Red Blood Cell Disorders Flashcards
Erythropoiesis
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Erythropoiesis and erythropoietin
- -Definition of erythropoiesis
a. Production of red blood cells (RBCs) in the bone marrow
b. Dependent on the release of erythropoietin (EPO) from the kidneys - EPO synthesized in the renal cortex by interstitial cells in the peritubular capillary bed.
EPO: synthesized in interstitial cells of peritubular capillary bed
3.Stimuli for EPO release include:
• Hypoxemia (↓arterial PO2), severe anemia, left-shifted O2-binding curve (OBC), high altitude, and decreased O2 saturation (SaO2; carbon monoxide poisoning, methemoglobinemia)
EPO stimuli: ↓PaO2/↓SaO2, left-shifted OBC, high altitude
4.Increased O2 content suppresses EPO release (e.g., polycythemia vera).
↑O2 content ↓EPO
Reticulocytes and the reticulocyte count
Reticulocytes and the reticulocyte count
- Importance of reticulocytes
a. Newly released RBCs from the bone marrow
b. Peripheral blood markers of effective erythropoiesis
c. Effective erythropoiesis refers to a good bone marrow response to anemia.
*Correlates with an increase in synthesis/release of reticulocytes from the bone marrow
Reticulocyte count: measure effective erythropoiesis
Effective erythropoiesis: good bone marrow response to anemia; ↑reticulocyte synthesis/release
2.Easily identified in the peripheral blood with supravital stains.
•Stains detect thread-like RNA filaments in the cytoplasm of young RBCs.
Tissue Hypoxia
A. Hypoxia
- Definition—inadequate oxygenation of tissue
- Factors contributing to the total amount of O2 carried in blood
a. Normally, O2 diffuses down a gradient from the atmosphere to the alveoli, to plasma, and into the red blood cells (RBCs), where it attaches to heme groups.
(1) In the alveoli, O2 increases the partial pressure of O2 (PAO2).
(2) In the plasma of the pulmonary capillaries, O2 increases the partial pressure of O2 (PaO2).
(3) In the RBC, O2 attaches to heme groups and increases the O2saturation (SaO2).
O2 diffusion: O2 in atmosphere → ↑PAO2 → ↑PaO2 → ↑SaO2
b. PaO2 and SaO2 are reported in arterial blood gas analyses.
c. O2 content is a measure of the total amount of O2 carried in blood and includes the hemoglobin (Hb) concentration as well as the PaO2and SaO2.
• Decrease in O2 content due to a decrease in Hb, PaO2, or SaO2causes an increase in erythropoietin (EPO).
O2 content = (Hb g/dL × 1.34) × SaO2 + PaO2 × 0.003
- In hypoxia, there is decreased synthesis of adenosine triphosphate (ATP).
a. ATP synthesis occurs in the inner mitochondrial membrane by the process of oxidative phosphorylation.
b. O2 is an electron acceptor located at the end of the electron transport chain (ETC) in complex IV of the oxidative pathway.
c. Lack of O2 and/or a defect in oxidative phosphorylation culminates in a decrease in ATP synthesis.
Thus–> Hypoxia: ↓ATP synthesis by oxidation phosphorylation.
What are the clinical findings of hypoxia?
1- Cyanosis (bluish discoloration of skin and mucous membranes).
2- Confusion
3- Cognitive impairment
4- Lethargy
Causes of hypoxemia:
Ischemia
1. Ischemia
Definition—decreased arterial blood flow to tissue or venous outflow of blood from tissue.
b. Examples—coronary artery atherosclerosis, decreased cardiac output, and thrombosis of the superior mesenteric vein
c. Consequences of ischemia
(1) Atrophy (reduction in cell/tissue mass)
(2) Infarction of tissue (localized area of tissue necrosis)
(3) Organ dysfunction (inability to perform normal metabolic functions)
Causes of hypoxia:
Hypoxemia
Definition—decrease in PaO2 measured in an arterial blood gas.
Hypoxemia: ↓PaO2
b.Normal PaO2 depends on percent O2 in inspired area, ventilation, perfusion, and diffusion of O2 from the alveoli into the pulmonary capillaries.
Causes of hypoxemia
(1) Decreased inspired PO2 (PiO2)
•Examples—breathing at high altitude and breathing reduced %O2 mist
(2) Respiratory acidosis
(a) Respiratory acidosis is defined as retention of CO2 in the lungs.
(b) Carbon dioxide (CO2) retention in the alveoli always produces a corresponding decrease in Alveolar PO2 (PAO2) which, in turn, decreases both PaO2 and SaO2.
