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Lymphatic System and Immunity. Chapter 16. Functions of Lymphatic System. Draining interstitial fluid Transporting dietary lipids Protection. Lymphatic Vessels. Begin as closed ended lymph capillaries in tissue spaces between cells NOT A CIRCULATING FLUID - PowerPoint PPT Presentation
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Lymphatic System and Immunity
Chapter 16
Functions of Lymphatic System
1. Draining interstitial fluid
2. Transporting dietary lipids
3. Protection
Lymphatic Vessels
• Begin as closed ended lymph capillaries in tissue spaces between cells
• NOT A CIRCULATING FLUID
• Interstitial fluid drains into lymphatic capillaries, forming lymph.
• Lymph capillaries merge to form lymphatic vessels
• Lymphatic vessels carry lymph into and out of lymph nodes
• and finally back to the vascular system.
Lymphatic capillaries
• Made of a single layer of squamous epithelial cells
• Slightly larger than blood capillaries
• Cells overlap and act as one-way valves
• Opened by pressure of interstitial fluid
• Anchoring filaments attach cells to surrounding tissue
Lymphatic vessels
• Resemble veins (same 3 layers)
• Found throughout body except:– Avascular tissues– Central nervous system– Splenic pulp– Bone marrow
Lymphatic vessels join to form lymphatic trunks.
Lymphatic trunks join to form :
Thoracic duct (3/4 of body)
Right lymphatic duct (drains right arm, and right side of head, neck and upper torso)
These empty into subclavian veins at junction with internal jugular vein.
Formation of lymph:Fluid leaves capillaries by diffusion and filtrationEscaped proteins
If lymph flow blocked = tissue swelling or edema
Specialized lymphatic capillaries in vili of small intestine transport lipids - they are called
lacteals, and the fluid is called chyle.
Lymphatic Organs
• Red bone marrow Primary organs
• Thymus gland
• Lymph nodes
• Lymph nodules Secondary organs
• Spleen
Lymph Nodes
• Lymph is filtered through lymph nodes
• Found in clusters
• “Waste water treatment plants”
• Vary in size
• Principal groupings in cervical, axillary and inguinal regions.
• Provide biological filtration
• Site of cancer growth and metastasis
• Vessels enter node on convex side
• Lymph passes through irregular channels called sinuses
• Leaves node through one or two efferent vessels at the hilum or hilus
• Capsule, cortex and medulla
• Cortex contains lymph nodules
• Follicular dendritic cells
• Germinal centers – B cells proliferate
Lymph nodules are also found singly or in groups throughout the mucous membranes of the respiratory, urinary, reproductive and digestive tracts.
MALT – mucosa associated lymphoid tissue
Peyer’s patches in ileum
Tonsils
Some in appendix
Tonsils – lymphoid tissue under the mucous membranes of the throat
palatine tonsils
pharyngeal tonsil – adenoid
lingual tonsils
First line of defense
Tonsillectomy
Thymus gland
• in mediastinum above the heart
• largest at age 10-12 then begins to atrophy
• Pre - T cells come from bone marrow and develop into T cells
• T cells then go to other lymphatic tissues
• Thymus produces hormone thymosin - aids maturation of T cells elsewhere in body
Spleen
• Largest lymphoid organ
• In upper left quadrant of abdomen
• Has a hilum and a capsule
• Sinuses contain blood instead of lymph
White pulp:
little islands, mostly B cells
Red pulp:
Venous sinuses
Splenic cords – RBCs, macrophages, lymphocytes, plasma cells and granulocytes
Functions of Spleen
• Blood formation –– All blood cells in fetus– Only lymphocytes and monocytes after birth
• Blood filtration– Removes bacteria, particles, worn out RBCs
and platelets (recycles iron)
• Blood storage – Can contain over one pint of blood
Nonspecific Resistance
The ability to ward off disease is called resistance.
Lack of resistance is susceptibility.
Nonspecific resistance refers to a wide variety of body responses against a wide range of pathogens. A pathogen is any microorganism that causes disease.
Immunity
Immunity involves activation of specific lymphocytes to combat a specific foreign agent.
Nonspecific Resistance
Species (Inborn) Resistance – certain species contract certain diseases, while other species do not.
Mechanical Barriers
• Skin and mucous membranes :– First line of defense– Physical barrier– Shedding of dead cells– Mucus– Hairs– Cilia– Coughing and sneezing, production of tears, saliva,
urine, defecation and vomiting physically remove harmful substances
Chemical ProtectionSebaceous glands produce sebum – fatty acids inhibit growth of bacteria and fungi
Lactic acid further decreases skin pH
Accumulation of salt
Vaginal secretions are also slightly acidic
Gastric juice – acid, enzymes and mucus
Lysozyme in tears, perspiration, saliva and tissue fluids
Normal Microbiota – bacteria living on skin inhibit the growth of pathogens by producing antibiotics
Antimicrobial Substances
Transferrins are proteins that tie up the free iron in the blood and interstitial fluid.
Interferon – “Paul Revere Chemical” – a glycoprotein produced by virus infected cells that cause neighboring cells to produce anti-viral proteins. These also enhance phagocytosis and can suppress growth of tumor cells.
The Complement System:
10- 20 normally inactive proteins
When activated, they “complement” or enhance certain immune, allergic and inflammatory reactions.
