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Nausea morphine

Hydromorphone has comparable side effects to those produced by morphine use. This is true for sedation, respiratory depression, and constipation, but hydromorphone is associated with less vomiting than morphine. Nausea caused by hydromorphone and other opioids can be minimized by administering the drug along with food and having the patient lie down following administration. [Pg.249]

Codeine, mol wt 299.3, is a significantly less potent analgesic than morphine, requiring 60 mg (0.20 mmol) to equal the effectiveness of 10 mg (0.04 mmol) of morphine. However, codeine is orally effective, and it is less addictive and associated with less nausea than morphine. Codeine is used as an antitussive agent, although newer, nonaddictive agents are preferred (see Expectorants, antitussives, and related agents). [Pg.381]

Morphine has certain undesirable side effects. Among these are respiratory depression, nausea, and vomiting, depression of the cough reflex, cardiovascular depression and hypotension, smooth muscle contraction (constipation), and histamine release (93). Morphine s onset of action, duration, and low therapeutic indices have prompted a search for a more effective opiate iv anesthetic. Extreme simplification of the complex morphine molecule has resulted in anilido —piperidines, the fentanyl class of extremely potent opiate iv anesthetics (118,119). [Pg.411]

This type of pain management is used for postoperative pain, labor pain, and cancer pain. The most serious adverse reaction associated with the administration of narcotics by the epidural route is respiratory depression. The patient may also experience sedation, confusion, nausea, pruritus, or urinary retention. Fentanyl is increasingly used as an alternative to morphine sulfate because patients experience fewer adverse reactions. [Pg.175]

Opium and its derivatives have been employed for centuries for the treatment of pain. Morphine was first synthesized in 1805 and has proven to be one of the most effective analgesic agents available [1], Morphine and its analogs are particularly useful because they diminish pain sensation while maintaining consciousness. However, opiates induce severe side-effects including respiratory depression, nausea, bradycardia and constipation and long-term use of opiates can cause addiction [2]. [Pg.461]

There are two main treatments for the opiate withdrawal syndrome. One is replacement therapy with methadone or other X agonists that have a longer half-life than heroin or morphine, and produce mild stimulation rather than euphoria. They also produce cross-tolerance to heroin, lessening heroin s effect if patients relapse. Withdrawal is also treated with the 0C2 agonist clonidine, which inhibits LC neurons, thus counteracting autonomic effects of opiate withdrawal — such as nausea, vomiting, cramps, sweating, tachycardia and hypertension — that are due in part to loss of opiate inhibition of LC neurons. [Pg.916]

Morphine is considered by many clinicians to be the first-line agent for moderate to severe pain. Nausea and vomiting are more likely in ambulatory patients and with the initial dose. [Pg.638]

Morphine is known to produce in human beings a multitude of different side reactions which vary from individual to individual. In a study in which several drugs were compared for their effects on 29 healthy students, using saline control tests, it was found that morphine caused nausea in 18, sleep in 16, drunkenness in 9, dizziness in 13, itching in 9, and indistinct speech in 7.23 The proneness to addiction to morphine is also known to vary from individual to individual and sometimes this drug excites instead of depressing the individual to whom it is administered. [Pg.151]

Morphine also causes nausea and vomiting by stimulation of the area postrema. Nausea is a common reaction to intravenous injection, but tolerance develops to this effect over repeated use. [Pg.310]

Morphine is an opioid analgesic that may be used for pain relief in myocardial infarction. However, diamorphine is usually preferred because it causes a lower risk of nausea and hypotension than morphine. [Pg.258]

Apomorphine hydrochloride (44 Apokyn Bertek, 2004), is a semisynthetic derivative of opium alkaloid morphine (43) isolated from poppy (Papaver somniferum), and it has long been known for its erectile activity at the effective dose of 2-6 mg physicians discovered the effect over 100 years ago, but found the drug, at a much higher dose (ca. 200 mg), to be more suitable for poison victims as an emetic because it also causes serious nausea and vomiting. Apomorphine exerts its erectile effect at the central nervous system the drug has been found to be a non-selective dopamine agonist which activates both Di-like and D2-like... [Pg.47]

Mediates its effects by activating the microopioid receptor it shows equivalent analgesia to morphine but to have a superior side-effect profile in terms of reduced liability to induce nausea and vomiting and respiratory depression. [Pg.63]

Levorphanol (Levo-Dromoran) is an L-isomer morphi-nan derivative of morphine that is five to seven times more potent than morphine. It produces all of the side effects associated with morphine but less nausea. It is indicated for moderate to severe pain as a preoperative anxiolytic. It is often used in combination with thiopental to reduce the latter drug s anesthetic dose and to decrease postoperative recovery time. The o-isomer of levorphanol, dextrorphan, does not possess opioid analgesic activity but is a useful antitussive. [Pg.323]

The most common side effect of pentazocine is sedation resulting from an interaction with the K-receptor. Also observed are sweating, dizziness, psychotomimetic effects, anxiety, nightmares, and headache. Nausea and vomiting are less frequent than with morphine. Respiratory depression and increased heart rate, body temperature, and blood pressure accompany overdose. Naloxone is effective in reducing the respiratory depression but requires the use of higher doses than for morphine overdose. [Pg.325]

Morphine stimulates CTZ and produces nausea and vomiting. These effects are more marked in upright position due to vestibular involvement. [Pg.77]

CNS side effects include confusion, anxiety, lethargy, nausea and vomiting. GIT related effect is constipation. Other side effects are urinary retention, dry mouth, miosis, dysphoria, hypotension, skin rash, itching and urticaria. Tolerance, drug dependence and drug abuse are the main drawbacks of morphine. [Pg.77]

Side-effects Morphine induces a variety of centrally- and peripherally-mediated side-effects. The most important of which is respiratory depression following parenteral administration, especially in the postoperative situation. Chronic oral application induces constipation and chronic treatment with oral morphine must be supplemented with laxatives. Other frequent side-effects are nausea, vomiting, dizziness and sedation. [Pg.208]

Side-effects Typical side-effects of tramadol are nausea, sweating and dizziness. In rare cases seizures after high i.v. doses are reported, mostly in combination with other proconvulsant componds or in patients with reduced seizure theshold (Gardner et al., 2000). Tramadol shows a reduced level of opioid side-effects, especially respiratory depression and constipation are less frequent and severe than with standard opioids such as morphine. Tramadol has a very limited abuse potential and is not subject to narcotic control (Cossmann et al., 1997). [Pg.230]

The effects of morphine, codeine, and heroin in the brain are dose-related. Small doses produce drowsiness, decreased anxiety and inhibition, reduced concentration, muscle relaxation, pain relief, depressed respiration, constricted pupils, nausea, and a decreased cough reflex, which is why codeine found its way into cough suppressants. At slightly higher doses, morphine and heroin can produce a state of intense elation or euphoria. [Pg.135]


See other pages where Nausea morphine is mentioned: [Pg.545]    [Pg.381]    [Pg.411]    [Pg.265]    [Pg.78]    [Pg.462]    [Pg.1274]    [Pg.932]    [Pg.20]    [Pg.236]    [Pg.253]    [Pg.27]    [Pg.127]    [Pg.321]    [Pg.42]    [Pg.353]    [Pg.29]    [Pg.126]    [Pg.133]    [Pg.695]    [Pg.720]    [Pg.179]    [Pg.159]    [Pg.181]    [Pg.189]    [Pg.218]    [Pg.462]    [Pg.637]    [Pg.91]    [Pg.50]    [Pg.149]   
See also in sourсe #XX -- [ Pg.216 ]




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