Believe that the smaller effect of clozapine on the extrapyramidal system due to its predominant influence on D4retseptor as well as its Mholinoblokiruyuschimi properties, in addition, clozapine blocks serotonin 5NT2aretseptor. In contrast, of tricyclic antidepressants, fluoxetine has no sedation (may show even a slight stimulating effect), does not here Mholinoblokiruyuschimi and aadrenoblokiruyuschimi properties does not lightpen cardiotoxic actions. One of the the first «atypical» antipsychotics was clozapine (leponeks). Some help can be intramuscular injection of physostigmine. Release: means that violate the neuronal capture of serotonin and norepinephrine, a means to selectively violate the neuronal capture of serotonin, and a means to selectively violate neuronal capture of norepinephrine. Funds violate the neuronal capture of serotonin and norepinephrine Imipramine (imipramine, Melipraminum) and amitriptyline attributed to tricyclic antidepressants. Since the volume of distribution of imipramine and amitriptyline than 1000 l, hemodialysis and hemosorbtion in such poisonings are ineffective. Olanzapine 5NT2retseptor blocks and to a lesser extent D2retseptor, adrenoretseptor, N1retseptor. Some antidepressants (especially MAO inhibitors) have also stimulating effect that helps eliminate lethargy, apathy. These drugs have anti-depressant and stimulating effect. MAOA acts predominantly on norepinephrine and serotonin, and IAIA - by Peroxidase By indiscriminate MAO inhibitors are irreversible inhibitor of MAO Nialamide and reversible MAO inhibitors phenelzine, pargilin, tranylcypromine (Transamin). If necessary, change the interval between antidepressants appointment of tricyclic antidepressants and MAO inhibitors should not be less than 3 weeks. Somewhat later emerged from the antidepressant group of monoamine oxidase inhibitors (MAOIs) - Nialamide, phenelzine, tranylcypromine, application of which is hampered by the need to diet (in combination with foods containing tyramine, such drugs cause hypertensive crisis). Side effects of MAO inhibitors: insomnia, anxiety, dysfunction liver, postural hypotension. Drugs in lightpen group due to their ability to inhibit microsomal liver enzymes increase the effect of barbiturates, analgesics lightpen . For tricyclic antidepressants with marked sedative and anxiolytic properties are trimipramin and doxepin, effective in depression accompanied by anxiety, agitation. Can not be used in combination with fluoxetine MAO inhibitors (the possibility of «serotonin syndrome» - psychomotor agitation, confusion, diarrhea, tremors, chills, pyrexia, collapse). Possess antidepressant and sedative (especially amitriptyline) properties. Monoamines serotonin and norepinephrine stand out from the presynaptic endings that act on specific receptors and subjected to reverse neuronal capture. In the application of tricyclic antidepressants may be manifestations of cardiotoxic actions: fibrillation ventricles, sudden cardiac arrest. K selective Umbilical Artery Catheter reuptake inhibitors also include fluvoxamine, Bronchiolitis Obliterans Organizing Pneumonia sertraline, citalopram. Patients with depression often take Estimated blood loss doses of tricyclic antidepressant drugs with suicidal purposes. If their regular reception of the antidepressant effect is seen in about 2 weeks. On pharmacological properties and applications similar to lightpen but the side effects (Mholinoblokiruyuschee effect, cardiotoxicity) are expressed to a lesser extent. These medications effectively reduce symptoms of depression, but lightpen expressed Mholinoblokiruyuschimi properties, block a, adrenergic receptors, may have lightpen cardiotoxic effect. Of the other tricyclic antidepressants are used clomipramine, desipramine. Therefore, they lightpen particularly indicated for depressions, which are accompanied by depression, lethargy. Tricyclic antidepressants also exhibit Mholinoblokiruyuschie and a1adrenoblokiruyuschie properties (can cause mydriasis, violations accommodation, dry mouth, tachycardia, delayed urination, decreased blood pressure, and orthostatic hypotension). Use of selective inhibitors of MAOA (moclobemide) is only lightpen Volume of Distribution on the lightpen supply. Monoamine oxidase (MAO) - an enzyme that produces inactivation (oxidative deamination), norepinephrine, serotonin, dopamine. Means to selectively violate neuronal serotonin capture Fluoxetine (Prozac) selectively breaks reverse neuronal capture of serotonin.
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