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EMERGENCY MEDICINE PRACTICE A N E V I D E N C E - B A S E D A P P ROAC H T O E M E RG E N C Y M E D I C I N E Pain Management In The ED: Prompt, Cost-Effective, State-Of-The-Art Strategies “Pain is inevitable; suffering is optional.” TINGY, miserly, parsimonious, chintzy, meagerly, closefisted, tight, “Spenurious, and frugal.” Does this describe some erstwhile Scrooge, or the modern emergency physician, gingerly dosing pain medication to the suffering? Perhaps both. Of all of the symptoms that prompt patients to seek emergency care, none is as prevalent as acute pain.1 Each year in the United States, millions of patients present to EDs for the treatment of acutely painful conditions. Pain costs millions of lost workdays and billions of dollars annually. Apart from the issues of compassion and patient satisfaction, there are positive physiologic benefits to treating acute pain. Conversely, there are abundant negative physiologic consequences to inadequately treating pain. In postoperative patients, effective early pain management will decrease postoperative complications and shorten ICU and hospital stays.2 Physiologically, unrelieved pain increases the metabolic rate, alters the immune response, and delays return to normal function. Acute pain has short-term psychological consequences, while chronic pain can cause depression and even suicide. Given the magnitude of painful conditions, and the wide availability of inexpensive analgesics, aggressive management of pain is humane and cost-effective. Unfortunately, emergency physicians often neglect to treat this symptom, needlessly prolonging suffering. This tendency to undertreat pain is called oligoanalgesia. In a frequently cited ED study, fewer than 50% of patients with painful conditions received any analgesia. Of those who were treated, more than half waited over an hour to receive their first dose of medication.3 Numerous studies echo these results. In one, fewer than one-tenth of patients in pain received analgesics in the ED.4 In another investigation, only 20% of patients with extremity fractures were given analgesics in the Editor-in-Chief Stephen A. Colucciello, MD, FACEP, Director of Clinical Services, Department of Emergency Medicine, Carolinas Medical Center, Charlotte, NC; Assistant Clinical Professor, Department of Emergency Medicine, University of North Carolina at Chapel Hill, Chapel Hill, NC. Editorial Board Judith C. Brillman, MD, Residency Director, Associate Professor, Department of Emergency Medicine, The University of New Mexico Health Sciences Center School of Medicine, Albuquerque, NM. W. Richard Bukata, MD, Assistant Clinical Professor, Emergency Medicine, Los Angeles County/ USC Medical Center, Los Angeles, CA; Medical Director, Emergency Department, San Gabriel Valley Medical Center, San Gabriel, CA. Francis M. Fesmire, MD, FACEP, Director, Chest Pain—Stroke Center, Erlanger Medical Center; Assistant Professor of Medicine, UT College of Medicine, Chattanooga, TN. Michael J. Gerardi, MD, FACEP, Clinical Assistant Professor, Medicine, University of Medicine and Dentistry of New Jersey; Director, Pediatric Emergency Medicine, Children’s Medical Center, Atlantic Health System; Chair, Pediatric Emergency Medicine Committee, ACEP. Michael A. Gibbs, MD, FACEP, Clinical Instructor, University of North Carolina at Chapel Hill; Medical Director, MedCenter Air, Department of Emergency Medicine, Carolinas Medical Center, Charlotte, NC. Gregory L. Henry, MD, FACEP, CEO, Medical Practice Risk Assessment, Inc., Ann Arbor, MI; Clinical Professor, Section of Emergency Services, Department of Surgery, University of Michigan Medical School, Ann Arbor, MI; President, American Physicians Assurance Society, Ltd., Bridgetown, Barbados, West Indies; Past President, ACEP. Jerome R. Hoffman, MA, MD, FACEP, Professor of Medicine/Emergency Medicine, UCLA School of Medicine; Attending Physician, UCLA Emergency Medicine Center; December 1999 Volume 1, Number 7 Author Michael A. Turturro, MD, FACEP Vice Chair and Director of Academic Affairs, Department of Emergency Medicine, The Mercy Hospital of Pittsburgh; Clinical Associate Professor of Emergency Medicine, University of Pittsburgh School of Medicine, Pittsburgh, PA. Peer Reviewer James Ducharme, MD, CM, FRCP Associate Professor, Department of Emergency Medicine, Dalhousie University, Saint John, New Brunswick, Canada. CME Objectives Upon completing this article, you should be able to: 1. discuss barriers to effective analgesia in the ED; 2. list advantages and disadvantages of opioid and non-narcotic analgesics; 3. discuss appropriate doses and routes of opioid analgesics; and 4. discuss the use of local anesthetics and sedative agents for pain control in the ED. Date of original release: December 1, 1999. Date of most recent review: November 24, 1999. See “Physician CME Information” on back page. Co-Director, The Doctoring Program, UCLA School of Medicine, Los Angeles, CA. Andy Jagoda, MD, FACEP, Associate Professor of Emergency Medicine, Mount Sinai School of Medicine, New York, NY. John A. Marx, MD, Chair and Chief, Department of Emergency Medicine, Carolinas Medical Center, Charlotte, NC; Clinical Professor, Department of Emergency Medicine, University of North Carolina at Chapel Hill, Chapel Hill, NC. Michael S. Radeos, MD, FACEP, Attending Physician in Emergency Medicine, Lincoln Hospital, Bronx, NY; Research Fellow in Emergency Medicine, Massachusetts General Hospital, Boston, MA; Research Fellow in Respiratory Epidemiology, Channing Lab, Boston, MA. Steven G. Rothrock, MD, FACEP, FAAP, Assistant Professor of Emergency Medicine, University of Florida; Orlando Regional Medical Center, Orlando, FL. Alfred Sacchetti, MD, FACEP, Research Director, Our Lady of Lourdes Medical Center, Camden, NJ; Assistant Clinical Professor of Emergency Medicine, Thomas Jefferson University, Philadelphia, PA. Mark Smith, MD, Chairman, Department of Emergency Medicine, Washington Hospital Center, Washington, DC. Thomas E. Terndrup, MD, Professor and Chair, Department of Emergency Medicine, University of Alabama at Birmingham, Birmingham, AL. Fear Of Obscuring The Diagnosis ED; just one-fifth were given a prescription (or even a recommendation) for an analgesic upon discharge.5 As many as 18% of patients surveyed in the ED have severe pain upon presentation, and 11% may have severe pain upon discharge.6 Children,7 the elderly,8 and certain ethnic groups9 are especially prone to oligoanalgesia in the ED. In one large ED, Hispanic patients were significantly less likely to receive analgesics for long bone fractures than non-Hispanic patients. Those lucky few who were treated rarely received parenteral or opioid agents.9 But why are physicians, who are so expansive in ordering tests, so miserly in analgesia? Some physicians believe they must have a firm diagnosis to treat pain; otherwise, the medication will obscure the clinical examination. Nowhere is this myth more prevalent than in the evaluation of abdominal pain. Physicians in training are frequently taught to withhold analgesics in patients with acute abdominal pain for fear of missing serious pathology. This dogma may stem from Zachary Cope’s 1921 monograph. The good doctor stated, “If morphine be given, it is possible for a patient to die happy in the belief that he is on the road to recovery, and in some cases the medical attendant may for a time be induced to share the delusive hope.”2 This observation (certainly not based on a doubleblinded, randomized, controlled trial) dates to an era in which advanced diagnostic techniques were not available. Fortunately, the latest edition of this classic surgical text now advocates reasonable doses of pain medication for patients with abdominal pain. In a dramatic reversal, the book now admonishes that withholding of analgesia is a “cruel practce” (although they imply that only a “responsible surgeon” should order the drugs).2 Another case of one step forward and two steps back. Recent studies suggest that opioid analgesics given to patients with acute abdominal pain do not alter diagnostic accuracy or delay surgical therapy. Pace studied 71 ED patients with acute undifferentiated abdominal pain and randomized patients to receive either saline placebo or morphine sulfate.11 The mean total dose of morphine administered in the experimental group was 15 mg. The patients who received morphine reported a greater degree of analgesia than placebo, and no patient had any serious pathology missed. The morphine did not mask physical findings such as peritoneal signs. Other studies have found similar results, and some suggest that the relief of pain may actually enhance the examination by reducing anxiety and increasing patient cooperation.12,13 These studies do not suggest that patients with acute abdominal pain should be simply medicated and released, but rather that analgesia be given while the cause for the pain is investigated. Analgesia In The ED: Habits And Facts Several reasons may account for the parsimonious treatment of pain in the ED. None are compelling. (See also Table 1.) Training The problem of oligoanalgesia begins with medical training. Pain management is frequently ignored in medical school and residency; physicians-in-training copy bad habits from colleagues and mentors. Nurses too are given inadequate training in assessing and treating pain.1 Fears Of Drug Dependence And Anger Toward Addicts Physicians may have irrational fears of regarding iatrogenic overdose or addiction. In reality, iatrogenic overdose