Pharmacologic Management of Acute and Chronic Pain.Focus on Drug Interactions and Patient-Specific Pharmacotherapeutic Selection PAIN is among the most common reasons patients seek medical care. Acute and chronic pain is debilitating de·bil·i·tat·ing adj. Causing a loss of strength or energy. Debilitating Weakening, or reducing the strength of. Mentioned in: Stress Reduction . Recovery is slow, interference with daily activities occurs, and pain manifests as a decremental change in the patient's quality of life. This is compounded by societal costs. [1-5] Acute pain is often associated with an identifiable injury or trauma as a known antecedent, responds to therapeutic options, and resolves in less than i to 3 months, chronic pain is more of a treatment challenge because the pathogenesis may be unclear, with less opportunity to predict the course of recovery. For patients already under great psychologic and financial stress, such an ambiguous prognosis is devastating. The goal of the clinician is to provide an opportunity for patients to regain some sense of control over their lives by providing the most effective pain treatment regimen possible. [1-5] Pain usually defined as chronic lasts longer than i to 3 months or exceeds the typical recovery time for an initial injury, chronic pain may be continuous or episodic or a combination of both. Overall, chronic pain is commonly accompanied by emotional stress, increased irritability, depression, social withdrawal, financial distress, loss of libido, disturbed sleep patterns, diminished appetite, and/or weight loss, chronic pain can have a wide-ranging impact; its management must therefore focus on multiple aspects of a patient's life. A multidisciplinary, comprehensive treatment plan is optimal, including (1) individual psychosocial counseling in conjunction with patient/family education; (2) noninvasive or minimally invasive procedures, such as massage therapy, physical therapy, transdermal or transcutaneous electrical nerve stimulation transcutaneous electrical nerve stimulation n. TENS. Transcutaneous electrical nerve stimulation (TENS) A method for relieving the muscle pain of TMJ by stimulating nerve endings that do not transmit pain. (TENS), or acupuncture; (3) up-to-date pharmacologic and/or anesthetic therapies; and (4) if necessary, surgical intervention and physical medicine with rehabilitation focused to enhance the patient's functional status. Health care practitioners must consider uniting these various options in tailoring a patient-specific treatment plan, addressing both physiologic and psychologic symptoms. [1-8] A pharmacotherapeutic plan begins with a thorough pain and pain medication history to identify the nature of the patient's pain (eg, acute versus chronic, acute and chronic, nociceptive no·ci·cep·tive adj. 1. Causing pain. Used of a stimulus. 2. Caused by or responding to a painful stimulus. versus neuropathic). The patient interview should focus on patient-reported pain descriptors (eg, exacerbation/modulation of pain; pain quality and intensity; pain sites as local, disseminated, or regional; characteristics and temporal relationships of pain), current pharmacotherapies (prescription, over-the-counter, phytopharmaceutical, and/or social/recreational agents), and past treatments (including successes and/or failures, adverse effects, and allergic reactions). A complete blood chemistry profile should be considered to determine if dosage changes are warranted. Health care practitioners should familiarize themselves with the pharmacodynamics pharmacodynamics /phar·ma·co·dy·nam·ics/ (-di-nam´iks) the study of the biochemical and physiological effects of drugs and the mechanisms of their actions, including the correlation of their actions and effects with their chemical , pharmacokinetics, and potential drugdrug or drug-food interactions and contraindications of any pharmacotherapy pharmacotherapy /phar·ma·co·ther·a·py/ (-ther´ah-pe) treatment of disease with medicines. phar·ma·co·ther·a·py n. Treatment of disease through the use of drugs. used by the patient. [1-3,7,9] Decisions about a polypharmaceutical or other complex regimen may be made jointly. Depending on the nature of the specific pain in a given patient, combinations of antidepressants Antidepressants Medications prescribed to relieve major depression. Classes of antidepressants include selective serotonin reuptake inhibitors (fluoxetine/Prozac, sertraline/Zoloft), tricyclics (amitriptyline/ Elavil), MAOIs (phenelzine/Nardil), and heterocyclics , anxiolytics, anticonvulsants Anticonvulsants Drugs used to control seizures, such as in epilepsy. Mentioned in: Antipsychotic Drugs, Osteoporosis , sedative/hypnotics, centrally acting agents, opiates/opioids, muscle relaxants, nonsteroidal anti-inflammatory drugs Nonsteroidal Anti-Inflammatory Drugs Definition Nonsteroidal anti-inflammatory drugs are medicines that relieve pain, swelling, stiffness, and inflammation. (NSAIDs), or other analgesics may be considered. Health care practitioners should also consider any factors that affect the likelihood of compliance (eg, patient age, frequency and/or complexity of the regimen, route of administration, tolerance of the regimen). [1-3,9] Pharmacologic Agents NONOPIOID ANALGESICS An extensive review of these agents has been published elsewhere. Aspirin (acetylsalicylic acid [ASA Asa (ā`sə), in the Bible, king of Judah, son and successor of Abijah. He was a good king, zealous in his extirpation of idols. When Baasha of Israel took Ramah (a few miles N of Jerusalem), Asa bought the help of Benhadad of Damascus and ]) is used to reduce inflammation, pain, and fever. It inhibits prostaglandin synthesis and acts on the hypothalamus hypothalamus (hī'pəthăl`əməs), an important supervisory center in the brain, rich in ganglia, nerve fibers, and synaptic connections. It is composed of several sections called nuclei, each of which controls a specific function. to reduce fever, to prevent the formation of the platelet aggregation substance thromboxane thromboxane /throm·box·ane/ (-bok´san) either of two compounds, one designated A2 and the other B2. Thromboxane A2 is synthesized by platelets and is an inducer of platelet aggregation and platelet release functions and is a , and to inhibit vitamin K--dependent and independent clotting factors. Renal elimination of ASA is primarily as free salicylic acids and conjugated conjugated adj. Conjugate. estrogens, conjugated Warning - Hazardous drug! C.E.S. metabolites Metabolites Substances produced by metabolism or by a metabolic process. Mentioned in: Interactions . Aspirin use should be avoided in end-stage renal disease End-stage renal disease (ESRD) Total kidney failure; chronic kidney failure is diagnosed as ESRD when kidney function falls to 5-10% of capacity. Mentioned in: Chronic Kidney Failure end-stage renal disease . The dose should be modified when aspirin is used for long-term therapy in the presence of hepatic compromise. Side effects of aspirin include gastrointestinal (GI) irritation, nausea, vomiting, tinnitus Tinnitus Definition Tinnitus is hearing ringing, buzzing, or other sounds without an external cause. Patients may experience tinnitus in one or both ears or in the head. , metabolic acidosis, acute respiratory distress syndrome acute respiratory distress syndrome n. See adult respiratory distress syndrome. , and occult GI blood loss. Both aspirin and salicylic acid enter the central nervous system (CNS See Continuous net settlement. CNS See continuous net settlement (CNS). ), and effects such as dizziness, vertigo, fatigue, insomnia, lethargy, confusion, depression, and headache may occur. [1-3,8,10,11] Caution should also be taken in treating patients with platelet or bleeding disorders or renal dysfunction. All patients receiving ASA for transient ischemic attacks or myocardial infarction who are prescribed a cyclooxygenase-2 (COX-2) agent must continue taking the ASA (80 ma to 325 mg). Patients with a history of nasal polyps, asthma, or rhinitis Rhinitis Definition Rhinitis is inflammation of the mucous lining of the nose. Description Rhinitis is a nonspecific term that covers infections, allergies, and other disorders whose common feature is the location of their symptoms. may have aspirin intolerance, leading to severe exacerbation of allergic symptoms, including potentially fatal bronchospasms. Acetaminophen acetaminophen (əsēt'əmĭn`əfĭn), an analgesic and fever-reducing medicine similar in effect to aspirin. It is an active ingredient in many over-the-counter medicines, including Tylenol and Midol. (APAP APAP Association of Performing Arts Presenters APAP Association of Physician Assistant Programs APAP Action Professionals' Association for the People APAP Associação Portuguesa das Empresas de Publicidade e Comunicação (Portugal) ) is an analgesic and antipyretic antipyretic /an·ti·py·ret·ic/ (-pi-ret´ik) 1. relieving or reducing fever. 2. an agent that so acts. an·ti·py·ret·ic n. An agent that reduces or prevents fever. agent that lacks anti-inflammatory properties. The APAP central mechanism may be mediated through central COX-2 mechanism. Metabolism occurs in the liver, primarily by cytochrome P450 (CYP-450) 1A2, 3A4, and 2E1. A slight increase in the dosing interval may be needed when renal dysfunction is present. Prolonged use of APAP in patients with severe liver disease is not recommended. Hepatotoxicity hepatotoxicity (hepˑ·  ·tō·t may occur with daily
long-term doses of more than 3,000 mg/day and short-term doses of 7 to 8
a and is exacerbated in patients with a history of alcohol abuse. No
more than 3 to 4 g of APAP daily is currently recommended. [1-3]
