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Trimipramine

Trimipramine is an tricyclic antidepressant with sedative and anxiolytic properties. more...

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Pharmacology

Trimipramine's mechanism of action differs from other tricyclic antidepressants. It is only a moderate reuptake inhibitor of norepinephrine, and a weak reuptake inhibitor of serotonin and dopamin. The main effects are due to considerable postynaptic blockage as follows:

  • strong : 5-HT2, Muscarinic, H1, H2, Alpha1
  • moderate : D2
  • weak : 5-HT1, Alpha2

The spectrum of effects (strong antidepressant activity, sedation and anxiolysis) and side-effects (strong anticholinergic and antiadrenergic side-effcts) is the same as with Doxepin. It is also a more effective sedative than Amitriptyline. Trimipramine is the only effective drug against insomnia known so far that does not alter the normal sleep architecture. In particular, it does not suppress REM-sleep. Moreover, dreams are said to brighten during treatment. Its relatively strong antagonistic activity at postsynaptic D2-receptors led to a clinical study trying Trimipramine as atypical neuroleptic. There it exerted good antipsychotic activity with a low incidence of extrapyramidal and other side-effects. But this study encompassed only 28 patients, so the use of Trimipramine as a neuroleptic needs further confirmation and can currently not be recommended. Trimipramine shows also useful activity against chronic pain.

Indications

  • Endogenous and neurotic depression with prominent agitation and anxiety
  • Depressive and non-depressive insomnia (suitable for long-term treatment)
  • Adjunctive therapy of alcohol and opioid withdrawal
  • Chronic pain of malignant and non-malignant origin

Trimipramine is an efficient antidepressant, sedative, and anxiolytic comparable to Doxepin.

Contraindications

absolute :

  • concomittant treatment with MAO-Inhibitors
  • known hypersensitivity to Trimipramine or other Tricyclics
  • acute intoxication with alcohol, sedatives, analgesics and other psychoactive drugs
  • acute Delirum tremens
  • untreated closed angle glaucoma
  • hypertrophy of the prostate with urine retention
  • paralytic ileus

relative :

  • hypertrophy of the prostate without urine retention
  • reduced function of the bone marrow
  • organic brain disorders
  • increased risk of seizures, preexisting epilepsy
  • preexisting cardial damage, particular some arrhythmias (impulse conductive disorders)

Side Effects

See the article on Doxepin. All side-effects of Doxepin are noted also during Trimipramine use with approximately the same frequency and intensity in equivalent doses.

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Low Risk From Antidepressants During Pregnancy - low risk of birth defects - Brief Article
From Family Pratice News, 3/15/00 by Heather Lindsay

Women who use antidepressants during pregnancy are not significantly increasing the risk of congenital malformations in their infants, according to the results of a large prospective study.

Dr. A. Ericson of the Centre for Epidemiology in Stockholm and colleagues followed 969 women who reported antidepressant use at a prenatal visit around weeks 10-12. There were 980 births, including 11 sets of twins.

The incidence of birth defects was 4%, and the incidence of infant mortality was 0.7%--no different from the rates in the general population (Eur. J. Chin. Pharmacol. 55[7]:503-08, 1999).

But Dr. Zachary Stowe, director of the Pregnancy and Postpartum Mood Disorders Program at Emory University, Atlanta, offered this caveat: "My only reservation about taking studies such as this one as prima facie evidence [that antidepressants are safe during pregnancy] is that they're uncontrolled case studies. We need more large prospective studies in this area," he said in an interview.

In the study the women who used antidepressants smoked more, had higher parity, and were significantly older (independent of parity) than women in the general population. They had a tendency to deliver preterm (before 37 weeks' gestation), and to deliver infants with lower birth weights--except for the subclass of women taking non-SSRI antidepressants, who had infants who were slightly heavier than the average.

The low birth weight in the antidepressant group was not significant after controlling for age, parity, and smoking habits. In fact, the mean birth weight was slightly higher than in the controls when these factors were accounted for. The tendency toward short gestation was not completely explained by these confounders.

The data came from the Swedish Medical Birth Registry, which includes information from prenatal visits, delivery, and from the first pediatric exam for nearly all of the births in Sweden.

A total of 531 women used SSRIs alone during pregnancy, 15 used SSRIs in combination with another antidepressant, and 423 used a non-SSRI antidepressant alone, Dr. Ericson and colleagues reported.

The SSRIs used were citalopram, fluoxetine, paroxetine, and sertraline. The non-SSRIs used were amitriptyline, clomipramine, imipramine, lofepramine, nortriptyline, maprotiline, mianserin, moclobemide, trimipramine, and venlaflaxine.

Citalopram, for which no previous data on teratogenic effects exist, was the most popular antidepressant and was used by 39% of the women. Congenital anomalies did not appear more frequently in the infants of these women than in infants exposed to other SSRIs.

More than 40% of the women reported using other medications during pregnancy including psycholeptics, analgesics, anti-asthmatic drugs, antibiotics, anti-inflammatory drugs, sex hormones, thyroid hormones, antiepileptics, and insulin.

Dr. Stowe said that it's nearly impossible to know how much the outcome is affected by the concurrent use of these medications, smoking and alcohol use, socioeconomic status, prenatal care, and underlying uncontrolled depression.

"There are just so many uncontrolled factors," he remarked.

In the meantime, women are getting a lot of mixed messages. Physicians are regularly treating pregnant women for their depression, but physicians often tell women that they have to stop taking antidepressants if they want to breast-feed.

"That makes no sense," Dr. Stowe declared. "She was probably taking that medication throughout pregnancy, and the dose [secreted in breast milk] is so low that she'd have to breast feed for 5 years to equal the dose the infant got during 1 month of pregnancy."

Dr. Stowe reminds his own patients that antidepressants have shown no effect on infant health at any dose.

He agreed with the suggestion of Dr. Ericson and colleagues that untreated depression can expose the mother and child to risks associated with substance abuse, poor nutrition, and suicidal tendencies.

"If they have a history of being able to come off [their antidepressant] and be OK, then do it. But if you take them off the medication and they get sick and need to go back on it, you're exposing the fetus both to antidepressant and to untreated depression," Dr. Stowe said. In his view, this is the worst of both worlds.

In a recent multicenter prospective study by Dr. Stowe, 112 women were taking antidepressants when they became pregnant, and all discontinued medication as soon as they discovered their pregnancy About 70% developed depressive symptoms during pregnancy; by the time their babies were born, 50% had started taking antidepressants again.

Even if a woman is able to stay off her antidepressant for the duration of pregnancy it may not help that much. Most women don't know they're pregnant until week 4 or 5, and even if they stop taking their medication immediately, it takes another week to clear the system, he explained. By that time, organogenesis is well underway and the critical period when antidepressants could have affected fetal development is over.

Another reason to keep women on antidepressants is Dr. Stowe's own finding that SSRIs and tricyclic antidepressants have incomplete placental passage. A fetus receives a very low dose of these drugs.

COPYRIGHT 2000 International Medical News Group
COPYRIGHT 2001 Gale Group

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