is easily avoided by the proper dose of medication in the proper route. Fostering addiction through emergency pain relief is virtually unheard of. In the Boston Collaborative survey, nearly 12,000 medical inpatients were treated with opioid analgesics for acute pain. Only four patients developed addiction.10 More realistically, emergency physicians are angered by patients whom they believe to be seeking drugs. While drug seekers populate every ED, it’s no shame to occasionally be “duped” into a narcotic prescription by these desperate (and sometimes innovative) characters. Certainly, it is better to err on the side of relieving true pain at the risk of being sporadically fooled by an addict. Fear Of Side Effects Analgesics are routinely withheld from patients with the potential for hemodynamic instability. While this is a theoretical concern, there’s no evidence to suggest that carefully titrated doses of analgesics will mask significant disease or contribute to instability once primary stabilization has occurred. The most recent edition of the American College of Surgeons’ Advanced Trauma Life Support (ATLS) course advocates the judicious use of analgesics in the multiple trauma patient, stating, “The relief of severe pain is an important part of the management of the trauma patient.”14 Table 1. Factors Contributing To Inadequate Analgesia In The ED. • Inadequate training in analgesic practices • Over-reliance on anecdotal experience • Irrational fears of overdosage and addiction • Focus on diagnostic work-up vs. treatment of symptoms • Fear of exacerbating hemodynamic instability • Unfounded concerns of masking intra-abdominal pathology • Overly suspicious that everyone with chronic pain is an addict Fear Of Voiding Informed Consent Analgesics are occasionally withheld from certain patients in whom surgical intervention is needed due to • Fear of confrontation with consultants Emergency Medicine Practice 2 December 1999 pain. The Agency for Health Care Policy and Research has published a clinical practice guideline that advocates this approach.16 Numerical pain rating scales, Likert scales, visual analog scales, and smiling face scales for children have all been used effectively to measure pain.2 Serial pain scales may be recorded on a designated area in the patient’s chart along with the vital signs. These scales will help the clinician gauge the response to therapy and use additional agents if necessary. concerns regarding consent. However, the mere fact that a patient has been given narcotic analgesia does not render them incapable of consenting to surgical procedures. Vessey and Siriwardena surveyed patients who underwent abdominal surgery, and the majority stated that the administration of pre-operative analgesia did not alter their ability to provide informed consent.15 In fact, withholding analgesics until consent is obtained may be coercion—a more serious breech of the physician-patient relationship than the failure to obtain informed consent. The safest approach is to use judicious titrated doses of analgesics to control the pain without excessively altering cognitive function. If possible, involve the family in the process of obtaining consent, and document the patient’s ability to understand the risks and benefits of the procedure. Establish Clinical Pathways And Educational Programs In Pain Management Clinical pathways for the management of acute pain can include pain scales, physician and nurse protocols, and other prompts to treat pain. (See Clinical Pathway on page 4.) Jones studied the use of a four-hour educational program on resident analgesic practices in the ED. After the program, a significantly greater proportion of patients had clinically important improvements in pain scores.17 Small enhancements in the ED processes and reeducation of staff are simple steps to enhance analgesia in the ED. Fear Of Angering Consultants Some physicians still feel that analgesics should be withheld until a diagnosis is established or consent for a procedure is obtained. This approach is not supported by the medical literature. Communication with and education of these consultants is essential. These discussions should lead to interdisciplinary pathways for the use of analgesics in patients with acute abdominal or other types of pain. Choosing Analgesic Agents: The Right Drug, The Right Route, In The Right Dose There are numerous means to control pain (see Table 2 on page 5). The emergency physician should use both pharmacologic and non-pharmacologic approaches. When selecting drugs to control pain, the physician should understand the advantages and disadvantages of the various agents. Peripheral analgesics such as the NSAIDs inhibit the synthesis of inflammatory mediators that stimulate pain fibers or lower the pain threshold. Centrally acting analgesics such as the opioids modulate the response of the CNS to a given painful stimulus. Many oral opioid preparations combine peripheral and central analgesics to control pain at both sites. Certain analgesics have advantages in particular clinical situations. For example, NSAIDs are useful in dysmenorrhea, since these agents inhibit prostaglandin- “Pain is real when you get other people to believe in it. If no one believes in it but you, your pain is madness or hysteria.” —Naomi Wolf, U.S. author. The Beauty Myth, “Violence” (1990).56 Improving Pain Management In The ED Use Pain Scores In the ED, it is commonplace to measure and recheck vital signs. In a similar fashion, pain scales measure the need for and response to analgesic therapy. The physician and nurse should record the pain score early during the patient encounter and assess the success or failure of pain interventions based upon subsequent scores. The first score may even be obtained at triage. Such a system is routinely used in many EDs for the treatment of chest Continued on page 5 Pearls To Improve Pain Management In The ED (The RELIEF Approach) • Record the pain score on the patient’s chart before and after treatment. • Ease the patient’s concerns—often the fear of pain is more distressing than the pain itself. Inform the patient that pain control is a goal of the ED patient care team. • Look and listen to the patient—they will be the best judge on how much pain they are having and how much relief they have obtained. • Inquire: Always ask the patient if they need pain medication. • Educate ED staff on proper analgesic techniques. • Facilitate multi-disciplinary protocols with nursing and other specialties to manage common painful conditions in the ED. December 1999 3 Emergency Medicine Practice Clinical Pathway: Recommended ED Analgesia Assumes hemodynamic stability In patients with complaint of pain, complete pain score. Re-assess after analgesics given. (Class IIa) Chest pain Yes → Suspect ischemia? No → → → Treat as indicated (Class I) Consider parenteral opioid or oral NSAID (Class IIa) Headache → Suspect migraine? No Yes → → → Consider specific antimigraine therapy (Class I) Consider parenteral opioid (Class IIa) → Female pelvic pain → Pregnant? Yes → → No Consider oral NSAID (Class IIa) Abdominal pain → Renal colic? No → → Yes → Consider parenteral fentanyl 1 mcg/kg (Class IIa) → Pharyngitis → Consider oral or parenteral analgesic in combination with steroids (Class IIa) → Musculoskeletal pain → Consider oral or parenteral analgesic (Class I) Severity of pain mild: Consider acetaminophen. Severe: Consider opioid. (Class IIa) Consider NSAID plus parenteral opioid (Class IIa) The evidenc e for recommendations is graded using the following scale. For complete definitions, see back page. Class I: Definitely recommended. Definitive, excellent evidence provides support. Class II a: Acceptable and useful. Very good evidence provides support. Class II b: Acceptable and useful. Fair-togood evidence provides support. Class III: Not acceptable, not useful, may be harmful. Indeterminate: Continuing area of research. Adapted from Department of Emergency Medicine Pain Management Guidelines, The Mercy Hospital of Pittsburgh. This clinical pathway is intended to supplement, rather than substitute, professional judgment and may be changed depending upon a patient’s individual needs. Failure to comply with this pathway does not represent a breach of the standard of care. Copyright 1999 Pinnacle Publishing, Inc. Pinnacle Publishing (1-800-788-1900) grants permission to reproduce this Emergency Medicine Practice tool for institutional use. Emergency Medicine Practice 4 December 1999 Continued from page 3 exist, the opioid analgesics are the most effective drugs for rapidly controlling pain in the ED. Unfortunately, many physicians have gross misconceptions about dosing, irrational fears regarding addiction, and rely upon the undependable intramuscular route. mediated cramping. These prostaglandin inhibitors are also very useful to control the colicky pain of biliary or ureteral origin. Pharmacokinetics of the drug are also important. Shortacting agents (such as fentanyl) are best used for the treatment of painful procedures, while longer-acting agents (such as oral opioid preparations and NSAIDs) are appropriate for outpatient use. Patients with chronic pain may benefit from sustained-release products and agents that alter monoamine reuptake, such as the tricyclic antidepressants. Although potent analgesics are effective in pain regardless of etiology, in certain conditions, diagnosticspecific therapy is useful. Examples include nitrates to treat cardiac ischemia pain, antacids for dyspepsia, and neuro-modulators or vasoactive agents to treat