Nonsteroidal anti-inflammatory drugs are antipyretic, anti-inflammatory, and analgesic agents that decrease prostaglandin production through their variable inhibition of cyclooxygenase-1 (COX-1) and COX-2. All NSAIDs carry the risk of GI, hepatic, hematologic hematological, hematologic pertaining to or emanating from blood cells. hematological tests total and differential white cell counts, hematocrit estimation, erythrocyte count. , and renal adverse effects, which should be considered when contemplating their use long-term for pain. Drug monitoring should include complete blood count, creatinine clearance, urinalysis, potassium level, liver function tests Liver Function Tests Definition Liver function tests, or LFTs, include tests for bilirubin, a breakdown product of hemoglobin, and ammonia, a protein byproduct that is normally converted into urea by the liver before being excreted by the kidneys. , occult fecal blood testing, and blood and urine testing for hematuria hematuria Blood in the urine. It usually indicates injury or disease of the kidney or another structure of the urinary system or possibly, in males, the reproductive system. It may result from infection, inflammation, tumours, kidney stones, or other disorders. and proteinuria proteinuria /pro·tein·uria/ (-ur´e-ah) an excess of serum proteins in the urine, as in renal disease or after strenuous exercise.proteinu´ric pro·tein·u·ri·a n. 1. . Gastrointestinal ulceration, bleeding, and perforation occur, often without warning symptoms. [1-3,11,12] Other adverse effects associated with NSAID NSAID: see nonsteroidal anti-inflammatory drug. use include reduced renal blood flow In the physiology of the kidney, renal blood flow (RBF) is the volume of blood delivered to the kidneys per unit time. In humans, the kidneys together receive roughly 20% of cardiac output, amounting to 1 L/min in a 70-kg adult male. and glomerular glomerular /glo·mer·u·lar/ (glo-mer´u-ler) pertaining to or of the nature of a glomerulus, especially a renal glomerulus. glo·mer·u·lar adj. filtration, interstitial nephritis, acute tubular necrosis acute tubular necrosis Nephrology A pathologic change of acute renal failure due to shock, crush injuries, hemoglobinuria, toxic nephrosis, sepsis, drugs-aminoglycosides, amphotericin B, cyclosporine, radiocontrast, ischemia in transplanted kidneys Predisposing , papillary necrosis, nephrotic syndrome, sodium and water retention (edema edema (ĭdē`mə), abnormal accumulation of fluid in the body tissues or in the body cavities causing swelling or distention of the affected parts. ), acute renal failure acute renal failure Acute kidney failure Nephrology An abrupt decline in renal function, triggered by various processes–eg, sepsis, shock, trauma, kidney stones, drug toxicity-aspirin, lithium, substances of abuse, toxins, iodinated radiocontrast. , hyperkalemia Hyperkalemia Definition The normal concentration of potassium in the serum is in the range of 3.5 to 5.0 mM. Hyperkalemia refers to serum or plasma levels of potassium ions above 5.0 mM. , and hypertension; NSAIDs also decrease the efficacy of diuretics Diuretics Definition Diuretics are medicines that help reduce the amount of water in the body. Purpose Diuretics are used to treat the buildup of excess fluid in the body that occurs with some medical conditions such as congestive heart , [beta]-blockers, and angiotensin-converting enzyme (ACE) inhibitors. Elderly patients, patients with diabetes mellitus, or those with mild to moderate renal insufficiency may be predisposed to hyperkalemia, as may patients receiving concomitant therapy with other hyperkalemia-inducing agents (ACE-inhibitors, potassium-sparing diuretics, salt substitutes). Local as well as systemic injury is caused by prostaglandin synthesis inhibition of gastric mucosa defense and platelet function, respectively. Inhibition of platelet aggregation can lead to enhanced bleeding. [1-3,11,12] Two isoenzymes of oral cyclooxygenase--COX-1 and COX-2--have been identified. Only two COX-2 specific agents are currently available in the United States. A comparison of these two agents is seen in the Table. The distribution, regulation, and function of cyclooxygenase, along with a complete review of COX-1 and COX-2 agents, has been fully described elsewhere." [11,12] Acute sodium retention is COX-2 inhibitor--mediated and clinically resolves with continuation of therapy. Glomerular filtration rate glomerular filtration rate n. Abbr. GFR The volume of water filtered out of the plasma through glomerular capillary walls into Bowman's capsules per unit of time. (GFR GFR - Grim File Reaper ) is influenced due to inhibition of COX-1; COX-2 specific agents spare the GFR, which decrementally deteriorates in the elderly. Both hypertension and edema are of minor clinical occurrence with COX-2 specific agents. As with all NSAIDs, COX-2 agents should be used with caution in patients with fluid retention, hypertension, or heart failure. Rofecoxib has been found to be opioid-sparing in postoperative treatment of pain. Rofecoxib has prominent pharmacologic, pharmacokinetic, pharmacodynamic, and pharmacotherapeutic advantages over the available COX-2 specific agents. [3,11,112] CENTRALLY ACTING ANALGESIC Tramadol is an atypical analgesic with a binary mechanism of action. The mechanism of action combines centrally acting opioid ([micro]) activity with a secondary spinal mechanism of monoamine monoamine /mono·amine/ (mon?o-ah-men´) an amine containing one amino group, e.g., serotonin, dopamine, epinephrine, and norepinephrine. mon·o·am·ine n. reuptake reuptake /re·up·take/ (re-up´tak) reabsorption of a previously secreted substance. re·up·take n. inhibition. With its weak affinity for [micro]-opioid receptors, in conjunction with serotonin and norepinephrine norepinephrine (nôr'ĕpīnĕf`rən), a neurotransmitter in the catecholamine family that mediates chemical communication in the sympathetic nervous system, a branch of the autonomic nervous system. reuptake blockade, tramadol interferes with pathways that mediate pain. Spinally and supraspinally, tramadol is associated with a lower degree of respiratory depression than opioids. It has a low potential for tachyphylaxis tachyphylaxis /tachy·phy·lax·is/ (-fi-lak´sis) 1. rapid immunization against the effect of toxic doses of an extract or serum by previous injection of small doses of it. 2. and abuse and is used for the long-term management of moderate to moderately severe pain and for acute pain. The concomitant use of tramadol and NSAIDs (eg, rofecoxib) may offer the therapeutic benefits of both central and peripheral analgesia analgesia /an·al·ge·sia/ (an?al-je´ze-ah) 1. absence of sensibility to pain. 2. the relief of pain without loss of consciousness. , though the requisite studies have not yet been concluded. Tramadol represents an option for patients who are at risk for the side effects of NSAIDs but are reluctant to take opioid analgesics. Only 20% is bound to plasma proteins. The activ e metabolite metabolite, organic compound that is a starting material in, an intermediate in, or an end product of metabolism. Starting materials are substances, usually small and of simple structure, absorbed by the organism as food. Ml and the parent exhibit linear pharmacokinetics, utilize the CYP CYP In currencies, this is the abbreviation for the Cyprus Pound. Notes: The currency market, also known as the Foreign Exchange market, is the largest financial market in the world, with a daily average volume of over US $1 trillion. 45O 3A4 and 2D6 hepatic enzyme substrate, respectively. Dialysis removes less than 10% of a given dose. Tramadol has been additionally studied in elderly populations and for a variety of conditions. It has been well tolerated overall and has proven to be effective in fibromyalgia, acute or chronic pain, osteoarthritis, back pain, and neuropathic pain. In the near future, tramadol will be available in combination with APAP (37.5 mg tramadol and 325 mg APAP), in a sustained-action dosage form, and in an oral liquid form. [1-3,6,13-18] OPIATES Opiates Analgesic, pain killing drugs, such as heroin and morphine that depress the central nervous system. Mentioned in: Withdrawal Syndromes AND OPIOIDS Probably the best-known class of medications used to treat pain is that of the opiates and opioids. When opiates are used for management of chronic pain, both chemical and psychologic dependence may ensue with chronic administration. Both practitioners and patients can have "opiophobia" (the patient's fear of opiate opiate /opi·ate/ (o´pe-it) 1. any drug derived from opium. 2. hypnotic (2). o·pi·ate n. 1. use, the physician's concern of "opiate addiction," and the pharmacist's cautions about dispensing the prescription), which leads to unnecessary underutilization of opiates in pain management. Opiates/opioids each uniquely produce a wide spectrum of pharmacologic effects, including analgesia, dysphoria dysphoria /dys·pho·ria/ (-for´e-ah) [Gr.] disquiet; restlessness; malaise.dysphoret´icdysphor´ic gender dysphoria , euphoria, somnolence somnolence /som·no·lence/ (som´no-lens) drowsiness or sleepiness, particularly in excess. som·no·lence n. 1. A state of drowsiness; sleepiness. 2. , respiratory depression, diminished GI motility motility /mo·til·i·ty/ (mo-til´ite) the ability to move spontaneously.mo´tile Motility Motility is spontaneous movement. , altered circulatory dynamics, urinary retention, histamine release, and physical dependence. [1-5,7,11,19-23] The analgesic effects appear to be a function of several factors, including affinity for specific receptor binding sites, intrinsic activity at respective receptors, and the pharmacokinetics and pharmacodynamics of the specific agents. The binding of [micro] receptors ([[micro].sub.1] and [[micro].sub.2]) produces euphoria and is associated with morphine-like analgesia, respiratory depression, miosis miosis /mi·o·sis/ (mi-o´sis) contraction of the pupil. mi·o·sis or my·o·sis n. pl. mi·o··ses 1. , and inhibited GI motility. The [[micro].sub.2] receptor has been associated with effects on GI motility, euphoria, respiratory depression, bradycardia bradycardia: see arrhythmia. , and psychologic aspects of chemical dependence. Codeine codeine (kō`dēn), alkaloid found in opium. It is a narcotic whose effects, though less potent, resemble those of morphine. An effective cough suppressant, it is mainly used in cough medicines. Like other narcotics, codeine is addictive. is metabolized to morphine, and hydrocodone is metabolized to hydromorphone. This hepatic metabolism occurs through the CYP-450 2D6 pathway. (A brief comment on each frequently prescribed opiate/opioid follows.) Hydrocodone, a phenanthrene phenanthrene /phe·nan·threne/ (fe-nan´thren) a tricyclic aromatic hydrocarbon occurring in coal tar; toxic and carcinogenic. phe·nan·threne