Protein Metabolism

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Protein Metabolism

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Title: Protein Metabolism

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Protein MetabolismUrea Cycle

By
Dr. Samer Zahran

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Learning Objectives

Describe the three mechanisms used by humans for
removal of the nitrogen from amino acids prior to
the metabolism of their carbon skeletons.
Outline the sequence of reactions in the urea
cycle and trace the flow of nitrogen from amino
acids into and out of the cycle.
Define the terms and give examples of glucogenic
and ketogenic amino acids

4
Learning Objectives ( cont. )

Summarize the sources and use of ammonia in
animals and explain the concept of nitrogen
balance.
Explain the biochemical basis and the therapeutic
rationale for treatment of phenylketonuria and
maple syrup urine disease.

Proteins or polypeptides are polymers of
amino acids.
They perform many essential functions in
mammalian body.
These functions are
I - Dynamic functions
II- Structural functions

I - Dynamic functions
a) Transport functions
Albumin that transports some drugs, calcium, bile
pigments and FFA
Hemoglobin that transports oxygen.
Transferrin that transports iron.
Lipoproteins that transport lipid.

b) Metabolic control as they enters in the
formation of enzymes and some hormones, e.g.
Insulin and glucagon.
c) Contraction , e.g. Proteins of muscles
(actin and myosin)
d) Protection, e.g. Immunoglobulins.
e)Blood clot e.g.Fibrinogen,thromboplastin, and
prothrombin.

II- Structural functions
a) Essential component of cell membrane
cytoplasm, cell organells and receptors.
b) Enter in the structure of collagen,
elastin, keratin, and rhodopsin

Sources of Dietary Proteins
1- Animal as milk, fish, meat and eggs.
2- Plant as cereals and beans.

Fate of absorbed amino acids
Anabolic pathway
Catabolic pathway

Anabolic pathway
Amino acids enter in the formation of
proteins for wear and tear, plasma proteins,
hemoglobin, enzymes, some hormones
also enter in the formation of non protein
nitrogenous compounds (NPN) as purines,
pyrimidines, creatine and thyroxine.

Catabolic pathway
a) Urea formed in the liver, is considered
as
the main metabolic endoproduct of protein
catabolism.
b) Supplying energy 1 gram protein yields
4.1 K cal, only if there is shortage in
carbohydrate and fats.

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Nitrogen Balance There is no storage (depot)
for protein, but there is a certain percentage of
protein that undergoes a constant process of
breakdown and resynthesis i.e. turnover. This is
a normal process an essential feature of what is
called "nitrogen balance". Nitrogen balance
is a comparison between the intake of nitrogen
(mainly in the form of dietary protein) and the
excretion of nitrogen (mainly in the form of
undigested protein in stool and urea and ammonia
in urine). Also nitrogen output is through nails,
hair and desquamated skin.
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Nitrogen equilibrium The normal adult
human will be in nitrogen equilibrium when N2
lost (in urine, feces and sweat) just balanced by
N2 in diet intake. N2 LOST
N2 INTAKE
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Positive nitrogen balance
A condition in which there is increase in
the N2 intake over the output.
N2 LOST lt N2
INTAKE
It may occur in growth, pregnancy or
convalescence from diseases.

Negative nitrogen balance
A condition in which there is either
decreased
N2 intake as in
starvation, poverty,
malnutrition,maldigestion, malabsorption,
severe vomiting, severe diarrhea
Or increased N2 output as in
hemorrhage, burns,
old age or debilitating disease.
N2 LOST gt N2
INTAKE

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N.B. 1- Daily protein needs are One
gram protein per kilogram body weight (i.e. about
70-100 gm protein per day). At least part of
this protein should be of high biological
value. A protein of high biological value
should contain all essential amino acids.
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2- essential amino acids are amino acids that are
not synthesized in our body and hence, must be
supplied in food.
They are arginine, histidine, valine, leucine,
isoleucine, lysine, methionine, threonine,
phenylalanine and tryptophan.
If nine of the ten essential amino acids are
present in certain type of food, this food is
considered to contain protein of low biological
value.