migraine. Dosing The effective dose of an analgesic differs between individuals, and standard doses or even weight-based doses may not be appropriate. Generally, lower doses are required in the elderly, although large individual variability exists. Many clinicians under-dose opioids in the emergency setting for fear of untoward side effects. In particular, meperidine (Demerol) is uniformly underdosed. Barsan studied the use of high-dose opioid analgesia in the emergency setting in which 72 patients aged 18-63 received 1.5-3.0/kg of meperidine.18 Although sedation was noted in most patients, none had significant respiratory depression. In most otherwise healthy ED patients, use starting doses of approximately 0.1 mg/kg of morphine or 1.0 mg/kg of meperidine by the intravenous route; titrate additional doses to the desired effect. However, many patients will require significantly higher doses to control their pain. Opioid Analgesics The ideal analgesic for emergency use would be highly effective, have rapid onset, be easily used, and titratable. This fabled agent would have a reliable duration of action, lack hemodynamic effects, have minimal to no side effects, and would not mask signs or symptoms of serious disease. Although this agent obviously does not Table 2. Mechanisms Of Pain Control. Mechanism Therapy Stimulate opiate receptors in the CNS Opioid analgesics Block inflammatory mediators that cause pain or lower pain threshold NSAIDs Block pain fiber transmission into the CNS Local anesthetics Stimulate descending serotonergic pathways Tricyclic antidepressants, Tramadol “Gate closing” at dorsal horn of spinal cord Transcutaneous electrical nerve stimulation; acupuncture Reinterpretation of painful stimulus Hypnosis; reassurance Table 3. Opioid Analgesics In Emergency Medicine. Route Typical Dose Range† Frequency† IV, IM, SQ* 0.1-0.2 mg/kg q3h Meperidine IV, IM, SQ* 1-2 mg/kg q2h Fentanyl†† IV, IM, SQ* 1-2 mcg/kg q1h Hydrocodone PO 5-10 mg q4h Codeine PO 30-60 mg q4h Oxycodone PO 5-10 mg q4h Propoxyphene PO 100-200 mg q6h Hydromorphone IV, IM, PO 2-4 mg q4h Tramadol PO 50-10 mg q6h Drug Morphine sulfate†† †† * IV preferred. When not possible or practical, SQ preferred over IM. † The appropriate amount and timing of opioids vary widely between individuals. IV opioids should be titrated to pain. The additional doses are given at fixed intervals only after pain is under control. †† Dosages for these analgesics apply to both adult and pediatric patients. December 1999 5 Emergency Medicine Practice Route Of Administration Specific Agents Opioid analgesics may be given by virtually any route, including oral, intramuscular, subcutaneous, intravenous, intrathecal, intranasal, rectal, and transdermal. In the ED, many clinicians over-rely on the intramuscular route. The major disadvantages of this mode of administration are its erratic absorption (resulting in unreliable onset/ duration) and the pain of administration. The intramuscular route is especially unpredictable in patients with hypovolemia or third spacing, such as patients with blood loss or those with large burns. Conversely, intravenous administration of opioid analgesics results in reliable onset and duration, allowing individualized titration. If intravenous access is difficult, use subcutaneous administration, which is effective and less painful than the intramuscular route. Here again, patients with peripheral vasoconstriction, such as those with hypovolemia, may have delayed or variable responses. There are several opioid analgesics available, for both oral and parenteral administration (see Table 3 on page 5). Fortunately, these highly effective agents are quite inexpensive (see Table 4). Parenteral Opioid Analgesics Morphine sulfate is the analgesic to which all others are compared. Despite certain agents having a higher potency per unit weight, all parenteral agents will be equianalgesic at properly used doses. The major advantages to morphine are its low cost and its half-life of 3-4 hours—longer than most other parenteral agents. The major disadvantage to morphine is its potential to release histamine, resulting in vasodilation or localized inflammatory reactions. Surgical legend suggests that it not be used in patients with suspected biliary disease because it may increase intrabiliary pressures. This concern is entirely theoretical—based solely on in vitro studies. In addition to sedation and respiratory depression in high doses, other common side effects include nausea and dysphoria. Many clinicians use meperidine in the ED, primarily out of habit. Meperidine has several disadvantages compared to morphine. Meperidine has a shorter duration of action, and it is metabolized to normeperidine. Normeperidine may cause CNS side effects such as disorientation, hallucinations, and can lower the seizure threshold, particularly in patients with renal failure or sickle cell disease.20 Meperidine may cause dangerous depressive or excitatory reactions such as hyperpyrexia, hyper- or hypotension, and coma when given with certain psychotropic agents, particularly the monoamine oxidase inhibitors (MAOIs). Fentanyl has several advantages in the ED. It is short-acting, and therefore useful in procedural sedation or in patients who require serial examinations. It causes little histamine release and no significant myocardial depression; therefore, it is safer than many other opioids when used in patients at risk for hemodynamic instability. In higher doses, it may cause apnea before sedation. Fentanyl can cause muscular rigidity when given by the parenteral route. However, this typically occurs with rapid administration at the very high doses used for induction of anesthesia (10 mcg/kg or more). The narcotic agonist-antagonist analgesics (see Table 5 on page 8) stimulate opioid receptors but have certain antagonist properties. This prevents respiratory depression despite high dosage. They also cause less sedation and euphoria than direct opioid agonists. However, due to their antagonist properties, they should not be used in opioid-dependent patients, as they may cause withdrawal. Agonists-antagonists have a high rate of side effects—butorphanol in some migraine studies had so many adverse effects that 60% of patients would not use it again. In one study, the most common side effects, compared to placebo, were dizziness (58% vs 4%), nausea Timing Clinicians also tend to prescribe these drugs on a “PRN” basis. However, more sustained analgesia occurs with “round-the-clock” dosing. This is presumably due to sustained plasma levels. Therefore, in patients with moderate to severe pain, prescribe outpatient analgesics on a regular basis based on the pharmacokinetics of the particular drug, rather than “PRN.” PCA pumps Patients who self-administer small opioid doses are able to control pain with fewer side effects than patients whose medication schedule is determined by a physician. This enhanced sense of personal control will also reduce anxiety and improve analgesia.19 PCA pumps allow patients to self-titrate opioids; in some hospitals, they are ubiquitous in postoperative and oncology wards. However, these pumps are rarely seen in the ED. Barriers to their use include equipment cost and maintenance, lack of familiarity, and pharmacy charges for filling the syringes. Nevertheless, the numerous advantages of the PCA pump make it likely that these devices will play a larger role in ED pain management in the coming decade, especially for patients who may have a prolonged ED stay. Table 4. Pharmacy Cost Of Selected Parenteral Opioid Analgesics (Single Dose). Drug Cost* Morphine 10 mg tubex $0.46 Meperidine 100 mg tubex $0.38 Fentanyl 100 mcg ampule $0.21 Hydromorphone 4 mg ampule $0.59 Nalbuphine 10 mg ampule $0.28 * These prices reflect pharmacy costs only; patient charges may vary. Emergency Medicine Practice 6 December 1999 lower dose of opioids) or to prophylactically treat opioidinduced nausea or vomiting. Hydroxyzine appears to have mild analgesic activity at very high doses (75-100 mg) when combined with opioid analgesics. These doses, which are much higher than typically used, can produce significant sedation and respiratory depression. The dose commonly used (50 mg) has no “opioid-sparing” effect but merely increases the cost of analgesia by 30-38%.22 In addition to the extra cost, hydroxyzine must be given by the painful intramuscular route (adding injury to insult). Promethazine (Phenergan) has an anti-analgesic effect and should not be used routinely.23 Since opioidinduced nausea is not universal, employ these agents as and/or vomiting (38% vs 18%), and drowsiness (29% vs 0%).21 Most of these agents (particularly pentazocine) have affinity for the sigma opiate receptor, which may result in dysphoria, disorientation, hallucinations, and panic. Reports of abuse of the intranasal preparation led butorphanol to be classified as a DEA schedule IV drug in 1997. Opiates And Antiemetics Many clinicians routinely prescribe antiemetics such as hydroxyzine (Vistaril) or promethazine (Phenergan) with opioid analgesics. This combination is selected for either a purported synergistic effect (supposedly requiring a Top 10 Myths Regarding Pain Management In The ED pain to be uncontrolled. Myth #1: Analgesics should not be given to patients with acute abdominal pain, as they may mask the signs of serious disease. Fact: In controlled studies, analgesics do not alter the ability to diagnose the cause of undifferentiated abdominal pain, and they may even improve diagnostic accuracy. Myth #6: The appropriate parenteral