Chapter 10: Tissue Response to Injury

About This Presentation

Title:

Chapter 10: Tissue Response to Injury

Description:

Chapter 10: Tissue Response to Injury Inflammatory Response Acute Inflammation Short onset and duration Change in hemodynamics, production of exudate, granular ... – PowerPoint PPT presentation

Number of Views:604

Avg rating:3.0/5.0

Slides: 69

Provided by: kentschoo8

Category:

more less

Transcript and Presenter's Notes

Title: Chapter 10: Tissue Response to Injury

1
Chapter 10Tissue Response to Injury
2
Inflammatory Response

Acute Inflammation
Short onset and duration
Change in hemodynamics, production of exudate,
granular leukocytes
Chronic Inflammation
Long onset and duration
Presence of non-granular leukocytes and extensive
scar tissue

3
Cardinal Signs of Inflammation

Rubor (redness)
Tumor (swelling)
Color (heat)
Dolor (pain)
Functio laesa (loss of function)

4
Phases of the Inflammatory Response

(3 separate phases)
1. Acute phase
2. Repair phase
3. Remodeling phase

5
Phase I Acute Phase

Initial reaction to an injury occurring 3 hours
to 4 days following injury
Goal
Protect
Localize
Decrease injurious agents
Prepare for healing and repair
Caused by trauma, chemical agents, thermal
extremes, pathogenic organisms

External and internal injury result in tissue
death and cell death
Decreased oxygen to area increases cell death
Phagocytosis will add to cell death due to excess
digestive enzymes
Rest, ice, compression elevation are critical
to limiting cell death

First hour
Vasoconstriction and coagulation occur to seal
blood vessels and chemical mediators are released
Immediately followed by vasodilation or blood
vessel
Second hour
Vasodilation decreases blood flow, increased
blood viscosity resulting in edema (swelling)

Second hour (continued)
Exudate increases (high concentration of RBCs)
due to increased vessel permeability
Permeability changes generally occur in capillary
and venules
Margination occurs causing leukocytes to fill the
area and line endothelial walls
Through diapedesis and chemotaxis leukocytes move
to injured area

Cellular response
Mast cells (connective tissue cells) and
leukocytes (basophils, monocytes, neutrophils)
enter area
Mast cells with heparin and histamine serve as
first line of defense
Basophils provide anticoagulant
Neutrophils and monocytes are responsible for
small and large particles undergoing phagocytosis
- ingestion of debris and bacteria

Cellular mediation
Histamine provided by platelets, mast cells and
basophils to enhance permeability and arterial
dilation
Serotonin provides for vasoconstriction
Bradykinin is a plasma protease that enhance
permeability and causes pain.
Heparin is provided by mast cells and basophils
to prevent coagulation
Leukotrienes and prostaglandins are located in
cell membranes and develop through the
arachadonic acid cascade
Leukotrienes alter permeability
Prostaglandin add and inhibit inflammation

Complimentary systems
Enzymatic proteins that destroy bacteria and
other cells through their impact on cell lysis
Bleeding and exudate
Amount dependent on damage
Initial stage thromboplastin is formed
Second stage Prothrombin is converted to
thrombin due to interaction with thromboplastin
Third stage thrombin changes from soluble
fibrinogen to insoluble fibrin coagulating into a
network localizing the injury

12
(No Transcript)
13
Phase II Repair Phase

Phase will extent from 48 hours to 6 weeks
following cleaning of fibrin clot, erythrocytes,
and debris
Repaired through 3 phases
Resolution (little tissue damage and normal
restoration)
Restoration (if resolution is delayed)
Regeneration (replacement of tissue by same
tissue)

14
(No Transcript)
15

Scar formation
Less viable than normal tissue, may compromise
healing
Firm, inelastic mass devoid of capillary
circulation
Develops from exudate with high protein and
debris levels resulting in granulation tissue
Invaded by fibroblasts and and collagen forming a
dense scar and while normally requiring 3-14
weeks may require 6 months to contract

Primary healing (healing by first intention)
Closely approximated edges with little
granulation tissue production
Secondary healing (heal by secondary intention)
Gapping, tissue loss, and development of
extensive granulation tissue
Common in external lacerations and internal
musculoskeletal injuries

Regeneration
Related to health, nutrition and tissue type
Dependent on levels of
debris (phagocytosis)
endothelial production (hypoxia and macrophages
stimulate capillary buds)
production of fibroblasts (revascularization
allows for enhanced fibroblast activity and
collagen production which is tied to Vitamin C,
lactic acid, and oxygen

18
Phase III Remodeling

Overlaps repair and regeneration
First 3-6 weeks involves laying down of collagen
and strengthening of fibers
3 months to 2 years allowed for enhanced scar
tissue strength
Balance must be maintained between synthesis and
lysis
Take into consideration forces applied and
immobilization/mobilization time frames relative
to tissue and healing time