n. derivative, is a dehydrogenated ketone ketone (kē`tōn), any of a class of organic compounds that contain the carbonyl group, C=O, and in which the carbonyl group is bonded only to carbon atoms. codeine derivative. Fixed hydrocodone analgesic combinations include APAP and ibuprofen. Most opioids have side effects, including sedation, nausea, vomiting, pruritus pruritus /pru·ri·tus/ (proo-ri´tus) itching.prurit´ic pruritus a´ni intense chronic itching in the anal region. pruritus hiema´lis xerotic eczema. , and urinary retention. Constipation is an adverse effect to which tolerance does not develop, so a laxative laxative, drug or other substance used to stimulate the action of the intestines in eliminating waste from the body. The term laxative usually refers to a mild-acting substance; substances of increasingly drastic action are known as cathartics, purgatives, and/or stool softener may be added to opiate/opioid therapy. Morphine dosage should be administered according to the patient's characteristics. Elderly patients are more sensitive to morphine. Dose adjustments are not necessary in mild hepatic disease, but excessive sedation occurs in cirrhotic patients. This is a function of the accumulation of the active analgesic metabolite, morphine-6-glucuronide (M-6-G), which is renally eliminated. Oxycodone oxycodone /oxy·co·done/ (-ko´don) an opioid analgesic derived from morphine; used in the form of the hydrochloride and terephthalate salts. ox·y·co·done n. is an analgesic metabolized by the CYP-450 2D6 isoenzyrne and is excreted renally. Oxymorphone is a minor active metabolite of oxycodone created through hepatic CYP-450 metabolism. Morphine acts as a pure agonist, binding with and activating opioid receptors at sites in the periaqueductal per·i·aq·ue·duc·tal adj. Situated around the aqueduct of the brain. and periventricular grey matter, ventromedulla, and spinal cord to produce analgesia. The principal therapeutic actions of morphine on the CNS are analgesia, sedation, and alterations of mood. The pharmacologic activity is primarily due to the parent compound morphine. One metabolite, M-6-G, has been shown to have analgesic activity, but it crosses the blood-brain barrier poorly and may accumulate during renal dysfunction or excessive administration. Elimination of morphine is primarily via hepatic metabolism by phase II process to glucuronide metabolites (55% to 56%), which are then renally excreted. The terminal half-life of morphine is 2 to 4 hours and up to 15 hours with linear pharmacokinetics over the dosage range of 30 to 100 mg. After the administration of oral morphine, approximately 50% of the morphine is not used, because of presystemic (CYP-50 metabolism, first pass) elimination; only abou t 20% to 40% of the administered dose reaches the systemic circulation. Morphine is 30% to 35% reversibly bound to plasma proteins. The major pathway of the detoxification of morphine is conjugation conjugation, in genetics conjugation, in genetics: see recombination. conjugation, in grammar conjugation: see inflection. . Virtually all morphine is converted to glucuronide metabolites, including morphine-3-glucuronide (M-3-G) (about 50%) and M-6-G (about 5% to 15%). While M-3-G has no significant, analgesic activity, M-6-G has been shown to have opioid agonist and analgesic activity in humans. Meperidine meperidine (me-per´i-den) an opioid analgesic, used as the hydrochloride salt as an analgesic and an anesthesia adjunct. meperidine a centrally acting analgesic with spasmolytic properties equal to those of atropine. is a synthetic opioid. Normeperidine is an active nonopioid metabolite that is clinically important in that it is not naloxone-reversible. The half-life of normeperidine is 15 to 30 hours, depending on the patient's renal function. After repeated dosing, normeperidine accumulates, and the concentration exceeds that of meperidine in the plasma. Resultant effects of normeperidine include respiratory arrest and excitatory ex·ci·ta·tive or ex·ci·ta·to·ry adj. Causing or tending to cause excitation. Adj. 1. excitatory - (of drugs e.g. neurotoxicity neurotoxicity /neu·ro·tox·ic·i·ty/ (noor?o-tok-sis´it-e) the quality of exerting a destructive or poisonous effect upon nerve tissue. (hyperreflexia, myoclonus myoclonus /my·oc·lo·nus/ (mi-ok´lo-nus) shocklike contractions of a muscle or a group of muscles.myoclon´ic essential myoclonus , grand mal seizures, and agitation). These effects have been reported after less than 24 hours of dosing in patients at all ages and in those with normal renal function as well as in those with impaired renal function. Anticholinergic anticholinergic /an·ti·cho·lin·er·gic/ (-ko?lin-er´jik) parasympatholytic; blocking the passage of impulses through the parasympathetic nerves; also, an agent that so acts. an·ti·cho·lin·er·gic n. effects of meperidine are serious enough that the patient may have urinary retention and need catheterization catheterization Threading of a flexible tube (catheter) through a channel in the body to inject drugs or a contrast medium, measure and record flow and pressures, inspect structures, take samples, diagnose disorders, or clear blockages. ; other effects include ventricular response to atrial flutter and supra-ventricular tachycardia tachycardia: see arrhythmia. tachycardia Heart rate over 100 (as high as 240) beats per minute. When it is a normal response to exercise or stress, it is no danger to healthy people, but when it originates elsewhere, it is an arrhythmia. . Meperidine also blocks the neuronal reuptake of serotonin with a serotonin syndrome produced by monoamine oxidase inhibitor monoamine oxidase inhibitor n. Abbr. MAOI Any of a class of antidepressant and hypotensive drugs that block the action of monoamine oxidase in the brain, thereby allowing the accumulation of monoamines such as norepinephrine. (MAOI MAOI monoamine oxidase inhibitor. MAOI abbr. monoamine oxidase inhibitor Monoamine oxidase inhibitor (MAOI) An older class of antidepressants. ) drug interactions. Deaths related to meperidine-MAOI interactions have been reported. Serotonin syndrome has also been reported with concomitant use of meperidine and fluoxetine fluoxetine /flu·ox·e·tine/ (floo-ok´se-ten) a selective serotonin reuptake inhibitor used as the hydrochloride salt in the treatment of depression, obsessive-compulsive disorder, bulimia nervosa, and premenstrual dysphoric disorder. . Meperidine use may aggravate preexisting pre·ex·ist or pre-ex·ist v. pre·ex·ist·ed, pre·ex·ist·ing, pre·ex·ists v.tr. To exist before (something); precede: Dinosaurs preexisted humans. v.intr. seizure disorders. Use of meperidine in chronic pain and acute pain is falling into disuse. [*] Propoxyphene propoxyphene /pro·poxy·phene/ (-pok´si-fen) an opioid analgesic structurally related to methadone, used as the hydrochloride and napsylate salts. propoxyphene an analgesic used as the hydrochloride and napsylate salts. is a synthetic opiate analgesic with chemical similarity to methadone methadone (mĕth`ədōn', –dŏn'), synthetic narcotic similar in effect to morphine. Synthesized in Germany, it came into clinical use after World War II. It is sometimes used as an analgesic and to suppress the cough reflex. . It is metabolized in the liver to norpropoxyphene, which is eliminated in urine. Norpropoxyphene is not an opioid but has proarrhythmic lidocaine-like effects and cardiac anesthetic effects similar to those of amitriptyline amitriptyline /am·i·trip·ty·line/ (am?i-trip´ti-len) a tricyclic antidepressant with sedative effects; also used in treating enuresis, chronic pain, peptic ulcer, and bulimia nervosa. . Because of its long half-life, norpropoxyphene accumulates if the parent drug is given repeatedly. Norpropoxyphene accumulation is associated with arrhythmias and pulmonary edema, and it is poorly dialyzed di·a·lyze tr. & intr.v. di·a·lyzed, di·a·lyz·ing, di·a·lyz·es To subject to or undergo dialysis. [Back-formation from dialysis. . There have also been reports of apnea, cardiac arrest, and death. Naloxone naloxone /nal·ox·one/ (nal-ok´son) an opioid antagonist, used as the hydrochloride salt in opioid toxicity, opioid-induced respiratory depression, and hypotension associated with septic shock. does not reverse the effects of norpropoxyphene. Long-term use of this agent is highly discouraged, and use in elderly patients is not recommended. The US General Accounting Office has listed propoxyphene among drugs "inappropriate for the elderly" and has emphasized that alternative analgesics are both more effective and safer. Propoxyphene use is generally discouraged. [1-4,7,8,10,11,19,25] Fentanyl fentanyl /fen·ta·nyl/ (fen´tah-nil) an opioid analgesic; the citrate salt is used as an adjunct to anesthesia, in the induction and maintenance of anesthesia, in combination with droperidol (or similar agent) as a neuroleptanalgesic, and is a highly lipophilic lipophilic, adj/n the ability to dissolve or attach to lipids. lipophilic (lipōfil´ik), adj 1. showing a marked attraction to, or solubility in, lipids. 