dose of meperidine (Demerol) is 50-75 mg. Fact: The effective dose can vary widely, and most patients will require at least 1.5 mg/kg. Myth #7: Meperidine (Demerol) is better than morphine in patients with suspected biliary colic. Fact: The increase in intrabiliary pressure is similar with meperidine and morphine. More importantly, it is of no clinical significance. Myth #2: Always give antiemetics such as Phenergan or Vistaril with opioid analgesics to enhance the analgesic effect. Fact: Antiemetics do not enhance the analgesic effects of opioids at the commonly used doses. Myth #3: Ketorolac is the strongest NSAID, so it is best for severe pain. Fact: There is no evidence that any NSAID provides any better analgesia than another. The analgesic effect from ketorolac is similar to other NSAIDs. Myth #8: All patients requesting pain medications in the ED are drug abusers. Fact: Opioid analgesics can be an important part of pain management in patients with chronic or recurrent pain syndromes. Myth #4: Acetaminophen with codeine is the first choice for an oral narcotic analgesic. Fact: Codeine has limited utility due to its low potency and frequent side effects. Myth #9: Prescriptions for opioid analgesics should be avoided due to the risk of addiction. Fact: When they’re prescribed in short courses to treat acute pain, iatrogenic addiction is a rare phenomenon. Myth #5: Pain medications should be prescribed “PRN.” Myth #10: Tramadol is useful in treating acute pain. Fact: In most studies, the analgesic effect of tramadol is equivalent or only slightly better than placebo. Fact: It is more effective to give pain medication on a regular dosing schedule rather than waiting for the December 1999 7 Emergency Medicine Practice (10 mg or more), and they may develop seizures that are difficult to control. Avoid using propoxyphene unless the patient has demonstrated prior success with this drug. Oxycodone is an excellent analgesic available alone or in combination with aspirin (Percodan) or acetaminophen (Tylox, Percocet, Roxicet). It may produce more euphoria than other oral opioid analgesics and may have a higher abuse potential. Consequently, it is a DEA schedule II drug. Hydromorphone (Dilaudid) is also an effective analgesic that may be given at similar doses both orally and parenterally. Like oxycodone, many believe it has a higher abuse potential, and it is a schedule II drug. The illegal street value in some cities may be more than $60 a pill.28 Hydromorphone is useful in patients with sustained pain (such as cancer pain). Because hydromorphone is not available as a combination product, the use of higher doses is not associated with acetaminophen or aspirin toxicity. Tramadol (Ultram) has weak opioid receptor agonist properties and inhibits serotonin and norepinephrine reuptake in the CNS. Consequently, it is sometimes used as an adjunct to treat chronic pain. Clinicians who use this drug to treat acute pain face disappointing results. Comparative studies in acute pain show tramadol only as effective as placebo,29 and less effective than hydrocodone with acetaminophen.30 In addition, it has a high CNS and gastrointestinal side-effect profile—the manufacturer reports that within the first week of use, 26% of patients experience dizziness, 24% nausea, 24% constipation, 18% headache, and 16% somnolence. Still, abuse of this drug has been reported. It should not be routinely used to treat acute pain in the ED, since other, more effective agents are available. The outpatient prices of selected opioid analgesics are listed in Table 6 on page 9. needed in symptomatic patients. Oral Opioid Analgesics The oral opioid analgesics are typically combined with peripheral analgesics such as aspirin, acetaminophen, or ibuprofen to treat pain both centrally and peripherally. This allows for a lower dose of each agent and decreased side effects. Codeine has been used for many years, and its familiarity has resulted in continued use. However, codeine has many disadvantages. Its analgesic effects are minimal at the typically used doses, while higher doses are associated with a lofty incidence of gastrointestinal and CNS side effects. Seven to 10 percent of Caucasian patients may not respond to the analgesic effects of codeine due to a genetically mediated inability to metabolize codeine to morphine.24 A meta-analysis of 24 studies comparing acetaminophen with and without codeine found the analgesic effects of the combination to be only slightly better than the acetaminophen alone. However, acetaminophen with codeine had a much higher incidence of side effects, such as nausea, vomiting, and sedation.25 Hydrocodone is available alone or in combination with either acetaminophen (Vicodin, Lorcet) or ibuprofen (Vicoprofen). Hydrocodone is better tolerated and more effective than codeine; in one randomized, double-blind clinical trial, CNS side effects were significantly lower with hydrocodone, and patient satisfaction was greater.26 Propoxyphene (Darvon, Darvocet) is a weak analgesic, but sedation is common. A recent meta-analysis of 26 randomized trials comparing propoxyphene-acetaminophen combination products to acetaminophen concluded that propoxyphene was no more effective than acetaminophen alone. Furthermore, the combination was associated with more dizziness and drowsiness.27 This drug is particularly dangerous in overdose. Patients with propoxyphene overdose may present without the classic pinpoint pupils of the narcotic toxidrome. They have notable sedation and respiratory depression requiring high doses of naloxone for reversal Nitrous Oxide Nitrous oxide has great potential in the ED. It is easy to administer, has a rapid onset, a short duration of action, Table 5. Narcotic Agonist/Antagonist Analgesics. Drug Dose Route(s) Frequency Pentazocine (Talwin) 12.5/325 mg ASA PO q4-6h (Talacen) 25 mg/650 mg APAP PO (Talwin Nx) 50 mg/0.5 mg naloxone PO Nalbuphine (Nubain) 10-20 mg IV/IM/SQ q3-4h Butorphanol (Stadol) 1-2 mg IV/IM/SC/ Intranasal q3-4h Buprenorphine (Buprenex) 0.3-0.6 mg IV/IM/SQ q4-6h Dezocine (Dalgan) 10-20 mg IV/IM/SQ q3-4h Emergency Medicine Practice 8 December 1999 renal failure, and anaphylactoid reactions may be severe, life-threatening, and difficult to treat. Peptic ulcer disease may occur after treatment with any NSAID, but the risk appears lowest with ibuprofen.32 Most patients in the ED with mild-to-moderate pain are candidates for an oral NSAID or acetaminophen. More severe pain mandates the use of titrated opioids. Avoid NSAIDs in patients at high risk for side effects, such as the elderly, those with peptic ulcer disease, renal failure or known hypersensitivity. In such patients, treatment with opioids is preferred. provides both sedation and analgesia, and has minimal cardiovascular effects. Because the 50/50 mixture of nitrogen and oxygen is not very effective in severe to moderate pain, some authorities recommend the 70/30 mixture. Be aware that the gas becomes less effective as altitude increases due to decrease in partial pressures. Nitrous oxide-oxygen mixtures with attached scavenging devices are commercially available for ED and prehospital use. These devices use a patientheld valve as fail-safe mechanism. If the patient becomes excessively sedated, the mask falls away and the patient recovers. Nitrous oxide should not be used in conditions in which the gas may expand, such as pneumothoraces, small bowel obstructions, air embolism, and decompression sickness. It is contraindicated in the first trimester of pregnancy due to the potential for teratogenic effects. Parenteral NSAIDs Ketorolac is the only NSAID available for parenteral administration in the United States. Initial studies comparing ketorolac to opioids showed equianalgesia in postoperative pain and renal colic. However, these studies did not account for the variability in opioid dosing or titratability of opioids to enhance analgesia, thus biasing the results in favor of ketorolac.33 Like other NSAIDs, ketorolac is useful in prostaglandin-mediated pain syndromes, such as postoperative pain, renal colic, and biliary colic. There is no evidence to suggest that ketorolac is more potent than the other NSAIDs. Several ED studies have compared ketorolac to oral NSAIDs in acute pain. The less expensive oral agents have the same effect on pain control as parenteral ketorolac.34-36 Furthermore, parenteral administration of NSAIDs does not offer enhanced potency over oral administration.37,38 As with other NSAIDs, adverse effects such as gastrointestinal bleeding, renal dysfunction and platelet inhibition may occur, even with single doses. Ketorolac is also quite expensive: the cost to the pharmacist for a 60 mg tubex is $6.70 and each 10 mg tablet is $1.07, while 800 mg of generic ibuprofen costs $0.04. Therefore, use ketorolac only in conditions where prostaglandin inhibition is needed to control pain and the patient is unable to tolerate oral NSAIDs (such as biliary or renal colic with vomiting). The maximum intravenous dose is 30 mg, half the maximum intramuscular dose. Non-narcotic Analgesics The non-narcotic analgesics consist of those with prostaglandin inhibitory properties (NSAIDs and COX-2 inhibitors) and acetaminophen. Prostaglandinmediated pain is frequent in the ED and includes ureteral colic, biliary colic, and dysmenorrhea. These conditions are particularly suited for treatment with NSAIDs. NSAIDs may be used alone or in conjunction with an opioid. They are widely available and are not associated with dependence, tolerance, or significant respiratory depression or