Upload
veronica-nichols
View
218
Download
4
Tags:
Embed Size (px)
Citation preview
Biology of Disease CH0576
The Inflammatory Response I
Dr Stephen Todryk
Inflammation:
•Painful•Unsightly•Essential process•Response to a foreign object or to damage
Major cells
Neutrophil50-70%(5000/mm3)
Eosinophil1-3%
Basophil<1%
polymorphonuclear
Major cells
Monocyte1-6%
macrophage
mast cell (tissue)
platelets
Inflammation - Introduction
• Inflammation is the local physiological tissue response to injury, cell death, infection and is classified according to duration
Acute inflammation:- Initial and often transient response. Short-lived.
Chronic Inflammation:- Subsequent and often prolonged response that follows acute stages.
Associated with / cause:cancer, atherosclerosis, asthma, psoriasis, arthritis
Inflammation - Introduction
• Inflammation is a reaction to trauma e.g.the invasion of microorganisms through the skin or through the epithelial layers of the respiratory, digestive, or urinary system
• characterized by four signs:
Acute Inflammation
� The ‘cardinal signs’ of inflammation were first described some 2000 years ago by the Roman Physician Celcus.
•Calor = Heat
•Rubor = Redness
•Tumor = Swelling
•Dolor = Pain
These normally give rise to a fifth: loss of function
Table 4. Cardinal Signs
English Greek/Latin Caused ByRedness Rubor HyperemiaWarmth Calor Hyperemia
Swelling TumorIncreased permeability
Pain Dolor Low pHLoss of function
Functio laesa Pain, swelling
Inflammation
•Usually localised, but can get whole body effects
•Multiple injuries•Systemic infection
•Multiple organ failure
Causes of Acute Inflammation
The causes of acute inflammation are
1. Physical agents (physical trauma, radiation, burns).
2. Chemical agents (corrosive chemicals).
3. Immunological mechanisms (hypersensitivity reactions - certain allergies).
4. Tissue necrosis (death of tissue from lack of nutrients or oxygen due to lack of blood flow – INFARCTION).
5. Microbial Infections (viruses, bacteria, fungi and parasites)
Acute Bronchitis
Medlineplus, National Library of Medicine, U.S.A.
Inflammatory Response
• Inflammatory response The body's reaction to trauma
• includes an increase in blood flow to the affected area (controlled by “chemicals”)
• release of “chemicals” to attract white blood cells (Neutrophils)
• an increased flow of plasma • the arrival of monocytes to clean up the
debris.
Functions of Acute Inflammation
The acute inflammatory response is relatively non-specific (primitive program; innate) and has three main functions:
1. Damaged tissue is broken down and dead cells and debris are removed from the site.
2. If an infective agent is present (bacteria) it can be destroyed and eliminated
3. Allows the immune response (cells and molecules)access to the damaged site. Focusing the immuneresponse.
Effects of Acute Inflammation
BENEFICIAL EFFECTS:
1. Dilutes toxins
2. Allows entry of antibodies to site of inflammation
3. Delivers nutrients and oxygen to site of inflammation (essential for cells such as neutrophils which have a high metabolic activity)
• BENEFICIAL EFFECTS :
• 4. Fibrin formation (Exuded fibrinogen, clot, may impede the movement of microorganisms, limitingtheir spread; facilitating phagocytosis)
• 5. Stimulation of the immune response (Drainage of fluid exudate to the lymphatics allows antigens to reach the local lymph nodes)
• 6. Promotes repair and healing
Effects of Acute Inflammation
Acute Inflammation
Effects of Acute Inflammation
HARMFUL EFFECTS:
1. Release of lysosomal enzymes by inflammatory cells can digest normal tissues (collagenases and proteases) as well as damaged tissue
2. Swelling of acutely inflamed tissue may be harmful e.g. Swelling of the epiglottis due to Haemophilus
influenzae infection may obstruct airway and causedeath. In Acute Meningitis inflammatory swelling is especially serious as it may impair blood flow to brain
3. Inappropriate inflammatory responses. (Type I hypersensitivity reactions to harmless antigen
- allergy)
Inflammatory Response
The inflammatory response consists of:
a) Vasodilation - causing increased blood flow (hyperaemia)
b) Increased vascular permeability - causing vessels to become leaky
c) Leakage of plasma from blood to tissues (fluid exudate)
d) Emigration of inflammatory cells (mostly neutrophils) from blood to tissues(cellular exudate)
Steps in the Inflammatory Response
Steps involved in the acute inflammatory response
a) Small blood vessels adjacent to the areaof tissue damage become dilated with increased blood flow which then slows down
b) Endothelial cells swell and partially retract so they no longer form a completely intact internal lining.
