Transcript 442 pain
Pain Management Dr. Lamya Alnaim Pain is a Very Significant Problem Pain has negative effects on sleep, work, enjoyment of activities, sexual function, and personal interactions Multiple studies show pain of all types is under treated Pain is a Very Significant Problem Good medications and treatments are available Barriers (patient and caregiver) include lack of education, attitudes (myths, cultural differences), and regulatory/legal issues Definition: Acute Pain An unpleasant sensory and emotional reaction/sensation secondary to tissue damage Arises from injury, trauma, spasm, or disease of the skin, muscles, somatic structure or viscera. Corresponds to the degree of injury Self limiting- limited duration Definition: Acute Pain Serves a purpose By inducing an organism to withdraw from or avoid a noxious stimulus. Responds to conventional therapy. Decreases in intensity as the damaged area heals and tissue repair takes place. Definition of Chronic Pain Any pain that Persists beyond the expected time after a physical or emotional injury Subjective complaints are magnified Pain is out of proportion to clinical signs Is accompanied by severe psycho-social issues Responds poorly to conventional therapy Persistent Pain SUFFERING DEPRESSION LOSS OF FUNCTION DRUG ABUSE FINANCIAL LOSS DOMESTIC DISRUPTION PAIN Who Gets Persistent Pain ? Systemic disease Diabetes mellitus hypothyroidism HIV/AIDS Hepatitis C Malignancy Neurological disease….ALS, MS Rheumatoid related syndromes Obesity Psychiatric co-morbidity ACUTE PAIN Meaningful, linear, reversible Well defined, recent onset, clear definable cause Observable responses Readily responds to analgesics Usually nociceptive in origin CHRONIC PAIN Meaningless, cyclical, irreversible Persists over time Adaptation Less amenable to analgesics alone Multiple etiologic components Cancer Pain 20-50 % at time of diagnosis Incidence varies with tumor type 55-95% with advanced disease 50-70% report pain of moderate to severe intensity 30% report excruciating pain Pain Experience in Ambulatory Cancer Patient Population Disease Pain 71% Pain due to Disease 83% Worst Pain >5 60% Negative PMI 43% Breast GI 61% 91% 58% 41% GYN 55% 80% 71% 54% GU 64% 84% 66% 38% Lymphoma 53% 66% 63% 63% Lung 74% 85% 63% 34% Other 74% 85% 64% 42% Pain Classification Schemes 1-Neurophysiologic: Nociceptive (somatic, visceral) Neuropathic 2-Duration: acute vs. chronic 3-Temporal pattern: continuous intermittent incident Breakthrough End-of-dose failure Pain Classification Schemes 4-Severity 5-Specific cancer pain syndromes (etiology): Tumor infiltration of bone, nerve, viscera. Treatment related. Types of Persistent Pain Nociceptive Musculo skeletal Joint Ligamentous Visceral Neuropathic Central Somatic Sympathetic Psychogenic Mixed Types of Pain: Nociceptive vs. Neuropathic Nociceptive mediated by normal nervous system: Somatic - dull, aching, well-localized. Bone metastasis, invasion of soft tissue Visceral - vague distribution, referred. Bowel obstruction, carcinomatosis, pleural effusion Types of Pain: Nociceptive vs. Neuropathic Neuropathic mediated by damaged nervous system: Localized to an area of sensory abnormality Pain in response to non-painful stimuli Pain in the absence of ongoing tissue damage Painful peripheral neuropathy, post mastectomy pain, brachial plexopathy Behavioral Physiologic Manifestations of Pain Acute Increased BP, P, R. Dilated pupils. Sweating. Focuses on pain Reports pain Crying, moaning restless Grimace Chronic Normal Normal Dry skin Easy distraction No report Quiet, sleep, rest Blank or normal facial expression Key Principles in Assessment Pain is a multidimensional, subjective, and uniquely personal experience Pain is what ever the person says it is, occurring whenever the person says it does Reliance on observable physiologic and behavioral manifestations in order to verify existence and severity of pain is inadequate Goals of Assessment Estimate severity of pain (0-10 scale, visual analog scale) Form clinical impression regarding