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Transcript
PART 2: DRUGS AFFECTING THE CENTRAL NERVOUS SYSTEM I: Analgesic drugs. Overview: Medications that relieve pain without causing loss of consciousness are classified as analgesics. They are also commonly to as painkillers. There are various classes of analgesics, determined by their chemical structures and mechanisms of action. Here we will focus on the opioid analgesics, which are normally used to treat moderate to severe pain. Often drugs from other chemical categories are added to the opioid regimen as adjuvant analgesic drugs. Opioid agonists: 1. 2. 3. 4. 5. 6. Codeine. Fentanyl. Meperidine (bethidine). Methadone. Morphine. Oxycodone. Partial agonist: 1. Buprenorphine. 2. Pentazocine. Opioid antagonists 3. Naloxone. 4. Naltrexone. Nonopioids 1. Paracetamol. 2. Tramadol. Pain is most commonly defined as an unpleasant sensory and emotional experience associated with either actual or potential tissue damage. It is a very personal and individual experience. Pain can be defined as whatever the patient says it is, and it exists whenever the patient says it does. GATE THEORY Several theories attempt to explain pain transmission and pain relief. The most common and well described is the gate theory. First, the tissue injury causes the release of several substances from injured cells, such as bradykinin, histamine, potassium, prostaglandins, and serotonin. The release of these pain-mediating chemicals initiates action potentials at the distal end of sensory nerve fibers through receptors known as nociceptores. These nerve impulses are conducted along sensory nerve fibers and activate pain receptors in the dorsal horn of the spinal cord. It is here that the so called gates are located. These gates regulate the flow of sensory nerve impulses. If impulses are stopped by a gate at this junction, no impulses are transmitted to the higher centers of the brain. Conversely, if the gates permit a sufficient number and intensity of action potentials to be conducted from the spinal cord to the cerebral cortex, the sensation of pain is then felt. The gate is innervated by nerve fibers that originate in the brain and modulate the pain sensation by sending impulses to the gate, either keeping the gate closed or allowing it to open so that the brain is stimulated and pain is sensed. The cells that control the gate have a threshold. Impulses that reach these cells must rise above this threshold before an impulse is permitted to travel up to the brain. The level of stimulus needed to produce a painful sensation is referred to as the pain threshold. PAIN RECEPTORS: There are three main receptors believed to be involved in pain. - The mu receptors. Less important but still involved in pain sensations are the kappa and delta receptors. Pain receptors are located in both the central nervous system (CNS) and various body tissues. When these receptors are stimulated transmission of nerve impulses related to pain are inhibited. Opioid drugs also react with these receptors and thus relieve pain, so these receptors also called OPIOID RECEPTORS. All opioids act by binding to specific opioid receptors in the CNS to produce effects that mimic the action of endogenous peptide neurotransmitters (for example, endorphins, enkephalins, and dynorphins) Figure below illustrate the four processes of nociception Endogenous analgesic substances (body’s pain killers): The body is equipped with certain endogenous neurotransmitters known as enkephalins and endorphins. These substances are produced within the body to fight pain and are considered the body’s painkillers. Both are capable of bonding with opioid receptors and inhibiting the transmission of pain impulses, in a manner similar to that of opioid analgesic drugs. These endogenous substances are released whenever the body experiences pain. Adjuvant analgesic drugs. The goals of pain management include reducing and controlling pain, improving body function and quality of life. Drugs from other chemical categories are often added to the opioid regimen as adjuvant drugs. This adjuvant drug therapy may include NSAIDs, antidepressants, anticonvulsants and corticosteroids. This approach allows the use of smaller dosages opioids. This reduces some of the adverse effects that are seen with higher doses of opioids. It permits drugs with different mechanisms of action to produce synergistic effects. Pharmacology overview: Opioid drugs: Opioid analgesics are very strong pain relievers. They can be classified according to their chemical structure or their action at specific receptors. Of the 20 different natural alkaloids available from the opium poppy plant, only three are clinically useful: morphine, codeine, and papaverine. Of these, only morphine and codeine are pain relievers; papaverine is a smooth muscle relaxant. Relatively simple synthetic chemical modifications of these opium alakaloids are produced the three different chemical classes of opioids: morphine-like drugs, meperidine-like drugs, and methadone-like drugs. Mechanism of action and drug effects: Opioid analgesics can be characterized according to their mechanism of action. They can be agonists, agonists-antagonists (partial agonists), or antagonists (nonanalgesic).Agonists: binds to a pain receptor in the brain and causes an analgesic response. Partial agonist: binds to a pain receptor but causes a weaker pain response than a full agonist. Antagonist: binds to a pain receptor but does not reduce pain signals, it reverses the effects of agonists and partial agonists at the receptor site. A. Agonists: morphine, meperidine (pethidine), methadone, fentanyl,codeine. B. Partial agonists: pentazocine, nalbuphine, buprenorphine, butorphanol. C. Antagonists: naloxone, naltrexone. Indications: Main use: to alleviate moderate to severe pain The degree to which pain is relieved or unwanted adverse effects occur depends on the specific drug, the preceptors to which it binds, and its chemical structure. Opioids are also used for: Cough center suppression Treatment of diarrhea Balanced anesthesia (use a combinations of drugs to produce anesthesia). 1- Morphine: They are often used to control postoperative and other types of pain. Because morphine is available in injectable form,is often first-line analgesics in the immediate postoperative setting. Morphine rapidly enters all body tissues, including the fetuses of pregnant women, and should not be used for analgesia during labor. 2- Codeine: Codeine is a naturally occurring opioid that is a weak analgesic compared to morphine. It should be used only for mild to moderate pain. Is the most commonly used opioid for cough suppression, sometimes opioid-related cough suppressants have a depressant effect on CNS and cause sedation. To avoid this problem, dextromethorphan a nonopioid cough suppressant, is often given instead. 3- Fentanyl: used commonly in combination with anesthetics during surgery, it not only used to relieve pain but also to maintain a balanced state of anesthesia. Used of fentanyl injection for management of postoperative and procedural pain has become popular due to its rapid onset and short duration. 