19
(No Transcript)
20
Chronic Inflammation

Result of failed acute inflammation resolution
within one month termed subacute inflammation
Inflammation lasting months/years termed chronic
Results from repeated microtrauma and overuse
Proliferation of connective tissue and tissue
degeneration

21
Characteristics of Chronic Inflammation

Proliferation of connective tissue and tissue
degeneration
Presence of lymphocytes, plasma cell,
macrophages(monocytes) in contrast to neutrophils
(during acute conditions)
Major chemicals include
Kinins (bradykinin) - responsible for
vasodilation, permeability and pain
Prostaglandin - responsible for vasodilation but
can be inhibited with aspirin and NSAIDs

22
Factors That Impede Healing

Extent of injury
Edema
Hemorrhage
Poor Vascular Supply
Separation of Tissue
Muscle Spasm
Atrophy

Corticosteroids
Keloids and Hypertrophic Scars
Infection
Humidity, Climate, Oxygen Tension
Health, Age, and Nutrition

23
Soft Tissue Healing

Cell structure/function
All organisms composed of cells
Properties of soft tissue derived from structure
and function of cells
Cells consist of nucleus surrounded by cytoplasm
and encapsulated by phospholipid cell membrane
Nucleus contains chromosomes (DNA)
Functional elements of cells (organelles) include
mitochondria, ribosomes, endoplasmic reticulum,
Golgi apparatus centrioles

24
Tissues of the Body

Bone - not classified as soft tissue
4 types of soft tissue
Epithelial tissue
Skin, vessel organ linings
Connective tissue
Tendons, ligaments, cartilage, fat, blood, and
bone
Muscle tissue
Skeletal, smooth, cardiac muscle
Nerve tissue
Brain, spinal cord nerves

25
Soft Tissue Adaptations

Metaplasia - transformation of tissue from one
type to another that is not normal for
that tissue
Dysplasia - abnormal development of tissue
Hyperplasia- excessive proliferation of normal
cells in normal tissue arrangement
Atrophy- a decrease in the size of tissue due to
cell death and re-absorption or
decreased cell proliferation
Hypertrophy - an increase in the size of tissue
without necessarily changing the number
of cells

26
Cartilage Healing

Limited capacity to heal
Little or no direct blood supply
Chrondrocyte and matrix disruption result in
variable healing
Articular cartilage that fails to clot and has no
perichondrium heals very slowly
If area involves subchondral bone (enhanced blood
supply) granulation tissue is present and healing
proceeds normally

27
Ligament Healing

Follows similar healing course as vascular tissue
Proper care will result in acute, repair, and
remodeling phases in same time required by other
vascular tissue
Repair phase will involve random laying down of
collagen which, as scar forms, will mature and
realign in reaction to joint stresses and strain
Full healing may require 12 months

28
Skeletal Muscle Healing

Skeletal muscle cannot undergo mitotic activity
to replace injured cells
New myofibril regeneration is minimal
Healing and repair follow the same course as
other soft tissues developing tensile strength
(Wolffs Law)

29
Nerve Healing

Cannot regenerate after injury
Regeneration can take place within a nerve fiber
Proximity of injury to nerve cell makes
regeneration more difficult
For regeneration, optimal environment is required
Rate of healing occurs at 3-4 mm per day
Injured central nervous system nerves do not heal
as well as peripheral nerves

30
Modifying Soft-Tissue Healing

Varying issues exist for all soft tissues
relative to healing (cartilage, muscle, nerves)
Blood supply and nutrients is necessary for all
healing
Healing in older athletes or those with poor
diets may take longer
Certain organic disorders (blood conditions) may
slow or inhibit the healing process

31
Management Concepts

Drug utilization
Anitprostaglandin agents used to combat
inflammation
Non-steroidal anti-inflammatory agents (NSAIDs)
Medications will work to decrease vasodilatation
and capillary permeability

Therapeutic Modalities
Thermal agents are utilized
Heat stimulates acute inflammation (but works as
a depressant in chronic conditions)
Cold is utilized as an inhibitor
Electrical modalities
Treatment of inflammation
Ultrasound, microwave, electrical stimulation
(includes transcutaneous electrical muscle
stimulation and electrical muscle stimulation

Therapeutic Exercise
Major aim involves pain free movement, full
strength power, and full extensibility of
associated muscles
Immobilization, while sometimes necessary, can
have a negative impact on an injury
Adverse biochemical changes can occur in collagen
Early mobilization (that is controlled) may
enhance healing