etiology Determine need for additional diagnostic testing Formulate therapeutic recommendations which take into account the patient’s medical and psychosocial status Symptom Assessment PQRST P: Palliative or precipitating factors Q: Quality R: Region or Radiation S: Subjective Description of severity T: Temporal factors Symptom Assessment Site Onset Temporal pattern Quality Relieving/Provoking factors Associated signs/ symptoms Impact of function and QOL. Impact on psychological state. Response to prior therapy. Treatment preferences. Pain Assessment Characterize the pain Location of the pain Past Medication and Current Medication Pain Intensity Pain Intensity Rating Scales • Visual Analogue Scale (VAS) No pain ----------------------------------- Worst pain • Numerical Rating Scale 0 ------------------------------------------- 10 Worst pain imaginable No pain • Categorical Scale None (0) Mild (1 – 4) Moderate (5 – 6) Severe (7 – 10) Guidelines in Pain Therapy Assess the pain frequently Pain assessment must be dynamic and not static Use around the clock therapy (ATC) Treat and assess breakthrough pain aggressively Where possible use oral route Consider age, previous drug usage, hepatorenal function Monitor for abuse Monitor and treat side effects Treatment Goals Decrease Intensity and duration of pain Decrease conversion from acute to chronic Decrease suffering and disability Decrease psychological and socioeconomic of sequel of untreated pain. Treatment Goals Optimize drug therapy Improve quality of life and optimize ability to perform activities of daily living Minimize adverse effects of therapy Minimize inappropriate use Overall Treatment Strategies Analgesic Physical and adjuvant medications therapies Psychological Anesthetic interventions and neurolytic procedures Mechanistic Approach To Therapy Modify expression..anxiolytics Decrease inflammatory response. NSAIDS, local anesthetics, steroids Increase inhibition.. Amitryptiline venlafaxine, clonidine Prevent centralization Decrease conduction gabapentin, carbamazepine,local anesthetics, opioids cox2,opioids, ketamine,alpha 2 agonists. WHO Three-Step Analgesic Ladder Step 1: Mild pain Non-opioid, + Adjuvant Step 2: Mild to moderate pain Opioid for mild to moderate pain, + nonopioid, + Adjuvant Step 3: Moderate to Severe Pain Opioid for moderate to severe pain , + non-opioid, + Adjuvant. WHO Analgesic “Ladder” for Cancer Pain Freedom from Pain Proposed 4th Step Intrathecal Opioid Delivery Pain persisting or increasing Step 3 Opioid for moderate to severe pain ± Nonopioid ± Adjuvant WHO 3-Step Analgesic Ladder Pain persisting or increasing Step 2 Opioid for mild to moderate pain ± Nonopioid ± Adjuvant Pain persisting or increasing Step 1 ± Nonopioid ± Adjuvant Pain Algorithm for Medication Selection in Various Pain Syndromes Neuropathic pain Shingles, DM, HIV, antiretroviral drugs, Vinca Alkaloids. Sharp, lancinating, burning, hot, electrical, shocking, paresthesia Myofascial pain From muscle, bone, joints, or connective tissue Muscle pain from exertion→NSAIDs myositis → injection of local anasthetic Inflammatory muscle disease → low dose steroids Sickle Cell Disease Acute infarctions and necrosis of organs Mild to moderate pain: NSAIDs, acetaminophen Sever acute pain: opiates Cancer Pain Cancer: Tumor expansion, nerve compression, infiltration by tumor, malignant obstruction, infection of malignant ulcers. Treatment: radiation → mucositis pain Principles of Analgesia for cancerRelated pain Follow WHO Ladder ATC dosing for continuous pain Rescue dosing for intermittent pain Oral route unless contraindicated No PRN It is reactive not preventive Requires larger doses to reestablish control which may lead to side effects Principles of Analgesia for cancerRelated pain ATC dosing Small fixed doses on a schedule to prevent pain Rescue dosing Fixed doses on a flexible schedule Analgesia is administered in response to pain or to prevent predictable pain Key to success of pain management Similar to NG in angina Use immediate release opioid or NSAIDs Calculating Rescue dosing 1. 