4- Methadone: Methadone is a synthetic, orally effective opioid that induces less euphoria and has a longer duration of action than morphine.can be used as analgesic and in the controlled withdrawal of dependent abusers from heroin and morphine. Oral methadone is administered as a substitute for the opioid of abuse, and the patient is then slowly weaned from methadone. The withdrawal syndrome with methadone is milder but more protracted (days to weeks) than that with other opioids. 5- Meperidine (Pethidine) it is used for acute pain. Can be administered orally or I.M. Meperidine is very lipophilic and has anticholinergic effects, resulting in an increased incidence of delirium as compared to other opioids. 6- Buprenorphine: partial agonists used for opioid detoxification Use with extreme caution if: Respiratory insufficiency Elevated intracranial pressure Sleep apnea Is contraindicated in: severe asthma and known allergy Adverse effects: Euphoria CNS depression leads to respiratory depression which is the most serious adverse effect Nausea and vomiting Urinary retention, Diaphoresis, flushing and constipation Toxicity and management of overdose: The opioid antagonists naloxone (IV) and naletroxone (PO) can reverse the adverse effects induced by the opioid drug, such as respiratory depression. These drugs are used in the management of both opioid overdose and opioid addiction. When treating an opioid overdose or toxicity, the nurse must recognize the signs and symptoms of withdrawal. A gradual dosage reduction after chronic opioid use, when possible, generally helps to minimize the risk and severity of withdrawal symptoms. Respiratory depression: Stimulation of the patient may be adequate to reverse mild hypoventilation. Is this is unsuccessful, ventilator assistance using a bag and mask or endotracheal intubation may be needed to support respiration. Administration of opioid anatagonists may also necessary to reverse severe respiratory depression. Naloxone half-life is about 1 hour. Interactions: Co-administration of opioids with alcohol, antihistamines, barbiturates, benzodiazepine and other CNS depressants can result in additive respiratory depression, seizures, and hypotension. Other analgesics (Tamadol and Paracetamol): A. Acetaminophen (paracetamol): -Mechanism of action: it blocks peripheral pain impulses by inhibition of prostaglandin synthesis. It also lowers febrile body temperatures by acting on hypothalamus. -Indications: Is indicated for the treatment of mild to moderate pain and fever is the drug of choice as antipyretic in children. -Contraindications: known allergy, severe liver disease and G-6-PD -Adverse effects: is generally well tolerated. Possible adverse effects include rash, nausea and vomiting. -Toxicity: the ingestion of large doses can cause hepatic necrosis. Acute hepatotoxicity can usually reverse with acetylcysteine, where as long-term toxicity is more likely to be permanent. The maximum daily dose is 4000mg and Acetylcysteine is more effective when given within 10 hours of overdose. It is available as IV and OP dose. B. Tramadol: It is a centrally acting analgesic creates a weak bond to the mu receptors and inhibit reuptake of both norepinephrine and serotonin. Is indicated for severe to moderately severe pain adverse effects are include drowsiness, dizziness, headache, nausea, constipation and respiratory depression. Drug is available as injection (IV, IM) and PO (tablet and capsules). Analgesics: Nursing implications: Perform a thorough pain assessment, including pain intensity and character, onset, location, description, precipitating and relieving factors, type, remedies, and other pain treatments Assessment of pain is now being considered a “fifth vital sign” Rate pain on a 0 to 10 or similar scale Be sure to medicate patients before the pain becomes severe so as to provide adequate analgesia and pain control Pain management includes pharmacologic and nonpharmacologic approaches; be sure to include other interventions as indicated Patients should not take other medications or over-the-counter preparations without checking with their physician Instruct patients to notify physician for signs of allergic reaction or adverse effects Acetaminophen: patient education about the signs and symptoms of hepatotoxicity (bleeding, loss of energy, fever, and sore throat). Maximum dose: 4 g. Tramadol: if dizziness, blurred vision, or drowsiness occurs, the nurse should assist the patient to minimize the risk of fall and injury. Opioids: Ensure safety measures, such as keeping side rails up, to prevent injury. Withhold dose and contact physician if there is a decline in the patient’s condition or if vital signs are abnormal, especially if respiratory rate is less than 10 to 12 breaths/min. Constipation is a common adverse effect and may be prevented with adequate fluid and fiber intake Monitor for Therapeutic Effects: Decreased complaints of pain Decreased severity of pain Increased periods of comfort Improved activities of daily living, appetite, and sense of well-being Decreased fever (acetaminophen) II: Anesthetics. Overview: Anesthetics are drugs that cause complete or partial loss of sensation. This state of reduced neurologic function is called anesthesia. Anesthesia is further classified as general or local. General anesthesia normally involves complete loss of consciousness, loss of body reflexes, elimination of pain and other sensations throughout the entire body, and skeletal and smooth muscle paralysis, including paralysis of respiratory muscles. This loss of normal respiratory function requires mechanical or manual ventilator support to avoid brain damage and suffocation (death from respiratory arrest). Local anesthesia does not involve paralysis of respiratory function but does involve elimination of pain sensation in the tissue innervated by anesthetized nerves. Pharmacology overview 1- General anesthetics: -General anesthetics are drugs that induce general anesthesia and are most commonly used to induce anesthesia during surgical procedures. -General anesthesia is achieved by the use of one or more drugs. Often a synergistic combination of drugs is used, which allows for smaller doses of each drug and better control of the patient’s anesthetized state. -Inhalational anesthetics are volatile liquids or gases that are vaporized or mixed with oxygen to induce anesthesia. General anesthetics:inhaled Nitrous oxide. Halothane. Isoflurane. Sevoflurane. General anesthetics:parenteral Ketamine Etomidate. Propofol. Thiopental. Adjunctive anesthetic drugs Benzodiazepines. Antihistamines. Opioids. Barbiturates.anticholinergics . Neuromascular blocking drugs Pancuronium. Vecuronium. Atracurium. Succinylcholine. Local anesthetics Bupivacaine. Lidocaine (Xylocaine) mepivacaine (Carbocaine) procaine (Novocain) tetracaine (Pontocaine) -Parenteral anesthetics usually given IV and are used for induction and/or maintenance of general anesthesia, induction of amnesia, and as adjuncts to inhalation anesthetic. The specific goal varies with the drug. In addition, there are also adjunct anesthetics. Adjunct drugs can be thought as “helper drugs” when their use complements the use