34
Fracture Healing

Potential serious bone fractures are part of
athletics
Time is necessary for proper bone union to occur
and is often out of the control of a physician
Conservative treatment will be necessary for
adequate healing to occur

Bone undergoes constant remodeling through
osteocyte activity
Osteocytes cellular component of bone
Osteoblasts are responsible for bone formation
while osteoclasts resorb bone
Cambium (periosteum)
A fibrous covering involved in bone healing
Vascular and very dense
Inner cambium
less vascular and more cellular.
Provides attachments for muscle, ligaments and
tendons

36
Acute Fracture of Bone

Follows same three phases of soft tissue healing
Less complex process
Acute fractures have 5 stages
Hematoma formation
Cellular proliferation
Callus formation
Ossification
Remodeling

37
(No Transcript)
38
Hematoma Formation

Trauma to the periosteum and surrounding soft
tissue occurs due to the initial bone trauma
During the first 48 hours a hematoma within the
medullary cavity and the surrounding tissue
develops
Blood supply is disrupted by clotting vessels and
cellular debris
Dead bone results in an inflammatory response
(vasodilation, exudate cell migration)

39
Cellular Formation

Granulation forms constructing fibrous union
between fractured ends
Capillary buds allow endosteal cells influx from
cambium layer
Cells evolve from fibrous callus to cartilage, to
woven bone
High oxygen tension fibrous tissue
Low oxygen tension cartilage tissue
Bone growth will occur with optimal oxygen
tension and compression

40
Callus Formation

Soft callus is a random network of woven bone
Osteoblasts fill the internal and external
calluses to immobilize the site
Calluses are formed by bone fragments that bridge
the fracture gap
The internal callus creates a rigid
immobilization early

Hard callus formation occurs after 3-4 weeks and
lasts 3-4 months
Hard callus is a gradual connection of bone
filaments to the woven bone
Less than ideal immobilization produces a
cartilagenous union instead of a bony union

42
Ossification

Adequate immobilization and compression will
result in new Haversian systems developing
Haversian canals allow for the laying down of
primary bone
Ossification is complete when bone has been laid
down and the excess callus has been resorbed by
osteoclasts.

43
Remodeling

Occurs following callus resorption and trabecular
bone is laid along lines of stress
Bioelectric stimulation plays a major role in
completing the remodeling process
Osteoblasts are attracted to the electronegative
(concave/compression) side
Osteoclasts are attracted to the electropositive
(convex/tension) side
The process is complete when the original shape
is achieved or the structure can withstand
imposed stresses

44
Acute Fracture Management

Must be appropriately immobilized, until X-rays
reveal the presence of a hard callus
Fractures can limit participation for weeks or
months
A clinician must be certain that the following
areas do not interfere with healing
Poor blood supply
Poor immobilization
Infection

Poor blood supply
Bone may die and union/healing will not occur
(avascular necrosis)
Common sites include
Head of femur, navicular of the wrist, talus, and
isolated bone fragments
Relatively rare in healthy, young athletes except
in navicular of the wrist
Poor immobilization
Result of poor casting allowing for motion
between bone parts
May prevent proper union or result in bony
deformity

Infection
May interfere with normal healing, particularly
with compound fractures
Severe streptococcal and staphylococcal
infections
Modern antibiotics has reduced the risk of
infections
Closed fractures are not immune to infections
within the body or blood
If soft tissue alters bone positioning, surgery
may be required to ensure proper union

47
Healing of Stress Fractures

Result of cyclic forces, axial compression or
tension from muscle pulling
Electrical potential of bone changes relative to
stress (compression, tension, or torsional)
Constant stress axially or through muscle
activity can impact bone resorption, leading to
microfracture

If osteoclastic activity is not in balance with
oesteoblastic activity bone becomes more
susceptible to fractures
To treat stress fractures a balance between
osteoblast and osteoclast activity must be
restored
Early recognition is necessary to prevent
complete cortical fractures
Decreased activity and elimination of factors
causing excess stress will be necessary to allow
for appropriate bone remodeling

49
Pain

Major indicator of injury
Pain is individual and subjective
Factors involved in pain
Anatomical structures
Physiological reactions
Psychological, social, cultural and cognitive
factors

50
Nociception

Pain receptors -free nerve endings sensitive to
extreme mechanical, thermal and chemical energy
Located in meninges, periosteum, skin, teeth, and
some organs
Pain information transmitted to spinal cord via
myelinated C fibers and A delta fibers
Nociceptor stimulation results in release of
substance P

Signal travels along afferent nerves to the
spinal cord
A delta fiber (fast) transmit information to the
thalamus concerning location of pain and
perception of pain being sharp, bright or
stabbing
C fibers (slower conduction velocity) deal with
diffused, dull, aching and unpleasant pain
C fibers signal also passed to limbic cortex
providing emotional component to pain
Nociceptive stimuli is at or close to an
intensity which would result in tissue injury

