Doxepin: Comprehensive Drug Monograph

Pharmacokinetic Profile

Half-Life

~15 h (doxepin); ~31 h (nordoxepin)

Metabolism

CYP2D6 (major); CYP1A2, CYP2C9, CYP2C19

Protein Binding

~80%

Bioavailability

~29% (high first-pass)

Volume of Distribution

~11,930 L (~20 L/kg)

Clinical Information

Drug Class

Tricyclic Antidepressant (dibenzoxepin)

Available Doses

Caps: 10, 25, 50, 75, 100, 150 mg; Tabs: 3, 6 mg; Solution: 10 mg/mL; Cream: 5%

Route

Oral, Topical

Renal Adjustment

No specific adjustment (minimal renal excretion)

Hepatic Adjustment

Initiate low; monitor closely

Pregnancy

Risk of neonatal adaptation syndrome

Lactation

Not recommended

Schedule / Legal Status

Not a controlled substance

Generic Available

Yes

Black Box Warning

Suicidality in youth (antidepressant doses)

Indications

Indication	Approved Population	Therapy Type	Status
Major Depressive Disorder	Adults	Monotherapy	FDA Approved
Insomnia (sleep maintenance difficulty)	Adults (including elderly)	Monotherapy (low-dose, Silenor)	FDA Approved
Pruritus (atopic dermatitis, lichen simplex chronicus)	Adults (topical 5% cream)	Short-term topical (up to 8 days)	FDA Approved

Doxepin occupies a distinctive position among the tricyclic antidepressants owing to its unusually potent histamine H1 receptor blockade, which gives it a dual clinical identity. At full antidepressant doses (75–300 mg/day), it acts primarily through norepinephrine and serotonin reuptake inhibition. At ultra-low doses (3–6 mg), its selectivity for the H1 receptor makes it an effective hypnotic without the anticholinergic burden that characterises higher doses. The topical formulation leverages its antihistaminic properties for itch relief in dermatological conditions.

Off-Label Uses

Chronic urticaria (refractory) — Doxepin 10–25 mg at bedtime may be effective when standard second-generation antihistamines and H2 blockers fail. AAAAI/ACAAI guidelines list it as a treatment option for refractory cases. (Evidence quality: Moderate)

Anxiety disorders — Used at doses of 25–150 mg/day for generalized anxiety, though SSRIs are preferred first-line. (Evidence quality: Moderate)

Chronic pruritus (neuropathic or systemic) — Oral doxepin 10–100 mg/day used by dermatologists for intractable itch conditions. (Evidence quality: Low)

Neuropathic pain — Some evidence for use at 25–150 mg/day as an adjunct analgesic. (Evidence quality: Low)

Dose

Dosing

Adult Dosing by Clinical Scenario

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Major depression — initial monotherapy	25 mg TID or 75 mg QHS	75–150 mg/day	300 mg/day	May give in divided doses or as a single bedtime dose to exploit sedation Titrate over 1–2 weeks based on response
Depression with prominent insomnia	25–50 mg QHS	75–150 mg QHS	300 mg/day	Single bedtime dosing preferred; sedation is a therapeutic advantage Full antidepressant response may take 2–4 weeks
Insomnia — sleep maintenance (Silenor)	6 mg QHS	3–6 mg QHS	6 mg/day	Take within 30 min of bedtime; avoid within 3 h of a meal Not a controlled substance; no abuse potential demonstrated
Anxiety disorders (off-label)	25 mg QHS	75–150 mg/day	300 mg/day	Increase by 25–50 mg every 3 days as tolerated Divided dosing (BID or TID) may reduce daytime sedation at higher doses
Chronic urticaria (off-label)	10 mg QHS	10–25 mg QHS	75 mg/day	Exploits potent H1/H2 blockade at low doses May combine with second-generation antihistamine during the day
Pruritus — topical (Zonalon 5% cream)	Thin film QID	Thin film QID	QID × 8 days max	Allow 3–4 h between applications; reduce BSA treated if excessive drowsiness occurs Drowsiness in 22% even with topical use

Special Population Adjustments

Population	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Elderly (≥65 years) — insomnia	3 mg QHS	3–6 mg QHS	6 mg/day	Clearance reduced by ~33% from age 20 to 75 Higher risk of confusion and oversedation (Beers Criteria)
Elderly (≥65 years) — depression	10–25 mg QHS	25–75 mg/day	150 mg/day	Listed as potentially inappropriate by AGS Beers Criteria Monitor for orthostatic hypotension and falls
Hepatic impairment	3 mg QHS (insomnia) or lowest available (depression)	Titrate cautiously	Individualize	Higher plasma concentrations expected; no formal dose-adjustment studies Monitor for excessive sedation and anticholinergic effects
CYP2D6 / CYP2C19 poor metabolizers	Reduce dose	Guided by doxepin plasma levels	Individualize	Up to 4-fold higher nordoxepin AUC in CYP2D6 PMs Consider pharmacogenomic testing before initiation if available

Clinical Pearl: Dose-Dependent Pharmacology

At doses below approximately 10 mg, doxepin acts as a highly selective H1 receptor antagonist with minimal anticholinergic, antiadrenergic, or serotonergic activity. This is the pharmacological basis for the Silenor formulation. As doses climb above 25 mg, affinity for muscarinic, alpha-1 adrenergic, and monoamine transporter sites becomes relevant, producing both the therapeutic antidepressant effect and the classical TCA side-effect burden. Matching the dose to the clinical scenario is therefore essential.