25-50% of the 4hrly ATC 2. 3. If ATC is 60 mg MS q 4 hrs, rescue can be 15 mg 2-5% of the 24 hr ATC dose Based on response, 50% relief from 2 mg morphine →4 mg should provide ≈ 100% relief All rescue should be prescribed q 4 hrs Titrating dosage If 3 or more rescue doses in 24 hr ↑ based upon total opioid dose ( ATC+ rescue) taken in the previous 24 hrs. ↑ both the ATC and breakthrough Calculate Increase by the following guidelines > 7 , ↑ dose by 50-100% Pain 4-7, ↑ dose by 25-50% Pain < 4, ↑ dose by 25% Pain When patient uses < 2 rescue, sustained release opioid should be started Mild-Moderate Pain NSAIDs Ceiling dose. Contraindications. Side effects Effective in bone metastasis because block PGE2 Reduce stiffness, swelling and tenderness ± Weak opioid Codeine, hydrocodone, propoxyphene. Limitation of combination formulations. Mild-Moderate Pain + Adjuvant Corticosteroids: inhibit PGE2 in bone Mets bisphosphonates Moderate to Severe Pain Strong Opioid Morphine, hydromorphone, fentanyl, methadone, oxycodone, levodromoran. Moderate to Severe Pain + Adjuvant NSAIDs or Corticosteroids 1. No data to support analgesic superiority among NSAIDs. Selection based on patient report, side effects, chemical class (ibuprofen, naprosyn) 2. Gastric protection: PPIs 3. If nerve compression use dexamethasone Opioids Morphine Sulphate Hydromorphone (Dilaudid) Strong Opioids Demerol Fentanyl Methadone Buprenorphine Partial agonists Pentazocine Oxycodone (Roxycodone, Tylox, Percocet) Weak Hydrocodone (vicodin, lortab, Norco) Propxyphene ( Darvon, Darvocet) opioids Codeine Opioids Three Classes: Phenanthrene: morphine, hydromophine, levorphanol Phenylpiperidines: mepridine,fentanyl Diphenylheptanes:methadone, prpoxyphene Opioids Opioid Agonist: bind w/ opioid receptor site in PNS & CNS = pain relief No Ceiling Titrate to pain relief or side effects Opioid Antagonist: blocks relief. Naloxone Opioid Agonist-antagonist: + pain relief. Stadol, Nubain, Talwin (not recommended) Opioids No rationale for combining two opioids, use same agent for ATC and rescue pain. Routes of Administration Intravenous PRN nurse administered PCA Oral PRN Around the clock Transdermal Rectal Transmucosal……oral or nasal Neuraxial Intrathecal epidural Potent Opiates: Morphine, Hydromorphone. µ-receptors, κ-receptors Treat acute, chronic, sever, or terminal malignant pain Orally, rectally, IV Infusion, epidural , intrathecal Immediate release analgesic effect 4 hrs Morphine, Hydromorphone. Doses according to Prior exposure Pain severity Hepatic, renal function Route of administration Oral: parental, 5:1 Morphine Opioid of choice Available in multiple routes and formulations Extensive clinical experience in dosing, route change and side effects. Meperidine…….Demerol Used for traumatic and postoperative pain 1/10 potency of morphine Oral or parenteral Short acting Toxic metabolites: nomeperidine Can accumulate in renal dysfunction and cause CNS stimulation and seizures Metabolites with long half life >12 hrs High addiction potential Expensive Methadone Equivalent potency to morphine Orally, IV, rectally, epidurally/intrathecally Long acting adjust dose q 5-7 days Lower addiction and tolerance potential Cheap No active or toxic metabolites 8-12 hour analgesic action ( give Q8-12 hrs) Longer intervals in hepatic failure Methadone CNS depression lasts for 36 hrs after overdose Needs CIVI Naloxone for reversing effect. No renal excretion Dependence on hepatic function (p-450) Watch for drug-drug interaction Fentanyl >100 potent than morphine IV, intraspinally as preoperative anesthetic agent Rapid onset, short duration of action Transdermal patch: Consistent dosing Oral lollipop The Fentanyl Patch Indications for use Severe nausea and vomiting Unable to swallow Children Patients with poor compliance Concern of drug diversion Beware Opioid naïve Febrile patient Elderly Drug abuser The Fentanyl Patch disadvantages Delay in onset of analgesia Residual activity after the patch is removed 25,50,75,100 