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College of Veterinary Medicine 4/10/2012
Dept. of Vet .Internal & Preventive Med.
Clinical Pathology
Introduction to Hematology
PowerPlugs: Templates
Content
– Introduction
–Red cell production (erythropoiesis)
–Erythrocyte lifespan
–Erythrocyte breakdown
–Control of erythropoiesis
Introduction
• Haematology is the study of the cellular elements of the blood, which can
be divided into three categories:
• (1)The erythrocytes or red blood cells (RBC).
• (2)The thrombocytes or platelets.
• (3)The leucocytes or white blood cells (WBC).
• Occasionally other cells which are not normally present in circulation can
also be detected in a blood sample, such as mast cells or plasma cells ,
usually because the cells are neoplastic.
• The red blood cells are responsible for oxygen transport from the lungs to
all the tissues of the body,
• The platelets are responsible for routine maintenance and repair of the
blood vessels,
• The white cells are responsible in various ways for repelling foreign
invaders.
• The "erythron" is the name given to the
organ of the body, technically classified as
connective tissue, which comprises all the
red cells plus all the red cell producing tissue
(essentially the relevant fractions of the
blood, the spleen and the bone marrow).
• The single function of the erythron is
oxygen/carbon dioxide transport between
the tissues and the lungs, with haemoglobin
as the O2/CO2 carrier.
– Red cell production (erythropoiesis)
• This takes place in the red (haemopoietic) bone marrow (not
in the white fatty marrow). This haemopoietic bone marrow is
much more extensive in young animals than in mature ones.
This tends to make effective bone marrow biopsy rather more
difficult in older animals. The stages of development of the red
cells are shown in Fig. 1.
• As the erythrocytes mature they become very readily
deformable (necessary in order to pass through small
capillaries) and when they are flexible enough they can slide
into the circulation through openings in the sinusoidal walls.
• The total maturation time varies between
species from about 4– 5 days in cattle to about
1 week in the dog. Normally about 10– 15% of
developing red cells die before reaching
maturity (ineffective erythropoiesis) and this
percentage can increase in certain disease
situations.
• When there is an increased demand for red
cells (e.g. in cases of haemorrhage or oxygen
starvation) the bone marrow deals with these
cases by one of the following ways :
• production is increased firstly by allowing younger
forms (reticulocytes, normoblasts) to enter the
circulation, but this is not seen in all species, e.g.
dogs demonstrate reticulocytosis very readily, cattle
only on extreme provocation such as severe acute
haemorrhage, and horses never.
• secondly by allowing the maturation stages to
merge and skip so that erythropoiesis speeds up.
This occurs in all species and sometimes leads to
the appearance of a few imperfect erythrocytes in
circulation, such as Howell– Jolly bodies,
poikilocytes and leptocytes.
Erythrocyte lifespan
• This varies between species from about 2 months
in pigs to over 5 months in cattle. Sheep are unique
in having two populations of red cells, one short-
lived (70 days), the other long-lived (150 days). In
certain disease situations the survival time of the
erythrocytes is shortened, particularly some
nutritional deficiencies (iron, vitamin B12, folic
acid), and congenital porphyria in cattle.
•
Erythrocyte breakdown
•  This occurs in three ways: 
• The cell may be fragmented into pieces small 
enough for the reticulo-endothelial system to take 
up, or 
• When the enzymes present in the cell membrane 
are used up the much more fragile cell breaks up 
and is phagocytosed, or 
• The whole cell may be phagocytosed directly.
•  The haemoglobin from a defunct red cell is also broken down. The 
(protein) globin fraction is lysed into its component amino acids and 
the carbohydrate residue entering the fuel metabolism pathways. 
