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Ch 16: Blood Plasma and Cellular Elements of Blood Hematopoiesis

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1 Ch 16: Blood Plasma and Cellular Elements of Blood Hematopoiesis
RBC Physiology Coagulation

2 Blood = connective tissue
Extracellular matrix: Specialized cells: Fig 16-1

3 Blood Components Overview
Plasma Blood 20-40% Total WBC: 4, ,000 2-8% Cellular Elements 50-70% Blood Components Overview 1- 4% Fig 16-1/3

4 Red Blood Cells O2 Fig 16-5

5 Hem(at)opoiesis = Blood Cell Formation
Few uncommitted stem cells in red bone marrow throughout life time (Fig 16-2) Controlled by cytokines. Examples: Erythropoietin CSFs and ILs: e.g. M-CSF, IL- 3 (= multi CSF) Thrombopoietin Leukemia vs. leukocytosis vs. leukopenia Any of various acute or chronic neoplastic diseases of the bone marrow in which unrestrained proliferation of white blood cells occurs, usually accompanied by anemia, impaired blood clotting, and enlargement of the lymph nodes, liver, and spleen. Leukemias (“white blood”) group of cancerous conditions of WBCs. Named according to the abnormal WBC type primarily involved (e.g. lymphocytic leukemia, myelocytic leukemia). Leukemia is acute (quickly advancing - mostly in children) if it derives from blast-type cells like lymphoblasts, and chronic (slowly advancing - mostly in adults) if it involves proliferation of later cell stages like myelocytes. Leukemia, lymphoma and myeloma are cancers that originate in the bone marrow (in the case of leukemia and myeloma) or in lymphatic tissues (in the case of lymphoma). Leukemia, lymphoma and myeloma are considered to be related cancers because they involve the uncontrolled growth of cells with similar functions and origins. The diseases result from an acquired (not inherited) genetic injury to the DNA of a single cell, which becomes abnormal (malignant) and multiplies continuously. The accumulation of malignant cells interferes with the body's production of healthy blood cells and makes the body unable to protect itself against infections. Leukemia - Leukemia is a malignant disease (cancer) that originates in a cell in the marrow Non-Hodgkin Lymphoma - Lymphoma is a general term for a group of cancers that originate in the lymphatic system Hodgkin Lymphoma - Hodgkin lymphoma (also known as Hodgkin's disease) is a specialized form of lymphoma and represents about 8 percent of all lymphomas diagnosed each year Myeloma - Myeloma is a cancer of plasma cells, a type of white blood cell found in many tissues of the body, but mainly in the marrow Myelodysplastic Syndromes - Myelodysplastic syndromes are a group of diseases that originate in an early blood-forming cell in the marrow Leukopenia at

6 Controlled by ____________,specifically CSFs and ILs
colony-forming unit CFU-GEMM, multipotent progenitor cells, give rise to erythroid, granulocyte-macrophage and megakaryo Compare to Fig 16-2

7 EPO Regulates RBC Production
“Hormone” synthesized by kidneys in response to hypoxemia EPO gene cloned in  Recombinant EPO now available (Epogen, Procrit) Use in therapy, abuse in sport EPO is not stored, only produced upon demand.

8 Erythropoiesis lifespan ~ 120 days Reticulocytes
EPO release Mitotic rate  Tissue O2  Maturation speed  RBC  bag of Hb for carrying O2 lifespan ~ 120 days source of ATP for RBC?  Tissue O2  Reticulocytes enter circulation

9 Hemoglobin (Hb) Requires iron (Fe) + Vit. B12 (cobalamin) p.698/Ch21
Quaternary protein structure ? Reversible binding between Fe & O2 CO: a toxic gas (not in book) Bilirubin to bile. Hyperbilirubinemia HbA vs. HbF HbF is designed to steal oxygen from maternal blood in placenta. Replaced shortly after birth. CO is a product of incomplete combustion (complete combustion producesCO2 and H2O.) This obviously includes exposures to fires by victims and fire fighters but also includes smokers (cigars produce more CO than cigarettes - up to 20% CO Hb possible). Exhaust fumes are a common source of CO exposure. A recent report detailed high levels of CO exposure in enclosed pickup truck beds from a backdraft of exhaust fumes into the back of the truck. Carbon monoxide also binds coordinately to heme iron atoms in a manner similar to that of oxygen, but the binding of carbon monoxide to heme is much stronger than that of oxygen. The preferential binding of carbon monoxide to heme iron is largely responsible for the asphyxiation that results from carbon monoxide poisoning.

