Micro Exam 3 Answers – Flashcards

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4 characteristic signs of inflammation
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  1. erythema - due to increased blood flow
  2. heat - due to increase in blood and more rapid metabolic processes
  3. edema - increased permeability, fluid moves from blood to tissue spaces
  4. pain - injury to nerve fibers or bacterial toxins
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Histamine
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Increase Vasodilation

Increase Permeability

Released by mast cells in connective tissue - basophils in the blood

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Prostaglandins
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Intensify the effects of histamine

Released by injured tissue

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Leukotrienes
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Increase Permeability

Released by mast cells and basophils

Function in adherence of phagocytes to pathogens

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Cytokines
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  • Released by monocytes, macrophages, lymphocytes
  • Regulators of inflammatory response
  • Attract leukocytes, initiate fever
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Complement
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  • Increase Vasodilation
  • Increase Permeability
  • Stimulates histamine release
  • Attract neutrophils
  • Promotes phagocytosis
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Examples and Function of Polymorphonuclear Cells
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Basophils, neutrophils, eosinophils, mast cells

Destroy intracellular pathogens (phagocytosis), release chemicals

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Examples and Function of Antigen Presenting Cells
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Macrophages, monocytes, dendritic cells

Present antigens to lymphocytes

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Neutrophils
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Short lived
Ingest, kill, and digest microbial pathogens
First to inflammatory sites
Granules contain antimicrobial agents, such as:

  1. lysozymes
  2. lactoferrin
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Eosinophils
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Mediate allergic reactions and defense against helminths
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Basophils
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Mast cells are tissue counterpart

Produce cytokines in defense against parasites

Responsible for allergic reaction

Secrete primary mediators (histamines) and secondary mediators (leukotrienes)

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Monocytes
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Macrophages are tissue counterpart

Phagocytosis and intracellular killing

Antigen presentation to T-cells

Recruit other immune cells through cytokine and production

Specialized Macrophages:

  1. Kupfer cells (liver)
  2. Glial cells (brain)
  3. Langerhans cells (skin)
  4. Osteoclasts
  5. Alveolar macrophages
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Dendritic cells
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these are differentiated macrophages that act as APCs to active T-helper cells, Cytotoxic T cells, B-cells

Found in most organs

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B lymphocytes
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Differentiate into plasma cells to secrete immunoglobulin glycoproteins that bind antigens with high degree of specificity

 

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T Lymphocytes
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immature thymocytes differentiate in the thymus

cell mediated immunity

help B-cells produces immunoglobulins

CD4 expressing T helper cells

CD8 expressing Cytotoxic T cells

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CD4 Expressing Cells
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  • T-Helper Cells
  • Regulators of delayed-type hypersensitivity responses
  • Assist in the stimulation of B cells

 

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CD8 Expressing Cells
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Cytotoxic T cells

Cytotoxic against tumor cells and host cells with intracellular pathogens

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Natural Killer Cells
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Large, granular lymphocytes

Kill tumor cells and pathogen-infected cells

Enhanced by IFN and IL

Lack the major B and T-cell markers

Kill by direct and antibody-dependent cytotoxicity

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Primary or Secondary Lymphoid Organ? Fetal Liver
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Primary
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Primary or Secondary Lymphoid Organ? Adult bone marrow
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Primary
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Primary or Secondary Lymphoid Organ? Thymus
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Primary
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Primary or Secondary Lymphoid Organ? Lymph Nodes
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Secondary
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Primary or Secondary Lymphoid Organ? Spleen
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Secondary
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Spleen: Red Pulp
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  • Has vascular sinuses with macrophages
  • Macrophages break down old RBCs and recycles hemoglobin - retrieval of iron
  • Macrophages also break down platelets

 

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Spleen: white pulp
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  • T and B cell area
  • Germinal centers w/ macrophages and dendritic cells --> present antigens to lymphocytes
  • B-cells become plasma cells so they can make immunoglobulins
  • Macrophages break down antigens

 

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Lymph Nodes: Function
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Filters antigen and debri from lymph

Macrophages and dendritic cells (primarily in medulla area) cleanse lymph

T cell and B cell maturation occurs here

 

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Primary or Secondary Lymphoid Organ? Mucosa Associated Lymphoid Tissue
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Secondary
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Musoca Associated Lymphoid Tissue (MALT): Examples
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Tonsils

Peyer's Patches (located in ileum)

Appendix

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Musoca Associated Lymphoid Tissue (MALT): general locations and functions
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  • These are cellular aggregates (non-encapsulated) in the lining of the respiratory and digestive tracts
  • They are strategically located to recognize antigens and respond with an appropriate immune response
  • Contain resident intraepithelial lymphocytes
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Omenn's Syndrome
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  • This is a form of SCID (Severe Combined Immunodeficiency)
  • An autosomal recessive disorder
  • Absence of germinal centers in lymph nodes --> replaced with a diffuse infiltrate of large cells with abundant cytoplasm
  • There is abnormal intra-thymic T-cell development plus inefficient and/or abnormal generation of TCR's as well as a deficiency of B-cells and receptors (antibodies)

;

