Antipsychotic Drugs

ByCarol Tamminga, MD, UT Southwestern Medical Dallas
Reviewed/Revised Apr 2022 | Modified Sept 2022
View Patient Education

    Antipsychotic drugs are divided into conventional antipsychotics and 2nd-generation antipsychotics (SGAs) based on their specific neurotransmitter receptor affinity and activity. SGAs may offer some advantages, both in terms of modestly greater efficacy (although recent evidence casts doubt on SGAs' advantage as a class) and reduced likelihood of an involuntary movement disorder and related adverse effects.

    Recent results suggest that new antipsychotic drugs with novel actions—namely, trace amines and muscarinic agonists—may become available. Currently, SGAs comprise about 95% of antipsychotics prescribed in the US. However, risk of metabolic syndromelong QT syndrome

    Conventional antipsychotics

    Conventional antipsychotics (see table Conventional Antipsychotics

    Different drugs are available in tablet, liquid, and short- and long-acting IM preparations. A specific drug is selected primarily based on the following:

    • Adverse effect profile

    • Required route of administration

    • The patient’s previous response to the drug

    Conventional antipsychotics may cause significant adverse effects, particularly some related to cognition and extrapyramidal movement disorders (eg, dystonia, tremor, tardive dyskinesia).

    Table
    Table
    Clinical Calculators

    Second-generation antipsychotics

    About 95% of all antipsychotics prescribed in the US are SGAs.

    positive symptoms and the adverse effect benefits of SGAs.

    SGAs also do the following:

    • Tend to alleviate positive symptoms

    • May lessen negative symptoms to a greater extent than do conventional antipsychotics (although such differences have been questioned)

    • May cause less cognitive blunting

    • Are less likely to have extrapyramidal adverse effects (including a much lower risk of tardive dyskinesia)

    • Can generate a metabolic syndrome

    SGAs may appear to lessen negative symptoms because they are less likely to have parkinsonian adverse effects than conventional antipsychotics.

    agranulocytosis

    Newer SGAs (see table Second-Generation Antipsychotics

    Table
    Table

    long-acting injectable formulation.

    Weight gain, hyperlipidemia, and elevated risk of type 2 diabetes are the major adverse effects of SGAs. Thus, before treatment with SGAs is begun, all patients should be screened for risk factors, including personal or family history of diabetes, weight, waist circumference, blood pressure, and fasting plasma glucose and lipid profile. Those found to have or be at significant risk of metabolic syndromesymptoms and signs of diabetes, including polyuria, polydipsia, weight loss, and diabetic ketoacidosis (nausea, vomiting, dehydration, rapid respiration, clouding of sensorium), should be provided. In addition, nutritional and physical activity counseling should be provided to all patients when they start taking an SGA. All patients taking an SGA require periodic monitoring of weight, body mass index, and fasting plasma glucose and referral for specialty evaluation if they develop hyperlipidemia or type 2 diabetes.

    Sometimes, combining an antipsychotic with another drug is beneficial (1). These drugs include

    • Antidepressants/selective serotonin-norepinephrine reuptake inhibitors

    • Another antipsychotic

    • Benzodiazepines

    2).

    Long-acting antipsychotic drugs

    Some conventional and second-generation antipsychotics (SGAs) are available as long-acting depot preparations (see table Depot Antipsychotic Drugs). These preparations are useful for eliminating drug nonadherence. They may also help patients who, because of disorganization, indifference, or denial of illness, cannot reliably take daily oral drugs.

    Table
    Table

    Adverse effects of antipsychotic drugs

    Conventional antipsychotics have several adverse effects, such as sedation, cognitive blunting, dystonia and muscle stiffness, tremors, elevated prolactin levels (causing galactorrhea), weight gain, and lowered seizure threshold in patients with seizures or at risk of seizures (for treatment of adverse effects, see table Treatment of Acute Adverse Effects of Antipsychotics

    Second-generation antipsychotics are less likely to cause extrapyramidal (motor) adverse effects, including tardive dyskinesia, but these may occur. Metabolic syndrome

    Table
    Table

    Tardive dyskinesia is an involuntary movement disorder most often characterized by puckering of the lips and tongue, finger movements, writhing of the arms or legs, or more. For patients taking conventional antipsychotics, the incidence of tardive dyskinesia is about 5% each year of drug exposure and incidence is considerably lower with SGAs. In about 2%, tardive dyskinesia is severely disfiguring. In some patients, tardive dyskinesia persists indefinitely, even after the drug is stopped. Because of this risk, patients receiving long-term maintenance therapy should be evaluated at least every 6 months. Rating instruments, such as the Abnormal Involuntary Movement ScaleQT prolongation, and parkinsonism.

    Neuroleptic malignant syndrome, a rare but potentially fatal adverse condition, is characterized by rigidity, fever, autonomic instability, and elevated creatine kinase.

    Table
    Table

    Antipsychotic drug references

    1. 1. Correll CU, Rubio JM, Inczedy-Farkas G, et al: Efficacy of 42 pharmacologic cotreatment strategies added to antipsychotic monotherapy in schizophrenia: Systematic overview and quality appraisal of the meta-analytic evidence. JAMA Psychiatry 74(7):675-684, 2017. doi: 10.1001/jamapsychiatry.2017.0624

    2. 2. Wang SM, Han C, Lee SJExpert Opin Investig Drugs 26(6):687-698, 2017. doi: 10.1080/13543784.2017.1323870

    quizzes_lightbulb_red
    Test your KnowledgeTake a Quiz!
    Download the free MSD Manual App iOS ANDROID
    Download the free MSD Manual App iOS ANDROID
    Download the free MSD Manual App iOS ANDROID