General Metabolism of Proteins
Complete breakdown of proteins and amino
acids give rise to
Urea Co2 H2O Energy.

The major pathway for amino acids excess after
protein synthesis is the removal of the amino
group and its conversion to ammonia (as there is
no amino acid storage).
The liver is the major site of removal of amino
group from amino acids..

The amino group is removed by different
mechanisms
1. Transamination
2. Oxidative deamination
3. Non-oxidative deamination
4. Transdeamination

I . Transamination
It transfers the amino group from an amino acid
to a -keto acid.
All the amino acids participate in the reaction
of transamination except threonine and lysine.
Vitamin B6 is required as a coenzyme.
Its enzymes are termed transaminases

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a) Aspartate transaminase (AST) or(GOT)
Glutamic acid Oxaloacetic acid
a-Ketoglutaric acid Aspartic acid
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b) Alanine transaminase (ALT)or(GPT)
Glutamic acid Pyruvic acid
a-Ketoglutaric acid Alanine
Transaminases are cytosolic and mitochondrial
enzymes. It is a freely reversible process.
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Biological importance of Transamination

1- Synthesis of new non-essential amino acids.
2- Degradation of most amino acids except lysine
and threonine.
3- Formation of components of citric acid cycle
(filling up reaction of citric acid cycle).
4-Transaminase enzymes are used in diagnosis and
prognosis of the diseases.

N.B. Transaminase enzymes are present inside the
cells and small traces are present in the blood
(5-40 IU/L).
The increase in their level denote cell damage
with the release of enzymes from the destructed
cells.
eg.
in cardiac infarction SGOT is increased
in hepatic infection, SGPT is increased above
the normal levels.

II. Oxidative deamination
It is catalyzed by Amino acid oxidases Occur
in liver and kidney.
It includes removal of hydrogen (oxidation) and
removal of NH3 (deamination).
There are D- and L-amino acid oxidases that
oxidizes D- and L-amino acids respectively, to
the corresponding a-keto acids and the amino
group is released as ammonia (NH3).

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Oxidative deamination
1
2
?
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D-amino acid oxidase uses FAD as coenzyme which
is of limited natural occurance in mammals and of
high activity,
L-amino acid oxidase uses FMN as coenzyme which
is of natural occurrance in mammals, but of low
activity.

III - Non-oxidative deamination
(direct deamination)
The a- amino group of serine and threonine
( amino acids containing hydroxyl group) can be
directly converted to NH3 without removal of
hydrogen.
This reaction is catalyzed by serine and
threonine dehydratase which need pyriodoxal
phosphate as coenzyme.

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Non-oxidative deamination (direct
deamination)
Non-oxidative deamination
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IV .Transdeamination (L-Glutamate dehydrogenase)
Vit B6
NAD NADP
Vit B6
NAD NADP
1
1
1
2
2
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Oxidative deamination
?-ketoglutaric acid
Glutamic acid

The reaction is both mitochondrial and
cytoplasmic, occurs mainly in the liver and
kidney.
ATP and GTP are allosteric inhibitors while ADP
and GDP activate the enzyme.
It is a reversible reaction.

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Metabolism of ammonia

Sources of blood ammonia
Fates of ammonia (Removal of ammonia)
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Sources of blood ammonia
1.From amino acids
Transdeamination
Oxidative deamination
Non-oxidative deamination .
2.From glutamine
Renal glutaminase
Intestinal glutaminase

3.From amines whether dietary amine or
monoamine hormones by amine oxidase.
4. From catabolism of purines and
pyrimidines .
5.From bacterial action in the intestine either
from dietary protein residue or from urea
diffuses into the intestine

(This is of significance in cases of kidney
failure )

Fates of ammonia (Removal of ammonia)
Amination of a-ketoacid to form non-essential
amino acids and other biosynthetic reactions.
Glutamine synthesis in the brain, liver, muscle
and renal tissues (4).
The majority of NH3 (90) will produce urea in
the liver by urea cycle.
Excretion in urine upto 1 gm /24 hours urine.
Traces in blood (up to 100 ug / dl).