of any other drug(s) and are used simultaneously with general anesthetics for anesthesia induction, sedation, reduction of anxiety, and amnesia. The simultaneous use of both general anesthetics and adjuncts is called balanced anesthesia. Adjuncts: Neuromuscular blocking agents. Sedative hypnotics or anxiolytics. Propofol, benzodiazepines, barbiturates, hydroxyzine and promethazine. Opioid analgesics. Anticholinergics (atropine). Antiemetics (ondansetron). Note that propofol can be used as a general anesthetic and/or sedative-hypnotic, depending on the dose. Mechanism of action and drug effects: The drugs vary widely in their chemical structures, and their mechanism of action is not easily explained by a structure-receptor relationship. The concentrations of various anesthetics required to produce a given state of anesthesia also differ greatly. Fat-soluble drugs are stronger anesthetics than water-soluble drugs. Nerve cell membranes have high lipid content, as does the blood-brain barrier. Lipid-soluble anesthetic drugs can therefore easily cross the blood-brain barrier to concentrate in nerve cell membranes. The overall effect of general anesthetics is a progressive reduction of sensory and motor CNS functions. The degree and speed of this process varies with the anesthetics and adjuncts used along with their dosages and routes of administration. General anesthesia initially produces a loss of the senses of sight, touch, taste, smell, and hearing, along with loss of consciousness. Cardiac and pulmonary functions are usually the last to be interrupted; these are the classical “stages” of anesthesia. Again, mechanical ventilator support is usually necessary. In more extensive surgical procedures, especially those involving the heart, pharmacologic cardiac support may also be required. Adverse Effects: Vary according to dosage and drug used Sites primarily affected o Heart, peripheral circulation, liver, kidneys, respiratory tract Myocardial depression is commonly seen Malignant hyperthermia is an uncommon, but potentially fatal. o Occurs during or after general anesthesia or use of the NMBC succinylcholine o Sudden elevation in body temperature (greater than 104° F) o Tachypnea, tachycardia, muscle rigidity o Life-threatening emergency o Treated with dantrolene (skeletal muscle relaxant) Drug profiles: The dose of any anesthetic depends on the complexity of the surgical procedure to be performed and the physical characteristics of the patient. With regard to pharmacokinetics, all of the general anesthetics have a rapid onset of action along with rapid elimination upon discontinuation. Anesthesia is maintained intraoperatively by continuous administration of the drug. Isoflurane: Is fluorinated ether that is a chemical isomer of the older fluorinated ether enflurane. It has a more rapid onset of action, causes less cardiovascular depression, and has a little or no associated toxicity. Sevoflurane: Is the newest fluorinated ether and is now widely used. Its pharmacokinetics, with rapid onset and rapid elimination, make it especially useful in outpatient surgery settings. It is also nonirritating to the airway, which greatly facilitates induction of an unconscious state, especially in pediatric patients. Ketamine: It is a unique drug with multiple properties. Given IV, it can be used for both general anesthesia and moderate sedation. This drug is highly lipid soluble and penetrates the blood-brain barrier rapidly, which results in a rapid onset of action. It has a low incidence of reduction of cardiovascular, respiratory, and bowel function. Adverse effects include hallucinations. Propofol (Diprivan): Is a parentral general anesthetic used for the induction and maintenance of general anesthesia and also for sedation for mechanical ventilation in ICU settings. In lower doses it can be used as a sedative-hypnotic for moderate sedation. Some states allow nurses to administer propofol as part of a moderate sedation protocol. Is also typically well tolerated, producing few undesirable effects. Moderate Sedation: It also called conscious sedation, and procedural sedation. It’s anesthesia that does not necessarily cause complete loss of consciousness and does not normally cause respiratory arrest. This technique uses combination of several drugs from different groups. Drugs may be given by IV, IM, spinal or oral routes. The net effect is a type of anesthesia that allows the patient to relax, yet still maintain his or her own open airway, as well as respond to verbal commands. Used for diagnostic procedures and minor surgical procedures that do not require deep anesthesia 2- Local anesthetics: Local anesthetics are the second major class of anesthetics. They reduce pain sensations at the level of peripheral nerves. They also called regional anesthetics because they render a specific portion of the body insensitive to pain. They do this by interfering with nerve transmission in specific areas of the body, blocking nerve conduction only in the area in which they are applied without causing loss of consciousness. They are most commonly used in clinical settings in which loss of consciousness is undesirable or unnecessary. These include childbirth, dental procedures, and diagnostic procedures. Types of local anesthesia: 1-Central: Spinal or intraspinal anesthesia: Anesthesia drugs are injected into the area near the spinal cord within the vertebral column. Intraspinal anesthesia is commonly accomplished by one of two injection techniques: intrathecal and epidural. Intrathecal anesthesia: involves injection of anesthesia into the subarachnoid space. Epidural anesthesia: involves injection of anesthesia via a small catheter into the epidural space without puncturing the dura. 2-Peripheral: Infilteration: small amounts of anesthetic solution are injected into the tissue that surrounds the operative site. Nerve block: anesthetic solution is injected at the site where the nerve innervates a specific are SUCH AS A tissue. Topical anesthesia: the anesthetic drug is applied directly onto the surface of the skin, eye, or any mucous membrane to relieve pain or prevent it from being sensed. Mechanism of action and drug effects: Local anesthetics work by rendering a specific portion of the body insensitive to pain by interfering with nerve transmission in that area. They block the generation and conduction of impulses through all types of nerve fibers by blocking the movement of certain ions important to this process. Adverse effects; Possible systemic effects of the administration of local anesthetics include effects on circulatory and respiratory function. The systemic adverse effects depend on where and how the drug is administered. Such adverse effects are somewhat unlikely unless large quantities of a drug that are injected. Drug profiles: Lidocaine: is one of the most commonly used local anesthetics. It is available in several strengths, both alone and in different concentrations with epinephrine, and is used for both infiltration and nerve block anesthesia. Lidocaine is also available in topical form. Parenteral lidocaine is also used to treat certain cardiac dysrhythmias. 