mcg Duration 72hrs Steady state requires 24 hrs, use supplemental short acting to cover initial period. Weak Opioids Codiene, oxycodone, propoxyphene For mild to moderate pain Oxycodone Analgesic effect 4 hrs High bioavailability compared to MSO4 No toxic metabolites Less tolerance compared to MSO4 Higher incidence of euphoria Expensive Tramadol Activity against opioid and serotonergic and noradrenergeric pathways in CNS. Moderate to sever pain Advantages Lower abuse liability Lower risk of respiratory depression Disadvantages Dizziness, dry mouth, sedation, constipation. Use lower doses in elderly Oral Opioid Comparison Oxycodone • Long track record • No toxic metabolites • Formulations –Immediate release –Controlled release Hydromorphone • Long track record • No toxic metabolites • Formulations –Immediate release –Sustained release Hydrocodone • Long track record • No toxic metabolites • Formulations – Immediate release – Combinations Acetaminophen o Ibuprofen Equianalgesic Dosing MEDICATION IV PO RATIO DURATION Morphine 10 30 3 4-5 Hydromorphone 1.5 7.5 5 3-6 Oxycodone Meperidine 15 75 Hydrocodone Codeine 300 3-5 4 200 130 200 2-4 4-6 .75 3-5 Dose Conversion Equianalgesic dose of current opioid 24 hrs dose current opioid Equianalgesic dose of desired opioid = 24 hrs dose current opioid Drug Delivery No evidence that other routes are superior or have less SE. Choice of route depends on pragmatic consideration e.g. inability to swallow Can only be done safely with knowledge of equianalgesic dosing. Oral Route of choice Simple, noninvasive Reasons for failure: inadequate dose, parenteral to oral conversion made too quickly, dosing intervals too long Formulation and dose dependent upon pattern of pain and severity Long Acting Combined with Short Acting for Chronic Pain Sublingual, buccal Simple, noninvasive Unable to tolerate oral dosing, unable to swallow rapid onset, drug not subject to first-pass effect fentanyl Intravenous Most efficient for rapid titration, dose finding, immediate analgesic effect. Bolus, continuous, PCA. Steady state better maintained with CI. Full effects of increase CI will not be felt until steady state or approximately 5-6 half-lives. Therefore with IV Morphine 12-18 hours. Morphine, hydromorphone, fentanyl, methadone Rectal Morphine, hydromorphone Conversion from oral at 1:1 ratio Sustained release tablets of morphine can be used by this route. Subcutaneous Morphine, hydromorphone Equivalent to IV in efficacy and side effects Conversion to Oral Calculate total daily requirement with PCA Convert to IV morphine Convert to Oral morphine Convert to alternate opioid 75 % as ATC 25% as rescue Prior to Oral Conversion Patient able to tolerate oral fluids Oral therapy started prior to removal of PCA Pain control predictable and stabilized IV to oral conversion calculated Side effects under control Example of Conversion Total morphine for 24 hours on PCA= 60mg Want to convert to Oxycodone. 60 mgm of MS IV( x 3) = 180 mgm oral. To convert to oxycodone x by 1.5 = 120 mg oxycodone 75% as ATC = 90 mg = 40 mg Q 12 , but factor in 50% less for ICT = 20 mg q 12 hourly 25% as rescue = 30 mg or 5 mg Q 4-6 hourly PRN Conversion Chart for Starting Dose of Transdermal Fentanyl Fixed-combination short-acting opioids (6/day): – Lorcet 5 mg/500 mg – Lortab 5 mg/500 mg – Percocet 5 mg/325 mg – Percodan 5 mg/325 mg – Tylenol + Codeine 30 mg/325 mg – Tylox 5 mg/500 mg – Vicodin 5 mg/500 mg One 25 mcg/h transdermal fentanyl patch/3 days (72 hours) Long-acting opioids(2/day): – OxyContin 20 mg – MS Contin 30 mg Multiple patches may be used for doses exceeding 100 mcg/h. Doses up to 6oo mcg/h have been evaluated in clinical trials. Renal Failure Methadone Dilaudid Oxycodone Hydrocodone Morphine Fentanyl Demerol NEUROTOXICITY SEDATION TOLERANCE Liver Failure Methadone Dilaudid Oxycodone Hydrocodone Morphine Fentanyl Demerol All pretty much OK, but halve dose Side effects of opioids Constipation Sedation Mental clouding Respiratory depression Nausea and vomiting Orthostatic hypotension