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1
4
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Sources and Fates of ammonia
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Glutamine synthesis and ammonia formation
Glutamine synthetase
glutaminase

H2O
ATP ADPp H2O
Glutamic acid
Glutamine
Glutamic acid
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Urea cycle

Definition
It is the conversion of ammonia to urea.
Site
Mitochondia and cytosol of liver cells only.
Structure of urea
O
H2N - C -NH2

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Krebs urea cycleor ornithine cycle for urea
formation

Urea is formed in the liver mainly ,some in the
brain and renal tubules from one molecule of CO2
and two molecules of NH3 using 3 ATP's.
It is released into the blood with a level of
15-40 mg/dL of serum.
It is the major end product of nitrogen
catabolism in humans representing 80-90 of the
nitrogen excreted.

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Urea formation

NH2
3ATP
CO2 2 NH3 CO
H2O
NH2

urea
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Five reactions each of them utilizes specific
enzyme in urea cycle.
The first 2 reactions of urea cycle are
mitochondrial and the rest 3 reactions are
cytoplasmic.

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Steps of Urea Cycle
1
2 ATP HCO3- NH3
Carbamoyl phosphate 2 ADP Pi
Pi
Mitochondrion

Ornithine
2
Citrulline
Citrulline
Ornithine
Urea cycle
ATP
Aspartate
3
AMP PPi
Urea
5
Cytosol
H2O
Arginino- succinate
Arginine
4
Fumarate
Oxaloacetate
Malate
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Sources of the Atoms of Urea

O
H2N- C -NH2

From Aspartate
From NH3
From Bicarbonate
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mitochondria
cytoplasm
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Five enzymes of urea cycle
Carbamoyl phosphate synthase 1
Ornithine transcarbamoylase (citrulline synthase)
Argininosuccinate synthetase.
Argininosuccinase.
Arginase.

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LINK BETWEEN KREBS' UREA CYCLE AND KREBS'
TRICARBOXYLIC ACID CYCLE
1
2ATP
CO2 NH3
2
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LINK BETWEEN KREBS' UREA CYCLE AND KREBS'
TRICARBOXYLIC ACID CYCLE
Malate
Oxalacetate
Glutamate
a-ketoglutarate
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1. The fumarate resulting from reaction
number 4 (in Krebs urea cycle), under the
influence of argininosuccinase, undergoes
conversion to malate by fumarase enzyme.
This malate forms oxaloacetate by malate
dehydrogenase. The oxaloacetate undergoes
Transamination by SGOT to form aspartate.
This aspartate is needed in urea cycle at
argininosuccinic synthase enzyme.

2.The CO2 used in urea cycle comes mainly
from Krebs' tricarboxylic acid cycle.
The first NH2 group comes from
L-glutamic acid by L-glutamate
dehydrogenase.
The second NH2 group comes from amino group
of aspartic acid.

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REGULATION OF UREA CYCLE

1. Excess ammonia formation stimulates urea
formation.
2. High arginine level stimulates N-acetyl
glutamate
synthase enzyme, thus increases urea
formation.
3. High urea level inhibits carbamoylphosphate
synthase (reaction 1), ornithine
transcarbamoylase
(reaction 2) and arginase enzymes
(reaction 5).
4. Carbamoylphosphate synthase is inactive in the
absence of activator, N-acetylglutamate.

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METABOLIC DISORDERS OF UREA CYCLE

There are five types of congenital
hyperammonaemia.
They affect children and manifested by
1.vomiting,
2.irritability,
3.ataxia,
4.lethargy coma ,
5.mental retardation,and death

1. Hyperammonaemia type I
It may be due to carbamoylphosphate synthase
deficiency.
It causes increase in blood ammonia level
(normally plasma ammonia is less than 100 µg/dL).
It is a familial disease.

