Transcript pain
Chapter 10: Tissue Response to Injury © 2009 McGraw-Hill Higher Education. All rights reserved. The Healing Process • Essential for ATC to possess in depth knowledge of healing process – Understand phases – Time frames physiological changes associated with each phase • Must create a conducive environment for healing • Healing is a continuum © 2009 McGraw-Hill Higher Education. All rights reserved. Figure 10-1 © 2009 McGraw-Hill Higher Education. All rights reserved. Cardinal Signs of Inflammation • • • • • Rubor (redness) Tumor (swelling) Color (heat) Dolor (pain) Functio laesa (loss of function) © 2009 McGraw-Hill Higher Education. All rights reserved. Phases of the Inflammatory Response (3 separate phases) • 1. Inflammatory response phase • 2. Fibroblastic repair phase • 3. Maturation and remodeling phase © 2009 McGraw-Hill Higher Education. All rights reserved. Phase I • Healing begins immediately • Injury results in altered metabolism and liberation of various materials • Initial reaction by leukocytes and phagocytic cells – Goal • • • • Protect Localize Decrease injurious agents Prepare for healing and repair © 2009 McGraw-Hill Higher Education. All rights reserved. • Chemical Mediators – Derived from invading organisms, damaged tissue, plasma enzyme systems and white blood cells (WBC’s) – Histamine (from mast cells) • Causes vasodilatation and changes cell permeability owing to swelling – Leukotrienes & prostaglandins – Impact margination (adherence along cell walls) • Increase permeability locally for fluid and protein passage (diapedisis) • Facilitates exudate formation and neutrophil entrance to injured site – Cytokines • Regulate leukocyte and phagocytic activity © 2009 McGraw-Hill Higher Education. All rights reserved. • Vascular Response – Vasoconstriction and coagulation occur to seal blood vessels and chemical mediators are released • Presses endothelial lining together to produce local anemia – Followed by vasodilation of blood vessel 5-10 minutes later • Initially increases blood flow (transitory) • Vasodilation decreases blood flow, increased blood viscosity resulting in edema (swelling) • WBC’s able to adhere to walls • Initial effusion of blood and plasma lasts 24-36 hours © 2009 McGraw-Hill Higher Education. All rights reserved. Figure 10-3 © 2009 McGraw-Hill Higher Education. All rights reserved. • Clot Formation – Platelets adhere to exposed collagen leading to formation of plug (clot) – Clots obstruct lymphatic fluid drainage and aid in localizing injury – Requires conversion of fibrinogen to fibrin • 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 © 2009 McGraw-Hill Higher Education. All rights reserved. © 2009 McGraw-Hill Higher Education. All rights reserved. • Chronic Inflammation – Occurs when acute inflammatory response does not eliminate injuring agent – Tissue not restored to normal physiologic state – Involves replacement of leukocytes with macrophages, lymphocytes and plasma cells – As inflammation persists necrosis and fibrosis prolong healing process – Granulation and fibrotic tissue continue to develop within highly vascular and loose connective tissue. – Cause for shift from acute to chronic is unknown – Typically associated with overuse, overload, cumulative microtrauma © 2009 McGraw-Hill Higher Education. All rights reserved. Phase II: Fibroblastic Repair Phase • Scar formation through 3 phases – Resolution (little tissue damage and normal restoration) – Restoration (if resolution is delayed) – Regeneration (replacement of tissue by same tissue) • Referred to as fibroplasia – Complaints of pain and tenderness gradually subside during this period © 2009 McGraw-Hill Higher Education. All rights reserved. © 2009 McGraw-Hill Higher Education. All rights reserved. • Scar formation – Capillary buds form – Formation of delicate connective tissue (granulation tissue) • Consists of fibroblasts extracellular matrix • Develop collagen, elastin, ground substance, proteoglycans, glycosaminoglycans – With proliferation of collagen scar tensile strength increases • # of fibroblasts gradually diminishes – Types of collagen • 16 types; body is 80-90% Types I, II, & III – Normal sequence = minimal scarring – Persistent inflammation = extended fibroplasia © 2009 McGraw-Hill Higher Education. All rights reserved. Phase III: Maturation & Remodeling • Long-term process • Realignment of collagen relative to applied tensile forces • Continued breakdown and synthesis of collagen = increased strength • Tissue will gradually assume normal appearance • May require several years to complete © 2009 McGraw-Hill Higher Education. All rights reserved. © 2009 McGraw-Hill Higher Education. All rights reserved. • Role of Progressive Mobilization – Initially must maintain some immobilization in order to allow for initial healing – As healing moves into repair phase controlled activity should be added • Work towards regaining normal flexibility and strength • Protective bracing should also be incorporated – During remodeling aggressive ROM and strength exercises should be incorporated • Facilitates remodeling and realignment – Must be aware of pain and other clinical signs – may be too much too soon © 2009 McGraw-Hill Higher Education. All rights reserved. 