin is around 2.
• Pepsin is an endopeptidase.
• Pepsin catalyzes hydrolysis of the bonds formed by carboxyl
groups of Phe, Tyr, Trp and Met.
• By the action of pepsin, proteins are broken into proteoses
and peptones.
Rennin is active in infants and is involved in the
curdling of milk. It is absent in adults. Milk protein,
casein is converted to paracasein by the action of
rennin.
Rennin and Renin are different
Rennin is the proteolytic enzyme present in gastric juice.
Renin is proteolytic enzyme, secreted by kidneys. It is
involved in the activation of angiotensinogen to angiotensin,
a hypertensive agent.
PANCREATIC DIGESTION OF PROTEINS
• The optimum pH for the activity of pancreatic enzymes
(pH 8) is provided by the alkaline bile and pancreatic juice.
• The secretion of pancreatic juice is stimulated by the peptide
hormones, Cholecystokinin and Pancreozymin.
• Pancreatic juice contains the important endopeptidases,
namely Trypsin, Chymotrypsin, Elastase and
Carboxypeptidase.
• These enzymes are also secreted as zymogens (trypsinogen,
chymotrypsinogen and proelastase), so that the pancreatic
acinar cells are not autolyzed.
• All the three are serine proteases, i.e. the active centers of
these enzymes contain serine residues.
TRYPSIN
• Trypsinogen is activated by enterokinase (enteropeptidase)
present on the intestinal microvillus membranes.
• Once activated, the trypsin activates other enzyme molecules.
• Trypsin is activated by the removal of a hexapeptide from N-terminal
end.
• Trypsin catalyzes hydrolysis of the bonds formed by carboxyl groups
of Arg and Lys.
• Acute pancreatitis: Premature activation of trypsinogen inside the
pancreas itself, will result in the autodigestion of pancreatic cells.
• The result is acute pancreatitis.
• It is a life-threatening condition.
CHYMOTRYPSIN
• Trypsin will act on chymotrypsinogen, in such a manner that
A, B and C peptides are formed.
• These 3 segments are approximated, so that the active site is
formed.
• Thus selective proteolysis produces the catalytic site.
CARBOXYPEPTIDASES
• Trypsin and chymotrypsin degrade the proteins into small
peptides; these are further hydrolyzed into dipeptides and
tripeptides by carboxypeptidases present in the pancreatic
juice.
• The procarboxypeptidase is activated by trypsin.
• They are metalloenzymes requiring zinc.
Pepsin (endopeptidase) aromatic (tyr,phe, trp)
acidic (glu)
Trypsin (endopeptidase) basic (arg, lys)
Chymotrypsin (endopeptidase)aromatic (trp, phe, tyr,met)
Elastase (endopeptidase) neutral (gly, ser, ala)
Carboxy-peptidase A tyr, phe, trp val, leu, ile
(exopeptidase)
Carboxy- peptidase B basic (arg, lys)
(exopeptidase)
ENZYMES DIGESTING DIFFERENT GROUPS OF
AMINIACIDS
INTESTINAL DIGESTION OF PROTEINS
• Complete digestion of the small peptides to the level of
amino acids is brought about by enzymes present in
intestinal juice (succus entericus).
• The luminal surface of intestinal epithelial cells contains the
following enzymes:
• Aminopeptidases release the N-terminal amino acids.
• Dipeptidases and tripeptidases will complete the digestion
of proteins.
Summary of Digestion of Proteins
Enzyme Digestivity juice Activator Bond specificity Products
Pepsin
Endopeptidase
Aspartyl
Protease
Gastric juice
HCl-Pepsinogen to
Pepsin
Peptide bonds formed
by carboxyl groups of
Phe, Tyr, Trp & Met
Proteoses and peptones
Rennin
Gastric Juice HCl-Curdles milk Casien to paracasienate
Trypsin
Endopeptidase
Serine preotease
Pancreatic juice
Enterokinase-
Trypsinogen to
trypsin
CCK
Peptide bonds formed by carboxyl
groups of basic amino acids Arg &
Lys
Proteoses and peptones and
peptides
Chymotrypsin
Endopeptidase
Serine preotease
Pancreatic Juice Trypsin
Peptide bonds of hydrophobic
amino acids, Met, Leu, and
aromatic amino acids
Proteoses and peptones and
peptides
Elastase
Endopeptidase
Serine preotease
Pancreatic juice Trypsin
Proteoses and peptones and
peptides
Carboxy peptidase
Exopeptidase
Pancreatic juice Trypsin C terminal amino acid Free amino acid
Amino peptidases Intestinal juice N terminal amino acid Free amino acid
Tri- and
Dipeptidases
Intestinal juice Peptide bonds of small peptides Free amino acids
ABSORPTION OF AMINO ACIDS
• The absorption of amino acids occurs mainly in the small
intestine.
