Metabolism of RBC

Metabolism of Red Blood Cell&Membrane StabilityProf Dr Kwan Teck KimDepartment of BiochemistryFaculty of MedicineMahsa University College

Learning outcomes On completion of this topic, the student will be able to:Discuss the role of glycolysis in erythrocytes with respect to ATP production, supply of intermediates for Rapoport-Luebering glycolytic shunt and Hexose monophosphate pathway. Explain the role of NADPH in glutathione metabolismExplain the role of ATP and glutathione in the maintenance of erythrocyte membrane stabilityExplain the molecular basis of hemolytic anemias

Red Blood CellThe red blood cell is simple in terms of its structure and function, consisting principally of a concentrated solution of hemoglobin surrounded by a membrane. The erythrocyte membrane is flexible because of its cytoskeletal structure.The red cell contains a battery of cytosolic enzymes, such as suproxide dismutase, catalase, and glutathione peroxidase, to dispose of powerful oxidants (ROS, reactive oxygen species) generated during its metabolism.Genetically determined deficiency of the activity of glucose-6-phosphate dehydrogenase, which produces NADPH, is an important cause of hemolytic anemia.

Glycolysis Pathway4Rapoport-Luebering glycolytic shuntTo generate 2,3-Bisphosphoglycerate (2,3-BPG)

2,3-BPG is important regulator of binding of O2 to Hb.

HbO2 + 2,3-BPG Hb-2,3-BPG + O2 (deoxyhemoglobin)

ADP ATP 2-2,3-Bisphosphoglycerate shunt2,3-Bisphosphoglycerate mutase/phosphataseThis enzyme is bifunctional, serving as mutase for the formation of 2,3-bisphosphoglycerate and also as a phosphatase.

Phosphatase hydrolyzes 2,3-bisphosphoglycerate to 3-phosphoglycerate and Pi .

Erythrocytes contain very high concentrations of 2,3-bisphosphoglycerate, which functions as important negative allosteric regulator of the binding of oxygen to hemoglobin. 2,3-Bisphosphoglycerate mutase/phosphatase (contd)15-25% of glucose converted to lactate in red blood cells goes by way of the BPG shuntfor the synthesis of 2,3-bisphosphoglycerate.

No net production of ATP occurs when glucose is converted to lactate by the BPG shunt as it bypasses the phosphoglycerate kinase step.

However, it does serve to provide 2,3-BPG, which binds to Hb, decreasing its affinity for O2, and so making O2 more readily available to tissues.

2,3-Bisphosphoglycerate (BPG) in Red Blood Cells Modulates Oxygen release from HemoglobinBPG dissociates as deoxy-Hb is converted to oxy-Hb. H+BPG + Hb + 4O2 Hb(O2)4 + BPG + nH+

Increased concns of BPG force the equilibrium to the left, and they correspondingly shift the saturation plot to the right with an increase in P50 (see Fig. 9.34).In contrast, lowered concns of BPG force this equilibrium to the right, & correspondingly shift the saturation plot to the left with a lower P50 .2,3-Bisphosphoglycerate (BPG) in Red Blood Cells Modulates Oxygen release from Hemoglobin (contd 1)BPG is formed in a minor pathway for glucose metabolism & is present in small amounts in all cells.

In rbc, this pathway is highly active, & BPG concns are approx. equimolar to that of Hb.

BPG binds to the deoxy (T) but not to oxy (R) conformation.

Binding of BPG to Hb stabilizes the T conformation & increases its concn relative to the R conformation.2,3-Bisphosphoglycerate (BPG) in Red Blood Cells Modulates Oxygen release from Hemoglobin (contd 2)Conditions that cause hypoxia (deficiency of oxygen) such as anemia, smoking, and high altitude increase BPG levels in rbc.

In turn, conditions leading to hyperoxia result in lower levels of BPG.

Changes in rbc levels of BPG are slow & occur over hours and days to compensate for chronic changes in pO2 levels.Glucose is translocated by Passive Transport

Glucose transport & metabolism Depending on the concn gradient, erythrocyte GLUT 1 (glucose transporter) facilitates transport of glucose in both directions Glucose is metabolized mainly by glycolysis in erythrocytes.Since erythrocytes lack mitochondria, the end product of glycolysis is lactic acid, which is released into the blood plasma. Glucose metabolism via PPPGlucose used by the Pentose Phosphate pathway in r.b.c. provides NADPH to keep glutathione in the reduced state, which has an important role in the destruction of organic peroxides and H2O2.

