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Title: Amino Acids:

1

Amino Acids
Disposal of Nitrogen

2
Overview

Amino acids are not stored in the body
So, Amino Acids must be obtained from
1-Diet
2-Synthesized de novo
3-produced from normal protein degradation
(turnover)
Amino Acids in excess of biosynthetic needs of
the cell
Not stored
But rapidly degraded
first step removal of the a-amino group
a-ketoacid
(of
a.a.)
ammonia
exc. in urine
UREA

3
Synthesis
of proteins

other
compoundsAmino Acid
Diet Degrad. of Proteins De novo synthesis

Degradation
a-Ketoacid
Ammonia
(carbon skeleton) (nitrogen of
a.a.)
Glucose Fatty acids other
exc. In urine UREA
ketone Bodies compounds
Glycogen
exc. in
urine
ENERGY

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Amino Acid Pool

100 grams of a.a.
Collected from
Dietary Proteins (by hydrolysis)
Degradation of Tissue Proteins
De novo synthesis of a.a.
Fate of amino acids obtained by tissue protein
hydrolysis
75 of amino acids used to
synthesize new proteins
25 of amino acids metabolized
precursor for other compounds
compensated by dietary proteins
---- amino acids

6
Protein Turnover

Protein turnover results from the simultaneous
synthesis degradation of tissue proteins
The total amounts of protein in the body is
constant because the rate of protein synthesis
is just sufficient to replace the degraded
protein
Protein turnover leads to hydrolysis synthesis
of 300-400 grams of body protein each day

7
Rate of Protein Turnover

Short-lived proteins minutes hours half-life
(as many regulatory proteins misfolded
proteins)
Long-lived proteins days weeks half-life
(majority of proteins in the cell)
Structural proteins months years half-live
(as collagen)

8
Protein Degradation

By Two Major Enzyme Systems
1- Ubiquitin-proteasome mechanism
energy-dependent
mainly for endogenous proteins
(proteins synthesized within the cell)
2- Lysosomes
non-energy-dependen
primarily for extracellular proteins as
- plasma proteins that are taken into cells
by endocytosis
- cell surface membrane proteins for
receptor-mediated endocytosis

9
Ubiquitin-proteasome pathway
10
Mechanism of action of ubiquitin-proteasome
system

Protein is covalently attached to ubiquitin
(small globular protein)
More ubiquitin is added to form polyubiquitin
chain (protein is tagged with ubiquitin)
Ubiquitin-tagged protein is recognized by the
proteasome (proteolytic molecule)
The proteasome cuts the target protein into
fragments
(requires ATP)
Fragments are cut by non-specific proteases to
amino acids

11
Chemical Signals for Protein Degradation

Protein degradation is influenced by some
structural aspect of the protein
Examples
The half-life of a protein is influenced by the
nature of the N-terminal
residue
with serine long-lived proteins (half-life
is more than 20 hours)
with aspartate short-lived (half-life is
about 3 minutes)
Proteins rich sequence containing PEST
rapidly degraded (i.e. with short
half-life)
PEST sequence proline, glutamate, serine
threonine

12
Digestion of Dietary Proteins

Most of the nitrogen in diet is consumed in the
form of protein
Dietary protein/day 70 100 grams
Dietary proteins must be hydrolyzed to amino
acids by proteolytic
enzymes
Proteolytic enzymes are produced by three
different organs
stomach
pancreas
small intestine

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1- Digestion of Proteins By Gastric Secretion

Gastric secretions contains
1- hydrochloric Acid - pH 2 3 (for activation
pepsinogen)
- kills
some bacteria
-
denature proteins
2- Pepsin secreted as peopsinogen (inactive
zymogen)
activated to pepsin by Hcl or
autocatalytically by pepsin
product of hydrolysis of
proteins peptides few free amino acids
(oligo- poly-)

15
2- Digestion of Proteins by Pancreatic Enzymes

On entering the small intestine
Pancreatic Proteases
Large polypeptides are further cleaved
to oligopeptides free amino acids
PROTEASES
Secreted as inactive zymogen from pancreatic
cells
Secretion of zymogens
is mediated by the secretion of
cholecystokinin secretin (polypeptide hormones
of GIT)
Activation of zymogen
by enteropeptidase (enterokinase) enzyme
present on the luminal surface of intestinal
mucosal cells
converts trypsinogen to trypsin (by
removal of hexapeptide from trypsinogen)
Trypsin converts other trypsinogen
molecules to trypsin
Trypsin activates all other pancreatic
zymogens (chymotrypsinogen, proelastase
procarboxypeptidases)
Specificity

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Abnormalities in Protein Digestion
Deficiency of pancreatic secretion
occurs due to chronic pancreatitis, cystic
fibrosis or
surgical removal of the pancreas
Digestion absorption of fat protein is
incomplete
Abnormal appearance of lipids (steatorrohea)
undigested protein in feces

18
3- Digestion of oligopeptides by enzymes of the
Small Intestine

Aminopeptidases
- on the luminal surface of the intestine
- is an exopeptidase
- cleaves the N-terminal residue from
oligopeptides
to produce free amino acids smaller
peptides