2. opioid analgesic with agonist activity at the [micro]-opioid receptor in the brain, spinal cord, and smooth muscle. The transdermal patch is applied to the skin on alternating sites and is replaced every 3 days. One week should be allowed before altering the dose, and equilibration equilibration /equi·li·bra·tion/ (e-kwil?i-bra´shun) the achievement of a balance between opposing elements or forces. occlusal equilibration is not reached until 6 days after a dosage change. The transdermal delivery system transdermal delivery system: see skin patch. offers continuous fentanyl administration. Increased fat stores, muscle wasting, or altered clearance should be a prescribing caution, and initial dosage should not be greater than 25 [micro]g/hr. A transmucosal (oral cavity) dosage form of fentanyl is also available. Pentazocine pentazocine /pen·taz·o·cine/ (pen-taz´o-sen) a synthetic opioid analgesic, used in the form of the hydrochloride and lactate salts as an analgesic and anesthesia adjunct. , nalbuphine, and butorphanol are the mixed opioid agonist-antagonists. Nalbuphine and pentazocine must be used with caution in patients receiving opioids, to avoid precipitating withdrawal and increasing pain. Pentazocine is an agonist at both K and [sigma] receptors. Dysphoria, nightmares, depersonalization depersonalization /de·per·son·al·iza·tion/ (de-per?sun-al-i-za´shun) alteration in the perception of self so that the usual sense of one's own reality is temporarily lost or changed; it may be a manifestation of a neurosis or another , and visual hallucinations Hallucinations Definition Hallucinations are false or distorted sensory experiences that appear to be real perceptions. These sensory impressions are generated by the mind rather than by any external stimuli, and may be seen, heard, felt, and even are other adverse effects caused by pentazocine. Pentazocine use is discouraged. [1-3,7,11] Butorphanol is an antagonist-agonist at the [micro] receptor. Therapeutic effects also may occur via agonist effects on the K receptor. Opiate abstinence may occur with coadministration of propoxyphene and methadone. Negative side effects can be minimized with administration in small doses, and a nasal deliver form is available. Nalbuphine has both agonist and antagonist properties. The most common adverse reaction is sedation. Buprenorphine is a partial agonist at the [micro] receptors and an antagonist at the K receptors. It may also have some antagonist activity at the [sigma] receptor but lacks dysphoric effects. Buprenorphine is anticipated to be available for oral administration. Buprenorphine has been used for analgesia without producing hemodynamic instability in the management of pain resulting from myocardial infarction. It has a lower incidence of nausea and vomiting Nausea and Vomiting Definition Nausea is the sensation of being about to vomit. Vomiting, or emesis, is the expelling of undigested food through the mouth. than other opioids. Opiate abstinence has not been a clinical event with any coadministered opiates in our clinical practice. [+] ANTIDEPRESSANTS Selective serotonin reuptake inhibitors Selective Serotonin Reuptake Inhibitors Definition Selective serotonin reuptake inhibitors are medicines that relieve symptoms of depression. Purpose (SSRIs) have a limited side-effect profile. Adverse effects most commonly reported include headache, insomnia, anxiety, dizziness, tremors, drowsiness, nausea, vomiting, diarrhea, dyspepsia dyspepsia: see indigestion. , xerostomia xerostomia /xe·ro·sto·mia/ (zer?o-sto´me-ah) dryness of the mouth due to salivary gland dysfunction. xe·ro·sto·mi·a n. , sexual dysfunction, anorexia, and diaphoresis diaphoresis /di·a·pho·re·sis/ (-fah-re´sis) sweating, especially of a profuse type. di·a·pho·re·sis n. Perspiration, especially when copious and medically induced. . Serotonin syndrome can occur when using SSRIs in combination with other medications, ie, MAOIs, dihydroergotamine, tryptophan tryptophan (trĭp`təfăn), organic compound, one of the 20 amino acids commonly found in animal proteins. Only the l-stereoisomer appears in mammalian protein. , dextromethorphan, lithium, nefazodone nefazodone /ne·fa·zo·done/ (ne-fa´zo-don) an antidepressant, used as the hydrochloride salt. ne·fa·zo·done n. , or "tryptans" that block the reuptake of serotonin. Selective serotonin reuptake inhibitors inhibit the CYP-450 enzyme system and cause delayed clearance of certain medications, especially those medications that use CYP-450 1A2, 2D6, and 3A4 enzymes as a substrate for their metabolism. All SSRIs can increase serum levels and decrease clearance of other substrate agents by way of these hepatic enzyme systems. The SSRIs are less effective than other antidepressants for the management of pain. A complete list of drug interactions involving the CYP-450 system and su bstrate drugs that may be used in the management of pain is provided in the Appendix. [1-3,5,7-10,25,27,29] Among the tricyclic antidepressants (TCAs) is amitriptyline, which is hepatically converted to an active metabolite, nortriptyline nortriptyline /nor·trip·ty·line/ (nor-trip´ti-len) a tricyclic antidepressant, used as the hydrochloride salt to treat depression and panic disorder and to relieve chronic severe pain. . Imipramine imipramine /imip·ra·mine/ (i-mip´rah-men) a tricyclic antidepressant of the dibenzazepine class, used as i. hydrochloride or i. pamoate. is transformed by the liver to desipramine desipramine /de·sip·ra·mine/ (des-ip´rah-men) a tricyclic antidepressant of the dibenzazepine class; used as the hydrochloride salt. desipramine a tricyclic antidepressant. . Trazodone trazodone /tra·zo·done/ (tra´zo-don) an antidepressant, used as the hydrochloride salt to treat major depressive episodes with or without prominent anxiety. (not a TCA TCA 1. trichloroacetic acid. 2. tricarboxylic acid cycle (Krebs cycle). TCA Tricyclic antidepressant, see there ) is hepatically converted to meta-chlorophenyl piperazine piperazine /pi·per·a·zine/ (-zen) an anthelmintic used against Ascaris lumbricoides and Enterobius vermicularis; used as the citrate salt. pi·per·a·zine n. (mCPP), a serotonin agonist, and is generally given at bedtime due to its sedative sedative, any of a variety of drugs that relieve anxiety. Most sedatives act as mild depressants of the nervous system, lessening general nervous activity or reducing the irritability or activity of a specific organ. properties. Generally, the adverse effects of TCAs result mostly from cholinergic/muscarinic receptor blockade, [[alpha].sub.2]-adrenergic blockade, histaminergic ([H.sub.1], [H.sub.2]) blockade, and dopaminergic dopaminergic /do·pa·min·er·gic/ (do?pah-men-er´jik) activated or transmitted by dopamine; pertaining to tissues or organs affected by dopamine. do·pa·mi·ner·gic adj. blockade. Receptor blockade of cholinergic cholinergic /cho·lin·er·gic/ (ko?lin-er´jik) 1. parasympathomimetic; stimulated, activated, or transmitted by choline (acetylcholine); said of the sympathetic and parasympathetic nerve fibers that liberate acetylcholine at a ! muscarinic muscarinic /mus·ca·rin·ic/ (mus?kah-rin´ik) denoting the cholinergic effects of muscarine on postganglionic parasympathetic neural impulses. receptors can produce blurry vision, xerostomia, sinus tachycardia, constipation, urinary retention, and memory dysfunction. Blockage of [H.sub.1] and [H.sub.2] receptors produces sedation, dizziness, weight gain, and hypotension hypotension or low blood pressure Condition in which blood pressure is abnormally low. It may result from reduced blood volume (e.g., from heavy bleeding or plasma loss after severe burns) or increased blood-vessel capacity (e.g., in syncope). and potentiates CNS depressant agents. [[alpha].sub.1]-Adrenergic blockade is often associated with postural hypotension and dizziness. Dopamine-receptor blockade has been associated with extrapyramidal syndrome, dystonia dystonia /dys·to·nia/ (-to´ne-ah) dyskinetic movements due to disordered tonicity of muscle.dyston´ic dystonia musculo´rum defor´mans , akathisia, rigidity, tremor, akinesia akinesia /aki·ne·sia/ (a?ki-ne´zhah) absence, poverty, or loss of control of voluntary muscle movements. akinesia al´gera , neuroleptic malignant syndrome neuroleptic malignant syndrome n. Hyperthermia in reaction to the use of neuroleptic drugs, accompanied by extrapyramidal and autonomic disturbances that may be fatal. , tardive dyskinesia, and endocrine changes. Tachycardia and prolonged PR and QRS QRS A pattern seen in an electrocardiogram that indicates the pulses in a heart beat and their duration. Variations from a normal QRS pattern indicate heart disease. Mentioned in: Bundle Branch Block intervals with membrane stabilization occur. Orthostatic hypotension and, in patients who have impaired left ventricular function, congestive heart failure congestive heart failure, inability of the heart to expel sufficient blood to keep pace with the metabolic demands of the body. In the healthy individual the heart can tolerate large increases of workload for a considerable length of time. may occ ur. Bupropion bupropion /bu·pro·pi·on/ (bu-pro´pe-on) a monocyclic compound structurally similar to amphetamine, used as the hydrochloride salt as an antidepressant and as an aid in smoking cessation. (not a TCA) blocks reuptake of both norepinephrine and dopamine and also has relatively few cardiac side effects, minimal (if any) effects on cardiac conduction, and no production of orthostatic hypotension. [1-4,7,28-30] Other receptor-specific antidepressants, such as venlafaxine venlafaxine /ven·la·fax·ine/ (ven?lah-fak´sen) an inhibitor of serotonin and norepinephrine reuptake that potentiates neurotransmitter activity in the central nervous system; used as the hydrochloride salt as an antidepressant and , nefazodone, and mirtazapine, do not currently fit into any broad antidepressant antidepressant, any of a wide range of drugs used to treat psychic depression. They are given to elevate mood, counter suicidal thoughts, and increase the effectiveness of psychotherapy. classification. Venlafaxine (serotonin and norepinephrine reuptake inhibitor Norepinephrine reuptake inhibitors (NRIs), also known as noradrenaline reuptake inhibitors (NARIs), are compounds that elevate the extracellular level of the neurotransmitter norepinephrine in the central nervous system by inhibiting its reuptake from the ), has a complex mechanism of action. It blocks the reuptake of serotonin at low doses, blocks the reuptake of norepinephrine at medium doses, and blocks the reuptake of dopamine at higher doses. Venlafaxine is in effect three drugs in one because of such dose-related, receptor-mediated events. Venlafaxine provides the therapeutic benefits of tertiary and secondary amine amine (əmēn`, ăm`ēn): see under amino group. amine Any of a class of nitrogen-containing organic compounds derived, either in principle or in practice, from ammonia (NH3). antidepressants without the TCA side-effect profile. Venlafaxine also is beneficial in chronic pain, since it lacks clinically relevant CYP-450 interactions and is available in an extended release dosage form. [1-3,30,31] Nefazodone is another antidepressant that acts dually on serotonin. Reuptake inhibition for 5-hydroxytryptamine (5-HT) and norepinephrine occurs, coupled with [5-HT.sub.2] receptor blockade. Some [[alpha].sub.1]-adrenergic inhibition produces orthostatic hypotension. This agent produces two active metabolites: the OH-nefazodone metabolite, which has activity similar to that of nefazodone, and the mCPP metabolite, which is the same metabolite found with trazodone. The mechanism of action of mCPP is that of a 5-HT agonist coupled with mild [5-HT.sub.2] and [5-HT.sub.3] antagonism. This agent shows zero-order kinetics. There is also relevant CYP-450 3A4 inhibition. [1-3,7] Mirtazapine is an atypical antidepressant described as a noradrenergic noradrenergic /nor·ad·ren·er·gic/ (-ah-dren-urj´ik) activated by or secreting norepinephrine. nor·ad·ren·er·gic adj. Stimulated by or releasing norepinephrine. serotonin-specific antagonist. This agent produces therapeutic antagonism at both [[alpha].sub.2] autoreceptors and heteroreceptors, thus facilitating enhanced noradrenergic and serotonin discharge. Mirtazapine's therapeutic benefits include a lack of sexual dysfunction, a decrease in migraine headache, and a decrease in anxiety, agitation, depression and insomnia. Further antagonism occurs at [5-HT.sub.2] receptors (decreasing anxiety and agitation) and at [5-HT.sub.3] receptors (decreasing nausea and GI distress). [H.sub.1]-receptor antagonism at low doses ([less than or equal to]30 mg) produces drowsiness, facilitating sleep and improving appetite. No clinically significant interactions are revealed in the CYP-450 system. A unique dissolve-in-mouth dosage form is available. Mirtazapine is a useful adjuvant agent in the management of chronic pain. [10-29-34] ANXIOLYTIC anxiolytic /anx·io·lyt·ic/ (ang?ze-o-lit´ik) 1. antianxiety. 