Urinary retention Pruritus Myoclonus Constipation Decreased gastric, pancreatic, biliary secretions. Decrease motility Delayed passage Tolerance does not develop Dose dependent Preventative approach Bulk and stimulant laxatives Sedation Common with start, increase, change drug, pain relief in sleep deprived. Tolerance to sedative effects 2-7 days. Other causes: sedatives, sepsis, metabolic imbalances, hypoxia. Strategies: change dose, frequency, type of opioid Stimulants: Caffeine, dextroamphetamines, methylphenidate Respiratory Depression Direct action on brain Rapid tolerance stem respiration Short acting receptors; decreased Goal: gradual reversal responsiveness to without analgesic CO2 levels withdrawal Pain is physiologic Naloxone 0.4 antagonist mg/10cc; 0.5 cc q 2-3 Risk factors mins Nausea - Vomiting Common with start or increase dose Tolerance within 2-3 days Rule out other causes Treatment: treat constipation, use antiemetics, change opioid Withdrawal Physical dependence Causes: abrupt discontinuation, rapid dose reduction, antagonist, agonistantagonist Onset dependent upon elimination halflife Signs and symptoms 25% of daily dose Dependence Physical dependence Psychological dependence Pseudo addiction Definitions Physical Dependence: involuntary, adaptation, withdrawal with abrupt reduction or discontinuation Psychological Dependence (addiction): compulsive use despite harm, for effects other than pain relief Definitions Tolerance: decreased effect over time (not universal) Pseudo addiction: behavioral manifestations of inadequate treatment Iatrogenic addiction: psychological dependence as consequence of exposure (RARE < 0.1%) Non Opioid Analgesics NSAIDS Acetominophen NSAIDS Mechanism of action - Inhibition of prostaglandin synthesis - Synergism with opioid analgesics Mild to moderate pain Different side effect profile from opioids No tolerance or dependence Ceiling effect Limited routes NSAIDS Pain from injury, surgery, trauma, arthritis, or cancer Very effective for bone pain Predominant effect on PNS→synergistic All are equipotent Patient response varies The Arachidonic Acid Cascade and COX-1 and COX-2 Inhibition Arachidonic acid COX-1 X Body Homeostasis • Gastric integrity • Renal function • Platelet function COX-2 Traditional NSAID X X Inflammation Pain Selective COX-2 Inhibitor The COX 2 Inhibitors Rofecoxib 25-50 mg daily (Vioxx) →W Celecoxib 100-200mg daily (Celebrex) Valdecoxib 10-20 mg daily (Bextra) →W Etrocoxib Paracoxib (iv use) The COX 2 Inhibitors Minimal effect on Gastric integrity Renal function Platelet function Potent inhibition of PGI2 →↑ risk if CV events (MI) Contraindications to COX2 I Previous side effects with COX2 inhibitors Allergy to sulpha drugs History of previous GI bleed pregnancy History of perforated gastric ulcer Esophageal varices Bronchospastic disease Renal dysfunction Coronary artery disease needing aspirin Congestive heart failure Acetaminophen Same analgesic potency as ASA No neuropsychological and little GI SE Orally, or rectally For musculoskeletal or visceral pain Can be used in 3 ways ATC 1g q 4 hrs as 5 doses in 24 hrs 2. As rescue with ATC opioid 1g q4 PRN 3. As an adjuvant analgesic 1. Adjuvant Medications Enhance analgesic effect of opioids Treat concurrent symptoms Provide independent analgesia Antidepressants Neuroleptics Anticonvulsants Local anesthetics Antispasmodics Muscle relaxants Psychostimulants Corticosteroids NMDA receptor antagonism Anticholinergics Bisphosphonates Antidepressant TCA, MAOIs, Clinical effects Improve mood Improve sleep Anoxiolytics Decreased pain perception TCA more easier to use Antidepressant TCA inhibit reuptake of serotonin and norepinephrine Serotogergic processes are part of endogenous pain inhibitory mechanisms TCA have analgesic properties related to ability to increase pain tolerance Faster onset than antidepressant effect Have local anesthetic properties Antidepressant Improve sleep disturbances and depression associated with chronic pain. 1-3 weeks for effect Amitriptyline most