19
Transport of Amino acids into cells

Movement of a.a. to cells is performed by active
transport (requires ATP)
Seven different transport systems
with overlapping specificity for different
amino acids
for example cystine, ornithine, argenine
lysine are transported in kidney tubules
by one transporter
In cystinuria Inherited disease , one of the
most common inherited dis.
1 7000 individuals
defective carrier
system for these 4 amino acids
appearance of all 4
amino acids in the urine
precipitation of
cystine to form kidney stones (may block urinary
tract)

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Removal of Nitrogen from Amino Acids

Removing the a-amino group
Essential for producing energy from any amino
acid
An obligatory step for the catabolism of all
amino acids

22
Amino Acids
23
Amino Acid
24
Amino Acid (deamination)removal of amino
group (nitrogen)

Amino group carbon
(nitrogen)
skeleton
(a-ketoacid)
incorporated
into
other excreted
catabolised synthesis
Compounds
of other compounds
(e.g. urea)
energy

25
Deamination Pathways

Amino group (nitrogen) is removed from an
amino acid by either
1- Transamination (BY
TRANSAMINASES)
2- Oxidative Deamination (BYGLUTAMATE
DEHYDROGENASE)

26
1- Transamination
Funneling of amino groups to glutamate

a-ketoglutarate accepts the amino group from
amino acids to become glutamate
By aminotransferases (transaminases)
Glutamate
Oxidat. Deam ammonia urea cycle
Or
gives amino group to oxalacetate to
produce aspartate--- urea cycle
Or
gives amino group to carbon skeleton to
produce new amino acid
All amino acids (with the exception of
lysine threonine) participate in transamination

27
Substrate Specificity of Aminotransferases

Each aminotransferase is specific for one or few
group of donors
Aminotransferase is named after the specific
amino group donor (amino acid that donates its
amino group)
The 2 most important aminotransferases
1- alanine aminotransferase (ALT)
2- aspartate aminotranspeptidase (AST)

28
ALanine AminoTransferase (ALT) ASpartate
AminoTransferase (AST)
amino acid Carbon skeleton of
alanine UREA CYCLE
29
Mechanism of Action of Aminotransferase
30
Equlibrium of Transamination Reactions

Equilibrium constant 1
Allowing the reaction to function in both
directions
after protein-rich meal
amino acid degradation
(removal of amino group from amino acid
a-keto acid)
supply of amino acids from diet is not adequate
amino acid biosynthesis
(addition of amino group to a-keto acid
amino acid)

31
Diagnostic Value of Plasma Aminotransferases

Aminotransferases are normally intracellular
enzymes
Plasma contains low levels of aminotransferases
representing release of cellular contents
during normal cell turnover
Elevated plasma levels of aminotransferases
indicate damage to cells rich in these
enzymes
(as physical trauma or disease to tissue)
Plasma AST ALT are of particular diagnostic
value

32
Diagnostic Value of Plasma Aminotransferases

1- liver disease
Plasma ALT AST are elevated in nearly all
liver diseases
but, particularly high in conditions that
cause cell necrosis as
viral hepatitis
toxic injury
prolonged circulatory collapse
ALT is more specific for liver disease than
AST
AST is more sensitive (as liver contains a
large amount of AST)
2- Nonhepatic disease
as myocardial infarction
muscle disorders
These disorders can be distinguished clinically
from liver disease

33
2- Oxidative deamination of amino acids By
Glutamate Dehydrogenase

Oxidative Deamination of glutamate by glutamate
dehydrogenase results in liberation of the amino
group as free ammonia
(i.e. no transfer of amino group)
primarily in the liver kidney (but can occur in
other cells of the body)
Oxi Deamin. Of Glutamate provides
1- a-ketoglutarate (can be reused for
transamination of a.a.)
2- free ammonia urea cycle
urea

GLUTAMATE (from
transamination)
Glutamate oxi.
deamin. (liver kidney (mainly) others)
Dehydrogenase
ammonia a-ketoglutarate
Urea Cycle
Urea used for tranasmination
of a.a.

35
OXIDATIVE DEAMINATIONbyGLUTAMATE DEHYDROGENASE
36
Glutamate Dehydrogenase

Amino group of most amino acids are funneled to
GLUTAMATE
(by transamination with a-ketoglutarate)
GLUTAMATE is the only amino acid that undergoes
oxidative deamination (by glutamate
dehydrogenase) to give a-ketoglutarate ammonia
Amino Acids donate their amino group to
a-ketoglutarate to produce glutamate
(Transamination)
Glutamate is oxi deamin. to a-ketoglutarate
ammonia
(by Glutamate dehydrogenase)

Amino acid a-ketoglutarate
ammonia
TRANS AMINASE
GLUTA MATE UREA
CYCLE
DEHYDROGENASE
a-keto acid Glutamate
(carbon Skeleton)
metabolized
UREA
Energy other compounds
(catab.)

38
Removal of Amino Group from an Amino Acid
UREA CYCLE
Amino acid
Carbon skelton of an amino acid
Coenzyme for glutamate dehydrogenase NAD
39
Synthesis of an Amino Acid from its carbon
skeleton(reductive amination)
Amino acid
Carbon skelton of an amino acid
Coenzyme for glutamate dehydrogenase NADPH
40
Combined Actions of Transaminases Glutamate
Dehydrogense reactions
41
Direction of Reactions