1 / 66

Red Blood Cells, Anemia and Polycythemia

Red Blood Cells, Anemia and Polycythemia. Prof. dr. Zoran Vali ć Department of Physiology University of Split School of Medicine. Red Blood Cells (Erythrocytes). functions: transport of hemoglobin (O 2 ) in some animals it circulates as free protein

atalo
Download Presentation

Red Blood Cells, Anemia and Polycythemia

An Image/Link below is provided (as is) to download presentation Download Policy: Content on the Website is provided to you AS IS for your information and personal use and may not be sold / licensed / shared on other websites without getting consent from its author. Content is provided to you AS IS for your information and personal use only. Download presentation by click this link. While downloading, if for some reason you are not able to download a presentation, the publisher may have deleted the file from their server. During download, if you can't get a presentation, the file might be deleted by the publisher.

E N D

Presentation Transcript


  1. Red Blood Cells, Anemia and Polycythemia Prof. dr. Zoran Valić Department of Physiology University of Split School of Medicine

  2. Red Blood Cells (Erythrocytes) • functions: • transport of hemoglobin (O2) • in some animals it circulates as free protein • in humans within RBC – loss by filtration 3% • large quantity of carbonic anhydrase (CO2 and H2O) • an excelent acid-base buffer (proteins)

  3. biconcave discs (φ=7,8 μm; V=90-95 μm3) • shape can change remarkably (squeeze through capillaries, excess of membrane) • M = 5,2x1012 • F = 4,7x1012 • chemoglobin in RBC < 340 g/L • Ht = 40-45% • chemohlobin in blood = 160-140 g/L

  4. yolk sac (few early weeks) • liver; spleen and lymph nodes(middle trimester of gestation) • bone marrow • beyond the age of 20 most RBC are produced in membranous bones (vertebrae, sternum, ribs and ilia)

  5. growth inducers – proteins which control growth and reproduction of stem cells • interleukin-3 – promotes growth and reproduction of virtually all stem cells • differentiation inducers (low oxygen, infectious diseases)

  6. 1% bone marrow

  7. tissue oxygenation – most essential regulator (viscosity) • hemorrhage, x-ray therapy, high altitudes, cardiac failure, lung diseases • erythropoietin (glycoprotein; 34000) • 90% is formed in kidneys (unknown, liver) • fibroblast-like interstitial cells surrounding the tubules? • renal tissue hypoxia (and some other)   HIF-1   erythropoietin • quick secretion (min – 24 h), RBC in 5 days • production of proerythroblasts, speeding up

  8. erythropoietic cells are among the most rapidly growing and reproducing cells • person’s nutritional status • vitamin B12 and folic acid (thymidine) • macrocytes – flimsy membrane and irregular, large shape – shorten life span (1/2-1/3 normal) • B12 – pernicious anemia (atrophic gastric mucosa; parietal cells – intrinsic factor) • folic (pteroylglutaminic) acid – widely spread but destroyed during cooking – sprue

  9. Formation of Hemoglobin • begins in proerythroblasts and continues even into the reticulocyte stage • succinyl-CoA from Krebs metabolic cycle • alpha, beta, gamma and delta chains • most common – hemoglobin A (2 alpha, 2 beta chains) • each hemoglobin molecule transports 4 molecules of oxygen

  10. sickle cell anemia –the amino acid valine is substituted for glutamic acid at one point in each of the two beta chains • 15 μm elongated crystals in low oxygen environment • loosely and reversibly combining with O2 • “coordination bond”, molecular oxygen

  11. Iron Metabolism • hemoglobin, myoglobin, cytochrome-oksidase, peroxidase and catalase • total iron in the body – 4-5g (65% in hemoglobin, 4% in myoglobin, 15-30% in reticuloendothelial system and liver parenchymal cells)

  12. transferrin molecule binds strongly with receptors in the cell membrane s of erythroblasts in bone marrow – endocytosis • inadequate quantities of transferrin – failure to transport iron to the erythroblasts – hypochromic anemia

  13. Absorption of Iron • liver secretes moderate amounts of apotransferrin into the bile – transferrin (with the iron, pinocytosis into enterocyts, plasma transferrin) • absorption is slow and limited; total body iron is regulated mainly by altering the rate of absorption

  14. Life Span of RBC • average circulating time  120 days • cytoplasmic enzymes: • maintaining pliability of the cell membrane • maintain membrane transport of ions • keep the iron in ferrous, rather than ferric form • prevent oxidation of the RBC proteins • many RBC self-destruct in the spleen (when squeezing through the red pulp)