Doxepin Pharmacology

Mechanism of Action

Doxepin is a dibenzoxepin-derivative tricyclic compound that exerts its effects through multiple receptor interactions. At antidepressant doses, it inhibits the reuptake of norepinephrine (primarily) and serotonin at presynaptic terminals, increasing their availability in the synaptic cleft. The active metabolite nordoxepin contributes additional norepinephrine reuptake blockade. Beyond monoamine reuptake, doxepin is among the most potent histamine H1 receptor antagonists known, with an in-vitro Ki of approximately 0.17 nM—far exceeding conventional antihistamines such as diphenhydramine (Ki ~16 nM). It also blocks muscarinic acetylcholine receptors, alpha-1 adrenergic receptors, and 5-HT2A serotonin receptors. Additionally, doxepin inhibits cardiac sodium and potassium channels, which accounts for its cardiotoxic potential in overdose. The clinical selectivity of doxepin is dose-dependent: at ultra-low doses (3–6 mg), H1 blockade predominates; at standard antidepressant doses, the full polypharmacology profile emerges.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Well absorbed orally; Tmax ~3.5 h; bioavailability ~29% (extensive first-pass ~55–87%); AUC increased ~41% with high-fat meal	For insomnia dosing, administer on an empty stomach (not within 3 h of a meal) to avoid delayed absorption and next-day hangover; food effect less relevant at antidepressant doses
Distribution	Vd ~11,930 L (~20 L/kg); protein binding ~80% (albumin and alpha-1 acid glycoprotein)	Very large volume of distribution indicates extensive tissue uptake; haemodialysis is ineffective for overdose removal
Metabolism	Hepatic via CYP2D6 (primary), CYP2C19, CYP1A2, CYP2C9; active metabolite: nordoxepin (t½ ~31 h); further glucuronidation	CYP2D6 and CYP2C19 poor metabolizers may have significantly elevated doxepin exposure (up to 4-fold increase in nordoxepin AUC); dose reduction and therapeutic drug monitoring advisable
Elimination	t½ ~15 h (doxepin), ~31 h (nordoxepin); <3% excreted unchanged in urine; primarily as glucuronide conjugates	Long active-metabolite half-life supports once-daily dosing; negligible renal excretion means no dose adjustment needed in renal impairment

Side Effects

The side-effect profile of doxepin is strongly dose-dependent. At ultra-low insomnia doses (3–6 mg), adverse events are comparable to placebo. The incidence data below are from clinical trials of antidepressant-dose doxepin (Sinequan PI, n = 1,635 patients with MDD) unless otherwise noted.

≥10% Very Common

Adverse Effect	Incidence	Clinical Note
Somnolence	17%	Most frequently reported effect; often diminishes over the first 1–2 weeks of therapy; dose-related
Dry mouth	15%	Due to muscarinic receptor blockade; oral hygiene counselling recommended to prevent caries

1–10% Common

Adverse Effect	Incidence	Clinical Note
Dizziness	6%	Related to alpha-1 adrenergic blockade; advise slow position changes
Constipation	5%	Anticholinergic effect; encourage fibre and hydration
Fatigue	5%	Distinct from somnolence; dose reduction may help
Blurred vision	3%	Anticholinergic; usually transient; rule out acute angle closure if eye pain present
Tachycardia	3%	Vagolytic anticholinergic effect on the heart; obtain ECG if clinically indicated
Hypotension	3%	Orthostatic; falls risk in elderly; measure standing blood pressure early in treatment
Insomnia	2%	Paradoxical; consider bedtime-only dosing
Tremor	2%	Fine postural tremor; may indicate serotonergic contribution
Nausea	2%	Usually resolves with continued use; take with food at antidepressant doses
Hyperhidrosis	2%	Noradrenergic effect; may persist long-term
Weight gain	2%	Related to H1 blockade and metabolic effects; monitor weight regularly