52
Endogenous Analgesics

Nervous system is electrochemical in nature
Chemicals called neurotransmitters are released
by presynaptic cell
Two types mediate pain
Endorphins
Seretonin
Neurotransmitters release stimulated by noxious
stimuli- resulting in activation of pain
inhibition transmission

Stimulation of periaqueductal gray matter (PGA)
and raphe nucleus of pons and medulla cause
analgesia
Analgesia is the result of opioids release
Morphine like substance manufactured in the PGA
and CNS
Endorphins and enkephalins
Other pain modulators
Norepinephrine (noradrenergic
Seretonin also will serve as neuromodulator

54
Pain Categories

Pain sources
Fast versus slow pain
Acute versus chronic
Projected or referred pain

Pain sources
Cutaneous, deep somatic, visceral and psychogenic
Cutaneous pain is sharp, bright and burning with
fast and slow onset
Deep somatic pain originates in tendons, muscles,
joints, periosteum and blood vessels
Visceral pain begins in organs and is diffused at
first and may become localized
Psychogenic pain is felt by the individual but is
emotional rather than physical

Fast versus Slow Pain
Fast pain localized and carried through A-delta
axons
Slow pain is perceived as aching, throbbing, or
burning (transmitted through C fibers)
Acute versus Chronic Pain
Acute pain is less than six months in duration
Chronic pain last longer than six months
Chronic pain classified by IASP as pain
continuing beyond normal healing time

Projected (Referred) Pain
Pain which occurs away from actual site of
injury/irritation
Unique to each individual and case
May elicit motor and/or sensory response
A-alpha fibers are sensitive to pressure and can
produce paresthesia
Three types of referred pain include myofascial,
sclerotomic, and dermatomic

Myofascial Pain
Trigger points or small hyperirritable areas
within muscle resulting in bombardment of CNS
Acute and chronic pain can be associated with
myofascial points
Often described as fibrositis, myositis, myalgia,
myofasciitis and muscular strain
Two types of trigger points (active and latent)
Active points cause obvious complaint
Latent points are dormant potentially causing
loss of ROM

Trigger points do not follow patterns
Trigger point area referred to as reference zone
which may or may not be proximal to the point of
irritation
Sclerotomic and dermatomic pain
Deep pain with slow or fast characteristics
May originate from sclerotomic, myotomic or
dermatomic nerve irritation/injury
Sclerotomic pain transmitted by C fibers causing
deep aching and poorly localized pain
Can be projected to multiple areas of brain
causing depression, anxiety, fear or anger

Autonomic changes result (vasomotor control, BP
and sweating
Dermatomic pain (irritation of A-delta fibers) is
sharp and localized
Projects to the thalamus and cortex directly

Gate Theory
Area in dorsal horn of spinal cord causes
inhibition of pain impulses ascending to cortex
T-cells will transmit signals to brain
Substantia gelatinosa functions as gate
determining if stimulus sent to T-cells
Pain stimuli exceeding threshold results in pain
perception
Stimulation of large fast nerves can block signal
of small pain fiber input
Rationale for TENS, accupressure/puncture,
thermal agents and chemical skin irritants

62
Central Biasing Theory
63
Release of B-Endorphins
64
Variation of Pain Sensitivity

Hyperesthesia, paresthia or analgesia
Pain modulation
Mixture of physical and psychological factors
Pain management is a challenge to treat
Generally acute pain management in athletic
training setting

Pain assessment
Self report is the best reflection of pain and
discomfort
Assessment techniques include
visual analog scales (0-10, marked no pain to
severe pain)
verbal descriptor scales (marked none, slight,
moderate, and severe)
Pain Treatment
Must break pain-spasm-hypoxia-pain cycle through
treatment
Agents used heat/cold, electrical
stimulation-induced analgesia, pharmacological
agents

Heat/Cold
Heat increases circulation, blood vessel
dilation, reduces nociception and ischemia caused
by muscle spasm
Cold applied for vasoconstriction and prevention
of extravasation of blood into tissue
Pain reduced through decrease in swelling and
spasm
Induced analgesia
Utilize electrical modalities to reduce pain
TENS and acupuncture commonly used to target Gate
Theory

Pharmacological Agents
Oral, injectable medications
Commonly analgesics and anti-inflammatory agents

68
Psychological Aspects of Pain

Pain can be subjective and psychological
Pain thresholds vary per individual
Pain is often worse at night due to solitude and
absence of external distractions
Personality differences can also have an impact
A number of theories relative to pain exist and
it physiological and psychological components
Athlete, through conditioning are often able to
endure pain and block sensations of minor injuries

Write a Comment

User Comments (0)