sedation. Unlike the opioids, in which escalating doses increase analgesic effects (in addition to side effects), non-narcotic analgesics have a therapeutic “ceiling.” However, chronic inflammatory conditions such as rheumatoid arthritis require higher-than-typical analgesic doses. Although the NSAIDs differ in pharmacokinetics and their ability to inhibit prostaglandin synthesis, there is no evidence to suggest that any one NSAID is more effective than another. However, for unclear reasons, certain patients may respond better to one class of NSAID vs. another.31 The NSAIDs have certain disadvantages. Dyspepsia is common. NSAID-associated gastrointestinal bleeding, COX-2 Inhibitors NSAIDs inhibit the enzyme cyclooxygenase (COX), which is required to synthesize prostaglandins. There are two isoforms, both of which are blocked by NSAIDs: COX-1 appears to be gastro-protective and is found in platelets, and COX-2 is induced at sites of inflammation. Recently, selective COX-2 inhibitors were developed to provide antiprostaglandin activity without the adverse effects on gastric mucosa and platelets. Celecoxib (Celebrex) was the first of these agents approved by the FDA. It is marketed for the treatment of osteoarthritis and rheumatoid arthritis. While it would seem that these agents could also treat acute pain with fewer adverse consequences, scientific support is lacking. In the single-dose trials with post-dental procedure pain, celecoxib was less effective than naproxen, while in post-surgical pain, it was no Table 6. Retail Prices Of Selected Oral Opioid Analgesics (15 Tablets). Drug DEA Schedule Price APAP—codeine (generic) III $7.00 Hydrocodone (generic) III $7.00 Oxycodone (generic) II $7.00 Tylenol #3 (brand name) III $8.00 Vicodin 5 mg III $8.00 Percocet II $8.00 Talwin-Nx IV $14.00 Dilaudid 4 mg II $15.00 Ultram 50 mg - $23.00 Stadol NS IV $64.00 December 1999 9 Emergency Medicine Practice better than placebo.39 Rofecoxib (Vioxx) has comparable efficacy to 400 mg ibuprofen in post-dental surgery pain.40 Although professed to lower the risk of gastrointestinal bleeding, clinically significant gastric bleeding has followed use of this drug.41 Its safety profile in doses required to treat acute pain is yet to be determined. It costs approximately $4.85 per 50 mg dose, as compared to $0.04 for 800 mg ibuprofen. Currently, there is no evidence to support the routine use of COX-2 inhibitors in the treatment of acute pain. appropriate doses of OTC NSAIDs whenever feasible. In order to reduce the risk of renal failure and GI hemorrhage, suggest or prescribe a maximum supply of five days, since the risk of these complications appears to increase after five days of use. Skeletal Muscle Relaxants Muscle relaxants are often used for myofascial strains; however, their major benefit may come from their sedative effects. Despite their suggestive name, there is no conclusive evidence that they relax skeletal muscle.42 In comparative studies, patients who received skeletal muscle relaxants reported greater analgesia vs. placebo.43,44 However, no particular agent is more effective than another. Cost And Duration Of Therapy The retail prices of nonnarcotic analgesics varies widely (see Table 7), and over-the-counter (OTC) agents are typically much less expensive than prescription agents. For example, two 200 mg OTC generic ibuprofen tablets cost far less than a single 400 mg generic ibuprofen by prescription. Since there are no proven differences in efficacy between NSAIDs, instruct patients to use Local Anesthetics In the ED, painful procedures such as laceration repair, nasogastric intubation, Foley catheter placement, joint reduction, and arterial and venous cannulation are frequently performed (see Table 8). The proper use of local anesthetics, either by direct infiltration, nerve block (see Table 9), field block, or intra-articular use can render these procedures painless. Always document distal neurologic function before performing local or regional anesthesia. In addition, local anesthetics can treat the pain of corneal abrasion so an adequate examination can be performed. Local anesthesia provide sustained pain relief in dentalgia using various nerve blocks. Femoral nerve blocks are an excellent means to Table 7. Retail Price Of Selected NSAIDs (Five-Day Supply). Drug/dose Quantity Price Aspirin 325 mg 40 $1.52 Ibuprofen 200 m (OTC) 40 $2.71 Naproxen 220 mg (OTC) 30 $3.11 Ibuprofen 400 mg 20 $7.00 Ibuprofen 800 mg 15 $7.00 Indomethacin 50 mg 15 $7.00 Naproxen 375 mg (generic) 15 $11.00 Relafen (nabumetone) 500 mg 10 $15.00 Naprosyn 375 mg 15 $21.00 Toradol 10 mg 20 $33.00 Table 9. Common Nerve Blocks In The ED. Extremities Fingers: Digital block Fingers/Metacarpals: Metacarpal block Table 8. Uses For Local Anesthetics In The ED. Hand: Ulnar, radial, median block Procedures: Femur/anterior thigh: Femoral block Wound repair Foot: Saphenous, superficial peroneal, deep peroneal, sural, tibial blocks Thoracostomy Abscess drainage Arthrocentesis Intraoral Lumbar puncture Upper lip/lateral nose: Infraorbital block Nasogastric intubation Lower lip/chin: Mental block Nasotracheal intubation Arterial blood gases Mandibular teeth, anterior 2/3 of tongue: Inferior alveolar block Venous cannulation Individual teeth: Periapical block Foley catheter placement Epistaxis management Other areas Joint reduction Frontal scalp: Supraorbital block Occipital scalp: Greater and lesser occipital block Symptom relief: Penis: Dorsal penile block Dentalgia Vulva/Vagina: Pudendal block Corneal abrasions Ribs: Intercostal blocks Emergency Medicine Practice 10 December 1999 it will not change the neurologic examination in the leg below the knee. control the agony of a femur fracture without the need for high doses of parenteral opioids.45,46 This type of block is particularly useful in multiple-trauma victims or in children. It should be performed after a detailed neurovascular examination of the lower extremity. Approach the femoral nerve lateral to the femoral artery at the inguinal crease. A dose of 5-10 cc of a long-acting local anesthetic such as bupivacaine will provide hours of relief. Although this block will temporarily affect the motor and sensory function of the thigh, Pain Of Injection Some patients report an allergy to local anesthetics, but true allergy to amide local anesthetics is rare; many patients who report allergy may have had an adverse effect to the preservative or received an inappropriately high dose. The major adverse effect of local anesthetics is the pain of administration. This can be minimized by Ten Excuses That Don’t Work In Court 6. “I didn’t know that Demerol interacted with Nardil.” This deadly drug interaction occurred in the highly publicized Libby Zion case. A fatal hyperpyrexic reaction can occur with this drug combination, presumably due to inhibition of serotonin reuptake. 1. “He got better after the Demerol. How was I supposed to know he had a subarachnoid hemorrhage?” Although controlling pain is a desirable goal, it must not be the only goal. Pain control does not preclude evaluation to rule out serious pathology. Opioid analgesia will relieve the pain of even life-threatening conditions such as subarachnoid hemorrhage and pulmonary embolism. Just because the pain is gone does not mean the patient is “fine.” 7. “I forgot to note he was numb in his fingers before I did the median block.” Always document prior neurologic status before using local anesthetics, particularly for regional anesthesia. 2. “Micrograms, milligrams—what’s the difference?” The difference is life and breath in the case of fentanyl. A 100 mg dose led to apnea in this patient. 8. “I didn’t realize I was in the artery when I injected the lidocaine.” When performing nerve blocks or using local anesthetics, aspirate before injecting, or continuously move the needle in and out. This will prevent intravascular injection. Ensure that infiltration does not occur and that the maximum dose is not exceeded, so toxicity does not develop. 3. “She never said she was allergic to Percodan—just to aspirin.” This patient was most upset about the emergency cricothyroidotomy performed after she arrested. While true allergy to the opioid component of combination products is uncommon, certain patients may have allergies to the non-narcotic component. 9. “We had already reduced the shoulder—it took 15 minutes of tugging and straining under conscious sedation. The procedure was over so I told the nurse she could take him off the pulse oximeter.” The several minutes after a procedure may be the most dangerous. During painful stimulation, the patient is unlikely to stop breathing (unless the physician is performing unconscious sedation). When a patient is heavily sedated for an especially painful procedure, apnea may occur when the stimulus is removed. Cardiorespiratory monitoring should continue until the patient is arousable to verbal commands. 4. “I didn’t think a three-week supply of indomethacin would be a problem for Mrs. Viejo. She bled down to a hemoglobin of what???” Four. Life-threatening complications of NSAID use increase in frequency after 5-7 days of use. The elderly are particularly prone to gastrointestinal hemorrhage from these agents. The bleeding is often painless. 