Acute Inflammation PDF

Summary

This document provides an overview of acute inflammation, including its features, mediators, and the key cells involved such as leukocytes and endothelial cells. The document discusses the stages of the inflammatory response and the specific functions of different cell types during these stages.

Full Transcript

Inflammation
PROF. DR. DALYA BASIL
 Introduction
Inflammation is a complex response intended to minimize the
effects of injury or infection, remove the damaged tissue, and
generate new tissue. It accomplishes this by diluting, destroying, or
otherwise neutralizing the harmful agents.
Inflammation is the reaction of vascularized tissues to cell injury or
death, characterized by the elaboration of inflammatory mediators
and the movement of fluid and leukocytes from the vascular system
into the extravascular tissues.
 General Features of Inflammation
Inflammatory conditions are commonly named by adding the suffix -itis to the
affected organ or system. For example, appendicitis refers to inflammation of
the appendix, pericarditis to inflammation of the pericardium, and neuritis to
inflammation of a nerve.
Inflammation can be acute or chronic. Acute inflammation is the adaptive
response that is triggered by noxious stimuli and conditions, such as infection
and tissue injury, and is of relatively short duration, lasting from a few minutes
to several days. It is characterized by the exudation of fluid and plasma proteins
and emigration of leukocytes, predominantly neutrophils.
Chronic inflammation is of a longer duration, lasting for days to years, and is
associated with the proliferation of blood vessels, tissue necrosis, and fibrosis
(scarring).
 Cells of Inflammation
Many cells and tissue components are involved in the inflammatory
process, including the endothelial cells that line blood vessels,
circulating platelets and leukocytes, connective tissue cells (mast
cells, fibroblasts, tissue macrophages), and components of the
extracellular matrix.
The principal leukocytes in acute inflammation are neutrophils,
whereas macrophages, lymphocytes and plasma cells, eosinophils,
and mast cells predominate in chronic inflammation.
 Cells of Inflammation
Endothelial Cells: Endothelial cells comprise the single-cell-thick epithelial lining
of blood vessels. They produce antiplatelet and antithrombotic agents that
maintain vessel patency, as well as vasodilators and vasoconstrictors that
regulate blood flow. Endothelial cells are also key players in the inflammatory
response.
As such, they provide a selective permeability barrier to exogenous (microbial)
and endogenous inflammatory stimuli; regulate leukocyte extravasation, and
release of inflammatory mediators; and regulate immune cell proliferation
through secretion of hematopoietic colony-stimulating factors (CSFs).
 Cells of Inflammation
Platelets or thrombocytes are small membrane-bound disks circulating in the
blood that play an active role in normal hemostasis. Activated platelets also
release a number of potent inflammatory mediators, thereby increasing
vascular permeability and altering the chemotactic, adhesive, and proteolytic
properties of the endothelial cells.
Leukocytes (WBCs) are the major cellular components of the inflammatory
response. They include the granulocytes (neutrophils, eosinophils, and
basophils), which contain specific cytoplasmic granules and a multilobed
nucleus, and the agranulocytes (monocytes/macrophages and lymphocytes),
which lack cytoplasmic granules and have a single nucleus.
 Cells of Inflammation
Neutrophils: Neutrophils are the most numerous leukocytes in the
circulating blood, accounting for 60% to 70%of all white blood cells. These
leukocytes are referred to polymorphonuclear neutrophils (PMNs).
Because of their ability to form pseudopods used in ameboid movement,
neutrophils are highly mobile and are therefore the first cells to appear at
the site of acute inflammation, usually arriving within 90 minutes of injury.
They are capable of engulfing bacteria and other cellular debris through
phagocytosis.
They have oxygen-dependent metabolic pathways that generate toxic
oxygen (e.g., hydrogen peroxide) and nitrogen (e.g., nitric oxide) products
that aid in the destruction of engulfed pathogens.
 Cells of Inflammation
Eosinophils: Eosinophils account for 2% to 3% of circulating leukocytes and are
recruited to tissues similar to neutrophils. Their appearance at the site of
inflammation occurs 2 to 3 hours after the neutrophils. This is, in part, because
of their slower mobility and comparatively slower reaction to chemotactic
stimuli.
The granules of eosinophils, which stain pink with the acid dye eosin, contain a
protein that is highly toxic to large parasitic worms that cannot be phagocytized.
Eosinophils have a longer life span than neutrophils and therefore present in
chronic inflammation.
 Cells of Inflammation
Basophils and Mast Cells: Basophils are account for less than 1% of the
circulating leukocytes, they are important participants in inflammatory reactions
and are most prominent in allergic reactions mediated by immunoglobulin E
(IgE).
Monocyte/Macrophages: Monocytes constitute 3%to 8% of the white blood cell
count. They have a single kidney-shaped nucleus and are the largest of the
circulating leukocytes. The half-life of circulating monocytes is about a day, after
which they begin to migrate to the site of injury and undergo transformation
into larger macrophages, which have a longer half-life and greater phagocytic
ability than do blood monocytes.
 Cells of Inflammation
Lymphocytes and Plasma Cells: Lymphocytes are participate in
immune-mediated inflammation caused by infectious agents as well as
non–immune-mediated inflammation associated with cell injury and death.
Both T and B lymphocytes (T and B cells) migrate into inflammatory sites using
some of the same adhesion molecules and chemokines that recruit neutrophils
and other leukocytes.
Plasma cells develop from activated B lymphocytes and produce antibodies
directed against persistent antigens in the inflammatory site and against altered
tissue components. In some intense chronic inflammatory reactions, the
accumulation of lymphocytes and plasma cells may assume the appearance of
lymphoid organs, such as lymph nodes. This pattern of lymphocyte
accumulation is often seen in the inflamed synovium of persons with
long-standing rheumatoid arthritis.
 Cells of Inflammation
Cell Adhesion Molecules and Leukocyte Recruitment: Several families of cell
adhesion molecules, including selectins, integrins, and the immunoglobulin
superfamily, are involved in leukocyte recruitment and trafficking.
The selectins are a family of three closely related proteins (E-selectin, L-selectin,
P-selectin) that differ in their cellular distribution but all function in adhesion of
leukocytes to endothelial cells. The integrin superfamily consists of 30
structurally similar proteins that promote cell-to-cell and cell–to–extracellular
matrix interactions.
 Cells of Inflammation
The importance of the leukocyte adhesion molecules is
demonstrated in persons with an inherited disorder called leukocyte
adhesion deficiency (LAD) type I, in which deficiency of a member of
the integrin superfamily leads to severe leukocytosis and recurrent
infections. A similar deficiency is seen in individuals with impaired
expression of a member of the selectin superfamily and has been
labeled LAD type 2. There is also evidence that excessive expression
of cell adhesion molecules or their receptors contributes to the
pathogenesis of some chronic inflammatory diseases such as
rheumatoid arthritis.
 Steps of inflammatory response