2. Hyperammonaemia type II
It is due to ornithine transcarbamoylase
deficiency.
It is X-chromosome linked deficiency.
There is increased glutamine in blood, CSF and
urine due to increased glutamine synthesis as
consequence of increased tissue levels of
ammonia.

3. Citrullinaemia type III
It is due to lack of argininosuccinic synthase .
It is recessive inherited disorder.
There is an increase in citrulline in plasma, CSF
and urine.

4. Argininosuccinic aciduria type IV
It is due to argininosuccinase deficiency.
It is recessive inherited disorder. There is
increase in argininosuccinic in plasma, CSF and
urine.
It is manifested at age of two years.
It usually ends in death early in life.

5. Hyperargininaemia type V
It is due to arginase deficiency.
There is increase in arginine in blood, CSF and
urine.
It affects children ( 1 30,000 ) leading to
mental retardation ,coma and death.

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Ammonia intoxication(Ammoniacal encephalopathy)

It is defined as toxicity of the brain due to
increase in NH3 level in the systemic blood.
This increased ammonia will be fixed to
a- ketoglutaric acid to form glutamic acid
then glutamine leading to interference with
citric acid cycle so decrease ATP production in
the brain cells.

Causes
I. Congenital The 5 types of hyperammonaemia
due to enzymes deficiencies in urea cycle.
(see urea cycle)
II. acquired
1. Liver disease as cirrhosis due to
failure
of urea formation and glutamine
synthesis.
2. Portocaval shunt as in
bilharziasis.
3. Gastrointestinal bleeding by action
of bacterial
flora on the blood urea and thus
NH3 is released
in large amounts.

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Manifestations of ammonia intoxication

1. Tremors
2. Blurred vision
3. Slurred speech
4. Vomiting
5. Confusion followed by coma
and death.

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Treatment

1. Injection of Glutamic acid and
?-ketoglutaric
acid
They act as a carrier for NH3 and combine
with it to form a nontoxic material
called
glutamine. Glutamine passes to the
kidney
and by glutaminase yielding glutamic acid
and NH3 excreted in urine as ammonium
salt.
(NH4cl).
2. Restrict protein diet.

3. Sodium benzoate and phenylacetate
are given to conjugate with glycine
and glutamine and rapidly the
conjugates are excreted in urine.
4. Frequent small meals to avoid sudden
increase in blood ammonia levels.
5. Removal of excess NH3 by dialysis in
acute cases.

CATABOLISM OF THE CARBON SKELETON OF AMINO ACIDS

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Catabolism of Amino Acids

It involves
I. Removal of the amino acid nitrogen (a-amino
group) by
a. Transamination or
b. Oxidative deamination.
These two reactions finally produce ammonia and
aspartate that are the sources of urea nitrogen.
II. Metabolism of the carbon skeleton of the
amino acid which includes either
a. Conversion into glucose, fatty acid or ketone
bodies or
b. Oxidation to CO2 and energy.

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Metabolism of Amino Acids
Amino Acid is composed of
AND
Amino group
Carbon skeleton

OR
OR
Converted to Glucose, fat, Or ketone bodies
Oxidized to CO2 Energy
Transferred to a keto acid to form a new amino
acid
Released as ammonia
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Catabolism of the Carbon Skeleton of Amino Acids

It results in the production of 7 intermediate
products that directly enter the pathways of
Intermediary metabolism, resulting either in the
synthesis of glucose or lipids, or in the
production
of energy through their oxidation by the citric
acid
cycle.

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Intermediate Products of Amino Acid Catabolism

These include the following seven intermediate
products
1. Pyruvate.
2. ?-ketoglutarate.
3. Succinyl CoA.
4. Fumarate.
5. Oxaloacetate.
6. Acetyl CoA.
7. Acetoacetyl CoA.