(c) A partial list of causes of respiratory acidosis includes depression of the medullary respiratory center (e.g., barbiturates), paralysis of the diaphragm (e.g., amyotrophic lateral sclerosis), and chronic bronchitis.
Causes of hypoxemia:
Ventilation Defect
Ventilation defect
(a) Definition—alveoli are perfused; however, there is impaired O2 delivery to alveoli.
(b) _Respiratory distress syndrome (_RDS; refer to Chapter 17) is an example of a diffuse ventilation defect, where a lack of surfactant causes collapse of the distal airways (called atelectasis) in both lungs (note the arrows in Fig. 2-3).
–Ventilation defect: lung perfused but not ventilated.
Diffuse ventilation defects produce intrapulmonary shunting of blood characterized by pulmonary capillary blood having the same PO2 and PCO2 as venous blood returning from tissue (i.e., a large fraction of pulmonary blood flow has not been arterialized).
Ventilation defect: produces intrapulmonary shunting
Causes of Hypoxemia:
Perfusion Defect
Perfusion defect
Definition—alveoli are ventilated but there is no perfusion of the alveoli
Examples—pulmonary embolus and fat embolism.
(b) Perfusion defects produce an increase in *pathologic dead space.
•In pathologic dead space, the exchange of O2 and CO2 does not occur (normal dead space includes the mouth to the beginning of the respiratory bronchioles).
Perfusion defect: ↑dead space
(c) Inspired %O2 from 24% to 28% or greater increases the PaO2 in perfusion defects, because they tend to be less extensive than ventilation defects.
•Other parts of ventilated and perfused lung have normal gas exchange; hence compensating for most perfusion defects (e.g., pulmonary embolus).
Causes of Hypoxemia:
Diffusion defect
Definition—decreased diffusion of O2 through the alveolar-capillary interface into the pulmonary capillaries
(b) Examples—interstitial fibrosis, pulmonary edema
Cyanotic congenital heart disease (Tetralogy of fallot) is another cause of hypoxia
• Shunting of venous blood into arterial blood causes a drop in the PaO2.
Causes of hypoxia related to Hemoglobin (Hb) abnormalities:
Anemia
Anemia
(1) Definition—decrease in Hb concentration
Anemia: ↓Hb concentration; ↓O2 content
(2) Causes of anemia
(a) Decreased production of Hb (e.g., iron deficiency)
(b) Increased destruction of RBCs (e.g., hereditary spherocytosis)
(c) Decreased production of RBCs (e.g., aplastic anemia)
(d) Increased sequestration of RBCs (e.g., splenomegaly)
Anemia: ↓production Hb/RBCs; ↑destruction/sequestration RBCs
(3) PaO2 and SaO2 are normal.
•Total amount of O2 delivered to tissue is decreased (↓O2content), which has no effect on normal O2 exchange in the lungs.
Anemia: normal Pao2/Sao2; ↓O2 content
Methemoglobinemia (metHb)
Methemoglobinemia (metHb)
(1) Definition—Hb with oxidized heme groups (Fe3+)
MetHb: heme Fe3+; cannot attach to O2
MetHb reduction: NADH electrons → cytochrome b5 → cytochrome b5 reductase → heme Fe2+
(2) Causes
(a) Oxidant stresses
• Examples—nitrite- and/or sulfur-containing drugs, nitrates (fertilizing agents), and sepsis
(b) Congenital deficiency of **cytochrome b5 reductase
(3) Pathogenesis of hypoxia
(a) Fe3+ cannot bind O2; hence PaO2 is normal, but SaO2 is decreased.
• ↓SaO2 decreases O2 content, causing an increase in EPO.
MetHb: heme Fe3+; normal PaO2, ↓SaO2
(b) Ferric heme groups impair unloading of O2 by oxygenated ferrous heme in the RBCs (impairs cooperativity).
• MetHb shifts the O2-binding curve to the **left.
MetHb: shifts OBC to left; lactic acidosis.
(4) Clinical findings
(a) Cyanosis at low levels (levels <20%)
(b) Headache, anxiety, dyspnea, tachycardia (levels >20%)
(c) Confusion, lethargy, lactic acidosis (levels >40%)
•Lack of O2 causes a shift to anaerobic glycolysis leading to lactic acidosis.
Carbon Monoxide poisoning
CO: leading cause of death due to poisoning
(2) Produced by incomplete combustion of carbon-containing compounds.
(3) Causes include:
•Automobile exhaust, smoke inhalation, wood stoves, indoor gasoline powered generators, and clogged vents for home heating units (e.g., methane gas)
↑CO: car exhaust, smoke inhalation, wood stoves
(4) Pathogenesis of hypoxia
(a) CO has a high affinity for heme groups and competes with O2for binding sites on Hb.