1.Activation of inflammation
2. Opsonization – enhances phagocytosis
3.Cytolysis – membrane attack complex
Fever :
Causes liver and spleen to sequester iron
Increases phagocytosis
Inhibits growth of microbes
Speeds up body repair
Inflammation:
Characterized by:
Heat, swelling, redness, and pain
(and sometimes loss of function)
calor, tumor, rubor and dolor
Stages of inflammation
1. Vasodilation and increased permeability of blood vessels
2. Phagocyte migration1. Neutrophils come first
2. Followed by macrophages
3. Tissue Repair
Phagocytosis
Three phases:
1. Chemotaxis
2. Adherence
3. Ingestion
Natural Killer Cells
• Next line of defense (with phagocytes)
• Lymphocytes – but do not respond to specific antigens
• Can kill a variety of microbes plus tumor cells.
• May release perforins, or attack directly
• Cell may not display correct MHC antigens
Immunity
• Specific resistance to disease involving the production of a specific lymphocyte or antibody against a specific antigen.
• An antigen is any substance that elicits an immune response. Best antigens are:– Large– Complex– Recognized as foreign
Haptens are molecules that are small, foreign and complex. To elicit an immune response, they must piggy-back on a larger molecule, often blood proteins.
Epitopes: a foreign protein may result in several different antibodies. Each antibody recognizes a different portion of the protein. These regions are called epitopes.
Two forms of immunity:
Humoral or antibody mediated immunity
B cells (mature in bone) make antibodies: specific proteins that bind to specific antigens
OR
Cell-mediated immunity
Tcytoxic lymphocytes attack virus infected or tumor cells directly
“The Story”
• Macrophage destroys a bacterium
• Takes bacterial antigen and fuses it with MHC II complex
• MHC II complex and antigen are placed on cell membrane.
• Displays antigen (like a proud cat) – so it is called an antigen presenting cell.
It shows antigen to helper T cells, until it finds one that has a receptor that matches the antigen complex.
The helper T cell binds to the antigen complex, and the macrophage is stimulated to produce the cytokine Interleukin -1
A cytokine is a protein hormone which regulates normal cell functions, like growth and differentiation.
Every step needs 2 signals to proceed.
IL-1 binds to receptors on the helper T cell, causing helper T-cell to clone itself and produce IL-2.
IL-2 causes lymphocytes to multiply.
These steps are common to both humoral and cell-mediated immunity.
Humoral or Antibody mediated immunity
In order for B cells to become activated and make antibodies against an antigen, two things must happen:
1. B cell must encounter the antigen
2. IL-2 produced by helper T cell must be present.
When both signals are present (the antigen and IL-2). The B cell becomes activated and forms two types of cells: plasma cells and memory cells.
Plasma cells produce large quantities of their specific antibody into the blood.
Memory cells lie in wait for the next infection.
Antibodies
“Y” shaped proteins – gamma globulins
have a variable region that matches a specific antigen (Fab region)
Have a constant region – activates complement (Fc region)
The first antibodies produced are IgM. Pentamers – with ten combining sites – very effective in opsonization and activating complement
Several days later, IgG is produced – single unit antibodies, abundant in serum, cross the placenta, and have the longest half-life.
Cell mediated immunity
A virus is a core of nucleic acid wrapped in a protein.
To reproduce, it must make use of a host cell to replicate the viral nucleic acids and proteins and assemble new viruses.
Infected cells put viral proteins on their membranes.
This antigen is processed by macrophages.
Antibodies can’t get at viruses inside a cell, so we need something different : a Tcytotoxic or Tc Cell.
The Tc encounters the viral antigen with the MHC -1 complex on the infected cell.
Now needs the second stimulus – IL-2 from the helper T cell.
Tc cell clones itself, and makes activated Tc cells and memory cells.
Tc Cells bind to antigens on infected cells and release:
Perforins – punch holes in cell membrane.
Lymphotoxins- activate the cell’s own self-destruct mechanism
Tc Cells are effective against bacteria which are intracellular parasites, viruses, fungi, cancer cells associated with viral infections, and transplanted cells.
Immune Response
The first time you encounter an antigen, you have few B cells or Tc cells against that antigen = primary response
The next time, you have many memory cells, so response is much quicker, so you don’t come down with the disease = secondary response
HIV/AIDS
Human immunodeficiency virus
Attacks helper T cells
Without production of IL-2, there is no second signal, and humoral and cell mediated immunity are shut off.See increase in rare diseases:
TB, Kaposi sarcoma, etc.
Hypersensitivity
“The immune system gone bad.”
Delayed Hypersensitivity
A type of cell mediated immunity.
Td cell – requires usual two signals
Second time antigen is encountered, Td cell produces several cytokines that attract and activate macrophages, resulting in an inflammatory reaction.
Examples: poison ivy (urushiol), TB skin test
Immediate Type Hypersensitivity
• Exposure to certain antigens (allergens) results in the formation of IgE antibodies
• IgE antibodies bind to mast cells by the Fc end.
• When the antigen is encountered again, binding with the antibody causes mast cell to release histamine granules.
May be able to desensitize individual by giving allergen to stimulate IgG antibodies. These tie up antigen before they can bind with IgE.
Acquired immunity
Active = person makes own antibodies
Passive = person receives antibodies from someone else
Natural = “just happens”
Artificial = caused by man (often using a needle)
Natural active acquired immunity:
person comes down with measles
Artificial active acquired immunity:
person is immunized with a vaccine
Artificial passive acquired immunity:
Person receives serum with antibodies
Natural passive acquired immunity:
Baby receives antibodies with mother’s milk - colostrum
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