3- Neuromuascular blocking drugs (NMBDs): These drugs prevent nerve transmission in skeletal and smooth muscles, leading to paralysis. They are often used as adjuncts with general anesthetics. NMBDs also paralyze respiratory muscles, so mechanical ventilation is required to prevent brain damage or death by suffocation. Mechanism of action: They are classified into two groups based on mechanism of action: depolarizing and nondepolarizing. Depolarizing work similarly to the neurotransmitter acetylcholine, they are competitive agonists. Nondepolarizing also bind to acetylcholine receptors at neuromuscular receptors at neuromuscular junction, and they block the usual action of acetylcholine, therefore these drugs are competitive antagonists of acetylcholine. NMBDs: Depolarizing: succinylcholine. Nondepolarizing: Short acting: mivacurium. Intermerdiate-acting drugs: atracurium, rocuronium and vecuronium. Long-acting drugs: dexacurium, pancuronium and tubocurarine. Indications: Main use: maintaining controlled ventilation during surgical procedures Endotracheal intubation (short-acting) To reduce muscle contraction in an area that needs surgery Diagnostic drugs for myasthenia gravis Adverse effects: Few when used appropriately May cause: Hypotension (blockade of autonomic ganglia) Tachycardia (blockade of muscarinic receptors) Hypotension (release of histamine) Drug profiles: Succinylcholine: Is the only currently available drug in the depolarizing subclass of NMBDs. This drug stimulates the same neuron as Ach and produces the same physiological responses initially. Succinylcholine is metabolized more slowly. Because of this slower metabolism, repolarizing cannot occur. As long as sufficient concentrations are present, the muscles lose its ability to contract, and flaccid muscle paralysis results. Because of its quick onset of action (less than 1 min), succinylcholine is most commonly used to facilitate endotracheal intubation. Pancuronium: Is a long-acting nondepolarizing NMBD. It’s used as an adjunct to general anesthesia to facilitate endotracheal intubation and to provide skeletal muscle relaxation during surgery or mechanical ventilation. Its most commonly employed for long surgical procedures that require prolonged muscle paralysis. Vancuronium: Is an intermediate-acting nondepolarizing NMBD. It is used as an adjunct to general anesthesia to facilitate tracheal intubation and to provide skeletal muscle relaxation during surgery or mechanical ventilation, and is one of the most commonly used NMBDs. Long-term used in the ICU setting has resulted in prolonged paralysis and subsequent difficulty in weaning. Nursing implications: Always assess past history of surgeries and response to anesthesia Assessment is vital during preoperative, intraoperative, and postoperative phases Vital signs Baseline lab work, ECG Oxygen saturation ABCs (airway, breathing, circulation) Monitor all body systems Nursing considerations during the perioperative phase include: Preoperative phase Intraoperative phase Postoperative phase Each phase has its own complex and very specific nursing actions Watch for sudden elevations in body temperature, which may indicate malignant hyperthermia During recovery, monitor for cardiovascular depression, respiratory depression, and complications of anesthesia Implement safety measures during recovery, especially if motor or sensory loss occurs because of local anesthesia Reorient patient to his or her surroundings Teach the patient about postoperative turning, coughing, deep breathing III. Antiepileptic drugs Traditional antiepileptic drugs: Disease overview: - Phenobarbital. Epilepsy: - Phenytoin . Epilepsy is the most common chronic neurologic illness. It results from excessive electrical activity of neurons located in the superficial area of the brain known as the cerebral cortex. The terms convulsive, seizure, and epilepsy are often used interchangeably, but they do not have the same meaning. -Benzodiazepines: diazepam, clonazepam A seizure is a brief episode of abnormal electrical active in the nerve cells of the brain, which may or may not lead to a convulsion. A convulsion is a more severe seizure characterized by involuntary spasmodic contractions of any or all voluntary muscles throughout the body. - Carbamazepine (Tegretol), Oxcarbazepine (Trileptal). - Valproic acid. Newer antiepileptic drugs: Gabapentin (neurontin). Lamotrigine (Lamictal), Levetiracetam (Keppra). Topiramate (Topamax). Epilepsy is chronic, recurrent pattern of seizures. These excessive electrical discharges can often be detected by an electroencephalogram (EEG), which is commonly obtained to help diagnose epilepsy. Because up to 50% of patients with epilepsy have normal EEGs, a careful history is important for accurate diagnosis. Other applicable diagnostic tests include skull radiography, computed tomography, and magnetic resonance imaging. -Primary epilepsy: Epilepsy without an identifiable cause is known as or idiopathic epilepsy. -Secondary epilepsy: Epilepsy has a distinct cause, such as trauma, infection, cerebrovascular disorder, or other illness, also some drugs can cause epilepsy. - Febrile seizure occurs in children aged 6 months to 5 years and by definition be caused by fever. Children usually outgrow the tendency to have such seizures, and thus these seizures do not constitute a chronic illness. Status epilepticus: In status epilepticus, two or more seizures occur without recovery of full consciousness in between episodes. These may be focal or primary generalized, convulsive or nonconvulsive. Status epilepticus is life threatening and requires emergency treatment usually consisting of administration of a fast-acting medication such as a benzodiazepine, followed by a slower-acting medication such as phenytoin. Pharmacology overview: Antiepileptic drugs: The goal of antiepileptic drug therapy is to control or prevent seizures while maintaining a reasonable quality of life. Many antiepileptic drugs have adverse effects. In most cases, the therapeutic goal is to maximally reduce the incidence of seizures while minimizing drug-induced toxicity. A number of antiepileptic drugs are available. Sometimes, a combination of drugs must be given to control the disorder. Generally, single-drug therapy must fail before two-drug or multidrug therapy is attempted. Antiepileptic drugs should never be stopped abruptly unless a severe adverse effect occurs. Therapeutic drug monitoring of serum drug concentrations provides a useful guideline in assessing the effectiveness of therapy. Maintaining serum drug levels within therapeutic ranges therapeutic ranges helps not only to control seizures but also to reduce adverse effects. However, each patient should be monitored individually, and the dosages adjusted based on the individual case. Successful control of a seizure disorder hinges on selection of the appropriate drug class and drug dosage, avoidance of drug toxicity, and patient compliance with the treatment regimen. Mechanism of action: As with many classes of drugs, the exact mechanism of action of the antiepileptic drugs is not known with certainty. However, strong evidence indicates that they alter the movement of