• It is an energy requiring process.
• These transport systems are carrier mediated and/or ATP sodium
dependent symport systems.
• There are 5 different carriers for amino acids:
1. Neutral amino acids (Ala, Val, Leu, Met, Phe, Tyr, Ile)
2. Basic amino acids (Lys, Arg) and Cysteine
3. Imino acids and Glycine
4. Acidic amino acids (Asp, Glu)
5. Beta amino acids (beta alanine).
MIESTER CYCLE (GAMMA-GLUTAMYL CYCLE)
• In intestines, kidney tubules and brain, the absorption of
neutral amino acids is effected by the gamma-glutamyl cycle.
• The tripeptide glutathione (GSH) (gammaglutamyl- cysteinyl
glycine) reacts with the amino acid to form gamma-glutamyl
amino acid.
• That is then cleaved to give the free amino acid.
• The net result is the transfer of an amino acid across the
membrane.
Gamma-glutamyl cycle (Meister cycle).
FOOD ALLERGY
• Dipeptides and tripeptides can enter the brush border of
mucosal cells; they are immediately hydrolyzed into single
amino acids.
• They are then transported into portal vein.
• These are immunogenic, causing antibody reaction, leading
to food allergy.
CLINICAL APPLICATIONS
1. The deficiency of the enzyme 5-oxoprolinase leads to
oxoprolinuria (pyroglutamic aciduria).
2. The allergy to certain food proteins (milk, fish) is believed to result from
absorption of partially digested proteins.
3. Defects in the intestinal amino acid transport systems are seen in
inborn errors of metabolism such as:
a. Hartnup disease
b. Imino glycinuria
c. Cystinuria
4. Partial gastrectomy, pancreatitis, carcinoma of pancreas and cystic
fibrosis may affect the digestion and absorption of proteins.
5. Protein-losing enteropathy: There is an excessive loss of proteins
through the gastrointestinal tract.
INTRACELLULAR PROTEIN DEGRADATION
• All proteins in the body are constantly being degraded.
• Half-life (t 1/2) of a protein is the time taken to lower its
concentration to half of the initial value.
• General tissue proteins have half lives of few hours.
• Key enzymes have half lives of about few minutes only.
• PEST sequence (areas rich in proline, glutamate, serine and threonine) on a
protein will give an inherent message to breakdown that protein very quickly.
• Proteins are taken by endocytosis and are fused with lysosomes.
• The half-life of proteins is highly variable.
• Ornithine decarboxylase has only 11 minutes.
• Half-life of hemoglobin depends on the lifespan of RBCs.
• The lens protein, Crystallin remains unchanged throughout the life of the
organism.
• Damaged or defective proteins are prematurely degraded.
CATHEPSINS
• In the phagolysosomes, the particles are broken down by
enzymes known as cathepsins.
• The term cathepsin is a Greek word, meaning ‘to digest'.
• Cathepsins are 18 in number, designated as A to T.
• Most of them are active at pH around 3 to 5.
UBIQUITIN
• Intracellular protein breakdown also occurs independent of
lysosomes.
• This involves ubiquitin.
• It is so named, because it is seen in all cells abundantly.
• It is a small protein with 76 residues (molecular weight, 8.5
kDa).
• Ubiquitin is attached to proteins.
PROTEASOMES
• Ubiquitin tagged proteins are immediately broken down
inside the proteasomes of the cells.
• Ciechanover, Hershko and Rose were awarded Nobel Prize in
2004 for their discovery of ubiquitin-mediated protein
degradation.
• There is a regular turnover of intracellular proteins.
• The half life of proteins is highly variable.
Examples:
• Ornithine decarboxylase has only 11 minutes.
• Insulin has a half-life of a few hours.
• Half-life of haemoglobin depends on the life span of RBCs.
• The lens protein, crystallin remains unchanged throughout the
life of the organism.
• Majority of proteins have a turnover rate of a few days.
Damaged or defective proteins are prematurely degraded.
Life Span of Proteins
Sources and fate of amino acid pool
Amino acid pool.