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 © 2009 McGraw-Hill Higher Education. All rights reserved. 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 © 2009 McGraw-Hill Higher Education. All rights reserved. Figure 10-4 © 2009 McGraw-Hill Higher Education. All rights reserved. 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 © 2009 McGraw-Hill Higher Education. All rights reserved. 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 © 2009 McGraw-Hill Higher Education. All rights reserved. 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 © 2009 McGraw-Hill Higher Education. All rights reserved. Ligament Healing • Follows similar healing course as other vascular tissues • Proper care will result in acute, repair, and remodeling phases in same time required by other vascular tissues • 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 © 2009 McGraw-Hill Higher Education. All rights reserved. • Factors affecting healing – Surgically repaired ligaments tend to be stronger due to decreased scar formation – With intra-articular tears synovial fluid will dilute hematoma and prevent clotting and spontaneous healing – Exercised ligaments are stronger • Exercise vs. Immobilization – Muscles must be strengthened to reinforce the joint • Increased tension will increase joint stability © 2009 McGraw-Hill Higher Education. All rights reserved. Skeletal Muscle Healing • Initial bleeding followed by proliferation of ground substance and fibroblast • Myoblastic cells form = regeneration of new myofibrils • Collagen will mature and orient along lines of tension • Healing could last 6-8 weeks depending on muscle injured © 2009 McGraw-Hill Higher Education. All rights reserved. Tendon Healing • Requires dense fibrous union of separated ends • Abundance of collagen is required for good tensile strength – Too much = fibrosis – may interfere with gliding • Initially injured tendon will adhere to surrounding tissues (week 2) • Week 3 – tendon will gradually separate • Tissue not strong enough until weeks 4-5 © 2009 McGraw-Hill Higher Education. All rights reserved. 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 © 2009 McGraw-Hill Higher Education. All rights reserved. Figure 10-5 © 2009 McGraw-Hill Higher Education. All rights reserved. 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 patients or those with poor diets may take longer • Certain organic disorders (blood conditions) may slow or inhibit the healing process © 2009 McGraw-Hill Higher Education. All rights reserved. Management Concepts • Drug utilization – Anitprostaglandin agents used to combat inflammation – Non-steroidal anti-inflammatory agents (NSAID’s) – Medications will work to decrease vasodilatation and capillary permeability © 2009 McGraw-Hill Higher Education. All rights reserved. • Therapeutic Modalities – Thermal agents are utilized • Heat facilitates acute inflammation • Cold is utilized to slow inflammatory process – Electrical modalities • Treatment of inflammation • Ultrasound, microwave, electrical stimulation (includes transcutaneous electrical muscle stimulation and electrical muscle stimulation) © 2009 McGraw-Hill Higher Education. All rights reserved. • 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 © 2009 McGraw-Hill Higher Education. All rights reserved. Bone Healing • Follows same three phases of soft tissue healing • Less complex process • Acute fractures have 5 stages – – – – – Hematoma formation Cellular proliferation Callus formation Ossification Remodeling © 2009 McGraw-Hill Higher Education. All rights reserved. © 2009 McGraw-Hill Higher Education. All rights reserved. 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 © 2009 McGraw-Hill Higher Education. All rights reserved. • 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 © 2009 McGraw-Hill Higher Education. All rights reserved. • Hard callus becomes more well-formed as osteoblasts lay down cancellous bone, replacing cartilage • With crystallization of callus remodeling begins • Less than ideal immobilization produces a cartilaginous union instead of a bony union © 2009 McGraw-Hill Higher Education. All rights reserved. • Ossification is complete when bone has been laid down and the excess callus has been resorbed by osteoclasts • Bone continually adapts to applied stresses – Balance between osteoblast and osteoclast activity • Time required is dependent on various factors – Severity and site of fracture – Age and extent of trauma • Time will range from 3-8 weeks © 2009 McGraw-Hill Higher Education. All rights reserved. Acute Fracture Management • Must be appropriately immobilized, until Xrays 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 © 2009 McGraw-Hill Higher Education. All rights reserved. • 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 © 2009 McGraw-Hill Higher Education. All rights reserved. • 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 © 2009 McGraw-Hill Higher Education. All rights reserved. 