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Glycine Cysteine Serine Alanine Threonine Tryptoph
an
Leucine Lysine Phenylalanine Tyrosine Tryptophan
Glucose
Isoleucine Leucine
Phosphoenol-pyruvate
Pyruvate
Asparagine Aspartate
Acetyl CoA
Acetoacetyl CoA
Oxaloacetate
Tyrosine Phenylalanine
Glutamate Glutamine Histidine Proline Arginine
Fumarate
Citrate
Isoleucine Valine Methionine Threonine
Succinyl CoA
?-keto-glutarate
Fates of the carbon skeletons of amino acids.
Glucogenic amino acids are shaded red, ketogenic
amino acids are shaded green and glucoketogenic
amino acids are shaded blue.
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Glucogenic (glycogenic) Amino Acids

Definition
- These are amino acids whose catabolism yields
pyruvate or one of the intermediates of the
citric
acid cycle which are substrates for gluconeo -
genesis and, therefore, can give rise to the
net
formation of glucose or glycogen.
- They include 14 amino acids.

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Ketogenic Amino Acid

Definition
- This is amino acid its catabolism yields to
either acetoacetate or one of its precursors.
- Leucine is the only exclusively ketogenic amino
acid found in proteins because Its carbon
skeletons is not substrates for gluconeogenesis
therefore, cannot give rise to the net formation
of glucose or glycogen.

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Both Glucogenic and Ketogenic (glucoketogenic)
Amino Acids

Definition
- These are amino acids whose catabolism yields
both glucose and ketone bodies.
- They include 5 amino acids isoleucine, phenyl-
alanine, tyrosine , tryptophan and lysine
because part of
their carbon skeleton can give glucose and the
other part can give ketone bodies.

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Classification of Amino Acids.
Biological value Ketogenic Glucogenic and ketogenic Glucogenic
Non-essential Tyrosine Glycine Alanine Serine Cysteine Proline Histidine Arginine Aspartate Asparagine Glutamate Glutamine
Essential Leucine Isoleucine Phenylalanine Lysine,Tryptophan Methionine Threonine Valine
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1- Amino Acids That Form Oxaloacetate
Aspartate
Asparagine
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2- Amino Acids That Form ?- Ketoglutarate
Glutamine
Glutamate
Histidine
Proline
Arginine
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3- Amino Acids That Form Pyruvate
Glycine
Serine
Alanine
Tryptophan
Cysteine
Threonine
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Biological functions of Glycine

1. Incorporated into proteins.
2. Glucogenic amino acid.
3. Source of energy.
4. Formation of serine.
5. Formation of bile acids (e.g. glycocholate).
6. Formation of Glutathione (GSH) which is a
tripeptide formed of glutamate, cysteine and
glycine.
7. Formation of Heme (succinyl COA Glycine).
8. Formation of purines.
9. Formation of creatine (synthesized from
glycine, arginine and methionine).
10. Detoxification of Benzoic acid (food
preservatve) by converting it into hippuric acid
which is excreted in urine

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Biological Functions of Cysteine

1. Incorporated into proteins.
2. Glucogenic amino acid.
3. Source of energy.
4. Formation of taurine (a component of the bile
acid taurocholate).
5. Formation of Glutathione.

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Biological Functions of Tryptophan

1. Formation of niacin.
- It is a member of vitamin B complex
- it is a component of NAD and NADP.
2. Formation of serotonin.
- It is a neurotransmitter that controls the
mood.
- It is a vasoconstrictor substance.
- It causes contraction of smooth muscles of
bronchi and intestine.
3. Formation of melatonin.
- It induces sleep.
- It is an antioxidant.
- It causes hypopigmentation.