Sources and fate of amino acid pool
INTER-ORGAN TRANSPORT OF AMINO ACIDS
• Breakdown of muscle protein is the source of amino acids for
tissues while liver is the site of disposal.
• In Fasting State
• The muscle releases mainly alanine and glutamine of which alanine is taken
up by liver and glutamine by kidneys.
• Liver removes the amino group and converts it to urea and the carbon
skeleton is used for gluconeogenesis.
• Students should also see glucose-alanine cycle, under gluconeogenesis.
• The brain predominantly takes up branched chain amino acids.
Inter-organ transport of amino acids during fasting
conditions
In the Fed State
• Amino acids absorbed from the diet are taken up by different
tissues.
• Both muscle and brain take up branched chain amino acids,
and release glutamine and alanine.
• The glutamine is delivered to kidneys to aid in regulation of
acid-base balance, while alanine is taken up by liver.
Inter-organ transport of amino acids after taking food
(post-prandial condition)
Sources and fate of ammonia

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Digestion of proteins (1).ppt

  • 1. General Amino Acid Metabolism Digestion & Absorption
  • 2. • The main role of amino acids is in the synthesis of structural and functional proteins. • A 70 kg man has an average protein turnover rate of 400 g per day (same amount synthesized and same amount broken down). • The nonessential amino acids are either derived from the diet or synthesized in the body. • The essential amino acids are obtained from the diet. • Even if one amino acid is deficient, protein synthesis cannot take place. • The body amino acid pool is always in a dynamic steady state. • In an adult, the rate of synthesis of proteins balances the rate of degradation, so that nitrogen balance is maintained proteins are generally not used for providing energy Introduction:
  • 3. Overview of metabolism of amino acids
  • 4. • Proteolytic enzymes are secreted as inactive zymogens. • These are then converted to their active form in the intestinal lumen. • This would prevent auto-digestion of the secretory acini. • Premature activation of trypsinogen results in acute pancreatitis. • It is a life-threatening condition. Introduction: Proteolytic enzymes
  • 5. • The proteolytic enzymes include: 1. Endopeptidases: They act on peptide bonds inside the protein molecule, so that the protein becomes successively smaller and smaller units. • This group includes Pepsin, Trypsin, Chymotrypsin and Elastase. 2. Exopeptidases: Which act only on the peptide bond located at at the ends of the polypeptide chain. • This group includes: a. Carboxypeptidase, which acts only on the peptide bond at the carboxy terminal end of the chain. b. Aminopeptidase, which acts only on the peptide bond at the amino terminal end of the chain.
  • 6. Action of proteases. The enzyme hydrolyses the peptide bond at the site of arrow
  • 7. Digestion of Proteins to Amino Acids • Stomach : HCl and Pepsin • Pancreas : Trypsin, Chymotrypsin, Elastase • Intestine: Carboxypeptidase, Amino peptidase, Dipeptidase
  • 8. GASTRIC DIGESTION OF PROTEINS • In the stomach, hydrochloric acid is secreted. • It makes the pH optimum for the action of pepsin and also activates pepsin. • The acid also denatures the proteins. Rennin • Rennin otherwise called Chymosin, is active in infants and is involved in the curdling of milk. • It is absent in adults. • Milk protein, casein is converted to paracasein by the action of rennin. • This denatured protein is easily digested further by pepsin.
  • 9. Pepsin • It is secreted by the chief cells of stomach as inactive pepsinogen. • The conversion of pepsinogen to pepsin is brought about by removal of 44 amino acids from the N-terminal end, by the hydrochloric acid. • The optimum pH for activity of pepsin is around 2. • Pepsin is an endopeptidase. • Pepsin catalyzes hydrolysis of the bonds formed by carboxyl groups of Phe, Tyr, Trp and Met. • By the action of pepsin, proteins are broken into proteoses and peptones.
  • 10. Rennin is active in infants and is involved in the curdling of milk. It is absent in adults. Milk protein, casein is converted to paracasein by the action of rennin. Rennin and Renin are different Rennin is the proteolytic enzyme present in gastric juice. Renin is proteolytic enzyme, secreted by kidneys. It is involved in the activation of angiotensinogen to angiotensin, a hypertensive agent.