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Omenn's Syndrome: Symptoms
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Chronic diarrhea

leukocytosis

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T-Helper Cells: Characteristics
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  1. Express the CD4 co-receptor
  2. Recognize antigens complexed with MHC II on B cells, macrophages, or other APCs
  3. Activate memory T helper cells and cytokine-secreting cells
  4. Stimulated B-cells
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Cytotoxic T cells: Characteristics
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  1. Express the CD8 co-receptor
  2. Dependent upon MHC I on APCs
  3. Are cytotoxic against tumor cells
  4. Are cytotoxic against host cells with intracellular pathogens --> causes them to undergo apoptosis
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What are the 3 groups of molecules that specifically recognize foreign antigens for the adaptive immune system?
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  1. T-cell receptors
  2. B-cell receptors
  3. MHC
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T/F: Not all TCR's expressed by a single T-cell are specific for the same antigen
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False

ALL TCR's expressed by a SINGLE T-CELL ARE SPECIFIC for the SAME ANTIGEN

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Endogenous (cytoplasmic) Antigen Processing: Characteristics
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MHC I are associated with this type of antigen processing

MHC I are found in all nucleated cells (excluding immunological cells)

MHC I participates in anitgen presentation to CD8 Cytotoxic T cells

Endogenous because the virus has already infected the cell and has started to make viral proteins that are in the cytoplasm (endogenous pathogens)

The viral protein is degraded by proteosomes and the degradation products of the viral protein are combined with MHC I --> sent to cell surface for presentation

This marks the cell for destruction by Cytotoxic T cells

 

 

 

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Exogenous (endosomal) Antigen Processing: Characteristics
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  • MHC II are associated with this type of antigen processing
  • MHC II molecules are found on APC's (macrophages, dendritic cells) and B-cells
  • MHC II participates in antigen presentation to CD4 T-Helper cells
  • Exogenous because the pathogen is outside the cells and is taken up by endosomes that break it down
  • The degradation products will be combined with MHC II and sent to the surface of the cell for presentation
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Cytokine-related disorder due to: Overproduction of IL-1, IL-6, TNF
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  1. Drop in BP
  2. Shock
  3. Fever
  4. Blood clotting

endotoxin stimulation of macrophages after G- bacterial infection --> septic shock

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Cytokine-related disorder due to: Massive release of cytokines
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superantigen stimulation of T-cells by bacterial toxins --> toxic shock
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Cytokine-related disorder due to: Decreased expression of IL-2 receptor
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Immune suppression

Caused by Trypanosoma cruzi --> Chagas

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IgD
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With IgM, it the major Ig expressed by mature B-cells

Functions in activation of B-cells by antigens

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IgG
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  • Protects fetus
  • Neutralizes bacterial toxins and viruses
  • Complement activator
  • Plays a huge role in persistent viral, bacterial, and fungal infections
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IgE
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Binds to allergens

Mediates hypersensitivity reactions (such as asthma, hives, hay fever) by inducing degranulation of basophils and mast cells

Protects against parasitic infections

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IgA
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Main Ig in external secretions (tears, saliva, breast milk, mucus)
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IgM
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  • Analagous to neutrophils in that they are the first to respond to an infection
  • Has 10 antigen binding sites
  • Activates complement pathway
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Phase of the Adaptive Immune Response
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  1. Antigen recognition
  2. Lymphocyte activation
  3. Effector Phase
  4. Decline (homeostatis)
  5. Memory
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What is the immunological basis for multiple myeloma?
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  • Cancer of the cells in the bone marrow --> results in an increase in plasma cells
  • There will be a decrease in polymorphonuclear cells

 

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In patients with multiple myeloma, why are patients considered more susceptible to bacterial infections?
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  • They have a marked increase in plasma cells, which results in an increase in IgG and they are producing only that particular Ig
    Their body is not producing any other Ig (such as IgA, IgD, IgM, etc.)
  • This leaves the patient susceptible to other pathogens that other Ig take care of (parasites, no added protection of IgA in tears, etc.)
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What are the two pathways of the complement system?
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  1. Alternate (innate) pathway
  2. Classical (humoral) pathway
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How is the alternate pathway activated?
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Most commonly activated by microbial surfaces or cell components (e.g. lipopolysaccharides)
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What type of immunity (innate or adaptive) is associated with the alternate pathway?
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Innate
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What type of immunity (innate or adaptive) is associated with the classical pathway?
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Adaptive (humoral)

 

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How is the classical pathway activated?
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  • It is activated by antigen/antibody complexes containing IgM or IgG
  • It is the major effector of the humoral immunity
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What are the two major biological activities of complement products?
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  1. Membrane Attack Complex acts as a molecular drill to puncture cell membranes
  2. Complement cleavage products promote: opsonization (enhancement of phagocytosis) inflammatory responses, degranulation, etc.
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What is the pathological basis of DiGeorge Syndrome and what is the result?
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  • Deletion of a portion of chromosome 22
  • Babies are born without a thymus
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For patients with DiGeorge Syndrome, what is the effect of thymus absence on maturation of T cells?
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  • Basically, patient will not have maturation of T-cells, because this is where T cells mature
  • Since the baby does not have a thymus, its body will rely on bone marrow
  • However, T-cells will not have their coreceptors (CD4 or CD8) and therefore no T-helper cells or Cytotoxic T cells
  • There will be an accumulation of B cells that won't be stimulated

 

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