• The haem fraction loses its iron atom, which is not excreted but is 
recycled into a new haemoglobin molecule. The remaining part of the 
haem complex becomes bilirubin which is non-water-soluble and so 
must be transported in the plasma bound to albumin. On reaching 
the liver it is conjugated to glucuronic acid or a similar substance, 
which renders it soluble so that it can be excreted in the bile. After 
some recycling round the hepatic circulation and further metabolism 
most of this is excreted in the faeces as urobilin and stercobilin – 
these give the faeces their characteristic colour. Some is also 
excreted in the urine as urobilinogen.
•  
– Control of erythropoiesis
•    Normally, production and destruction of red cells are 
kept in balance so that total erythrocyte numbers (i.e. 
erythron size) are constant – in a 15 kg dog about 800 
000 red cells die and are replaced every second.
•    The hormone responsible for the regulation of the rate 
of erythropoiesis is a glycoprotein called erythropoietin. 
Fetal and maternal erythropoietin are quite separate 
because the hormone does not cross the placenta. The 
principal site of erythropoietin production is the kidney – 
in dogs this is the only site and thus the hormone is 
totally absent in nephrectomized animals, but there is an 
additional extra-renal site in some species (e.g. rats) 
which has not been identified.
•  The fundamental stimulus to erythropoietin production 
is tissue hypoxia, and so the concentration in plasma is 
related to the ratio of oxygen supply to oxygen demand.
• Erythropoietin affects red cell production in four ways:
• (1)More stem cells differentiate to red cell precursors.
• (2)Stages of red cell development are speeded up.
• (3)Transit time out of bone marrow is reduced.
• (4)Immature red cells are released (depending on 
species).
• The endocrine organs involved in the modification of
erythropoietin production are the pituitary, adrenals,
thyroid and gonads. The hormones in question actually
affect cell metabolism and hence tissue oxygen
requirements, and so have a feedback on EP synthesis.
• (1)Hormones which increase EP production: androgens,
cortisol, thyroxine, adrenaline, noradrenaline, angiotensin,
prolactin, growth hormone, thyroid-stimulating hormone
(TSH) and adrenocorticotrophic hormone (ACTH).
• (2)Hormones which decrease EP production: oestrogens.
•

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Introduction to veterinary hematology / Assist.Prof.Sr. Salah Al - Kubaisi

  • 1. College of Veterinary Medicine 4/10/2012 Dept. of Vet .Internal & Preventive Med. Clinical Pathology Introduction to Hematology
  • 2. PowerPlugs: Templates Content – Introduction –Red cell production (erythropoiesis) –Erythrocyte lifespan –Erythrocyte breakdown –Control of erythropoiesis
  • 3. Introduction • Haematology is the study of the cellular elements of the blood, which can be divided into three categories: • (1)The erythrocytes or red blood cells (RBC). • (2)The thrombocytes or platelets. • (3)The leucocytes or white blood cells (WBC). • Occasionally other cells which are not normally present in circulation can also be detected in a blood sample, such as mast cells or plasma cells , usually because the cells are neoplastic. • The red blood cells are responsible for oxygen transport from the lungs to all the tissues of the body, • The platelets are responsible for routine maintenance and repair of the blood vessels, • The white cells are responsible in various ways for repelling foreign invaders.
  • 4. • The "erythron" is the name given to the organ of the body, technically classified as connective tissue, which comprises all the red cells plus all the red cell producing tissue (essentially the relevant fractions of the blood, the spleen and the bone marrow). • The single function of the erythron is oxygen/carbon dioxide transport between the tissues and the lungs, with haemoglobin as the O2/CO2 carrier.
  • 5. – Red cell production (erythropoiesis) • This takes place in the red (haemopoietic) bone marrow (not in the white fatty marrow). This haemopoietic bone marrow is much more extensive in young animals than in mature ones. This tends to make effective bone marrow biopsy rather more difficult in older animals. The stages of development of the red cells are shown in Fig. 1. • As the erythrocytes mature they become very readily deformable (necessary in order to pass through small capillaries) and when they are flexible enough they can slide into the circulation through openings in the sinusoidal walls.