sodium, potassium, calcium, and magnesium. The changes in the movement of these ions induced by antiepileptic drugs result in more stabilized and less excitable cell membranes. Regardless of mechanism, however, the overall effect is that antiepileptics stabilize neurons and keep them from becoming hyper excited and generating excessive nerve impulses to adjacent neurons. Some work by enhancing the effects of the inhibitory neurotransmitter gamma-aminobutyric acid (GABA). Indications: Antiepileptic drugs are chiefly used for the long-term maintenance treatment of epilepsy. However, they are also useful for the acute treatment of convulsions and status epilepticus. In these cases the therapy is typically diazepam, which is considered by many to be the drug of choice. Once status epilepticus is controlled, long-term drug therapy is begun with other drugs for the prevention of future seizures. Drug profiles: A. Benzodiazepines Benzodiazepines bind to GABA inhibitory receptors to reduce firing rate. Most benzodiazepines are reserved for emergency or acute seizure treatment due to tolerance. However, clonazepam and clobazam may be prescribed as adjunctive therapy for particular types of seizures. Diazepam is also available for rectal administration when oral administration is not possible. B. Carbamazepine (Tegretol): - - It was marketed in the late 1960s for the treatment of epilepsy in adults after its efficacy and safety for the treatment of trigeminal neuralgia was proved. Carbamazepine blocks sodium channels, thereby inhibiting the generation of repetitive action potentials in the epileptic focus and preventing their spread. Carbamazepine is effective for treatment of focal seizures and, additionally generalized tonic–clonic seizures, trigeminal neuralgia, and bipolar disorder. Carbamazepine is associated with autoinduction of hepatic enzymes. Autoinduction is a process in which, over time, a drug stimulates the production of enzymes that enhance its own metabolism, which leads to lower than expected drug concentrations. Hyponatremia may be noted in some patients, especially the elderly, and may necessitate a change in medication. C.Gabapentin: - - Gabapentin is a chemical analogue of GABA, a major neurotransmitter that inhibits brain activity. It is indicated as an adjunct drug for the treatment of partial seizures and for prophylaxis of partial seizures. Its precise mechanism of action is not known. Also gabapentin is effective as a single-drug therapy for the new-onset epilepsy. It is also commonly used to treat neuropathic pain. Adverse effects include CNS and GI symptoms. D.Phenobarbital: - Phenobarbital is used primarily in the treatment of status epilepticus when other agents fail. Is an effective prophylactic drug for the control of febrile seizures In developing countries, however, oral Phenobarbital is often the drug of choice for routine seizure prophylaxis because of its lower cost compared with the newer drugs. Phenobarnital associated with physical dependence and withdrawal syndrome. The most common adverse effect is sedation. Contraindications include known drug allergy, liver or kidney impairment, and respiratory illness. Phenobarbital interacts with many drugs because it is a major liver enzyme inducer. Phanobarbital is available in oral and injectable forms. E.Phenytoin: - - Phenytoin is primarily indicated for the management of tonic-clonic and partial seizures. Contraindications include known drug allergy and heart conditions that involve bradycardia. The most common adverse effects are lethargy, abnormal movements, and mental confusion. Long-term phenytoin therapy can cause gingival hyperplasia, acne, and hirsutisim. Phenytoin can interact with other medications for two reasons. First, it is highly bound to plasma proteins and competes with other highly protein-bound medications for binding sites. Second, it induces hepatic enzymes. Phenytoin is generally well tolerated, highly effective, and relatively inexpensive. It can also be given intravenously if needed. Most often, however, phenytoin is taken orally. Valproic acid: - Valproic acid is used primarily in the treatment of generalized seizures. It has also been shown to be effective in controlling partial seizures. Contraindications include known drug allergy, liver impairment, and urea cycle disorders. Common adverse effects include drowsiness; nausea, vomiting, and other GI disturbances; tremor; weight gain; and transient hair loss. The most serious adverse effects are hepatotoxicity and pancreatitis. The main reason for the drug interactions with valproic acid are protein binding and liver metabolism. The drug is available in both oral and injectable. Nursing Implications: Oral drugs Take regularly, same time each day with meals to reduce GI upset Do not crush, chew, or open extended-release forms Intravenous forms Follow manufacturer’s recommendations for IV delivery—usually given slowly and monitor vital signs during administration Avoid extravasation of fluids Teach patients to keep a journal to monitor: Response to AED (Antiepileptic drugs) Seizure occurrence and descriptions Adverse effects Instruct patients to wear a medical alert tag or ID and AEDs should not be discontinued abruptly Driving may be impaired until drug levels stabilize Teach patients that therapy is long term and possibly lifelong (not a cure) Monitor for therapeutic effects: Decreased or absent seizure activity Monitor for adverse effects Mental status changes, mood changes, changes in level of consciousness. Eye problems, visual disorders, Sore throat, fever (blood dyscrasias may occur with hydantoins) Many others Benzodiazepines: IV. Sedatives and hypnotics. Overview: Drugs that have a calming effect or that depress the CNS are referred to as sedatives and hypnotics. Anxiolytic: drug used to depress the central nervous system (CNS); prevents the signs and symptoms of anxiety. Sedatives reduce nervousness, excitability, and irritability without causing sleep. Hypnotics cause sleep and have a much more potent effect on the CNS than do sedatives. Many drugs can act in the body as either a sedative or a hypnotic, depending on dose and patient responsiveness, and for this reason are called sedative-hypnotics. -Long acting: Diazepam, lorazepam -Short acting: Alprazolam, Midazolam Nonbenzodiazepines: Zaleplon. Zolpidem. Ramelteon. Barbiturates: Ultrashort acting: thiopental. Short acting: pentobarbital, secobarbital. Intermediate acting: butabarbital. Long acting: Phenobarbital. Sedative-hypnotics can be classified chemically into three main groups: barbiturates, benzodiazepines, and miscellaneous drugs. 1- Anxiety: Anxiety is the unpleasant state of mind chiefly characterized by a sense of dread and fear. Persistent anxiety is divided clinically into several distinct disorders, including the following: Obsessive-compulsive disorder. Post-traumatic stress disorder. Generalized anxiety disorder. Panic disorder with or without agoraphobia. Social phobia. Simple phobia. Anxiety is a normal physiologic emotion. Anxiety may occur as a result of a wide range of medical illness (e.g., cardiovascular or pulmonary disease, hypothyroidisim and hypoglycemia). - 1- Anxiolytic drugs: Benzodiazepines. Buspirone. Beta-blockers. Antideprassants. 