APRN Ebook Continuing Education

FDA Approved Benzodiazepines

Healthcare Considerations: In an emergency setting, treatment for benzodiazepine and barbiturate intoxication is primarily supportive. In cases of severe benzodiazepine intoxication, particularly if the patient is becoming hypoxic, flumazenil may be administered (Jahan & Burgess, 2022). Sedative, hypnotic, and anxiolytic withdrawal The severity of withdrawal varies with dose and duration; however, it can occur with short-term, relatively low dose BZDs (Boland & Verduin, 2022). Withdrawal symptoms include: ● Autonomic hyperactivity (diaphoresis, tachycardia). ● Hand tremors. ● Insomnia. ● Nausea/vomiting. ● Transient visual, tactile, or auditory hallucinations. ● Psychomotor agitation. ● Anxiety. ● Grand mal seizures. Deprescribing benzodiazepines is an important clinical skill and the first goal of treatment in detoxification (Drugs.com, 2022). Certain individuals may not require long term BZDs. When deprescribing BZDs, consider duration of treatment, dose, and half-life of the BZD. Consider a taper over several weeks or months. Often switching to a long-acting BZD is an effective method in an individual who has serious abuse problems. Tapering is effective in cases of long active benzodiazepines, but not as effective in short-acting benzodiazepines. Example: An individual who has been taking a BZD for 12 weeks, taper for 10- 25% per week (PsychDB, 2021). Common adverse effects of BZDs include respiratory arrest, drowsiness, confusion, headache, syncope, nausea/vomiting, diarrhea, and tremors (Bounds & Nelson, 2022). Central nervous system (CNS) adverse effects include euphoria, diplopia, ataxia, and cognitive impairment with long-term use. BZDs are contraindicated in angle-closure glaucoma and have a black box warning with concomitant use of opioids, which leads to severe respiratory depression, coma, and death (Bounds & Nelson, 2022). Several groups are at high risk for abuse; caution is essential when prescribing. Individuals who consume large amounts of alcohol often present for treatment of anxiety and insomnia, and there is a high likelihood of abuse (Ciraulo, 2014). Polysubstance use frequently involves benzodiazepines, especially in methadone clinics. Individuals self-medicate for insomnia, anxiety, and withdrawal; additionally, benzodiazepines increase hedonistic effects of methadone (Ciraulo, 2014). Older individuals utilize benzodiazepines more than younger individuals. The greatest concern in this population is risk of falls and cognitive impairment and is not recommended according to Beers’ Criteria (Ciraulo, 2014).

Generic

Trade

Indication

Alprazolam Xanax

Anxiety, panic disorders, agoraphobia.

Chlordiazepoxide Librium

Alcohol withdrawal syndrome.

Clonazepam

Klonopin Panic disorder and

agoraphobia; myoclonic and absence seizures.

Quazepam Doral

Chronic insomnia.

Temazepam

Restoril

Onset and sleep maintenance in insomnia.

Diazepam

Valium Alcohol withdrawal management.

Lorazepam Midazolam (in-patient) Triazolam

Ativan

Anxiety disorders.

Versed Procedural sedation.

Halcion

Sleep onset in insomnia.

Note . Bounds & Nelson, 2022. Non-benzodiazepines including zolpidem, zaleplon, and eszopiclone (Z-drugs) have clinical effects similar to BZDs but are more prone to misuse and dependence (Borland & Verduin, 2022). Anxiolytics or sedative-hypnotic drugs can be viewed on a continuum based on sedating properties of the class. Physical and psychological dependence does occur, and all these drugs have withdrawal symptoms. Alcohol with other drugs in this class has additive effects (Boland & Verduin, 2022). The essential features of this drug class are maladaptive behavioral or psychological changes. Memory impairment causes anterograde amnesia similar to blackouts (Boland & Verduin, 2022). Sedative, hypnotic, or anxiolytic intoxication Low doses of sedative, hypnotic, or anxiolytic drugs can lead to intoxication during or shortly after use. Clinically maladaptive behavior or psychological changes can lead to: ● Drowsiness or sedation.

● Slurred speech. ● Incoordination. ● Unsteady gait. ● Nystagmus. ● Impaired cognition. ● Stupor or coma.

STIMULANT RELATED DISORDERS

Stimulant use disorders include a range of issues related to illicit cocaine, methamphetamine, ecstasy, as well as prescription stimulants, including methylphenidate and amphetamine. Approximately 5 million individuals misused prescription amphetamines ages 12 and older (CDC, 2020). Stimulant use and disorders are associated with physical, psychological, and societal harm. Acute adverse effects can cause acute conditions, including tachycardia, vasoconstriction, and bronchodilation, as well as hyperthermia. Psychological and neurological effects include panic attacks, hostility, paranoia, psychosis, and even violent behavior (SAMSHA, 2020). The highs and lows from these drugs create a binge and crash pattern (NIDA, 2019). Chronic stimulant use can alter brain structures with decreased attention span, confusion, impaired memory, inhibited impulse, and reduced motor skills (SAMSHA, 2020).

Stimulant Drugs by Schedules

Schedule I

Aminorex; methyl-aminorex; methcathinone, animal use only (3,4-Methylenedioxymethamphetamine) commonly known as MDMA. Amphetamines, dextroamphetamine; methamphetamine, methylphenidate; phentermine, cocaine. Clortermine, not currently in use Phendimetrazine, weight loss; benzphetamine, weight loss.

Schedule II

Schedule III

Schedule IV Schedule V

Diethylpropion, weight loss; Modafinil.

Pyrovalerone. Cocaine is a naturally occurring alkaloid obtained from the Erythroxylon coca shrub (Holstege et al., 2021). After its first

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Book Code: AUS3024

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