Transcript Hemoglobin
Hemoglobin
Structure & Function
Objectives of the Lecture
1- Understanding the main structural & functional details of
hemoglobin as one of the hemoproteins.
2- Identify types & relative concentrations of normal adult
hemoglobin with reference to HBA1c with its clinical application.
3- Recognize some of the main genetic & biochemical aspects of
hemoglobinopathies with some implications on clinical features
(with focusing on thalassemias).
Hemoglobin is a globular hemoprotein
• Hemeproteins are a group of specialized proteins that contain heme as
a tightly bound prosthetic group.
• Heme is a complex of protoporphyrin IX & ferrous iron (Fe2+) .
• The iron is held in the center of the heme molecule by bonds to the four
nitrogens of the porphyrin ring. The heme Fe2+ can form two
additional bonds, one on each side of the planar porphyrin ring.
One of these positions is coordinated to the side chain of a histidine
amino acid of the globin molecule, whereas the other position is
available to bind oxygen
Globin of hemoglobin
is a globular protein with a quaternary structure
Structure & function of hemoglobin
• Hemoglobin is found exclusively in RBCs.
• Its main function is to transport oxygen from lungs to the tissues &
carbon dioxide & hydrogen protons from tissues to lungs.
• Hemoglobin A is the major hemoglobin in adults, is composed of four
polypeptide chains, 2 alpha (a) & 2 beta (b) chains, held together by
noncovalent interactions
• Each day, 6-7 grams of hemoglobin is synthesized to replace lost
through normal turn over of RBCs.
• Each subunit has stretches of a-helical structure & a heme binding
pocket.
Quaternary structure of hemoglobin
• The hemoglobin tetramer can be envisioned as being composed of two
identical dimers, (αβ)1 and (αβ)2, in which the numbers refer to
dimers one and two.
• The two polypeptide chains within each dimer are tightly held
together, primarily by hydrophobic interactions
• In contrast, the two dimers are able to move with respect to each other,
being held together primarily by polar bonds.
• The weaker interactions between these mobile dimers result in the two
dimers occupying different relative positions in deoxyhemoglobin as
compared with oxyhemoglobin
oxygenation & deoxygenation of hemoglobin
(oxyhemoglobin & deoxyhemoglobin)
Deoxyhemoglobin
Taut structure
Oxyhemoglobin
Relaxed structure
Types of adult hemoglobin
< 5%
HBA1:
HBA2:
HBF:
the major hemoglobin in humans
3–6 %
first appears 12 weeks after birth
- a minor component of normal adult HB increased in b-thalassemia
normally synthesized only during fetal development
in fetus and newborn infants Hb F binds O2 at lower tension than Hb A
→ Hb F has a higher affinity to O2
After birth, Hb F is replaced by Hb A during the first few months of life.
HBA1C : has glucose residues attached to b-globin chains
– increased amounts in DM
Hemoglobin A1c (HBA1c)
Some of hemoglobin A is glycosylated
Extent of glycosylation depends on the plasma
concentration of a particular hexose (as glucose).
The most abundant form of glycosylated hemoglobin is
HBA1c which has a glucose residues attached to bglobin chains in hemoglobin RBCs.
Increased amounts of HBA1c are found in RBCs of
patients with diabetes mellitus (DM).
HbA1c could be used as a monitor for the control of the blood glucose level
during the last 2 months for diabetic patients
Derivatives of hemoglobin
Oxyhemoglobin (oxyHb) =
Hb with O2
Deoxyhemoglobin (deoxyHb) =
Hb without O2
Methemoglobin (metHb)=
Fe3+ instead of Fe2+ in heme groups
Carbonylhemoglobin (HbCO) =
CO binds to Fe2+ in heme in case of CO poisoning or smoking.
CO has 200x higher affinity to Fe2+ than O2.
Carbaminohemoglobin (HbCO2) =
CO2 is non-covalently bound to globin chain of Hb.
HbCO2 transports CO2 in blood (about 23%).
Glycohemoglobin (HbA1c) is formed spontaneously by
nonenzymatic reaction with Glucose. People with DM have more
HbA1c than normal (› 7%). Measurement of blood HbA1c is
useful to get info about long-term control of glycemia.
Hemoglobinopathies
Hemoglobinopathies are members of a family of genetic disorders
caused by:
1- Production of a structurally abnormal hemoglobin molecule
(Qualitative hemoglobinopathies): HbS, HbC, HbSC & HbM.
Or: 2- Synthesis of insufficient quantities of normal hemoglobin
(Quantitative hemoglobinopathies): thalasaemias
Or: 3- both (rare).
1-Thalassemias
• Thalassemias are hereditary hemolytic diseases in which an
imbalance occurs in the synthesis of globin chains.
• They are most common single gene disorders in humans.
• Normally, synthesis of a- and b- globin chains are coordinated,
so that each a-globin chain has a b-globin chain partner.
This leads to the formation of a2b2 (HbA).
•
In thalassemias, the synthesis of either the a- or b-globin chain
is defective.
Thalassemia can be caused by a variety of mutations, including:
1- Entire gene deletions (whole gene is absent)
Or
2- Substitutions or deletions of one or more nucleotides in DNA
Each thalassemia can be classified as either:
1- A disorder in which no globin chains are produced
(ao- or bo -thalassemia)
Or: 2- Some b-chains are synthesized, but at a reduced rate.
(a+- or b+- thalassemia).