1- Recognition of injurious agent
2- Recruitment of leukocytes
3- Removal of the agent
4- Regulation of response
5- Resolution
 Acute Inflammation
Acute inflammation is the early (almost immediate) reaction of local
tissues and their blood vessels to injury. It typically occurs before the
adaptive immune response becomes established and is aimed
primarily at removing the injurious agent and limiting the extent of
tissue damage. Acute inflammation can be triggered by a variety of
stimuli, including infections, immune reactions, blunt and
penetrating trauma, physical or chemical agents (e.g., burns,
frost-bite, irradiation, caustic chemicals), and tissue necrosis from
any cause.
 Cardinal Signs of Inflammation
Pain: the inflamed area is likely to be
painful, especially when touched.
Chemicals that stimulate nerve endings
are released, making the area much more
sensitive.
Redness: this is because the capillaries
are filled up with more blood than usual.
Swelling: caused by an accumulation of
fluid.
Heat: as with the reason for the redness,
more blood in the affected area makes it
feel hot to the touch.
Immobility: there may be some loss of
function.
 Vascular and Cellular Stages
Acute inflammation has two stages: the vascular stage, which is
characterized by increased blood flow (vasodilation) and structural
changes (increased vascular permeability) that allow plasma proteins
to leave the circulation, and the cellular stage, which involves the
emigration of leukocytes (mainly neutrophils) from the
microcirculation and their accumulation at the site of injury or
infection.
 Vascular Stage
Vascular Stage: The vascular changes that occur with inflammation involve the
arterioles, capillaries, and venules of the microcirculation. These changes begin
almost immediately after injury and are characterized by vasodilation and
changes in blood flow followed by increased vascular permeability and leakage
of protein-rich fluid into the extravascular tissues. Vasodilation, which is one of
the earliest manifestations of inflammation, follows a transient constriction of
the arterioles, lasting a few seconds.
As a result, the area becomes congested, causing the redness (erythema) and
warmth associated with acute inflammation. Vasodilation is induced by the
action of several mediators, most notably histamine and nitric oxide.
 Vascular Stage
Vasodilation is quickly followed by increased permeability of the microvasculature,
with the outpouring of a protein-rich fluid (exudate) into the extravascular spaces.
The loss of fluid results in an increased concentration of blood constituents (red blood
cells, leukocytes, platelets, and clotting factors), stagnation of flow, and clotting of
blood at the site of injury. This aids in localizing the spread of infectious
microorganisms.
The loss of plasma proteins reduces the intracapillary osmotic pressure and increases
the osmotic pressure of the interstitial fluid, causing fluid to move from the vascular
compartment into the tissues and produce the swelling, pain, and impaired function
that are the cardinal signs of acute inflammation. The exudation of fluid into the tissue
spaces also serves to dilute the offending agent.
The most common mechanism of vascular leakage is elicited by histamine, bradykinin,
leukotrienes, and many other classes of chemical mediators.
 Vascular Stage
Depending on the severity of injury, the vascular changes that occur with
inflammation follow one of three patterns of responses.
1. The first pattern is an immediate transient response, which occurs with minor
injury. It develops rapidly after injury and is usually reversible and of short
duration (15 to 30 minutes). Typically, this type of leakage affects venules 20 to
60 µm in diameter, leaving capillaries and arterioles unaffected.
Although the precise mechanism for restriction of this effect to the venules is
unknown, it may reflect the greater density of receptors in the endothelium of
the venules. It has also been suggested that the later leukocyte events of
inflammation (i.e., adhesion and emigration) also occur predominantly in the