2. an antianxiety agent. anx·i·o·lyt·ic n. A drug that relieves anxiety. AGENTS The principal modulatory site of the [gamma] aminobutyric acid (GABA GABA ?. GABA abbr. gamma-aminobutyric acid GABA (gamma-aminobutyric acid) A neurotransmitter that slows down the activity of nerve cells in the brain. ) receptor complex is found on its [alpha] subunit and is referred to as the benzodiazepine benzodiazepine (bĕn'zōdīăz`əpēn'), any of a class of drugs prescribed for their tranquilizing, antianxiety, sedative, and muscle-relaxing effects. Benzodiazepines are also prescribed for epilepsy and alcohol withdrawal. or [omega] receptor. Three subtype [omega] receptors have been identified, and it is thought that the [[omega].sub.1] receptor is associated with sedation and that [[omega].sub.2] is associated with anticonvulsant anticonvulsant /an·ti·con·vul·sant/ (-kon-vul´sant) inhibiting convulsions, or an agent that does this. an·ti·con·vul·sant n. A drug that prevents or relieves convulsions. , anxiolytic, and myorelaxant effects. The clinical effects of the [[omega].sub.3] receptor have not yet been thoroughly investigated. The [[omega.sub.2] receptors are associated with memory dysfunction, such as forgetfulness and/or amnesia, because of anterograde anterograde /an·tero·grade/ (an´ter-o-grad?) extending or moving anteriorly. an·ter·o·grade adj. Moving forward. anterograde extending or moving forward. amnesic effects. Clonazepam clonazepam /clo·naz·e·pam/ (klo-naz´e-pam) a benzodiazepine used as an anticonvulsant and as an antipanic agent. clo·naz·e·pam n. offers a therapeutic option among other benzodiazepines Benzodiazepines Definition Benzodiazepines are medicines that help relieve nervousness, tension, and other symptoms by slowing the central nervous system. Purpose Benzodiazepines are a type of antianxiety drugs. . Lorazepam lorazepam /lor·a·ze·pam/ (lor-az´e-pam) a benzodiazepine used as an antianxiety agent, sedative-hypnotic, preanesthetic medication, and anticonvulsant. lor·az·e·pam n. , temazepam temazepam /te·maz·e·pam/ (te-maz´e-pam) a benzodiazepine used as a sedative and hypnotic in the treatment of insomnia. te·maz·e·pam n. , and oxazepam oxazepam /ox·az·e·pam/ (ok-saz´e-pam) a benzodiazepine tranquilizer, used as an antianxiety agent and as an adjunct in the treatment of acute alcohol withdrawal symptoms. ox·az·e·pam n. may be especially useful to patients with liver impairment, because these drugs do not have any active metabolites and are metabolites and are metabolized by phase II processes. [**] ANTICONVULSANTS Anticonvulsants, or antiepileptic drugs (AEDs), have produced therapeutic benefits in a variety of painful neuropathic syndromes. Such agents include carbamazepine carbamazepine /car·ba·maz·e·pine/ (kahr?bah-maz´e-pen) an anticonvulsant and analgesic used in the treatment of pain associated with trigeminal neuralgia and in epilepsy manifested by certain types of seizures. , phenytoin phenytoin /phen·y·to·in/ (fen´i-toin?) an anticonvulsant used in the control of various kinds of epilepsy and of seizures associated with neurosurgery. phen·y·to·in n. , vaiproic acid, tiagabine, gabapentin, oxcarbazepine, vigabatrin, zonisamide, lamotrigme, and topiramate and have been described elsewhere. [1-3] Topiramate has several mechanisms of action (1) diminishing action potential by sodium channel blockade, (2) increasing GABA frequency activation at GABA receptor sites, (3) selectively antagonizing kainate activation at kainate/[alpha]-amino-3-hydroxy-5-methyl-4-isoxazolepropinate (AMPA AMPA Alpha-Amino-3-Hydroxy-5-Methyl-4-Isoxazole Propionic Acid AMPA A-Amino-3-Hydroxy-5-Methyl-4-Isoxazolepropionic Acid AMPA Agricultural Marketing Programs Act (Canada) AMPA American Medical Publishers Association ) receptor sites, (4) providing glutamate antagonism, (5) calcium channel blockade, and (6) producing an acidosis acidosis /ac·i·do·sis/ (as?i-do´sis) 1. the accumulation of acid and hydrogen ions or depletion of the alkaline reserve (bicarbonate content) in the blood and body tissues, decreasing the pH. 2. that results in diminished N-methyl-D-aspartate (NMDA NMDA N-methyl-D-asparate ) mediated excitation and increased [GABA.sub.A] mediated inhibition. Additionally, some carbonic anhydrase inhibition occurs. Absorption is rapid with bioavailability bioavailability /bio·avail·a·bil·i·ty/ (bi?o-ah-val?ah-bil´i-te) the degree to which a drug or other substance becomes available to the target tissue after administration. bi·o·a·vail·a·bil·i·ty n. of about 80%. The AMPA and kainate receptors have a role in mediating neuropathic pain. Pharmacokinetics are linear, with dose-proportional increases in plasma concentration, and the steady state is achieved in about 4 days. Plasma protein binding A drug's efficacy may be affected by the degree to which it binds to the proteins within blood plasma. The less bound a drug is, the more efficiently it can traverse cell membranes or diffuse. is only 13% to 17%. Metabolism is minimal, with 70% of a dose recovered unchanged in the urine; elimination half-life is 18 to 23 hours. The drug is cle ared by hemodialysis. Clearance is diminished in those patients with moderate renal impairment and/or hepatic impairment. Side effects of topiramate include paresthesia paresthesia /par·es·the·sia/ (par?es-the´zhah) morbid or perverted sensation; an abnormal sensation, as burning, prickling, formication, etc. par·es·the·sia or par·aes·the·sia n. and anorexia, to name a few. A [less than or equal to]% incidence of renal calculi requires adequate hydration hydration /hy·dra·tion/ (hi-dra´shun) the absorption of or combination with water. hy·dra·tion n. 1. The addition of water to a chemical molecule without hydrolysis. 2. . Central nervous system-related side effects are dose-related and are generally not observed at doses of less than 250 mg/day. Cognitive motor slowing and speech or work difficulty are seen only in a minimal percentage of patients when high doses are initiated, with rapid incremental dose changes, or with coprescription of other AEDs. In our clinical practice with a large number of patients, CNS event occurrence was not a clinically relevant finding. Clinical applications may be available for bipolar disorder, neuromodulation, neurostabilization and disease modification, obesity treatment, epilepsy, bulimia, neuropathic pain syndromes, essential tremor, and migraine headache. SKELETAL MUSCLE RELAXANTS Baclofen acts as a [GABA.sub.B] agonist in hyperpolarized membranes. Carisoprodol is metabolized in the liver by CYP-450 2C19 to an active metabolite, meprobamate meprobamate (məprō`bəmāt'), tranquilizing drug that acts as a depressant of the central nervous system and is commonly used in the treatment of anxiety and sometimes schizophrenia. . It should be avoided in patients with renal or hepatic disease. With prolonged use, this drug is associated with dependence. Use of carisoprodol is discouraged. Cyclobenzaprine, a frequently used muscle relaxant, is structurally similar to TCAs. Side effects include drowsiness, dizziness, confusion, ataxia ataxia (ətăk`sēə), lack of coordination of the voluntary muscles resulting in irregular movements of the body. Ataxia can be brought on by an injury, infection, or degenerative disease of the central nervous system, e.g. , xerostomia, and anticholinergic effects. Contraindications are similar to those of TCAs. Long-term use of cyclobenzaprine should be avoided, and the manufacturer recommends that administration not exceed a 3-week period. [1-3] TOPICAL AGENTS Capsaicin capsaicin /cap·sa·i·cin/ (kap-sa´i-sin) an alkaloid irritating to the skin and mucous membranes, the active ingredient of capsicum; used as a topical counterirritant and analgesic. cap·sa·i·cin n. is a topical analgesic that may inhibit the synthesis, transport, and release of substance P, a peripheral neurotransmitter of pain. Capsaicin is used to treat pain associated with neuralgia neuralgia (n  răl`jə, ny–), acute paroxysmal pain along a peripheral sensory nerve. ,
neuropathy, and arthritis. Lidocaine lidocaine /li·do·caine/ (li´do-kan) an anesthetic with sedative, analgesic, and cardiac depressant properties, applied topically in the form of the base or hydrochloride salt as a local anesthetic; also used in the latter form as a (5%) topical patches are available
for the relief of allodynia (painful hypersensitivity hypersensitivity, heightened response in a body tissue to an antigen or foreign substance. The body normally responds to an antigen by producing specific antibodies against it. The antibodies impart immunity for any later exposure to that antigen. ) and chronic
painful postherpetic neuralgia; the patches are to be applied for 12
hours daily only.