1
b-thalassemias:
Synthesis of b-globin chains are decreased or absent, whereas a-globin synthesis is
normal.
a-globin chains cannot form stable tetramers & therefore precipitate causing
premature death of RBCs ending in chronic hemolytic anemia
Also, a2g2 (HbF) & a2d2 (HbA2 ) are accumulated.
There are only two copies of the b -globin gene in each cell (one on each chromosome 11)
So, individuals with b -globin gene defects have either:
1- b-thalassemia minor (b -thalassemia trait):
if they have only one defective b-globin gene.
2- b- thalassemia major (Colley anemia):
if both genes are defective.
Mutation in one of
b-globin genes
Mutation in both
b-globin genes
b-thalassemia
minor
b-thalassemia
major
b-thalassemia
Some clinical aspects of b-thamassemias:
1- As b-globin gene is not expressed until late fetal gestation, the
physical manifestations of b -thalassemias appear only after birth.
2- Individuals with b -thalassemias minor, make some b-chains, and
usually require no specific treatment.
3- Infants born with b - thalassemias major seem healthy at birth, but
become severely anemic during the first or second years of life. They
require regular transfusions of blood.
2- a-thalassemia:
Synthesis of a-globin chains is decreased or absent. Each individual's genome
contains four copies of the a-globin (two on each chromosome 16), there are
several levels of a-globin chain deficiencies
Types a-thalassemia :
If one of the four genes is defective: The individual is termed a silent
carrier as no physical manifestations of the disease
If two a-globin genes are defective: The individual is designated as
having a-thalassemia trait with mild anemia
If three a-globin genes are defective; Synthesis of unaffected g- and
then b- globin chains continues, resulting in the accumulation of g
tetramer in the newborn (g4, Hb Bart's) or b-tetramers (b4, HbH). The
subunits do not show heme-heme interactions. So, they have very high
oxygen affinities. Thus, they are essentially useless as oxygen carriers to
tissues (clinically severe marked anemia).
If four a-globin genes are defective: hydrops fetalis & fetal death
occurs as a-globin chains are required for the synthesis of HbF
3-Sickle cell anemia
Definition: Sickle cell anemia is a genetic disorder of the blood caused by
a single nucleotide alteration (a point mutation) in the b-globin gene.
Inheritance of sickle cell anemia:
Sickle cell disease is a homozygous recessive disorder:
i.e. It occurs in individuals who have inherited two mutant genes (one from each
parent) that code for synthesis of the b chains of the globin molecule. RBCs of
homozygous is totally HB S (a2bs2 )
Heterozygotes individuals:
Have one normal and one sickle cell gene.
RBCs of heterozygotes contain both HB S (a2bs2 ) & HB A (a2b2 )
These individuals have sickle cell trait
Clinical manifestations of sickle cell anemia
Homozygous individuals
An infant (first 2 years of life) begins
show manifestations when
sufficient HbF is replaced by HbS
Clinical manifestations:
- Chronic hemolytic anemia
- Lifelong episodes of pain
- Increased susceptibility to infection.
- Acute chest syndrome
- Stroke
- Splenic & renal dysfunction
- Bone changes due to bone marrow
hyperplasia
Heterozygote individuals
Usually do not show clinical symptoms
Amino acid substitution in HB S b chains
HB S contains two mutant b-globin chains (bs ). In mutant chains,
glutamate (polar) at position 6 is replaced with valine (nonpolar)
resulting in:
Formation of a protrusion on the b-globin that fit into a
complementary site on the a chain of another hemoglobin molecule
in the cell.
In low oxygen tension, deoxy HB S polymerize inside the red blood
cell leading to stiffening & distorting of the cell ending in production
of rigid misshapen RBCs.
Sickle cells block the flow of blood in narrow capillaries
resulting in interruption of oxygen supply (localized anoxia) in
tissues causing pains.
Finally, cell death occurs due to anoxia (infarction)
Also, RBCs of HB S have shorter life span than normal RBCs (less
than 20 days, compared to 120 of normal)
Hence, anemia is a consequence of HB S.
• Factors that increase sickling
The extent of sickling is increased by any factor that increases the
proportion of HB S in the deoxy state as in cases of
1- Decreased oxygen tension:
in high altitudes
flying in a nonpressurized plane
2- Increased pCO2
3- Decrease pH
4- Increased 2,3- BPG in RBCs
Diagnosis of HB S
Hemoglobin Electrophoresis
HB S migrates more slowly
towards anode (+ve electrode)
than normal hemoglobin
Why?
due to absence of negatively charged
glutamate resulting in decrease of
negativity of hemoglobin
4- Methemoglobinemia
• Methemoglobin results from oxidation of the ferrous ion (Fe2+) of
heme of hemoglobin to ferric (Fe3+) ion
• Methemoglobinemia is characterized by “chocolate cyanosis” i.e. brownblue coloration of skin & membranes & chocolate colored blood
• Causes of oxidation of ferrous ions:
1- Drugs as nitrates
2- Endogenous products (as reactive oxygen species )
3- Inherited defects (as in certain mutations of a or b chains)
4- Deficiency of NADH-Met HB reductase :enzyme for reduction of Fe3+ of Met HB
• RBCs of newborns have ½ capacity of adults to reduce Met HB & therefore
they are more susceptible to Met HB formation by previous factors.
• Clinically, symptoms are due to tissue hypoxia
• Treatment: Methylene blue (to reduce the ferric ions)