Peroxides cause irreversible damage to membranes, DNA and other cellular components and must be removed to prevent cell damage and death.

Erythrocyte and Pentose Phosphate Pathway Glucose 6-phosphate dehyrogenase deficiency causes drug induced hemolytic anemia

Patients administered the drug pamaquine experienced drastic loss of Hb

Role of NADPH in RBCs is to reduce gluthathione to sulfhydryl form

Essential for maintaining structure of Hb (keeps Hb in ferrous state) [ G-S-S-G 2G-SH ]Energy generation

Generates ATP for energy to maintain RBC shape and flexibility

Via anaerobic glycolytic pathway

2 ATP for each molecule glucoseReduced nicotinamide adenine dinucleotide phosphate (NADPH)

Overview of erythrocyte metabolism gOverview of erythrocyte metabolismMature erythrocytes contain no intracellular organelles, so metabolic enzymes of rbc are limited to those found in cytoplasm.Glycolysis is the major pathway, with branches for the hexose monophosphate shunt (for protection against oxidizing agents) andRapoport-Luebering shunt (which generates 2,3-BPG, which moderates oxygen binding to Hb).The NADH generated from glycolysis can be used to reduce methemoglobin (Fe3+) to normal Hb (Fe2+) orTo convert pyruvate to lactate, so that NAD+ can be regenerated and used for glycolysis.

RBC Membrane IntegrityGlutathione is present in RBCs. This is used for inactivation of free radicals formed inside RBC.The enzyme used is glutathione peroxidase.The glutathione is regenerated by an NADPH dependent glutathione reductase.The NADPH is derived from the glucose 6-phosphate dehydrogenase shunt pathway.The occurrence of hemolysis in G6PD deficiency is attributed to the decreased regeneration of reduced glutathione.

Pentose phosphate pathway (Hexose monophosphate shunt) 6-Phosphogluco- lactonase 6-Phosphogluconate dehydrogenase Oxidative phase Non-Oxidative Phase C5 + C5 C3 + C7 Transketolase

C7 + C3 C4 + C6 Transaldolase

C5 + C4 C3 + C6 Transketolase Transketolase & transaldolase reactionsC5 + C5 C3 + C7 (transketolase)

C7 + C3 C4 + C6 (transaldolase)

C5 + C4 C3 + C6 (transketolase)

Transketolase- transfers 2 carbon units.

Transaldolase transfers 3 carbon units. Pentose Phosphate PathwayThe oxidative branch consists of 3 irreversible reacns.

Glucose-6-phosphate dehydrogenase (G6PD), the rate-limiting enzyme, converts glucose 6-phosphate to 6-phosphogluconolactone, which is further converted in a series of reacns to ribulose 5-phosphate.

The 2 NADPH formed are used for reductive biosynthesis and for maintaining the anti-oxidant glutathione in the reduced form.Pentose Phosphate Pathway (contd)All of the reacns of the non-oxidative branch are reversible and produce ribose 5-phosphate for RNA and DNA synthesis.

Also produced are the intermediates fructose 6-phosphate and glyceraldehde 3-phosphate for glycolysis (fed state) or gluconeogenesis (fasting state).

Agents that affect oxygen binding31

Effect of H+ on oxygen binding by HbEffect of H+ on oxygen binding by HbA. In the tissues, CO2 is released. In rbc, this CO2 forms carbonic acid, which releases protons. The protons bind to Hb, causing it to release oxygen to the tissues.

B. In the lungs, the reacns are reversed. O2 binds to protonated Hb, causing the release of protons. They bind to HCO3- , forming carbonic acid, which is cleaved to water and CO2 , which is exhaled.

ReferencesLieberman, M. & Marks, A. (2009). Marks Basic Medical Biochemistry: A clinical approach (3rd edition), Lippincott, Williams & Wilkins, Philadelphia.

Harvey, R.A. & Ferrier, D.R. (2011). Lippincotts Illustrated Reviews: Biochemistry (5th edition), Lippincott, Williams and Wilkins, Philadelphia.

Vasudeven, D.M., Sreekumari, S. & Vaidyanathan, K. (2011). Textbook of Biochemistry for Medical Students (6th edition), Jaypee Brothrs Medical Publishers Ltd, New Delhi.