venules of most organs.
 Vascular Stage
2. The second pattern is an immediate sustained response, which
occurs with more serious types of injury and continues for several
days. It affects all levels of the microcirculation (arterioles,
capillaries, and venules) and is usually due to direct damage of the
endothelium by injurious stimuli, such as burns or the products of
bacterial infections. Neutrophils that adhere to the endothelium
may also injure endothelial cells.
 Vascular Stage
3. The third pattern is a delayed hemodynamic response, in which
the increased permeability begins after a delay of 2 to 12 hours, lasts
for several hours or even days, and involves venules as well as
capillaries. A delayed response often accompanies injuries due to
radiation, such as sun-burn. The mechanism of the leakage is
unknown, but it may result from the direct effect of the injurious
agent, leading to delayed endothelial cell damage.
 Cellular Stage
- Leukocytes emigration, accumulation, activation of leukocytes,
enabling them to eliminate the offending agent. Principal leukocytes
are polymorpho nuclear leukocytes (Neutrophils).
- Leukocyte recruitment In this step there is sequence of events:
1) Margination and rolling: as blood flows, circulating cells are swept
by laminar flow against the vessel wall.
Larger leukocytes are pushed out of central axial column and thus
interact with lining endothelial cells (margination).
 Cellular Stage
If endothelial cells are activated by cytokines and mediators--express
adhesion molecules to which leukocytes attach loosely, these cells
bind and detach and thus begin to tumble on endothelial surface, a
process called rolling.
Mediated by selectin family of adhesion molecules, three members
are- E-selectin (on endothelial cells), P- selectin (on platelets and
endothelium), and L selectin (on surface of most leukocytes). All
selectins are induced after stimulation.
 Cellular Stage
2) Adhesion:
Rolling leukocytes sense changes, then initiate firm adhesion which
is mediated by integrins - leukocyte cell surfaces and ligands on
endothelial cells.
Cytokine stimulated increased integrin affinity and increased
expression of integrin ligands provides stable attachment of
leucocytes to endothelial cells at sites of inflammation.
 Cellular Stage
3) Transmigration:
By squeezing between cells at intercellular junctions called diapedesis, mainly in
venules of systematic vasculature. Leucocytes secrete collagenases, pass
through the vascular basement membrane.
4) Chemotaxis:
After extravasating from blood, leukocytes move toward sites of infection or
injury along a chemical gradient by a process called chemotaxis.
Chemotactic substances: such as soluble bacterial products, cytokines and
others.
 Cellular Stage
Leukocytes move by extending pseudopods that anchor to ECM and then pull
the cell in direction of extension.
Neutrophils predominate in inflammatory infiltrate during first 6 to24 hours and
are replaced by monocytes in 24 to 48 hours.

5) Leukocyte activation:
Cellular receptors responses in leukocytes result in defensive function and
leukocyte activation.
Functions:
- Phagocytosis of particles
- Intracellular destruction of phagocytosed microbes and dead cells.
- Liberation of substances that destroy extracellular microbes and dead tissues
- Production of mediators.
Phagocytosis steps:
1) Recognition and attachment
2) Engulfment, with subsequent formation of a phagocytic vacuole
3) Killing and degradation of ingested material.
* Key to the normal function of leukocytes in host defense
is to ensure that they are
recruited and activated only when needed.
Local manifestation of Acute Inflammation

Local manifestation of acute inflammation can be range from mild swelling and
redness to abscess or ulceration.
Charactestically the acute inflammatory response involves the production of
exudates, which vary in terms of fluid type, plasma protein content, and
presence or absence of cells. Exudates can be:
Serous
Hemorrahgic
Fibrinous
Membranous
Purulant
Resolution
THANK YOU