  • 6. • The total maturation time varies between species from about 4– 5 days in cattle to about 1 week in the dog. Normally about 10– 15% of developing red cells die before reaching maturity (ineffective erythropoiesis) and this percentage can increase in certain disease situations. • When there is an increased demand for red cells (e.g. in cases of haemorrhage or oxygen starvation) the bone marrow deals with these cases by one of the following ways :
  • 7. • production is increased firstly by allowing younger forms (reticulocytes, normoblasts) to enter the circulation, but this is not seen in all species, e.g. dogs demonstrate reticulocytosis very readily, cattle only on extreme provocation such as severe acute haemorrhage, and horses never. • secondly by allowing the maturation stages to merge and skip so that erythropoiesis speeds up. This occurs in all species and sometimes leads to the appearance of a few imperfect erythrocytes in circulation, such as Howell– Jolly bodies, poikilocytes and leptocytes.
  • 8. Erythrocyte lifespan • This varies between species from about 2 months in pigs to over 5 months in cattle. Sheep are unique in having two populations of red cells, one short- lived (70 days), the other long-lived (150 days). In certain disease situations the survival time of the erythrocytes is shortened, particularly some nutritional deficiencies (iron, vitamin B12, folic acid), and congenital porphyria in cattle. •
  • 9. Erythrocyte breakdown •  This occurs in three ways:  • The cell may be fragmented into pieces small  enough for the reticulo-endothelial system to take  up, or  • When the enzymes present in the cell membrane  are used up the much more fragile cell breaks up  and is phagocytosed, or  • The whole cell may be phagocytosed directly.
  • 10. •  The haemoglobin from a defunct red cell is also broken down. The  (protein) globin fraction is lysed into its component amino acids and  the carbohydrate residue entering the fuel metabolism pathways.  • The haem fraction loses its iron atom, which is not excreted but is  recycled into a new haemoglobin molecule. The remaining part of the  haem complex becomes bilirubin which is non-water-soluble and so  must be transported in the plasma bound to albumin. On reaching  the liver it is conjugated to glucuronic acid or a similar substance,  which renders it soluble so that it can be excreted in the bile. After  some recycling round the hepatic circulation and further metabolism  most of this is excreted in the faeces as urobilin and stercobilin –  these give the faeces their characteristic colour. Some is also  excreted in the urine as urobilinogen. •  
  • 11. – Control of erythropoiesis •    Normally, production and destruction of red cells are  kept in balance so that total erythrocyte numbers (i.e.  erythron size) are constant – in a 15 kg dog about 800  000 red cells die and are replaced every second. •    The hormone responsible for the regulation of the rate  of erythropoiesis is a glycoprotein called erythropoietin.  Fetal and maternal erythropoietin are quite separate  because the hormone does not cross the placenta. The  principal site of erythropoietin production is the kidney –  in dogs this is the only site and thus the hormone is  totally absent in nephrectomized animals, but there is an  additional extra-renal site in some species (e.g. rats)  which has not been identified.
  • 12. •  The fundamental stimulus to erythropoietin production  is tissue hypoxia, and so the concentration in plasma is  related to the ratio of oxygen supply to oxygen demand. • Erythropoietin affects red cell production in four ways: • (1)More stem cells differentiate to red cell precursors. • (2)Stages of red cell development are speeded up. • (3)Transit time out of bone marrow is reduced. • (4)Immature red cells are released (depending on  species).
  • 13. • The endocrine organs involved in the modification of erythropoietin production are the pituitary, adrenals, thyroid and gonads. The hormones in question actually affect cell metabolism and hence tissue oxygen requirements, and so have a feedback on EP synthesis. • (1)Hormones which increase EP production: androgens, cortisol, thyroxine, adrenaline, noradrenaline, angiotensin, prolactin, growth hormone, thyroid-stimulating hormone (TSH) and adrenocorticotrophic hormone (ACTH). • (2)Hormones which decrease EP production: oestrogens. •