1- Benzodiazepines: Diazepam, lorazepam, midozolam. Mechanism of action and drug effects: All anxiolytic drugs decrease anxiety by reducing overactivity in the CNS. Benzodiazepines seem to exert their effects by depressing activity in the areas of the brain called the brainstem and the limbic system. Benzodiazepines are believed to accomplish this by increasing the action of gammaaminobutyric acid, which is an inhibitory neurotransmitter in the brain that inhibits nerve transmission in the CNS. Indications: Benzodiazepines have a variety of therapeutic applications. They are commonly used for: - - - - Anxiety relief. Sleep disorders--- Commonly prescribed benzodiazepines for sleep disorders include intermediate-acting temazepam and short-acting triazolam Skeletal muscle relaxation-----Diazepam is useful in the treatment of skeletal muscle spasms Treatment of seizure disorders----Clonazepam is occasionally used as an adjunctive therapy for certain types of seizures, whereas lorazepam and diazepam are the drugs of choice in terminating status epilepticus Amnesia---The shorter-acting agents are often employed as premedication for anxietyprovoking and unpleasant procedures, such as endoscopy, dental procedures, and angioplasty. Midazolam is a benzodiazepine used to facilitate amnesia while causing sedation prior to anesthesia. Finally, benzodiazepines receptors in the CNS are in the same area as those that play a role in alcohol addiction. Therefore, some benzodiazepines are used in the treatment and prevention of the symptoms of alcohol withdrawal--- chlordiazepoxide, clorazepate, diazepam, lorazepam, and oxazepam are useful in the acute treatment of alcohol withdrawal and reduce the risk of withdrawal-related seizures. When these drugs are used to treat insomnia, it is generally recommended that they be used in short term to avoid dependency. Contraindications: Contraindications to the use of benzodiazepines are known drug allergy, narrow-angle glaucoma, and pregnancy. Adverse effects: The adverse effects are associated with their use are usually mild and primarily involve the CNS. The more commonly reported undesirable effects are headache, drowsiness, paradoxical excitement or nervousness, dizziness or vertigo, cognitive impairment, and lethargy. Also they can create a significant fall hazard in elderly patient. Toxicity and management of overdose: Somnolence, Confusion, Coma, and Diminished reflexes Do not cause hypotension and respiratory depression unless taken with other CNS depressants Treatment: symptomatic and supportive. Use Flumazenil as an antidote. Drug profiles: Diazepam: Diazepam was the first clinically available benzodiazepine drug. It has varied uses, including treatment of anxiety, procedural sedation and anesthesia adjunct, anticonvulsant therapy, and skeletal muscle relaxation. It is available in oral, rectal and injectable forms. 2- Buspirone: Buspirone is an attempt to produce an anxiolytic drug without adverse effects. It appears to have no sedative action or risk of dependence; its only adverse effects appear to be occasional nausea and headache. 3- Antidepressants: - Will be discussed in the next chapter. 2- Insomnia: - Insomnia can, however, cause feelings of anxiety, inability to concentrate and general debility. It is necessary to find out if there is some reason for failing to sleep. These reasons may include: Anxiety and stress. Depression. Physical illness. Pain. physiology of sleep: Sleep is defined as a transient, reversible, and periodic state of rest in which there is a decrease in physical activity and consciousness. Sleep research involves study of the patterns of sleep, or what is sometimes referred to as sleep architecture. The architecture of sleep consists of two basic elements that occur cyclically: rapid eye movement (REM) sleep and non-rapid eye movement (non-REM) sleep. Prolonged sedative-hypnotic use may reduce the cumulative amount of REM sleep; this is known as REM interference. This can result in daytime fatigue. On discontinuance of a sedative-hypnotic drug, REM rebound can occur in which the patient has an abnormally large amount of REM sleep, often leading to frequent and vivid dreams. Pharmacology overview: 1- Benzodiazepines. Benzodiazepines (BDZ) are classified as either sedatives-hypnotics or anxiolytics depending on their primary usage. However, any of these drugs can function along a continuum as a sedative and/or hypnotic and/or anxiolytic depending on the dosage and patient sensitivity to drug action. 2- Nonbenzodiazepines. Zaleplon and zolpidem. Benzodiazepines used to be the most commonly prescribed sedative-hypnotic drugs; however, the nonbenzodiazepine drugs are now the most frequently used. There are five benzodiazepines commonly used as sedative-hypnotic drugs. In addition, there are several miscellaneous drugs that are used primarily as hypnotics. They function much like benzodiazepines but are chemically distinct from them. Zolpidem: It is also a short-acting hypnotic. It’s has a lower incidence of daytime sleepiness compared to benzodiazepines. 3- Ramelteon: - Is the newest prescription hypnotic. This drug is structurally similar to the hormone melatonin, which is believed to regulate daynight sleep cycles in the body. Ramelteon works as agonist at the body’s melatonin receptors in the CNS. Is used as hypnotic, its lack dependency effect. It potentially has a shorter duration of action than other hypnotics and is therefore indicated primarily for patients who have difficulty with sleep onset rather than sleep maintenance. Its use is contraindicated in cases of severe liver disease. 4- Barbiturates: They were first introduced into clinical use in 1903 and were the standard drugs for treating insomnia and producing sedation. Barbiturates can produce many unwanted adverse effects. They are habit forming and have a low therapeutic index. Barbiturates can be classified into four groups based on their onset and duration of action. Mechanism of action and drug effects: They act primarily on the brainstem in an area called the reticular formation. Their sedative and hypnotic effects are dose related, and they act by reducing the nerve impulses traveling to the area of the brain called the cerebral cortex. Their ability to inhibit nerve impulse transmission is in part due to their ability to potentiate the action of inhibitory neurotransmitter GABA. Indications: Ultra short-acting: thiopental Anesthesia for short surgical procedures, anesthesia induction, and control of convulsions. Short-acting and intermediate Sedation/sleep induction and control of convulsive conditions Long-acting: Phenobarbital. Sleep induction, epileptic seizure prophylaxis Contraindications: Contraindications to barbiturate include known drug allergy, significant respiratory difficulties, pregnancy and severe kidney or liver disease. Adverse effects: They are enzyme inducers, they stimulate the action of enzymes in the liver for the metabolism of many drugs, and this shortens the duration of action of many drugs. Body System CNS Respiratory GI Other Adverse Effects