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 © 2009 McGraw-Hill Higher Education. All rights reserved. • 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 © 2009 McGraw-Hill Higher Education. All rights reserved. Pain • Major indicator of injury • Pain is individual and subjective • Factors involved in pain – Anatomical structures – Physiological reactions – Psychological, social, cultural and cognitive factors © 2009 McGraw-Hill Higher Education. All rights reserved. Pain Categories • • • • Pain sources Fast versus slow pain Acute versus chronic Projected or referred pain © 2009 McGraw-Hill Higher Education. All rights reserved. • 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 © 2009 McGraw-Hill Higher Education. All rights reserved. • 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 International Association for the Study of Pain (IASP) as pain continuing beyond normal healing time © 2009 McGraw-Hill Higher Education. All rights reserved. • 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 © 2009 McGraw-Hill Higher Education. All rights reserved. • 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 – Active points cause obvious complaint – 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 © 2009 McGraw-Hill Higher Education. All rights reserved. • 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 may result (vasomotor control, BP and sweating – Dermatomic pain (irritation of A-delta fibers) is sharp and localized – Projects to the thalamus and cortex directly © 2009 McGraw-Hill Higher Education. All rights reserved. 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 (first-order afferent fibers) • Nociceptor stimulation results in release of substance P © 2009 McGraw-Hill Higher Education. All rights reserved. • Second order afferent fibers – Sensory message from dorsal horn to brain (nociceptive specific) – Receive input from A- beta, delta and C-fibers – Overlapping receptive field – Nociceptive-specific second order afferents receive input only from A-delta and C-fibers – All of these neurons synapse with third order neurons • Transmit information to brain centers via ascending spinal tracts • Information is integrated, interpreted and acted upon © 2009 McGraw-Hill Higher Education. All rights reserved. Facilitators and Inhibitors of Synaptic Transmission • Nervous system is electrochemical in nature • Chemicals called neurotransmitters are released by pre-synaptic cell to transmit message • Two types mediate pain – Endorphins – Seretonin • Neurotransmitters release stimulated by noxious stimuli- resulting in activation of pain inhibition transmission © 2009 McGraw-Hill Higher Education. All rights reserved. Mechanisms of Pain Control © 2009 McGraw-Hill Higher Education. All rights reserved. • Gate Theory – Sensory information from cutaneous receptors enters A-Beta afferents to dorsal horn of spinal cord – Pain simultaneously travels along A-delta and c-fibers – Sensory information overrides pain information, closing gate – Pain message never received – Gate control occurs at the level of the spinal cord © 2009 McGraw-Hill Higher Education. All rights reserved. Gate Control Theory Figure 10-7 © 2009 McGraw-Hill Higher Education. All rights reserved. Central Biasing Theory © 2009 McGraw-Hill Higher Education. All rights reserved. • Central Biasing – Stimulation of descending pathways used to inhibit A-delta and C-fiber pain transmission – Involves release of enkephalin and norepinephrine release in dorsal horn blocking and inhibiting synaptic transmission • Release of B-endorphins – – – – Noxious stimuli can trigger endorphin release Stimulation of pain sensory fibers required Causes release from hypothalamus Strong analgesic effects © 2009 McGraw-Hill Higher Education. All rights reserved. Release of BEndorphins © 2009 McGraw-Hill Higher Education. All rights reserved. • Pain assessment – Self report is the best reflection of pain and discomfort – Utilize multi- and uni-dimensional questionnaires – Assessment techniques include: • Visual analog scales (0-10, marked no pain to severe pain) • Pain charts • McGill Pain questionnaire • Activity pain indicator profiles • Numeric rating scale © 2009 McGraw-Hill Higher Education. All rights reserved. Treating Pain • Modalities – Must have clear rationale for use – Used to relieve pain and control other signs and symptoms of injury/surgery – Must use in conjunction with exercise – Induced analgesia • Introduce thermal agents for pain control • Utilize electrical modalities to reduce pain • TENS, superficial heat/cold, massage used to target Gate Theory • Acupuncture, electrical stimulation, deep massage used to stimulate endorphin release © 2009 McGraw-Hill Higher Education. All rights reserved. • Pharmacological Agents – Oral, injectable medications – Commonly analgesics and anti-inflammatory agents – Important to work with referring physician or pharmacist to ensure patient is taking appropriate medications © 2009 McGraw-Hill Higher Education. All rights reserved. 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 – Physiological and psychological components • Patients, through conditioning are often able to endure pain and block sensations of minor injuries © 2009 McGraw-Hill Higher Education. All rights reserved.