5. “I was going to check his pressure before giving 15 mg of IM morphine. But he was in a lot of pain from that leaking aneurysm.” Opioid analgesics have vasodilatory effects and may blunt the secretion of catecholamines. In the patient with potential hemodynamic instability, use only small intravenous doses and balance pain control with clinical effects. Patients who are overtly hypotensive require intravenous fluids and other stabilizing measures before giving opioids. December 1999 10. “I didn’t know he was driving home after we gave him the morphine. I was shocked when I saw him in the trauma room an hour later.” I’ll bet you were also shocked by the lawsuit. Patients who receive opioids or other sedative agents in the ED should not drive home. Give them verbal and written instructions before leaving the ED, warning them not to drive or operate power tools while under the influence of these medications. 11 Emergency Medicine Practice of these dangers, and the abuse potential of a cocainebased drug, TAC use is disappearing in most EDs. Instead, a solution of lidocaine 4%, epinephrine 1:2000, and tetracaine 1% (LET) is as effective and less expensive ($3 vs $35 for TAC).53 EMLA cream (lidocaineprilocaine emulsion) is useful for anesthetizing the skin before venipuncture and may anesthetize wounds. However, its utility in the ED is limited, since it typically using buffered solution, warming, and injecting slowly with a long, narrow-gauge needle.47-49 (See Table 10.) The rate of administration has the greatest effect on reducing the pain of infiltration, followed by buffering and warming, respectively. Topical Anesthetics Since there are many indications for local and topical anesthetics in the ED, and they are relatively simple to use, employ them routinely for procedures listed in Table 11 on page 13. Topical lidocaine may be used alone to anesthetize the mucosa in procedures such as nasogastric tube insertion and Foley catheter insertion, or combined with a topical sympathomimetic such as phenylephrine for cauterization of anterior epistaxis. As with infiltration of local anesthetics, wait at least five minutes after the application before beginning the procedure. Both proparacaine and tetracaine may be used in the eye, but proparacaine may be less painful to instill.50 A solution of topical tetracaine 0.5%, epinephrine 1:2000 and cocaine 10.4% (TAC) will effectively and painlessly anesthetize wounds of the scalp and face. However, TAC can cause seizures or even death in children if they leak onto mucous membranes.51,52 Because Table 10. Tips On Using Local Anesthetics For Infiltration. Methods to Render Solution Less Painful Warming (to 37˚C) Buffering (1 mL of 1 meq/mL NaHCO3 in 10 mL of 1% lidocaine) Lower concentration Methods to Render Infiltration Less Painful Long, narrow-gauge needle Slow infiltration Subcutaneous infiltration Counterirritation Cost-Effective Strategies In Pain Management 1. Use oral rather than parenteral NSAIDs when indicated. Oral NSAIDs are as effective in controlling pain as intravenous or IM ketorolac (Toradol). The parenteral formulation is indicated when the patient is vomiting or otherwise unable to take PO. The pharmacy cost of ketorolac is more than 100 times that of a generic ibuprofen, not to mention the cost of an IV or the needle-stick risks associated with IM injections. Risk Management Caveat: Many patients with renal or biliary colic may be vomiting or intolerant of PO medications. nausea, or develops it after the opioid, an antiemetic may be helpful. 4. Use morphine. Morphine is an outstanding analgesic. It is potent, safe, and predictable. From a cost-effective perspective, it is almost free. Morphine is far less expensive than any other opioid. Risk Management Caveat: Rare patients have dysphoric reactions to morphine. Ask patients if they have ever received it in the past and determine any prior side effects. 2. Recommend over-the-counter NSAIDs instead of writing a prescription. OTC NSAIDs such as ibuprofen (Advil, Nuprin, etc.) or naproxen (Aleve) cost far less than their prescription counterparts, even accounting for the need to take several OTC pills to equal a single prescription tablet. Risk Management Caveat: Patients who come to an ED for pain may expect or insist upon a prescription. (“You mean I could have stayed home and taken some Tylenol instead of coming down here and waiting four hours!?” ) 5. Remember the simple things. Simple, non-pharmacologic interventions can profoundly decrease pain—and cost little or nothing. Ice, elevation, and splinting early in the ED stay can provide enormous relief for a patient with soft-tissue or skeletal injury. Reassure the patient and let him or her know that you will take care of their pain. Fear of remaining in pain and the anxiety associated with anticipation of further suffering can only decrease the patient’s distress. Tell the patient we have more drugs than they have pain.55 In pain management, talk is cheap (but valuable!). Risk Management Caveat: Reassurance and a kind demeanor alone cannot relieve the torment of renal colic. For patients in moderate-to-severe pain, pharmacologic relief is usually required in addition to non-drug interventions. 3. When giving opioids for pain control, avoid routine use of Vistaril (hydroxyzine) or Phenergan (promethazine). These medications significantly increase the cost of pain relief and provide no routine benefit. Promethazine may actually decrease the efficacy of the opioid. Risk Management Caveat: If the patient has significant Emergency Medicine Practice 12 December 1999 movement. Radiolucent splints applied before obtaining x-rays can relieve the unnecessary suffering that comes with radiographic positioning. Manipulative therapy is an example of a physical technique used to relieve musculoskeletal pain. The ancient art of acupuncture may relieve pain by stimulating inhibitory fibers that attenuate pain fiber transmission into the CNS. Similarly, transcutaneous electrical nerve stimulation (TENS) and percutaneous electrical takes 45-60 minutes for full effect. In addition, the cost of each application is approximately $20. Non-pharmacologic Therapy Of Acute Pain Although physicians traditionally use drugs to treat pain, we must not overlook the non-pharmacologic interventions. Simple interventions include ice and elevation for soft-tissue injuries and fractures. Immobilization of fractures can profoundly decrease pain associated with Table 11. Topical Anesthetics. Drug Use on mucous membranes Use in laceration repair Lidocaine jelly 2% + _ Benzocaine 20% + _ TAC (tetracaine, adrenaline, cocaine) _ + LET (lidocaine, epinephrine, tetracaine) _ + EMLA _ + Tool 1. Sample Discharge Instructions For Patients Who Have Received Sedatives Or Opioid Pain Medicine. Copyright 1999 Pinnacle Publishing, Inc. Pinnacle Publishing (1-800-788-1900) grants permission to reproduce this Emergency Medicine Practice tool for institutional use. You (or your child) have received a medicine that can cause a person to be sleepy or clumsy. You or your child must be extra careful in the next several hours. If you have any questions, call the Emergency Department at (_____) ___________. The following things are very important: Children 1. 2. 3. 4. 5. 6. 7. No eating or drinking for the next two hours. If your child is an infant, they may be fed half their normal feeding one hour after discharge. If sleepy, children should be awakened from sleep every hour for the next four hours. No play that requires coordination, such as bike riding, skating, swing sets, or climbing, for the next 24 hours. No playing for the next 24 hours without an adult to watch them. Return to the Emergency Department IMMEDIATELY for vomiting more than once, excessive sleepiness, trouble breathing, strange behavior, or any worrisome symptoms. No swimming, baths, showers, or hot objects (curling irons, etc.) for the next 24 hours, without an adult to watch them. Your child should eat liquids and light foods to start, then increase as tolerated. Adults 1. 2. 3. 4. 5. 6. 7. Do not drive, operate machinery, use power tools, cook, climb, or ride a bicycle for the next 24 hours. Go directly home, rest inside, watch TV or sleep. Do not do any activity in which dizziness or sleepiness would be dangerous. No alcohol for 24 hours. No nonprescription drugs except acetaminophen (Tylenol), aspirin, or ibuprofen (Advil, Nuprin). Eat liquids and light foods to start, then increase as tolerated. Have a responsible person with you at all times for the next 24 hours. No swimming, no taking baths (showers okay). Return to the Emergency Department IMMEDIATELY for vomiting more than once, excessive sleepiness, trouble breathing, strange behavior, or any worrisome symptoms. Remember that the emergency department is open 24 hours a day, every day, and we are always glad to see you. December 1999 13 Emergency Medicine Practice references cited in the paper, as determined by the authors, will be noted by an asterisk (*) next to the number of the reference. nerve stimulation (PENS) will diminish musculoskeletal pain by this mechanism. “It is by poultices, not by words, that pain is ended, although pain is by words both eased and diminished.” —Petrarch Letter to Guido Sette, 1359.54 1. Walsh M. Pain and anxiety in A & E attenders. Nursing Stand 1993;7: 40-42. (Article; 200 patients) 2. Silen W, revised by. Cope’s Early Diagnosis of the Acute Abdomen, ed 19. New York: Oxford University Press; 1996. (Book) *3. Wilson JE, Pendleton JM. Oligoanalgesia in the emergency department. Am J Emerg Med 1989;7:620-623. (Retrospective; 198 patients) 4. Ducharme J, Barber C. A prospective blinded study on emergency pain assessment and therapy. J Emerg Med 1995;13:571-575. (Prospective, blinded; 42 patients) 5. Ngai B, Ducharme J. Documented use of analgesics in the emergency department and upon release of patients