Drowsiness, lethargy, vertigo, mental depression. Respiratory depression, apnea, bronchospasms, cough. Nausea, vomiting, diarrhea, constipation Agranulocytosis, hypotension, Stevens-Johnson syndrome 5- Antihistamines like promethazine. Nursing implications: Give hypnotics 30 to 60 minutes before bedtime for maximum effectiveness in inducing sleep (depends on drug’s onset) Most benzodiazepines cause REM rebound and a tired feeling the next day; use with caution in the elderly Instruct patients to avoid alcohol and other CNS depressants Check with physician before taking any other medications, including over-the-counter medications Rebound insomnia may occur for a few nights after a 3- to 4-week regimen has been discontinued Safety is important: - Keep side rails up, or use bed alarms and keep call light reach. Assist patient with ambulation (especially the elderly) V: Antipsychotics and antidepressants. ANTIDEPRESSANTS: Selective serotonine reuptake inhibitors SSRIs A. Antidepressants: Overview: Depression: affective disorder in which a person experiences sadness that is much more severe and longer lasting than is warranted by the event that seems to have precipitated it, with a more intense mood; the condition may not even be traceable to a specific event or stressor. The etiology of depression is not known but there is evidence that a major factor is a reduction in the amount of neurotransmitters such as serotonin 5-HT or norepinephrine at the junctions between neurons in the brain. Antidepressants are the pharmacologic treatment of choice for major depressive disorders. Many of the drugs currently used to treat effective disorders increase the levels of serotonin, dopamine, and norepinephrine concentrations in the CNS. This treatment is based on the belief that alterations in the levels of these neurotransmitters are responsible for causing depression. Citalopram. Escitalopram. Fluoxetine. Paroxetine. Sertraline. Serotonine norepinephrine reuptake inhibitors SNRIs. Duloxetine. Venlafaxine. Tricyclic antidepressant TCA Amitriptyline. Clomipramine. Imipramine. Tetracyclic antidepressants Mirtazapine. Monoamine oxidase inhibitors MAOIs Recent research data indicate that early and aggressive antidepressant treatment increases the chances for full remission. The first 6-8 weeks of therapy constitute the acute phase. The primary goals during this time are to obtain a response to drug therapy and to improve the patient’s symptoms. It is currently recommended that antidepressant drug therapy be maintained at the effective dose for an additional 8-14 months after remission of depressive symptoms. Therapeutic response is measured primarily by subjective patient feedback. A therapeutic non-response to antidepressant drug therapy is defined as failure to respond to at least 6 weeks of therapy with adequate drug dosages. Therefore, dosage optimization, which involves careful upward titration of medication dose for several weeks, is recommended before concluding that a given drug is ineffective in treating a particular patient. Pharmacology overview: - Older generation: tricyclic antidepressant TCA drugs, monoamine oxidase inhibitors MAOIs Newer generation: selective serotonine reuptake inhibitorsSSRIs, serotonine norepinephrine reuptake inhibitors SNRIs, miscellaneous. 1- Monoamine oxidase inhibitors MAOIs: - Isocarboxazid, phenelzine, and tranylcypromine. They are now rarely used. This is partly because newer, safer drugs are now available A serious disadvantage to MAOI use is their potential to cause a hypertensive crisis when taken with a substance containing tyramine, which is found in many common foods and beverages. 2- Tricyclic antidepressants: Amitriptyline. Clomipramine. Imipramine. - Now TCAs are generally considered second-line drug therapy for patients for whom the newer drugs are ineffective or as adjunct therapy with newer drugs. TCAs are so named because of their characteristic three-ring chemical stricture. Mechanism of action: TCAs are believed to work by correcting imbalance in the neurotransmitter concentrations of serotonin and norepinephrine at the nerve endings in the CNS (the biogenic amine hypothesis). This is accomplished by blocking presynaptic reuptake of the neurotransmitters, which makes them available for transmission of nerve impulses to adjacent neurons in the brain. Some also believe that these drugs may help regulate malfunctioning neurons (the dysregulation therapy). Indications Originally used to treat depression currently, TCAs are most commonly used to treat neuropathic pain syndromes and insomnia. Some of the TCAs have additional specific indications. For example, imipramine is used as an adjunct in the treatment of childhood enuresis (bedwetting), and clomipramine is useful in treatment of obsessive-compulsive disorder. Contraindications Contraindications include known drug allergy, and pregnancy. TCAs are also not recommended in patient with any acute or chronic cardiac problems or history of seizures, because both conditions are associated with a greater likelihood of death upon TCA overdose. Adverse effects: The most common adverse effects have being constipation and urinary retention. Also they can lead to disturbances in cardiac conduction, hypotension, and sexual dysfunction. 3- Tetracyclic antidepressants: Maprotiline Mirtazapine. Drug profile: Mirtazapine (remeron): - Associated with sedation due to histamine H1 receptor activity. Dosed once daily at bedtime. Increase appetite. 4- Selective serotonin reuptake inhibitors SSRIs Citalopram, Escitalopram, Fluoxetine, Paroxetine, Sertraline. 5- Serotonin norepinephrine reuptake inhibitors SNRIs Duloxetine, Venlafaxine. They are associated significantly fewer and less severe systemic adverse effects, compare with older-generation. Mechanism of action: They inhibit the serotonin reuptake; this seems the primary mechanism of action of the SSRIs. Other drugs have weak effects on norepinephrine and dopamine reuptake and called SNRIs. Patients should be educated that antidepressant drugs commonly must be taken for several weeks before full therapeutic effects are realized. This requires some patience and faithful dosing on the part of patients. Indications: - Depression is their primary indication. - Have shown benefit in treating a variety of other mental and physical disorders (bipolar disorder, eating disorders, and obsessive-compulsive disorder.