  15. hemoglobin is phagocytized by macrophages (Kupffer cells of the liver)  iron and bilirubin (from porphyrin portion)

  16. Anemias (deficiency of hemoglobin) • microcytichypochromic anemia – blood loss anemia (acute and chronic) • aplastic anemia – bone marrow aplasia (high-dose radiation, chemotherapy, drugs, toxic chemicals – insecticides or benzene) • megaloblastic anemia (lack of B12 (pernicious) or folic acid)

  17. hemolytic anemia (abnormalities (hereditary) of RBC) • hereditary spherocytosis (small and spherical RBC) • sickle cell anemia (hemoglobin S, crisis) • erythroblastosis fetalis

  18. Effects of Anemia on Circulation • viscosity of blood depends largely on RBC • fall in blood viscosity  decrease in total resistance (added tissue hypoxia – vasodilation)  increase in CO (3-4x)  increased pumping workload on the heart • problems during exercise – acute cardiac failure

  19. Polycythemia • secondary polycythemia – due to hypoxia (at high altitude, cardiac failure) – 6-7 x 1012 (30%) • polycythemiavera (erythremia) – 7-8 x 1012 (Ht = 60-70%) – genetic aberration in the hemocytoblastic cells • increased viscosity – CO almost normal (decreased venous return, but increased blood volume), ruddy complexion with a bluish (cyanotic) tint to the skin)

  20. BloodTypes; Transfusion; Tissueand Organ Transplatation

  21. Antigenicity • first attempts were unsuccessful • transfusion reaction and death • blood posses antigenic and immune properties • at least 30 commonly occurring, and hundreds of other antigens • most of antigens are week, used to establish parentage • systems: O-A-B and Rh

  22. OAB system is discovered by Austrian scientist Karl Landsteiner 1900. (three types, awarded Nobel prize 1930; simultaneously with Czech serologist Jan Janský) • also with Alexander S Wiener identified Rh factor 1937.

  23. O-A-B Blood Types • antigens A i B (also called agglutinogens – cause blood cell agglutination) occur on the surface of the RBC • because of the way of inheritance people may have neither of them on their cells, they may have one or they may have both simultaneously

  24. when neither A or B agglutinogen is present – blood (person) is blood type O • only agglutinogen A – blood is type A • only agglutinogen B – blood is type B • when both agglutinogens are present – blood is type AB

  25. antigen H – essential precursor of OAB blood antigens • located on chromosome 19, posses 3 exons which are coding enzyme fucosyltransferase • enzyme creates H antigen on RBC • carbohydrate chain: β-D-galactose, β -D-N-acetilglucosamine, β -D-galactoseiα-L-fucose (connection with protein or ceramid)

  26. OAB locus is on chromosome 9, has 7 exons • exon 7 is the biggest and contains the greatest portion of coding sequence • OAB locus has 3 allele types: O, A, B

  27. allele A codes glycosyltransferase which bindes N-acetylgalactosamine on D-galactose end of H antigen • allele B codes glycosyltransferase which bindesα -D-galactose on D-galactose end of H antigen • allele 0 has deletion in exon 6 – loss of enzimatic activity – only H antigen is present

  28. Relative Frequencies of the Different Blood Types: 0 47% A 41% B 9% AB 3% • there are 6 different allele types among white population: (A1, A2, B1, O1, O1v i O2), in Asian population B type is more frequent

  29. Agglutinins • antibodies directed at agglutinogens • immediately after birth – not present • they are formed 2-8 month after the birth • maximum titer is reached 8-10 years of age • gamma-globulins (IgMiIgG) • why are they produced? • environmental antigens (bacteria, viruses, plants, foods)

  30. for anti-A agglutinins – influenza • for anti-B agglutinins – gram-negative bacteria (E. coli) • “light in the dark” theory – viruses during replication process incorporate parts of host membrane

  31. Agglutination Process • agglutinins have 2 (IgG) or 10 (IgM) binding sites for agglutinogens • attaching to two or more RBC – bounding together (clump of cells) – agglutination • plugging of small blood vessels throughout the circulation – physical distortion of the cells or phagocytosis – hemolysisof the RBC

  32. Acute Hemolysis • on rare occasion • hemolysis occurs immediately in circulating blood • activation of the complement system – release of proteolytic enzymes (the lytic complex) – rupture of the cell membranes (existence of high titer of IgM antibodies – hemolysins)

  33. Blood Typing • blood typing and blood matching • RBC are separated from the plasma and diluted with saline; mixing with anti-A and anti-B agglutinins

More Related