with extremity fractures. Acad Emerg Med 1997;4:1176-1178. (Letter) 6. Johnston CC, Gagnon AJ, Fullerton L, et al. One week survey of pain intensity on admission to and discharge from the emergency department. J Emerg Med 1998;16:377-382. (Pilot study—all patients at two university hospitals, 1 general and 1 pediatric) 7. Selbst SM, Clark M. Analgesic use in the emergency department. Ann Emerg Med 1990;1010-1013. (Retrospective; 268 patients) 8. Jones JS, Johnson K, McNinch M. Age as a risk factor for inadequate emergency department analgesia. Am J Emerg Med 1996; 157-160. (Retrospective; 231 patients) 9. Todd KH, Samaroo N, Hoffman JR. Ethnicity as a risk factor for inadequate emergency department analgesia. JAMA 1993;269:15371539. (Retrospective; 139 patients) 10. Porter J, Jick H. Addiction rare in patients treated with narcotics. N Engl J Med 1980;302:123. (Letter) *11. Pace S. Intravenous morphine for early pain relief in patients with acute abdominal pain. Acad Emerg Med 1996;3:1086-1092. (Prospective; 71 patients) 12. Attard AR, Corlett MJ, Kidner NJ, et al. Safety of early pain relief for acute abdominal pain. BMJ 1992;305:554-556. (Prospective, randomized, placebo-controlled; 100 patients) 13. LoVecchio F, Oster N, Sturmann K, et al. The use of analgesics in patients with acute abdominal pain. J Emerg Med 1997;15:775-779. (Prospective; 48 patients) 14. Subcommittee on Advanced Trauma Life Support, Committee of Trauma, American College of Surgeons: Advanced Trauma Life Support for Doctors Student Manual. Chicago: American College of Surgeons; 1997. (Book) 15. Vessey W, Siriwardena A. Informed consent in patients with acute abdominal pain. Br J Surg 1998;85:1278-1280. (Prospective; 49 patients) *16. Acute Pain Management Guideline Panel: Acute Pain Management: Operative or Medical Procedures and Trauma. AHCPR Pub. No. 920032. Rockville, MD: Agency for Health Care Policy and Research, Public Health Service, U.S. Department of Health and Human Services. Feb. 1992. (Review) 17. Jones JB. Assessment of pain management skills in emergency medicine residents: The role of a pain education program. J Emerg Med 1999;17:349-354. (Prospective; 126 patients) *18. Barsan W. Safety assessment of high-dose narcotic analgesia for emergency department procedures. Ann Emerg Med 1993;22:1444-1449. (Prospective; 5 EDs, all patients) 19. Portenoy RK. Clinical application of opioid analgesics. In: Sinatra RS, Hord AH, Ginsberg B, Preble LM, eds. Acute Pain: Mechanisms and Management. St. Louis: Mosby Year Book; 1992:93-101. 20. Clark RF. Meperidine: Therapeutic use and toxicity. J Emerg Med 1995;13:797-802. (Review of controlled trials) 21. Hoffert MJ, Couch JR, Diamond S, et al. Transnasal butorphanol in the treatment of acute migraine. Headache 1995;35(2):65-69. 22. Glazier HS. Potentiation of pain relief with hydroxyzine: A therapeutic myth? Ann Pharmacother 1990;24:484-488. (Review) 23. McGee JL, Alexander MR. Phenothiazine analgesia—fact or fantasy? Am J Hosp Pharm 1979;36(5):633-640. (Review) 24. Eckhardt K, Li S, Ammon S, et al. Same incidence of adverse drug events after codeine administration irrespective of the genetically determined differences in morphine formation. Pain 1998 May;76(12):27-33. (Double-blind study) 25. de Craen AJ, DiGiulio G, Lampe-Shoenmaeckers JE, et al. Analgesic efficacy of paracetamol-codeine combinations versus paracetamol alone: A systematic review. BMJ 1996;313:321-325. (Review) 26. Turturro MA, Paris PM, Yealy DY, et al. Hydrocodone versus codeine in acute musculoskeletal pain. Ann Emerg Med 1991;20-1100-1104. (Double-blind, prospective; 50 patients) 27. Li Wan Po A, Zhang WY. Systematic overview of co-proxamol to assess analgesic effects of addition of dextropropoxyphene to paracetamol. BMJ 1997;315:1565-1571. (Review) Although formal hypnosis is rarely practiced in the ED, we must never underestimate the power of suggestion. Higher brain functions can actively modulate the response to painful stimuli. If patients believe a medication will control their pain, they are more likely to respond to the drug. A physician who suggests, “Maybe this will help—maybe not” is less likely to relieve suffering than one who affirms, “We will make you feel better.” A reassuring manner, distracting attention from the painful stimulus, and the use of adjuncts such as music, television, and videos in the ED will ease pain’s dolorous sting. Summary Most patients come to EDs because of pain. Sadly, many physicians fall short when it comes to pain management. Numerous misconceptions and bad habits cripple their practice. Common failings include not making pain management a priority, the routine use of intramuscular agents to treat pain, frequent use of less effective agents such as codeine or propoxyphene, and under-dosing of opioid analgesics. When a patient arrives in the ED acutely short of breath, no physician waits for a final diagnosis before giving oxygen. Similarly, when a patient presents to the ED in pain, treat it quickly, and aggressively. In most situations, treatment of pain should occur in parallel to patient evaluation.. In the case of abdominal pain, studies show that pain relief does not obscure the diagnosis. If necessary, remind the consultant that CT scans are not influenced by administration of morphine. Routinely incorporate pain measurement into patient evaluation. Be proactive—don’t wait for the patient to ask for pain medication, but offer analgesics early during care. It’s useful to remember that our calling remains “To cure sometimes, to relieve often, and to comfort always.”54 ▲ References Evidence-based medicine requires a critical appraisal of the literature based upon study methodology and number of subjects. Not all references are equally robust. The findings of a large, prospective, randomized, and blinded trial should carry more weight than a case report. To help the reader judge the strength of each reference, pertinent information about the study, such as the type of study and the number of patients in the study, will be included in bold type following the reference, where available. In addition, the most informative Emergency Medicine Practice 14 December 1999 28. 29. 30. 31. *32. 33. *34. 35. 36. 37. 38. 39. *40. 41. 42. 43. 44. 45. 46. 47. 48. *49. 50. 51. 52. *53. 54. 55. 56. Physician CME Questions Web site of the Metropolitan Nashville Police Department (http:// www.nashville.net/~police/citizen/vice.htm.) Moore PA, Crout RJ, Jackson DL, et al. Tramadol hydrochloride: Analgesic efficacy compared with codeine, aspirin with codeine, and placebo after dental extraction. J Clin Pharm 1998;38:554-560. (Randomized, double-blind clinical trial; 200 patients) Turturro MA, Paris PM, Larkin GL. Tramadol versus hydrocodone with acetaminophen in acute musculoskeletal pain: A randomized, controlled clinical trial. Ann Emerg Med 1998;32:139-143. (Randomized, double-blind clinical trial; 68 patients) Brooks PM, Day RO. Nonsteroidal anti-inflammatory drugs— differences and similarities. N Engl J Med 1991;324:1716-1725. (Review) Griffin MR, Piper JM, Daugherty JR, et al. Nonsteroidal antiinflammatory drug use and increased risk for peptic ulcer disease in elderly persons. Ann Intern Med 1991;114:257-263. (Case-controlled study; 8478 patients) Catapano MS. The analgesic efficacy of ketorolac for acute pain. J Emerg Med 1996;14:67-75. (Review) Turturro MA. Intramuscular ketorolac versus oral ibuprofen in acute musculoskeletal pain. Ann Emerg Med 1995;26:117-120. (Prospective; 82 patients) Shrestha M. Randomized double-blind comparison of the analgesic efficacy of intramuscular ketorolac and oral indomethacin in the treatment of acute gouty arthritis. Ann Emerg Med 1995;26:682-686. (Comparative study; 20 patients) Wright JM. NSAID use and efficacy in the emergency department: Single doses of oral ibuprofen versus intramuscular ketorolac. Ann Pharmacother 1994;28:309-312. (Comparative study) Tramer MR, Williams JE, Carroll D, et al. Comparing analgesic efficacy of nonsteroidal anti-inflammatory drugs given by different routes in acute and chronic pain: A qualitative systematic review. Acta Anaesth Scand 1998;42:71-79. (Review) Schwartz N, Istvan D, Turturro MA, et al. Perceived mode of NSAID administration and its effect on analgesia. Acad Emerg Med (in press). Celecoxib for arthritis. Med Lett Drugs Ther 1999;41:11-12. (Review) Morrison BW, Christensen S, Yuan W, et al. Analgesic efficacy of the cyclooxygenase-2-specific inhibitor rofecoxib in post-dental surgery pain: A randomized, controlled trial. Clin Ther 1999;21:943-953. (Randomized, controlled trial; 151 patients) Mohammed S, Croom DW 2d. Gastropathy due to celecoxib, a cyclooxygenase-2 inhibitor. N Engl J Med 1999;340:2005-2006. (Letter) DeLee JC, Rockwood CA. Skeletal muscle spasm and a review of muscle relaxants. Curr Ther Res 1980;27:64-74. (Review) Borenstein DG, Lacks S, Wiesel SW. Cyclobenzaprine and naproxen versus naproxen alone in the treatment of acute low back pain and muscle spasm. Clin Ther 1990;12:125-131. (Comparative study; 40 patients) DiPallma JR, DiGregorio GJ. Management of low back pain by analgesics and adjuvant drugs. Mt Sinai J Med 1991;58: 101-108. (Review) Ronchi L, et al. Femoral nerve blockade in children using bupivacaine. Anesthesiology 1989;70:622-624. McGlone R, Sadhra K, Hamer DW, et al. Femoral nerve block in the initial management of femoral shaft fractures. Arch Emerg Med 1987;4(3):163-168. Colaric KB, Overton DT, Moore K. Pain reduction in lidocaine administration through buffering and warming. Am J Emerg Med 1998;16:353-356. (Comparative