  • 11. PANCREATIC DIGESTION OF PROTEINS • The optimum pH for the activity of pancreatic enzymes (pH 8) is provided by the alkaline bile and pancreatic juice. • The secretion of pancreatic juice is stimulated by the peptide hormones, Cholecystokinin and Pancreozymin. • Pancreatic juice contains the important endopeptidases, namely Trypsin, Chymotrypsin, Elastase and Carboxypeptidase. • These enzymes are also secreted as zymogens (trypsinogen, chymotrypsinogen and proelastase), so that the pancreatic acinar cells are not autolyzed. • All the three are serine proteases, i.e. the active centers of these enzymes contain serine residues.
  • 12. TRYPSIN • Trypsinogen is activated by enterokinase (enteropeptidase) present on the intestinal microvillus membranes. • Once activated, the trypsin activates other enzyme molecules. • Trypsin is activated by the removal of a hexapeptide from N-terminal end. • Trypsin catalyzes hydrolysis of the bonds formed by carboxyl groups of Arg and Lys. • Acute pancreatitis: Premature activation of trypsinogen inside the pancreas itself, will result in the autodigestion of pancreatic cells. • The result is acute pancreatitis. • It is a life-threatening condition.
  • 13. CHYMOTRYPSIN • Trypsin will act on chymotrypsinogen, in such a manner that A, B and C peptides are formed. • These 3 segments are approximated, so that the active site is formed. • Thus selective proteolysis produces the catalytic site.
  • 14. CARBOXYPEPTIDASES • Trypsin and chymotrypsin degrade the proteins into small peptides; these are further hydrolyzed into dipeptides and tripeptides by carboxypeptidases present in the pancreatic juice. • The procarboxypeptidase is activated by trypsin. • They are metalloenzymes requiring zinc.
  • 15. Pepsin (endopeptidase) aromatic (tyr,phe, trp) acidic (glu) Trypsin (endopeptidase) basic (arg, lys) Chymotrypsin (endopeptidase)aromatic (trp, phe, tyr,met) Elastase (endopeptidase) neutral (gly, ser, ala) Carboxy-peptidase A tyr, phe, trp val, leu, ile (exopeptidase) Carboxy- peptidase B basic (arg, lys) (exopeptidase) ENZYMES DIGESTING DIFFERENT GROUPS OF AMINIACIDS
  • 16. INTESTINAL DIGESTION OF PROTEINS • Complete digestion of the small peptides to the level of amino acids is brought about by enzymes present in intestinal juice (succus entericus). • The luminal surface of intestinal epithelial cells contains the following enzymes: • Aminopeptidases release the N-terminal amino acids. • Dipeptidases and tripeptidases will complete the digestion of proteins.
  • 17. Summary of Digestion of Proteins Enzyme Digestivity juice Activator Bond specificity Products Pepsin Endopeptidase Aspartyl Protease Gastric juice HCl-Pepsinogen to Pepsin Peptide bonds formed by carboxyl groups of Phe, Tyr, Trp & Met Proteoses and peptones Rennin Gastric Juice HCl-Curdles milk Casien to paracasienate Trypsin Endopeptidase Serine preotease Pancreatic juice Enterokinase- Trypsinogen to trypsin CCK Peptide bonds formed by carboxyl groups of basic amino acids Arg & Lys Proteoses and peptones and peptides Chymotrypsin Endopeptidase Serine preotease Pancreatic Juice Trypsin Peptide bonds of hydrophobic amino acids, Met, Leu, and aromatic amino acids Proteoses and peptones and peptides Elastase Endopeptidase Serine preotease Pancreatic juice Trypsin Proteoses and peptones and peptides Carboxy peptidase Exopeptidase Pancreatic juice Trypsin C terminal amino acid Free amino acid Amino peptidases Intestinal juice N terminal amino acid Free amino acid Tri- and Dipeptidases Intestinal juice Peptide bonds of small peptides Free amino acids
  • 18. ABSORPTION OF AMINO ACIDS • The absorption of amino acids occurs mainly in the small intestine. • It is an energy requiring process. • These transport systems are carrier mediated and/or ATP sodium dependent symport systems. • There are 5 different carriers for amino acids: 1. Neutral amino acids (Ala, Val, Leu, Met, Phe, Tyr, Ile) 2. Basic amino acids (Lys, Arg) and Cysteine 3. Imino acids and Glycine 4. Acidic amino acids (Asp, Glu) 5. Beta amino acids (beta alanine).