commonly used for painful conditions 50-150 mg/day Anticholinergic side effects TCA: Adverse Effects Commonly reported AEs Fewest (generally anticholinergic): AEs blurred vision cognitive changes constipation dry mouth orthostatic hypotension sedation sexual dysfunction Most tachycardia AEs urinary retention Desipramine Nortriptyline Imipramine Doxepin Amitriptyline Caveats With the Antidepressants •Start at lowest dose available •Escalate slowly…every 10 -14 days •Slow weaning, over a week •Beware of drug interactions •Check for •Glaucoma •Prostatic obstruction •Heart block Drug Interactions With Antidepressants Coumadin Alcohol ( cold medications) Appetite suppressants Quinolone antibiotics Antihistamines Tramadol Anti epileptics Bronchodilators Neuroleptics Fluphenazine, methotrimeprazine For mild to moderate pain Improve sleep Similar analgesic effects to morphine without addictive properties or respiratory depression Side effects High sedative and anticholinergic effects Extrapyramidal Anticonvulsants Carbamazapine (Tegretol) Gabapentin (Neurontin) Oxcarbezapine (Trileptal) Topiramate ( Topramax) Zonisamide ( Zonergan) Levetiracetam( Keppra) Lamotragine ( Lamictal) Valproate ( Depakote) Anticonvulsants Carbamazapine and valproate for lancinating, burning pain. (neuropathic) Neural invasion by cancerous tumor Surgical scarring Trigeminal neuralgia For opioid induced myoclonus dosing start at 100-200mg/d in cancer pain Plasma levels need to be monitored Anticonvulsants Carbamazapine and valproate Side effects Bone marrow suppression Ataxia, diplopia, Nausea lymphadenopathy, hepatic dysfunction Monitoring LFTs CBC Serum Drug levels Gabapentin in Neuropathic Pain Disorders FDA approved for postherpetic neuralgia Neuropathic pain in patients who do not respond to CBZ and TCA. Neuropathy, multiple sclerosis, migraine Usually well tolerated; serious adverse effects rare dizziness and sedation can occur No significant drug interactions Peak time: 2 to 3 h; elimination half-life: 5 to 7 h Usual dosage range for neuropathic pain up to 12004800 mg/d Suggestions with Gabapentin Start as low as possible…..100 mgm q HS Increase slowly by 100 mgm every three days Caution regarding driving ( sedation) Increase to 1200 mgm and assess pain relief If > 50% relief, wait two weeks and reassess Increase to maximum of 3600 mgm Do not exceed 1200 mgm in elderly Elixir in children mgm/kilo Local anesthetics Lidocaine For neuropatheic pain Short duration Mexiletine longer acting Doses same as antiarrhythmic dose Side effects Dizziness, lightheadedness, ataxia, N/V High dose lead to tremor and convulsion Lidocaine available as patches which have lower SE Local anesthetics Ketamine At the N-methyl-D-aspartate (NMDA) receptor Analgesic at subanesthetic doses For neuropathetic pain 25 mg q 6 hrs , titrate by 25 mg q 24-48hrs Side effects Psychotomimetic, tachycardia, high BP , ↑ intracranial pressure Benzodiazepines Diazepam, midazolam Skeletal muscle relaxant and anxiolytic → ↑ pain threshold. Side effects Sedation, cognitive impairment, depression Addictive Serious withdrawal symptoms such as seizures Corticosteroids Prednisone, Dexamethasone No ceiling effect Opioid sparing effect Dexamethasone 4-16 mg/d in divided doses Oral or IV Other non-analgesic effects Relief of nausea and vomiting Increase energy Corticosteroids Indications Bone metastases Visceral pain Neuropathic pain Nerve compression from tumor Soft tissue or musculoskeletal pain from inflammatory lesions Headache from ↑ intracranial pressure Pain from spinal cord compression Bisphosphonates Analgesic and prevents skeletal complications of malignancy Treatment of hypercalcemia Indications Wide spread painful bone metastases at risk of complications Multiple painful sites of disease at risk of hypercalcemia Osteolytic bone disease where radiation is CI Bisphosphonates Pamidronate, zoledronic acid given IV q 4 wks Nonpharmacologic therapy Surgery Neuroablative blocks and neurolysis Central and peripheral nervous system stimulation Physical therapy