• This decreases SaO2 (if blood is measured with a co-oximeter) without affecting the PaO2.
(b) CO inhibits cytochrome oxidase in the ETC.
- Cytochrome oxidase normally converts O2 into water.
- Inhibition of the enzyme prevents O2 consumption, shuts down the ETC, and disrupts the diffusion gradient that is required for O2 to diffuse from the blood into the tissue.
(c) Similar to metHb, CO attached to heme groups impairs unloading of O2 from oxygenated ferrous heme in RBCs into tissue (impairs cooperativity).
• CO shifts the O2-binding curve to the left.
(d) ↓SaO2 decreases O2 content causing an increase in EPO.
(5) Clinical findings
(a) Cherry-red discoloration of the skin and blood.
(b) Headache (first symptom at levels of 10%–20%)
(c) Dyspnea, dizziness (levels of 20%–30%)
(d) Seizures, coma (levels of 50%–60%)
(e) Other findings—atraumatic rhabdomyolysis (myoglobin binds CO and prevents normal muscle function), delayed neurologic deficits (e.g., memory deficits, apathy)
Laboratory findings
a) ↑CO levels in blood if measured with a co-oximeter.
(b) Lactic acidosis (shift to anaerobic glycolysis)
CO poisoning: normal PaO2, ↓SaO2, lactic acidosis (hypoxia)
Treatment
(a) Administer 100% O2 therapy with nonrebreather mask or endotracheal tube.
(b) Hyperbaric oxygen therapy
Factors causing a left-shift of the OBC
Decreased 2,3-bisphosphoglycerate (2,3-BPG)
(a) 2,3-BPG is an intermediate of glycolysis in RBCs and is formed by conversion of 1,3-BPG to 2,3-BPG.
(b) Stabilizes the taut form of Hb, which ↓O2 affinity and allows O2 to move into tissue.
(2) Other factors include CO, alkalosis, metHb, fetal Hb, and hypothermia
COHb and MetHb: ↓SaO2, normal PaO2, left-shifted OBC
(3) All factors that shift the OBC to the left increase affinity of Hb for O2 with less release of O2 to tissue.
•Example—at the capillary PO2 concentration in tissue, a right-shifted OBC (↑2,3-BPG, acidosis, fever) has released most of its O2 to tissue (80% to tissue), whereas a left-shifted OBC still has most of its O2 attached to heme groups (only 20% to tissue; see Fig. 2-5).
Right-shifted OBC: ↑2,3-BPG, fever, acidosis, high altitude
Thalassemia
- Epidemiology
a. Definition—decrease in α- or β-globin chain synthesis
b. Autosomal recessive disorders
c. α-thal is common in Southeast Asians, people who live on the African west coast, and in blacks (prevalence of 5%).
d. β-thal is common in blacks, Greeks (prevalence 15% to 30%), and Italians.
Blacks can have α- or β-thalassemia
What is the Pathogenesis of alpha-Thalassemia?
Decrease in α-globin chain synthesis is due to gene deletions.
- Four genes control α-globin chain synthesis.
b. One gene deletion produces a silent carrier.
•Not associated with anemia
c. Combination of two gene deletions is called α-thal trait.
(1) Produces a mild anemia with a normal to increased RBC count.
•There is no consensus as to why the RBC count is normal to increased, when the Hb and Hct are decreased; however, it is a very useful clinical finding.
α-thal trait: mild anemia; N/↑RBC count.
(2) In the black population, it is associated with a loss of one gene on each chromosome (trans: α/− α/−; see Fig. 12-11A)
Black α-thal trait: trans α/− α/−
(3) In the Southeast Asian population, it is associated with a loss of both genes on the same chromosome (cis: −/− α/α; see Fig. 12-11B)
•Increased risk for developing more severe types of α-thal, because one chromosome completely lacks α-globin genes.
Southeast Asian α-thal trait: cis −/− α/α; danger severe types
d. Combination of three gene deletions is called HbH (four β-chains) disease.
(1) Associated with a severe hemolytic anemia
• Excess β-chain inclusions cause macrophage destruction of RBCs (hemolytic anemia).
(2) Hb electrophoresis detects HbH.
HbH: 3 gene deletions; 4 β-chains; severe hemolytic anemia.
e. Combination of four gene deletions is called Hb Bart (four γ-chains) disease
(1) This combination is incompatible with life.
(2) Hb electrophoresis shows an increase in Hb Bart.
Hb Bart: 4 γ-chains; incompatible with life.