  • 19. MIESTER CYCLE (GAMMA-GLUTAMYL CYCLE) • In intestines, kidney tubules and brain, the absorption of neutral amino acids is effected by the gamma-glutamyl cycle. • The tripeptide glutathione (GSH) (gammaglutamyl- cysteinyl glycine) reacts with the amino acid to form gamma-glutamyl amino acid. • That is then cleaved to give the free amino acid. • The net result is the transfer of an amino acid across the membrane.
  • 21. FOOD ALLERGY • Dipeptides and tripeptides can enter the brush border of mucosal cells; they are immediately hydrolyzed into single amino acids. • They are then transported into portal vein. • These are immunogenic, causing antibody reaction, leading to food allergy.
  • 22. CLINICAL APPLICATIONS 1. The deficiency of the enzyme 5-oxoprolinase leads to oxoprolinuria (pyroglutamic aciduria). 2. The allergy to certain food proteins (milk, fish) is believed to result from absorption of partially digested proteins. 3. Defects in the intestinal amino acid transport systems are seen in inborn errors of metabolism such as: a. Hartnup disease b. Imino glycinuria c. Cystinuria 4. Partial gastrectomy, pancreatitis, carcinoma of pancreas and cystic fibrosis may affect the digestion and absorption of proteins. 5. Protein-losing enteropathy: There is an excessive loss of proteins through the gastrointestinal tract.
  • 23. INTRACELLULAR PROTEIN DEGRADATION • All proteins in the body are constantly being degraded. • Half-life (t 1/2) of a protein is the time taken to lower its concentration to half of the initial value. • General tissue proteins have half lives of few hours. • Key enzymes have half lives of about few minutes only. • PEST sequence (areas rich in proline, glutamate, serine and threonine) on a protein will give an inherent message to breakdown that protein very quickly. • Proteins are taken by endocytosis and are fused with lysosomes. • The half-life of proteins is highly variable. • Ornithine decarboxylase has only 11 minutes. • Half-life of hemoglobin depends on the lifespan of RBCs. • The lens protein, Crystallin remains unchanged throughout the life of the organism. • Damaged or defective proteins are prematurely degraded.
  • 24. CATHEPSINS • In the phagolysosomes, the particles are broken down by enzymes known as cathepsins. • The term cathepsin is a Greek word, meaning ‘to digest'. • Cathepsins are 18 in number, designated as A to T. • Most of them are active at pH around 3 to 5.
  • 25. UBIQUITIN • Intracellular protein breakdown also occurs independent of lysosomes. • This involves ubiquitin. • It is so named, because it is seen in all cells abundantly. • It is a small protein with 76 residues (molecular weight, 8.5 kDa). • Ubiquitin is attached to proteins.
  • 26. PROTEASOMES • Ubiquitin tagged proteins are immediately broken down inside the proteasomes of the cells. • Ciechanover, Hershko and Rose were awarded Nobel Prize in 2004 for their discovery of ubiquitin-mediated protein degradation.
  • 27. • There is a regular turnover of intracellular proteins. • The half life of proteins is highly variable. Examples: • Ornithine decarboxylase has only 11 minutes. • Insulin has a half-life of a few hours. • Half-life of haemoglobin depends on the life span of RBCs. • The lens protein, crystallin remains unchanged throughout the life of the organism. • Majority of proteins have a turnover rate of a few days. Damaged or defective proteins are prematurely degraded. Life Span of Proteins
  • 28. Sources and fate of amino acid pool
  • 29.
  • 30. Amino acid pool. Sources and fate of amino acid pool
  • 31. INTER-ORGAN TRANSPORT OF AMINO ACIDS • Breakdown of muscle protein is the source of amino acids for tissues while liver is the site of disposal. • In Fasting State • The muscle releases mainly alanine and glutamine of which alanine is taken up by liver and glutamine by kidneys. • Liver removes the amino group and converts it to urea and the carbon skeleton is used for gluconeogenesis. • Students should also see glucose-alanine cycle, under gluconeogenesis. • The brain predominantly takes up branched chain amino acids.
  • 32. Inter-organ transport of amino acids during fasting conditions
  • 33. In the Fed State • Amino acids absorbed from the diet are taken up by different tissues. • Both muscle and brain take up branched chain amino acids, and release glutamine and alanine. • The glutamine is delivered to kidneys to aid in regulation of acid-base balance, while alanine is taken up by liver.
  • 34. Inter-organ transport of amino acids after taking food (post-prandial condition)
  • 35. Sources and fate of ammonia