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4- Amino acids that form Fumarate
Phenylalanine
Tyrosine
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Functions of Phenylalanine and Tyrosine

1. Synthesis of catecholamines
a. Adrenaline (epinephrine).
b. Noradrenaline (norepinephrine).
c. Dopamine.
2. Synthesis of thyroid hormones
a. Tri-iodothyronine (T3).
b. Tetra-iodothyronine (T4, thyroxine).
3. Synthesis of melanin pigments.
4. Synthesis of tissue proteins.
5. Source of energy.

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Phenylalanine hydroxylase
Phenylalanine
Tyrosine
?-KG
O2
H2O
Phenylketonuria
Tyrosine transaminase
PLP
Glu
P-Hydroxyphenyl-pyruvate hydroxylase
Homogentisate
P- Hydroxyphenyl pyruvate
Ascorbate Cu2
O2
CO2
O2
Homogentisate dioxygenase
Alkaptonuria
Maleylacetoacetatecis- trans isomerase
Ascorbate
Fe2
Maleylacetaoacetate
Fumarylacetoacetate
Fumarylacetoacetate hydrolase
GSH
H2O
Acetoacetate
Fumarate
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Characteristics of Phenylketonuria

1. phenylalanine in blood, urine, and tissues.
2. phenylpyruvate, phenylacetate
phenyllactate in urine musty
(mousey) odor of urine.
3. CNS manifestations
a. Mental retardation (low IQ) by the age of 1
year
due to the toxic effects of phenylalanine
possibly
on the transport and metabolism of other
aromatic
amino acids (as tyrosine and tryptophan) in the
brain resulting in deficiency of
neurtransmitters
such as catecholamines and serotonin.
b. Failure to grow, walk or talk.
c. Seizures, tremors, hyperactivity
microcephaly.

4. Hypopigmentation
- It is due to competitive inhibition of
tyrosinase ( that catalyzes the first step
in the formation of melanin pigment from
tyrosine) by the high level of phenylalanine.
-There is fair hair, light skin color, and blue
eyes.

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Diagnosis of Phenylketonuria

A. Neonatal diagnosis
- Infants with PKU frequently has normal blood
phenylalanine level at birth because the mother
clears the increased blood phenylalanine in her
affected fetus through the placenta thus showing
false negative results.
- There is blood phenylalanine level in newborn
fed
with breast milk or formula for 48 hours.
B. Antenatal diagnosis
- It is done by in vitro detection of PKU gene
mutation in cells of amniotic fluid.

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Treatment of Phenylketonuria

- It must begin during the 7-10 days of life to
prevent
mental retardation.
- Treatment involves the following
1. Feeding a diet low in phenylalanine at least
till the
age of 8 years or better life-long to keep
blood
phenylalanine within the normal range. This
diet
includes synthetic amino acid preparations and
natural foods low in their phenylalanine
content
such as fruits, vegetables and certain cereals.
2. Supplementation with tyrosine that becomes an
essential amino acid in classic PKU.

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Alkaptonuria

It is a rare autosomal recessive metabolic
disease.
Cause
Deficiency of homogentisate dioxygenase
(oxidase).
Characteristics
1. Elevated level of homogentisic acid in urine
(homogentisic aciduria) which is oxidized to a
dark
pigment on standing giving urine a black color.
2. Large joint arthritis.
3. Black pigmentation of cartilage and
collagenous
tissue.
Treatment
Giving diet low in phenylalanine and tyrosine to
reduce the level of homogentisic acid.

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Albinism

Cause
Deficiency of tyrosinase that is involved in the
synthesis of melanin pigments.
Manifestations
Absence of melanin pigments from hair, iris of
eyes,
and skin results in
a- Fair (blond) hair, white eyebrows and lashes.
b- white color of the iris that reflects the red
color of blood vessels of the retina behind.
c- Photophobia.
d- Skin burns and skin cancer.

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Synthesis of Melanin Pigments

Melanin pigments
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5- Amino acids that form succinyl CoA
Methionine
Threonine
Valine
Isoleucine
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Methionine