SLEEP-PROMOTING AGENTS Treating disorders of initiating and maintaining sleep due to pain requires pharmacologic intervention when sleep hygiene methods have proved less than satisfactory. Selection of a pharmacologic agent necessitates pharmacodynamic and pharmacokinetic decisions that address a patient's specific needs. Zaleplon, a nonbenzodiazepine hypnotic, effects the [[omega].sub.1] receptor. Absorption is rapid, bioavailability is about 30%, and metabolism is primarily by aldehyde oxidase and by minor CYP-450 3A4 substrate-forming inactive metabolites. The mean half-life is about 1 hour. Therefore, the rapid onset, absence of active metabolites, absence of CYP-450 drug interactions of clinical consequence, rapid clearance from the body, and absence of major memory impairments make this agent highly suitable for use in patients with insomnia due to pain. [1-3] MISCELLANEOUS AGENTS Several other medications can be used to relieve pain. Clonidine clonidine /clo·ni·dine/ (klo´ni-den) a centrally acting antihypertensive agent, used as the hydrochloride salt; also used in the prophylaxis of migraine and the treatment of dysmenorrhea, menopausal symptoms, opioid withdrawal, and and tizanidine are both imidazole imidazole /im·id·az·ole/ (im?id-az´ol) 1. a heterocyclic organic compound in which two of five ring atoms are nitrogen; used as an insecticide. 2. any of a class of antifungal compounds containing this structure. [[alpha].sub.2]-agonists and are believed to inhibit pain transmission by modulating norepinephrine and 5-HT release in the dorsal horn on the lamina LAMINA - A concurrent object-oriented language. ["Experiments with a Knowledge-based System on a Multiprocessor", Third Intl Conf Supercomputing Proc, 1988]. of the spinal cord. Potentiation potentiation /po·ten·ti·a·tion/ (po-ten?she-a´shun) 1. enhancement of one agent by another so that the combined effect is greater than the sum of the effects of each one alone. 2. posttetanic p. of [micro]-opioid receptors and a decrease in the wide range of neuron excitability excitability readiness to respond to a stimulus; irritability. are additional mechanisms of [[alpha].sub.2] agonists, which also modulate specific calcium channels. Botulinum toxin type A botulinum toxin type A Botox, Botox Cosmetic, Dysport (UK), Vistabel (UK) Pharmacologic class: Neurotoxin Therapeutic class: Neuromuscular blocker Pregnancy risk category C Actionhas been used investigationally for some painful syndromes.CONCLUSION By following this pharmacologic review, the clinician is able to evaluate pharmacotherapies for a specific patient's needs, basing the selection on personal clinical experiences, patient-specific concerns, sides effects, adverse effects, drug interaction, pharmacodynamics, pharmacokinetics, and pharmacotherapeutics. From the Departments of Anesthesiology, Family Medicine, Pharmacology, and Psychiatry, Rush Medical College and The Rush Pain Center at Rush Presbyterian St. Luke's Medical Center, Chicago, Ill; and The Pain Center of Rush North Shore, Skokie, Ill. Reprint requests to Robert L. Barkin, MBA MBA abbr. Master of Business Administration Noun 1. MBA - a master's degree in business Master in Business, Master in Business Administration , PharmD, Rush Pain Center, 1725 w Harrison, Professional Bldg 3, Suite 550, Chicago, IL 60612. (*.) Reference [1-3,5,7,8,10,11,19-22,24]. (+.) References [1-4,7,10,11,18-20,22,25,26]. (**.) References [1-3,9,19,21,27,28,31,35,36]. References (1.) Barkin RL, Lubenow TR, Bruehl S, et al: Management of chronic pain. Part I. Dis Mon 1996; 42:389-454 (2.) Barkin RL, Lubenow TR, Bruehl S, et al: Management of chronic pain. Part II. Dis Mon 1996; 42:457-507 (3.) Barkin RL, Oetgen J, Barkin SJ: Pharmacotherapeutic management opportunities utilized in chronic nonmalignant pain. Supplement to Drug Topics. Montvale, NJ, Medical Economics Publishers, 1999 (4.) Schwer WA, Barkin RL, Katz WA, et al: The Management of Chronic Pain in the Elderly. Langhorne, Pa, Medical Communications Inc, 2000 (5.) McCarberg BH, Barkin RL: Long-acting opioids for chronic pain: pharmacotherapeutic opportunities to enhance compliance, quality of life, and analgesia. Am J Ther 2001; 8:181-186 (6.) Barkin RL: Pharmacotherapy for nonmalignant pain (Letter) . Am Fam Phys 2001; 63:848 (7.) Barkin RL, Schwer WA, Barkin SJ: Recognition and management of depression in primary care: a focus on the elderly. a pharmacotherapeutic overview of the selection process among the traditional and new antidepressants. Amf Ther 2000; 7:205-226 (8.) Barkin RL, Fawcett J: The management challenges of chronic pain: the role of antidepressants. Am J Ther 2000; 7:31-47 (9.) Barkin RL, Barkin DS: Pharmacotherapeutic challenges in the elderly: polypharmacy, drug interactions, compliance and side effects/adverse-effects predictions. Anesth Today 1998; 9:12-19 (10.) Barkin RL, Chor PN, Braun BG, et al: A trilogy case review highlighting the clinical and pharmacologic applications of mirtazapine in reducing polypharmacy for anxiety, agitation, insomnia, depression, and sexual dysfunction. primary care companion. J Clin Psychiatry 1999; 1:172-175 (11.) Barkin RL, Barkin DS, Barkin SJ, et al: Opiate, opioids, and centrally acting analgesics and drug interactions: the emerging role of the psychiatrist. emergency medicine update. Medical Update for Psychiatrists 1998; 3:196-202 (12.) Barkin RL, Sable KS: Caution recommended for prescribing and administering COX 1/COX 2 and COX 2 specific NSAIDs. Pharmacol Ther 2000; 25:196-202 (13.) Gaynes BL, Barkin RL: Analgesics in ophthalmic practice: a review of the oral non-narcotic agent tramadol. Optom Vis Sci 1999; 76:455-461 (14.) Barkin RL: Three challenging, diverse pain patients' requirements for patient-specific treatment, economic and therapeutic implications of analgesia in hospital pharmacy. (Poster presentation) Annual Meeting, American Society of Hospital Pharmacists, Atlanta, Ga, December 8, 1997 (15.) Barkin RL: Focus on tramadol: a centrally acting analgesic for moderate to moderately severe pain. Analgesic Dig 1996;1:11-12 (16.) Barkin RL: Cancer pain treatment insights. Pharmacotherapy 1997; 17:397-398 (17.) Barkin RL: Focus on tramadol: a centrally acting analgesic for moderate to moderately severe pain. Formulary 1995; 30:321-325 (18.) Barkin RL: Alternative dosing for tramadol aids effectiveness. Formulary 1995; 30:542-543 (19.) Huff J, Barkin RL, Lagatuta F: A primary care clinician's and consultant's guide to medicating for pain and anxiety associated with outpatient procedures. Am J Ther 1994; 1:186-190 (20.) Loh VT, Barkin RL: Appropriate use of opiates/opioids in migraine headache pain management. Continuing Pharmacy Education Monograph, Princeton, NJ, Bristol-Myers Squibb Co, 1998, pp 1-28 (21.) Barkin RL, Richtsmeier AY: Alternative agents in pharmacologic management of sickle cell pain crisis complicated by acute pancreatitis. Am J Ther 1995; 2:819-823 (22.) Leiken J, Barkin RL: Nalbuphine vs meperidine in sickle cell anemia sickle cell anemia n. A chronic, usually fatal inherited form of anemia marked by crescent-shaped red blood cells, occurring almost exclusively in Blacks, and characterized by fever, leg ulcers, jaundice, and episodic pain in the joints. DICP DICP Defense Intelligence Counterdrug Program DICP Dublin Inner City Partnership DICP Drop In Communications Package (MKV SOC) . Ann Pharmacother 1990; 24:781-782 (23.) Barkin RL: Pain management update: IV. Morphine infusions in children. Resident Staff Phys 1988; 34:11-13 (24.) Richtsmeier A, Barnes SD, Barkin RL: Ventilatory arrest with morphine patient-controlled anesthesia in a child with renal failure. Am J Ther 1997; 4:255-257 (25.) Hahn A, Oestreich S, Barkin RL: Pharmacology in Nursing. St. Louis, CV Mosby Co, 16th Ed, 1986 (26.) Barkin RL: Withdrawal syndrome is not precipitated when butorphanol is added to opiate or opioid therapy. a comment on intranasal butorphanol-induced apraxia apraxia Disturbance in carrying out skilled acts, caused by a lesion in the cerebral cortex; motor power and mental capacity remain intact. Motor apraxia is the inability to perform fine motor acts. Ideational apraxia is loss of the ability to plan even a simple action. reversed by naloxone. Pharmacotherapy 1996; 16:969 (27.) Bone RC, Hayden WR, Levine RL, et al: Recognition, assessment and treatment of anxiety in the critical care patient. Dis Mon 1995; 41:293-359 (28.) Barkin RL, Braun BG, Kluft RP: The dilemma of drug therapy for multiple personality disorder Multiple Personality Disorder Definition Multiple personality disorder, or MPD, is a mental disturbance classified as one of the dissociative disorders in the fourth edition of the Diagnostic and Statistical Manual of Mental Disorders (DSM-IV). patients. Treatment of Multiple Peronality Disorders. Braun BG (ed) . Washington, DC, American Psychiatric Press, 1986, pp 107-132 (29.) Braverman B, O'Connor C, Barkin RL: Pharmacology, physiology and anesthetic management of antidepressants. Pharmacology and Physiology in Anesthesia. Philadelphia, Lippincott Health Care Publications, 1993, pp 1-15 (30.) Fawcett J, Barkin RL: Efficacy issues with antidepressants. J Clin Psychiatry 1997; 58 (suppl 6) :32-39 (31.) Bhatia S, Bhatia S, Barkin R: Mirtazapine revisited (Letter) . Am Fam Phys 1997; 56:2190-2192 (32.) Fawcett J, Barkin RL: A meta-analysis of eight randomized ran·dom·ize tr.v. ran·dom·ized, ran·dom·iz·ing, ran·dom·iz·es To make random in arrangement, especially in order to control the variables in an experiment. , double-blind, controlled clinical trials of mirtazapine for the treatment of patients with major depression and symptoms of anxiety. J Clin Psychiatry 1998; 59:123-127 (33.) Davis J, Barkin RL: Clinical pharmacology of mirtazapine: revisited (Letter) . Am Fam Phys 1999; 60:1101 (34.) Fawcett J, Barkin RL: Review of the results from clinical studies on the efficacy, safety and tolerability of mirtazapine for the treatment of patients with major depresson. J Affect Disord 1998; 51:267-285 (35.) Barkin RL, Leikin JB, Barkin SJ: Noncardiac chest pain: a focus upon psychogenic psychogenic /psy·cho·gen·ic/ (-jen´ik) having an emotional or psychologic origin. psychogenic (sī´kojen´ik), adj causes. Am J Ther 1994; 1:321-326 (36.) Richtsmeier HA, Barkin RL, Alexander M: Benzodiazepines for acute pain in children. J Pain Symptom Manage 1992; 7:492-495
TABLE. Pharmacokinetics of COX-2 Inhibitors
Celecoxib
Bioavailability NA
[T.sub.max] median (hr) -2.8
[C.sub.max] ([micro]g/mL) 0.7 ([greater than]65 yr, 40%
higher)
AUC ([micro]g/hr/mL) 6.3 (40% increase in black patients
and 50% increase in patients
[greater than or euqal to] 65 yr)
Volume of distribution at steady
state (L/kg) 400
Plasma protein binding
(%) -97
Concentration at steady state [greater than or equal to]5
(days)
Elimination half-life (hr) 11.2 (fasting state)
GYP-45O substrate hepatic 2C9
metabolism
Inhibition of hepatic CYP-450 2D6
Metabolism Oxidation
Elimination by urine (%) 27
Elimination by feces (%) 57
Sulfonamide allergy Yes
Dosages
Osteoarthritis 200 mg/day or 100 mg twice daily
Rheumatoid arthritis 100 or 200 mg twice daily
Acute pain and primary -
dysmenorrhea
Familial adenomatous polyposis 200 mg twice daily
Rofecoxib
Bioavailability 93%
[T.sub.max] median (hr) 2.0-3.0
[C.sub.max] ([micro]g/mL)
0.2
AUC ([micro]g/hr/mL)
3.3
Volume of distribution at steady
state (L/kg) 91
Plasma protein binding
(%) 87
Concentration at steady state 4
(days)
Elimination half-life (hr) 17
GYP-45O substrate hepatic None
metabolism
Inhibition of hepatic CYP-450 None
Metabolism Reduction (extrahepatic)
Elimination by urine (%) 72
Elimination by feces (%) 14
Sulfonamide allergy None
Dosages
Osteoarthritis 12.5 mg/day; increase
to 25 mg in PM
Rheumatoid arthritis -
Acute pain and primary 50 mg/day; additional dose
dysmenorrhea of 50 mg/day PM
Familial adenomatous polyposis -
COX-2 = Cyclooxygenase-2; NA = not applicable; [T.sub.max] =
time to maximum concentration; [C.sub.max] = maximum serum
concentration; AUC = area under the curve; CYP-450 = cytochrome
P-450.