study; 20 volunteers) Bartfield JM, Crisafulli KM, Raccio-Robak N, et al. The effects of warming and buffering on pain of infiltration of lidocaine. Acad Emerg Med 1995;2:254-258. Scarfone RJ, Jasani M, Gracely EJ. Pain of local anesthetics: Rate of administration and buffering. Ann Emerg Med 1998;31:36-40. (Comparative study; 42 adult volunteers) Bartfield JM, Holmes TJ, Raccio-Robak N. A comparison of proparacaine and tetracaine eye anesthetics. Acad Emerg Med 1994;1:364-367. Daya MR, Burton BT, Schleiss MR, et al. Recurrent seizures following mucosal application of TAC. Ann Emerg Med 1988;17(6):646-648. Dailey RH. Fatality secondary to misuse of TAC solution. Ann Emerg Med 1988;17(2):159-160. Ernst A, Marvez-Valls E, Nick TG. LAT (lidocaine-adrenalinetetracaine) versus TAC (tetracaine-adrenaline-cocaine) for topical anesthesia in face and scalp lacerations. Am J Emerg Med 1995;13:151-154. Strauss MB, ed. Familiar Medical Quotations. Boston: Little, Brown and Company; 1968. Henry G, personal communication. The Columbia Dictionary of Quotations is licensed from Columbia University Press. Copyright © 1993, 1995 by Columbia University Press. All rights reserved. December 1999 57. All of the following have been identified as risk factors for oligoanalgesia except: a. age. b. gender. c. ethnicity. d. abdominal pain. 58. The most appropriate initial dose of morphine sulfate in an 80 kg 28-year-old male with an isolated upper extremity fracture is: a. 2 mg IV. b. 4 mg IV. c. 8 mg IV. d. 15 mg IV. 59. All of the following are opioid agonist/antagonist analgesics except: a. pentazocine. b. butorphanol. c. dezocine. d. tramadol. 60. Which of the following is a schedule II opioid analgesic? a. Hydromorphone. b. Hydrocodone. c. Pentazocine. d. Codeine. 61. Which of the following is not true regarding ketorolac 60 mg IM? a. It’s the only injectable NSAID available in the U.S. b. It’s as effective as escalating titrated doses of morphine. c. The pharmacy cost is approximately $7. d. It may cause gastrointestinal distress. 62. Which agent has weak opioid receptor agonist properties and inhibits monoamine reuptake? a. Meperidine b. Tramadol c. Ketorolac d. Amitriptyline 63. Which is not true regarding meperidine? a. Its metabolite may be a CNS irritant. b. It can have a dangerous interaction with MAO inhibitors. c. It is frequently underdosed in the ED. d. It has a longer duration of action than morphine. 64. Which local anesthetic is absorbed and effective in intact skin? a. Bupivacaine b. TAC c. Benzocaine d. EMLA 15 Emergency Medicine Practice Physician CME Information 65. Which is not a property of morphine? a. Histamine release b. Lowering of seizure threshold c. Sedation d. Inexpensive compared to other narcotic agents This CME enduring material is sponsored by Carolinas HealthCare System and has been planned and implemented in accordance with the Essentials and Standards of the Accreditation Council for Continuing Medical Education. Credit may be obtained by reading each issue and completing the post-tests administered in December and June. 66. Which agent has a synergistic analgesic effect if given with an opioid? a. Acetaminophen b. Promethazine c. Hydroxyzine d. Midazolam Target A udienc e: This enduring material is designed for emergency medicine physicians. Needs A ssessmen t: The need for this educational activity was determined by a survey of medical staff, including the editorial board of this publication; review of morbidity and mortality data from the CDC, AHA, NCHS, and ACEP; and evaluation of prior activities for emergency physicians. Date of O riginal R elease: This issue of Emergency Medicine Practice was published December 1, 1999. This activity is eligible for CME credit through December 1, 2000. The latest review of this material was November 24, 1999. Discussion of I nvestiga tional I nformation: As part of the newsletter, faculty may be presenting investigational information about pharmaceutical products that is outside Food and Drug Administration approved labeling. Information presented as part of this activity is intended solely as continuing medical education and is not intended to promote off-label use of any pharmaceutical product. Disclosure of Off-Label Usage: This issue of Emergency Medicine Practice discusses no offlabel use of any phamaceutical product. Facult y Disclosur e: In compliance with all ACCME Essentials, Standards, and Guidelines, all faculty for this CME activity were asked to complete a full disclosure statement. The information received is as follows: Dr. Turturro and Dr. Ducharme report no significant financial interest or other relationship with the manufacturer(s) of any commercial product(s) discussed in this educational presentation. Accreditation: Carolinas HealthCare System is accredited by the Accreditation Council for Continuing Medical Education to sponsor continuing medical education for physicians. Credit D esigna tion: Carolinas HealthCare System designates this educational activity for up to 2 hours of Category 1 credit toward the AMA Physician’s Recognition Award. Each physician should claim only those hours of credit actually spent in the educational activity. Emergency Medicine Practice is approved by the American College of Emergency Physicians for 24 hours of ACEP Category 1 credit (per annual subscription). Earning C redit: Physicians with current and valid licenses in the United States, who read all CME articles during each Emergency Medicine Practice six-month testing period, complete the CME Evaluation Form distributed with the December and June issues, and return it according to the published instructions are eligible for up to 2 hours of Category 1 credit toward the AMA Physician’s Recognition Award (PRA) for each issue. You must complete both the post-test and CME Evaluation Form to receive credit. Results will be kept confidential. CME certificates will be mailed to each participant scoring higher than 70% at the end of the calendar year. This test concludes the first semester testing period of Emergency Medicine Practice. The answer form for this semester and a postage-paid return envelope have been included with this issue. All paid subscribers are eligible to take this test. You will need the customer number printed on the outer envelope to submit the post-test. Please refer to the instructions printed on the answer form. Class Of Evidence Definitions Each action in the clinical pathways section of Emergency Medicine Practice receives an alpha-numerical score based on the following definitions. Class I • Always acceptable, safe • Definitely useful • Proven in both efficacy and effectiveness • Must be used in the intended manner for proper clinical indications Level of Evidence: • One or more large prospective studies are present (with rare exceptions) • Study results consistently positive and compelling Class IIa • Safe, acceptable • Clinically useful • Considered treatments of choice Level of Evidence: • Generally higher levels of evidence • Results are consistently positive Class IIb • Safe, acceptable • Clinically useful • Considered optional or alternative treatments Level of Evidence: • Generally lower or intermediate levels of evidence • Generally, but not consistently, positive results Emergency Medicine Practice Class III: • Unacceptable • Not useful clinically • May be harmful Level of Evidence: • No positive high-level data • Some studies suggest or confirm harm Indeterminate • Continuing area of research • No recommendations until further research Level of Evidence: • Evidence not available • Higher studies in progress • Results inconsistent, contradictory • Results not compelling Publisher : Robert Williford. Vice Presiden t/General Manager : Connie Austin. Executiv e Editor: Heidi Frost. Direct all editorial or subscription-related questions to Pinnacle Publishing, Inc.: 1-800-788-1900 or 770-565-1763 Fax: 770-565-8232 Pinnacle Publishing, Inc. P.O. Box 72255 Marietta, GA 30007-2255 E-mail: emer gmed@pinpub .com Adapted from: The Emergency Cardiovascular Care Committees of the American Heart Association and representatives from the resuscitation councils of ILCOR: How to Develop Evidence-Based Guidelines for Emergency Cardiac Care: Quality of Evidence and Classes of Recommendations; also: Anonymous. Guidelines for cardiopulmonary resuscitation and emergency cardiac care. Emergency Cardiac Care Committee and Subcommittees, American Heart Association. Part IX. Ensuring effectiveness of community-wide emergency cardiac care. JAMA 1992;268(16):2289-2295. Pinnacle Web Site: http://www .pinpub .com Emergency Medicine Practice (ISSN 1524-1971) is published monthly (12 times per year) by Pinnacle Publishing, Inc., 1503 Johnson Ferry Road, Suite 100, Marietta, GA 30062. Opinions expressed are not necessarily those of this publication. Mention of products or services does not constitute endorsement. This publication is intended as a general guide and is intended to supplement, rather than substitute, professional judgment. It covers a highly technical and complex subject and should not be used for making specific medical decisions. The materials contained herein are not intended to establish policy, procedure, or standard of care. Emergency Medicine Practice is a trademark of Pinnacle Publishing, Inc. Copyright 1999 Pinnacle Publishing, Inc. All rights reserved. No part of this publication may be reproduced in any format without written consent of Pinnacle Publishing, Inc. Subscription price: $249, U.S. funds. (Call for international shipping prices.) 16 December 1999