…. Etc) Adverse effects: Some of the most common adverse effects are insomnia, weight gain, and sexual dysfunction. Interactions: The newer-generation antidepressants are highly bound to albumin. When given with other drugs that are also highly protein bound (e.g., warfarin and phenytoin), they compete for binding sites for binding sites on the surface of albumin. This results in a more free unbound drug and therefore a more pronounced drug effect. Some of these drugs may also inhibit cyt P-450 enzymes, inhibition of these enzymes results in higher levels of drugs that metabolized by this system. B. Antipsychotic drugs: Overview: Mental disorders are now thought to be caused by some inherent dysfunction within the brain that leads to abnormal thought processes and responses. Psychosis is a severe mental disorder that often impairs mental function to the point of causing significant disability in performing the activities of daily living. A hallmark of psychosis is a loss of contact with reality. The primary psychotic disorders are schizophrenia and depressive and drug –induced psychoses. The dopamine hypothesis of psychotic illness grows out of the observation that psychotic patients often have excessive dopaminergic activity in the brain. Drug therapy is therefore aimed at reducing this activity. Because no diagnostic laboratory tests are available, patient assessment and response must be carefully evaluated to determine the basis of a particular problem. Selected disorders are discussed here. Schizophrenia, the most common type of psychosis, can be very debilitating and prevents affected individuals from functioning in society. Characteristics of schizophrenia include hallucinations, paranoia, delusions, speech abnormalities, and affective problems. This disorder, which seems to have a very Antipsychotics: - Older generation: Thioridazine. Trifluoperazine. Chlorpromazine. Haloperidol. - Newer generation: Clozapine. Olanzapine. Risperidone. Aripiprazole. Drugs used to treat mania and bipolar disorder Lithium Carbamazepine. Lamotrigine. Valproic acid. Mania, with its associated bipolar illness (i.e., manicdepressive illness), is characterized by periods of extreme overactivity and excitement. Bipolar disorder involves extremes of depression alternating with hyperactivity and excitement. This condition may reflect a biochemical imbalance followed by overcompensation on the part of neurons and their inability to re-establish stability. Pharmacology overview: Antipsychotics: There are few overall differences between antipsychotics in terms of mechanism of action. Therefore, selection of an antipsychotic is based primarily on the patient’s tolerance and the need to minimize adverse effects, it should also stressed that antipsychotic drug therapy does not normally provide a cure for psychoses but is a way of chemically controlling the symptoms of the illness. The newer-generation antipsychotics are referred to as atypical antipsychotics, as opposed to the older-generation drugs, which can also be thought of as conventional antipsychotics. Atypical antipsychotics differ from conventional drugs in that they tend to have better adverse effects. Mechanism of action: One thing that all antipsychotics have in common is some degree of blockage of dopamine receptors in the brain, which decrease the dopamine concentration in the CNS. Specifically, the older phenothiazines block the receptors to which dopamine normally binding postsynaptically in certain areas of the CNS, such as the limbic system and the basal ganglia. These are the areas associated with emotions, cognitive function, and motor function. The newer atypical antipsychotic drugs block specific dopamine receptors called dopamine 2 receptors, as well as specific serotonin receptors in the brain known as serotonin 2 receptors. These more refined mechanisms of action of atypical are responsible for their improved efficacy and safety profiles, compared with older drugs. Adverse effects: Common adverse effects include CNS effects like drowsiness, neuroleptic malignant syndrome (is a potentially lifethreatening adverse effect may include high fever, unstable blood pressure), extrapyramidal symptoms (they are involuntary motor symptoms similar to those associated with parkinson’s disease). Theoretically these effects are possible with atypical antipsychotics as well as older drugs. However, evidence suggests that the incidence is lower with the newer drugs. Cardiovascular effects include postural hypotension, in addition, electrocardiogram changes. Lithium The original drugs still currently available that can effectively alleviate the symptoms of acute mania are the lithium salts lithium carbonate and lithium citrate. Lithium is also effective for the maintenance treatment of bipolar disorder. One possible explanation for its effectiveness is that it potentiates serotonergic neurotransmission. A variety of medications may be used in conjunction with lithium to regulate mood or achieve stability in manic or hypomanic patients include benzodiazepines, antipsychotic drugs, antiepileptic drugs, and dopamine receptor agonists. The antiepileptic valproic acid, lamotrigine, and carbazepine are commonly preferred to lithium because lithium has a narrow therapeutic range and requires blood level monitoring. These drugs are often effective in treating mania, hypomania, and to lesser degree, depressive symptoms. Other evidence has shown that the atypical antipsychotic drugs risperidone, olanzapine,and ziprasidone can also be effective in treating mania and hypomania. Nursing Implications: Provide simple explanations about the drug, its effects, and the length of time before therapeutic effects can be expected Advise patients to avoid abrupt withdrawal Advise patients to change positions slowly to avoid postural hypotension and possible injury The combination of drug therapy and psychotherapy is emphasized because patients need to learn and acquire more effective coping skills Only small amounts of medications should be dispensed at a time to minimize the risk of suicide attempts Simultaneous use of these drugs with alcohol or other CNS depressants can be fatal Antidepressants Inform patients that it may take several weeks to see therapeutic effects, monitor patients closely during this time, assess for suicidal tendencies, and provide support Tricyclics may need to be weaned and discontinued before undergoing surgery to avoid interactions with anesthetic drugs Monitor for adverse effects, and discuss with patients Encourage patients to wear medication ID badges naming the drugs being taken Caffeine and cigarette smoking may decrease effectiveness of medication therapy Antipsychotics Instruct patients to wear sunscreen because of photosensitivity Tell patients to avoid taking antacids or antidiarrheal preparations within 1 hour of a dose Long-term haloperidol therapy may result in tremors, nausea, vomiting, or uncontrollable shaking of small muscle groups; report these symptoms to the physician Oral forms may be taken with meals to decrease GI upset These drugs may cause drowsiness, dizziness, or fainting; instruct patients to change positions slowly Monitor for therapeutic effects Monitor mental alertness, cognition, affect, mood, ability to carry out activities of daily living, appetite, and sleep patterns Monitor potential for self-injury during the delay between the start of therapy and symptomatic improvement For antidepressants Improved sleep patterns and nutrition Increased feelings of self-esteem Decreased feelings of hopelessness Increased interest in self and appearance Increased interest in daily activities Fewer depressive manifestations or suicidal thoughts/ideations For antipsychotics Improved mood and affect Alleviation of psychotic symptoms and episodes Decreased hallucinations, paranoia, delusions, garbled speech, and inability to cope For lithium Less mania Therapeutic lithium levels of 0.6 to 1.2 mEq/L