Laboratory findings in alpha-thal trait:
f. Laboratory findings in α-thal trait
(1) Decreased MCV, Hb, and Hct
(2) Increased RBC count
(3) MCV/RBC count ratio <13.
(4) Target cells inconsistently present
(5) Teardrop RBCs inconsistently present
(6) Normal RDW, serum ferritin, serum FEP, and Hb electrophoresis.
α-thal trait: ↓HbA, HbA2, HbF (normal electrophoresis); ↑RBC count
Hemoglobin electrophoresis is normal in α-thal trait, because all Hb types require α-globin chains. The Hb concentration is decreased; however, the relative proportions of the normal Hbs remains the same.
g.α-thal trait is a diagnosis of exclusion.
•Usually there is a family history of members with a mild microcytic anemia, normal Hb electrophoresis, and normal iron studies.
h.There is no treatment
What si the pathogenesis of Beta-thalassemia?
a. Decrease in β-globin chain synthesis.
(1) Mild anemia is most often due to DNA splicing defects.
(2) Severe anemia is due to a nonsense mutation with formation of a stop codon.
•Premature termination of β-globin chain synthesis or absent β-globin chain synthesis
β-thal: mild—DNA splicing defect; severe—stop codon
b.Normal synthesis of α-, δ-, and γ-globin chains
*Normal β-globin chain synthesis is designated β; some β-globin chain synthesis is designated β+; absence of β-globin chain synthesis is designated β°.
β-thal minor: β/β+
(1) Mild microcytic anemia
(2) Decreased MCV, HB, and Hct
(3) Increased RBC count
(4) MCV/RBC count ratio <13
(5) Target cells consistently present
6) Teardrop RBCs present (see Fig. 12-12B)
•Due to damage of the RBC membrane from removal of excess globin chains by splenic macrophages
(7) Normal RDW, serum ferritin, and serum FEP
•Serum FEP is normal because heme synthesis is normal.
(8) Hb electrophoresis (see Fig. 12-7C)
(a) HbA (α2/β2) is decreased, because β-globin chains are decreased.
(b) Corresponding increase in HbA2 (2α/2δ) and HbF (2α/2γ)
β-thal minor: ↓HbA; ↑RBC count, HbA2, HbF; normal RDW; target cells, tear drop cells
(9) No treatment
Beta-thalassemia Major (Cooley anemia)
β-Thal major (Cooley anemia; βo/βo or βo/β+)
β-thal major: β°/β° or βo/β+
(1) Severe hemolytic anemia
(a) RBCs with α-chain inclusions are removed by splenic macrophages
•Marked increase in unconjugated bilirubin (UCB; jaundice)
(b) RBCs with α-chain inclusions undergo apoptosis in the bone marrow (ineffective erythropoiesis).
β-thal major: severe hemolytic anemia; EMH; **hair-on-end skull x-ray
(2) EMH and accelerated erythropoiesis
(a) Hepatosplenomegaly from excessive hematopoiesis
(b) Radiographs of the skull show a hair-on-end appearance (see Fig. 12-3).
(3) Increased RDW due to increased size variation (see Fig. 12-12B)
(4) Increase in reticulocytes, teardrop cells, Howell-Jolly bodies (nuclear remnants), and nucleated RBCs (see Fig. 12-12B)
(5) Hb electrophoresis (see Fig. 12-7D)
(a) No synthesis of HbA
(b) Corresponding increase in HbA2 and HbF
β-thal major: no HbA; ↑HbA2, HbF, RDW, reticulocytes
(6) Treatment
(a) Blood transfusion
- Danger of iron overload (called hemosiderosis)
- Requires chelation therapy with desferrioxamine
(b)Bone marrow transplantation (only curative approach)
Laboratory findings in sickle cell trait and disease
a.Sickle cell screen
•Sodium metabisulfite reduces O2 tension, which induces sickling in a test tube.
Screen: sodium metabisulfite ↓O2 tension, induces sickling
b. Hb electrophoresis (see Fig. 12-7E and F)
(1) HbAS (trait) profile: HbA 55% to 60%, HbS 40% to 45%
(2) HbSS (disease) profile: HbS 90% to 95%, HbF 5% to 10%, no HbA
c. Peripheral blood findings
(1) Normal peripheral blood smear in HbAS
(2) Sickle cells, target cells, nucleated RBCs, and Howell-Jolly bodies in HbSS (seeFig. 12-24A)
d. Prenatal screening
•Analysis of fetal DNA is used to detect the point mutation.
HbAS: HbA 55%–60%, HbS 40%–45%
HbSS: HbS 90%–95%, HbF 5%–10%, no HbA
Target cells: excess RBC membrane; sign hemoglobinopathy or alcohol excess