10 Hb Structure Porphyrin ring with Fe in center
How many O2 can 1Hb carry?

11 RBC Disorders Anemias (O2 carrying capacity too low)
Polycythemia vera (PCV ~ 60-70%) Anemias (O2 carrying capacity too low) Hemorrhagic anemia  Fe deficiency anemia Hemolytic anemia, due to genetic diseases (e.g. Hereditary spherocytosis) or infections Pernicious anemia Renal anemia Polycythemia vera most commonly due to bone marrow cancer. Hematocrit can become as high as 80%. Secondary poycytemia when less oxygen is available (high altitudes) or EPO production increased. Polycythemia vera is a clonal stem cell disorder characterized by excessive erythrocyte production. Its etiology is not fully established, but hypersensitivity to interleukin-3 may play a role in the sustained erythrocytosis observed in this disease. Polycythemia vera usually occurs within the age range of 20-80, with 60 being the mean age of onset. The disease is slightly more common in males than in females. Clinical features include headaches, weakness, weight loss, and pruritus (itching without visible eruption on the skin). Major Criteria total RBC vol men > 36 mg/kg; women >32 mg/kg arterial 02 saturation > 92% Splenomegaly Fe deficiency anemia USUALLY A SECONDARY RESULT OF HEMORRHAGIC ANEMIAS. But also due to inadequate intake of iron containing foods or impaired absorption. Results in microcytes (pale small RBCs) Pernicious anemia (p.621) leads to large pale cells due to developing RBCs not dividing. Aplastic anemia due to some toxic chemicals and drugs and ionizing radiation. E.g.: arsenic, chloramphenicol. Fallout from nuclear bomb, excessive exposure to X-rays. Cancer and cancer chemotherapy. Marrow destruction of course affects all formed elements, anemia is just one symptom.

12 Sickle Cell Anemia 1st genetic illness traced to a specific mutation:
Sickle cell anemia HbS instead of normal HbA. One in 100 black newborns in US. Malaria connection: RBCs loose potassium which is essential for survival of parasite (plasmodium) DNA: CAC CTC aa: glutamic acid valine (aa #6 of 146) HbA HbS  crystallizes under low oxygen conditions

13 Platelets = Thrombocytes
Megakaryocytes (MKs) are polyploid. Mechanism? MK produces ~ 4,000 platelets which live an average of 10 days. Platelets contain gra- nules filled with clotting proteins & cytokines Activated when blood vessel wall damaged

14 Hemostasis Vasoconstriction Platelet plug (temporary blockage of hole)
= Opposite of hemorrhage  stops bleeding Too little hemostasis  too much bleeding Too much hemostasis  thrombi / emboli Three major steps: Vasoconstriction Platelet plug (temporary blockage of hole) Coagulation (clot formation seals hole until tissues repaired)

15 Steps of Hemostasis Vessel damage exposes collagen fibers
Platelets adhere to collagen & release factors local vasoconstriction & platelet aggregation decreased blood flow platelet plug formation + feedback loop Fig 16-11

16 Platelet Plug Formation
Platelet activating factor (PAF)

17 Steps of Hemostasis cont.
Two coagulation pathways converge onto common pathway Intrinsic Pathway. Collagen exposure. All necessary factors present in blood. Slower. Extrinsic Pathway. Uses TF released by injured cells and a shortcut. Usually both pathways are triggered by same tissue damaging events. Fig 16-12

18 The Coagulation Cascade
“Cascade” is complicated network! Numbering of coagulation factors according to time of discovery Fig 16-12

19 Common Coagulation Pathway
Intrinsic pathway Extrinsic pathway Active factor X Prothrombin  thrombin fibrinogen  fibrin reinforces platelet plug clot

20 Structure of Blood Clot
Plasmin, trapped in clot, will dissolve clot by fibrinolysis Clot formation limited to area of injury: Intact endothelial cells release anticoagulants (heparin, antithrombin III, protein C). SEM x 4625

21 Clot Busters & Anticoagulants
Dissolve inappropriate clots Enhance fibrinolysis Examples: Urokinase, Streptokinase & t-PA Prevent coagulation by blocking one or more steps in fibrin forming cascade Inhibit platelet adhesion  plug prevention Examples: Coumarin and warfarin block Vit K action (Vitamin K is cofactor in synthesis of several coagulation factors. Ca chelators (EDTA and citrate) only in vitro Heparin inhibits activity of thrombin (produced by basophils) Aspirin prevents platelet plug fomation

22 Hemophilia It is sometimes called Christmas disease after Stephen Christmas, the first patient described with this disease. In addition, the first report of its identification was published in the Christmas edition of the British Medical Journal. In more recent history, royal watchers know that Queen Victoria of Britain's son Leopold had hemophilia, and that two of her daughters, Alice and Beatrice, were carriers of the gene. Through them, hemophilia was passed to the royal families in Spain and Russia, leading to one of the most famous young men with the disease, Tsar Nicholas II's only son Alekei.

23 Hemophilia A (Factor VIII Deficiency)

24 Blood Doping the end


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