Steps in Inflammatory Response
c) The vessels become leaky, allowing the passage of water, salts and some small plasma proteins
into the damaged area (EXUDATION)
d) Circulating neutrophils adhere to swollenendothelial cells (MARGINATION) then migrate through the vessel basement membrane(EMIGRATION) passing into area of tissue damage
e) Small numbers of macrophages and lymphocytes migrate in a similar way as do neutrophils.
Chemical Mediators in Acute Inflammation
Vascular response to injury is mediated by a wide range of soluble mediators generated at thesite of tissue injury PHASE CHEMICAL MEDIATORVascular Dilation Histamine, Prostoglandins, Complement components: C3a and C5a.
Increased vascular Histamine, Kinins, Prostaglandins.permeability
Emigration of C5a, leukotrienes, IL-8, cationic proteinsleukocytes of neutrophils.
Fluid Movement Across Capillaries
• Under physiological conditions there is a continuous movement of fluid between capillaries and extravascular tissues.• The movement of fluid is dependent upon differential pressure gradients across the vessel wall.• The high colloid osmotic pressure inside the vessel (due to plasma proteins) favours fluid return to the vessel.• Normally there is fluid movement OUT of capillary at arteriolar end and INTO it at the venous end.
Non-inflammatory Oedema
• In certain circumstances fluid can move into the tissues at a greater rate than it can be removed.
• This results in OEDEMA e.g. pulmonary oedema due to left ventricular cardiac failure.
Non-inflammatory Oedema
• Obstruction to lymphatic drainage from a particular site can also result in oedema – LYMPHODEMA – following surgery, in tumour metastasis or elephantiasis due to parasitic worm infection e.g. filiarisis
Inflammatory Oedema
• Oedema which occurs due to increased vascular permeability following tisssue injury.
• Various vasoactive mediators originating from plasma and cellular sources, also from injured cells, are generated at the site of tissue injury.
• Their main site of action is at the post capillary venule
Inflammatory Oedema
• The mediators induce changes in endothelial cell wall of vessels, altering its permeability
• Binding of vasoactive mediators to their specific receptors on endothelial cells results in endothelial cell retraction and formation of gaps
• The integrity of the endothelial cell layer is lost.
• Endothelial cell retraction and gap formation are reversible processes
Inflammatory Oedema
Experimental studies have shown three patterns of oedema which occur at differenttimes following injury:
1. IMMEDATE - This is transient and lasts for 30-60 minutes after injury and is mediated by HISTAMINE acting on endothelium.
Inflammatory Oedema
• 2. DELAYED - starts 2-3 hours after injury and lasts for up to 8 hours. This is mediated by factors synthesised by local cells e.g. BRADYKININ, Complement breakdown products and factors released by dead neutrophils
• 3. An immediate response that is prolonged for over 24 hours and is seen if there has been severe direct injury to the endothelium e.g. by burns or caustic chemicals.
Mediators of Increased VascularPermeability
• The primary sources of these mediators are either plasma or various cells types e.g. Platelets, Tissue mast cells, Basophils, Polymorphonuclear Leucocytes (neutrophils), Endothelial cells, Monocytes and macrophages and injured cells themselves
Mediators of Increased VascularPermeability
• Plasma derived factors are mostly precursor
proteins or zymogens, activated by proteolytic
enzymes. • Once activated they generally have
a short half life. • They are rapidly inactivated
in tissues by a variety of systems.
Cellular Mediators
The mediators of increased vascular permeabilityreleased by cells are either preformed and storedwithin the cell as cytoplasmic granules, e.g. HISTAMINE, SERATONIN, LYSOSOMAL HYDROLASES or are derived from the metabolism of phospholipidsand arachidonic acid e.g. PROSTAGLANDINS, PLATELET ACTIVATING FACTOR (PAF), LEUKOTRIENES and THROMBOXANES
Outcomes of Acute Inflammation
• Foreign and/or infectious agents removed and debris
• Damaged area regrows and trauma resolved
• Scar (collagenous) formed
• Formation of abscess
• Chronic inflammation
Time for a break…….
Glossary
• Post capillary venule: Arteries bringing blood from heart divide into smaller arterioles which then divide into capillaries when they enter tissue. Capillaries exchange substances with tissue then reunite into small veins – venules
• zymogen (or proenzyme): The inactive or nearly inactive precursor of an enzyme, converted into an active enzyme by proteolysis
http://www.whfreeman.com/kuby/content/anm/kb01an01.htm