Adapted from Barkin and Sable. [12]
APPENDIX: Pharmacotherapeutic Inhibitors, Inducers, and
Substrates of Cytochrome P-450 (CYP-450) Enzyme With a
Focus on Agents Used in Pain Management
Xenobiotic
CYP-450 Enzyme Inhibitor
IA2
Polymorphism: No Anastrozole
Cimetidine
Ciprofloxacin
Citalopram
Clarithromycin
Diethyldithiocarbamate
Diltiazem
Enoxacin
Erythromycin
Fluoroquinolones
Fluvoxamine
Grapefruit juice
(6',7'-dihydroxybergamotin)
Grepafloxacin
Isoniazid (INH)
Ketoconazole
Levofloxacin
Mexiletine
Mibefradil
Mirtazapine (very weak)
Moclobemide
Nalidixic acid
Norfloxacin
Omeprazole
Paroxetine
Propranolol
Ritonavir
Sertraline
Tacrine
Zileuton
IIA6
Diethyldithiocarbamate
Ketoconazole
Letrozole
Methoxsalen
Miconazole
Pilocarpine
Ritonavir
IIB6
Diethyldithiocarbamate
Ketoconazole
Orphenadrine
Quinidine
Xenobiotic
CYP-450 Enzyme Inducer
IA2
Polymorphism: No Bupropion (possible)
Caffeine
Carbamazepine (CBZ)
Charcoal-broiled foods
Cigarette smoke
Cruciferous vegetable
Dihydralazine
Omeprazole
Phenobarbital
Phenytoin
Primidone
Rifampin
Ritonavir
IIA6
IIB6
Bupropion (possible)
Carbamazepine (CBZ)
Phenobarbital
Phenytoin
Primidone
Xenobiotic
CYP-450 Enzyme Substrate
IA2
Polymorphism: No Acetaminophen (APAP)
Antipyrine
Bupropion (possible)
Caffeine
Chlorzoxazone
Clozapine
Cyclobenzaprine (demethylation)
Dantrolene
Diazepam
Diethylstilbestrol (DES)
Estradiol
Flutamide
Fluvoxamine
Grepafloxacin
Haloperidol
Isotretinoin
Lidocaine
Methadone
Mexiletine
Mirtazapine
Naproxen
Olanzapine
Ondansetron
Phenacetin
Phenothiazines
Pramipexole
Procarbazine
Propafenone
Propranolol
Prostaglandins
Riluzole
Ritonavir
Ropinirole
Ropivacaine
Tacrine
Tamoxifen
Testosterone
Theophylline
Tiagabine
TCAs (N-demethylation)
Amitriptyline
Clomipramine
Desipramine
Imipramine
Nortriptyline
Verapamil
Warfarin (R form)
Zileuton
Zolpidem
IIA6
Letrozole
Nicotine
Ritonavir
Tamoxifen
IIB6
Bupropion
Cyclophosphamide
Diazepam (demethylation)
Halothane
Ifosfamide
Mianserin
Mephenytoin (S-isomer
demethylated)
Tamoxifen
Temazepam
IIC8, IIC9, IIC1O
Polymorphism: Yes Anastrozole (2C8/2C9)
(poor metabolizers); Amiodarone (2C9)
[greater than or equal to]20% Cannabinols
Whites,
2% Asians, Chloramphenicol (2C9)
2% African Americans Cimetidine (2C9)
Clopidogrel (2C9)
Delavirdine
Diclofenac (2C9)
Diethyldithiocarbamate (2C8)
Disulfiram (2C9)
Efavirenz (2C9)
Felbamate (2C8)
Fluconazole (2C9)
Fluoxetine (suspected) (2C9)
Flurbiprofen (2C9)
Fluvastatin (2C9)
Fluvoxamine (2C9)
Isoniazid (INH)
Ketoconazole
Ketoprofen (2C9)
Leflunomide
Metronidazole (2C9)
Miconazole (2C9)
Omeprazole (2C8/2C9)
Phenylbutazone (2C9)
Ritonavir (2C9, 2C1O)
Sertraline (suspected)
Sulfonamides (2C9)
Topiramate
Trimethoprim/sulfamethiazole
(TMP/SMX) (2C9)
Troglitazone (2C9)
Zafirlukast (2C9)
IIC18-19
Polymorphism: Cimetidine (2C18)
Yes (2C19); Citalopram (2C19)
18% Japanese, Delavirdine
20% African Americans, Efavirenz (2C19)
20% Asians, Felbamate (2C19)
3%-5% Whites Fluoxetine (2C19)
IIC8, IIC9, IIC1O
Polymorphism: Yes Barbiturates
(poor metabolizers); Bupropion (possible)
[greater than or equal to]20% Carbamazepine (2C9) (CBZ)
Whites,
2% Asians, Clopidogrel (2C9)
2% African Americans Dexamethasone
Ethanol (2C9)
Phenobarbital (2C9)
Phenytoin (2C9)
Rifampin (2C9)
Rifapentine (2C8/2C9)
IIC18-19
Polymorphism: Bupropion (possible)
Yes (2C19); Rifampin (2C19)
18% Japanese,
20% African Americans,
20% Asians,
3%-5% Whites
IIC8, IIC9, IIC1O
Polymorphism: Yes Amitriptyline (2C9)
(poor metabolizers); Aspirin (ASA)
[greater than or equal to]20% Barbiturates (2C9)
Whites,
2% Asians, Benzphetamine (2C8)
2% African Americans Bupropion
Carbamazepine (CBZ)
Carvedilol (2C9)
Celecoxib (2C9)
Clomipramine (2C9)
Cyclophosphamide
Dapsone (2C9)
Delavirdine (2C9)
Diazepam (2C8/2C9)
Diclofenac (2C8/2C9)
Donepezil
Dronabinol (2C9)
Efavirenz (2C9)
Ethosuximide
Flurazepam
Flurbiprofen (2C9)
Fluoxetine (2C9)
Fluvastatin (2C9)
Glimepiride (2C9)
Glipizide
Glyburide
Hexobarbital (2C9)
Ibuprofen (2C9)
Imipramine (2C8/2C9)
Indomethacin (2C8/2C9)
Irbestartan
Isotretinoin (2C8)
Lansoprazole
Leflunomide (2C9)
Losartan (2C9)
Mefenamic acid (2C9)
Mephenytoin (2C9)
Mephobarbital (2C9)
Mirtazapine (2C9)
Montelukast (2C9)
Naproxen (2C9)
Nifedipine
NSAIDs (2C9)
Omeprazole (2C8)
Paclitaxel (2C8)
Phenytoin (2C9)
Piroxicam (2C9)
Propranolol
Retinoic acid (2C8)
Ritonavir (2C9)
Sildenafil (2C9, minor)
Sulfonamide (including celecoxib)
Tamoxifen (2C9)
TCAs (tertiary amines) (2C9)
Terbinafine (2C9)
Tetrahydrocannabinol ([delta]THC)
(2C9)
Tolbutamide (2C8/2C9)
Tolcapone
Torsemide (2C9)
Valproic acid
Warfarin S-form (more active) (2C9)
Zafirlukast (2C9)
Zileuton (2C9)
IIC18-19
Polymorphism: Amitriptyline (2C19)
Yes (2C19); Barbiturates (2C19)
18% Japanese, Carisoprodol (2C19)
20% African Americans, Carvedilol
20% Asians, Citalopram (minor) (2C19)
3%-5% Whites Clomipramine (2C19)
Fluvoxxamine (2C19)
Ketoconazole
Letrozole
Omeprazole (2C19)
Oxcarbazepine (2C19)
Ritonavir (2C19)
Telmisartan (2C19)
Topiramate (2C19) minor
Tolbutamide (2C19)
Tranylcypromine (2C19)
Troglitazone (2C19)
IID6
Subject to genetic Amiodarone None
Polymorphism sublet Amitriptyline
Of 5%-10% of Whites, Bupropion
1%-10% Asians; Celecoxib
2%-8% African Americans: Chloroquine
Poor metabolizers or Cimetidine
Deficits in activity Citalopram (weak)
Clomipramine
Codeine
Delavirdine
Desipramine
Dextropropoxyphene
Diphenhydramine
Doxorubicin
Fenfluramine
Flecainide
Fluoxetine
Fluphenazine
Fluvoxamine
Haloperidol
Imipramine
Lomustine
Methadone
Metoprolol
Mexiletine
Mibefradil
Mirtazapine (very weak)
Moclobemide
Nicardipine
Norfluvoxamine
Norfluoxetine
Nortriptyline
Parpxetine
Perphenazine
Primaquine
Propafenone
Propafenone
Propoxyphene
Quinidine
Ranitidine
Ritonavir
Sertraline (suspected)
TCAs
Thioridazine
Diazepam (2C19)
Divalproex sodium VPA (2C19)
Hexobarbital (2C19)
Irbesatan
Imipramine (2C19)
Lamsoprazole (2C19)
Moclobemide (N-demethylation)
Omeprazole (2C19)
Naproxen (2C18)
Nordazepam (2C19)
Pantoprazole (2C19)
Phenytoin
Piroxicam (2C18)
Propranolol (2C19)
Retinoic acid (2C18)
Ritonavir (2C19)
Tertiary amines TCA (2C19)
Tiagabine
Tolbutamide (2C19)
Topirmate
Valproate VPA (2C19)
Valproic acid (2C19)
Tetrahydrocannabinol ([detla]THC)
S-isomer (2C18)
