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Chapter 10: Tissue Response to Injury

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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

6
  • 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

7
  • 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)

8
  • 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

9
  • 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

10
  • 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

11
  • 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
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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)

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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

16
  • 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

17
  • 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

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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

32
  • 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

33
  • 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

35
  • 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
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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

41
  • 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

45
  • 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

46
  • 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

48
  • 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

51
  • 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

53
  • 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

55
  • 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

56
  • 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

57
  • 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

58
  • 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

59
  • 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

60
  • 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

61
  • 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

65
  • 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

66
  • 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

67
  • 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
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