Warfarin S-isomer (2C18)
IID6
Subject to genetic Amiodarone
Polymorphism sublet Antidysrhythmics, type IC
Of 5%-10% of Whites, [beta]-A Adrenergic blockers (some)
1%-10% Asians; Bisoprolol
2%-8% African Americans: Bupropion
Poor metabolizers or Captopril
Deficits in activity Carvedilol
Chloroquine
Chlorpeniramine
Chlorpormazine
Citalopram (minor)
Clomipramine
Clozapine
Codeine
Cyclobenzaprine (hydroxylation)
Debrisoquine
Delavirdine
Dexfenfluramine
Dextromethorphan (DM)
Dolasertron
Donepezil
Encainide
Ethylmorphine
Fenfluramine
Flecainide
Fluozetine
Fluphenazine
Fluvoxamine
Halofantrine
Haloperidol
Hydrocodone
Hydroxyamphetamine
Labetalol
Lansoprazole
Lidocaine
Loratadine
Maprotiline
MCPP (metabolite of
trazodone & nefazodone)
Meperidine
Methadone
Methamphetamine
Metoprolo (R&S enantiomers)
Mexiletine
Timolol
Venlafaxine (very weak)
Vinblastine
Vinorelbine
Yohimbine
Ziprasidone
IIE1
Polymorphism: Yes Diethyldithiocarbamate Ethanol (ETOH)
Disulfiram Isoniazid (INH)
Ritonavir
IIA1
Spironolactone
Mirtazapine
Morphine (major pathway
phase II glucuronidation
to M-6-G and M-3-G)
Neuroleptics
Nicotine
Nortriptyline
Olanzipine
Omeprazole
Ondansetron
Opiate analgesics
Oxamniquine
Oxycodone
Paroxetine
Pentazocine
Perphenazine
Phenformin
Phenothiazines
Pindolol
Primaquine
Proguanil
Propafenone
Propoxyphene
Propranolol (minor)
Risperidone
Ritonavir
Ropivacaine
Selegiline
Sertraline
Sparteine
Tamoxifen
TCAs (hydroxylation/high
first-pass effeccs)
Amitriptyline
Clomipramine
Desipramine
Doxepin
Imipramine
Nortriptyline
Thebaine
Tiagabine
Timolol
Tolterodine
Tramadol (M1 metabolite zone)
Trazodone
Trimipramine
Venlafaxine
Zolpidem
Zonisamide
IIE1
Polymorphism: Yes Acetaminophen (hepatotoxic
metabolite-NAPQI)
Benzene
Bupropion
Carbon tetrachloride
Chlorzoxazone
Dapsone
Enflurane
Ethanol (minor)
Halothane
Isoflurane
Isoniazid (INH)
Methoxyflurane
Mexiletine
Mirtazapine (minor)
Ondansetron
Ritonavir
Sevoflurane
Tamoxifen
Theophylline
IIA1
IIIA3
Cimetidine
Nefazodone
Ranitidine
Sertraline
IIIA4
Polymorphism: No Acetaminophen (APAP)
(Significant differences in Amiodarone
CYPIII A4 expression Anastrozole
among patients) Antibiotics
Calcium channel
blockers (some)
Cannabinol
Cimetidine
Clarithromycin
Clotrimazole
Danazol
Delavirdine
Dextropropoxyphene
Diethyldithiocarbamate
Dihydroergotamine (DHE)
Diltiazem
Efavirenz
Erythromycin
Ethinyl-estradiol
Fluconazole
Fluoxetine
Fluvoxamine
Gestagen
Grapefruit juice
(6,7-dihydroxybergamotin)
Indinavir
Interferon-y
Itraconazole
Ketoconazole
Lovastatin
Macrolide antibiotics
Metronidazole
Mibefradil
Miconazole
Mirtazapine (very weak)
Naringerin
Nefazodone
Nelfinavir
Nevirapine
Nifedipine
Norfloxacin
Norfluoxetine
Omeprazole
Paroxetine
Propanolol
Propoxyphene
Quinidine
Quinine
Ranitidine
Ritonavir
Saquinavir
Sertraline
Troglitazone
Trolcandomycin
Verapamil
Zafirlukast
Ziprasidone
IIIA3
Erythromycin
IIIA4
Polymorphism: No Aconiazide
(Significant differences in Barbiturates
CYPIII A4 expression Carbamazepine (CBZ)
among patients) Dexamethasone
Efavirenz
Ethosuximide
Glucocorticoids
Griseofulvin
Macrolide antibiotics
Nevirapine
Oxcarbazpine
Phenobarbital
Phenylbutazone
Phenytoin (PHT)
Prednisone
Primidone
Quinidine
Rifabutin
Rifampicin
Rifampin
Rifapentine
Sulfinpyrazone
Troglitazone
Verapamil
IIIA3
Midazolam
IIIA4
Polymorphism: No Acetaminophen (APAP)
(Significant differences in Alfentanil
CYPIII A4 expression Alprazolam
among patients) Amiodarone
Amlodipine
Androgens
Antiarrhythmics
Astemizole
Atorvastatin
Azithromycin
Azole antifungals
Benzndiazepincs (short-acting
triazole type)
Benzphetamine
Bromocriptine
Bupropion (possible)
Busulfan
Caffeine
Calcium channel
blockers (most)
Cannabinol ([delta]THC)
Carbamazepine (CBZ)
Carvedilol
Cerivastatin
Chlorpromazine
Cisapride
Citalopram
Clarithromycin
Clindamycin
Clonazepam
Clotrimazole
Clozapine
Cocaine
Codeine (demethylation)
Corticosteroids
Cortisol
Cyclobenzaprine
(demethylation)
Cyclophosphamide
Cyclosporine (CSP)
Dantrolene
Dapsone
Delavirdine
Dexametbasone
Dextromethorphan (DM)
Diazepam (minor)
Digitoxin
Digoxin
Dihydroergotamine (DHE)
Dihydropteridine calcium
channel blockers
Diltiazem
Disopyramide
Docetaxel
Dolasetron
Domperidone
Donepezil
Doxorubicin
Dronabinol
Enalapril
Erythromycin
Estradiol
Estrogens (oral contraceptives)
Ethinyl estradiol
Ethosuximide
Xenobiotic
CYP-450 Enzyme Inhibitor Inducer
Ethylmorphine
Etoposide
Felodipine
Fentanyl
Fexofenadine
Fluoxetine
Flutamide
Fluvoxamine
Glyceryl trinitrate
Granisetron
Grepafloxacin
Halofantrine
Haloperidol
Hydrocortisone (cortisol)
Irbesartan
Ifosfamide
Indinavir
Isradipine
Ketoconazole
Lansoprazole (minor)
Letrozole
Lidocaine
Lorasadine
Losartan
Macrolide antibiotics
Mephenytoin
Metronidazole
Mibefradil
Miconazole
Midazolam (3A5)
Mifepristone
Mirtazapine
Montelukast
Navelbine
Nefazodone
Nelfinavir
Nevirapine
Nicardipine
Nifedipine
Nimodipine
Nisoldipine
Nitrendipine
Omeprazole
Ondansetron
Paclitaxel
Pantoprazole
Phenobarbital
Phenytoin (PHT)
Pimozide
Pravastatin
Prednisone
Primidone
Progesterone
Propafenone
Protease inhibitor (HIV-1)
Quetiapine
Quinine
Retinoic acid
Rifampin
Ritonavir
Ropivacaine
RU 486
Salmeterol
Saquinavir
Sertindole
Sertraline
Sibutramine
Sildenafil
Simvastatin
Sufentanil
Tacrolimus (FK506)
III A5-7
Clotrimazole Phenobarbital
Ketoconazole Phenytoin (PHT)
Metronidazole Primidone
Miconazole Rifampin
Troleandomycin
Tamoxifen
TCAs (demethylation)
Amitriptyline (minor)
Clomipramine
Imipramine
Teniposide
Terfenadine
Testosterone
Theophylline
Thiothixene
Tiagabine
Tolterodine
Toremifene
Tramadol (Ml metabolite)
Trazodone
Tretinoin
Triazolam
Troglitazone
Troleandomycin
Venlafaxine (N-demethylation)
Verapamil
Vinbiastine
Vincristine
Vindesine
Warfarin (less active, R form)
Zileuton
Zolpidem
Zonisamide
III A5-7
Ethinyloestradiol
Lovastatin (3A5)
Midazolam (3A5)
Nifedipine (3A5)
Quinidine
Terfenadine
Testosterone
Triazolam
Vinblastine
Vincristine
TCA = Tricyclic antidepresant; ASA = acetylsalicylic acid; NSAID =
nonsteroidal anti-inflammatory drug; VPA = valproic acid; mCPP =
metacholorophenyl piperazine; m-6-G = morphine-6-glucuronider; M-3-G =
morphine-3-glucuronide; HIV-1 = human immunodeficiency virus-1.
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