Serious Serious (regardless of frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Suicidal ideation / behaviour	Uncommon (age-dependent)	First weeks to months	Close monitoring especially in patients <25 years; consider stopping if emergent suicidality
Serotonin syndrome	Rare	Hours to days after adding serotonergic drug	Discontinue doxepin and all serotonergic agents immediately; supportive care; cyproheptadine
Cardiac arrhythmia / QRS prolongation	Rare (dose-dependent)	Any time; increased risk in overdose	Baseline and follow-up ECG; discontinue if QRS >120 ms or new arrhythmia; cardiology consult
Seizures	Rare	Any time; more common at high doses or in overdose	Discontinue doxepin; manage seizures per protocol; avoid rechallenge
Angle-closure glaucoma	Rare	Any time	Urgent ophthalmology referral; discontinue doxepin; contraindicated in glaucoma
Agranulocytosis / severe cytopaenia	Very rare (postmarketing)	Weeks to months	Urgent FBC; discontinue doxepin; haematology review
SIADH / hyponatraemia	Very rare (postmarketing)	Weeks	Check sodium; fluid restriction; discontinue if severe
Mania / hypomania activation	Uncommon	First weeks	Discontinue doxepin; evaluate for bipolar disorder; initiate mood stabiliser

Discontinuation Discontinuation & Withdrawal

Antidepressant Doses

Taper required

Gradual reduction recommended. Abrupt discontinuation may cause nausea, headache, malaise, and sleep disturbance. Symptoms typically mild due to long metabolite half-life.

Low-Dose Insomnia (Silenor)

~1% vs 0.6% placebo

Very low discontinuation rate. No rebound insomnia or withdrawal syndrome demonstrated in clinical trials up to 3 months. No taper needed at ultra-low doses.

Reason for Discontinuation	Incidence	Context
Somnolence / excessive sedation	<1%	Most common reason at antidepressant doses; not clinically significant at low doses
Anticholinergic effects (dry mouth, constipation, urinary retention)	<1%	Usually dose-related; dose reduction often sufficient
Weight gain	<1%	Long-term concern that may affect adherence

Managing Sedation

Sedation is the most clinically significant side effect and is strongly dose-dependent. At antidepressant doses, consolidating the entire daily dose at bedtime can transform this side effect into a therapeutic advantage for patients with comorbid insomnia. If persistent daytime drowsiness occurs, dose reduction is often more effective than adding a stimulant. At insomnia doses (3–6 mg), next-day residual sedation is not significantly different from placebo.

Int

Drug Interactions

Doxepin is primarily metabolised by CYP2D6, with secondary contributions from CYP2C19, CYP1A2, and CYP2C9. It does not appear to inhibit or induce CYP enzymes at therapeutic concentrations. The most clinically important interactions involve MAOIs, other serotonergic agents, and CYP2D6 inhibitors.

Major MAO Inhibitors

MechanismCombined serotonergic and noradrenergic excess

EffectLife-threatening serotonin syndrome and hypertensive crisis

ManagementContraindicated: 14-day washout required between doxepin and any MAOI (including linezolid and IV methylene blue)

FDA PI

Major Serotonergic Drugs (SSRIs, SNRIs, triptans, tramadol)

MechanismAdditive serotonergic activity

EffectRisk of serotonin syndrome; SSRIs also inhibit CYP2D6, compounding exposure

ManagementIf combination necessary, start low and monitor closely; allow 5-week washout after fluoxetine before starting doxepin

FDA PI

Major Strong CYP2D6 Inhibitors (fluoxetine, paroxetine, quinidine, bupropion)

MechanismInhibition of CYP2D6-mediated doxepin metabolism

EffectSubstantially increased doxepin and nordoxepin plasma concentrations

ManagementReduce doxepin dose guided by plasma levels; monitor for anticholinergic toxicity and sedation

FDA PI

Moderate Cimetidine

MechanismBroad CYP inhibition (2D6, 1A2, 3A4)

EffectApproximately 2-fold increase in doxepin Cmax and AUC

ManagementFor insomnia dosing: max 3 mg/day with cimetidine. For antidepressant doses: reduce dose and monitor plasma levels

FDA PI

Moderate Carbamazepine

MechanismCYP enzyme induction accelerating doxepin clearance

EffectReduced doxepin exposure, potentially subtherapeutic levels

ManagementMonitor plasma levels; dose increase may be necessary

FDA PI

Moderate Alcohol & CNS Depressants

MechanismAdditive CNS depression

EffectPotentiated sedation, respiratory depression, impaired psychomotor function

ManagementAvoid alcohol; reduce dose of doxepin or co-administered sedative as tolerated

FDA PI

Moderate Tolazamide / Sulfonylureas

MechanismUncertain; possibly enhanced insulin secretion or altered glucose metabolism

EffectSevere hypoglycaemia reported (case reports)

ManagementClosely monitor blood glucose; reduce doxepin dose as needed

FDA PI

Minor Anticholinergic Agents

MechanismAdditive muscarinic receptor blockade

EffectWorsened dry mouth, constipation, urinary retention, delirium (especially in elderly)

ManagementMinimise anticholinergic burden; review medication list using an anticholinergic scoring tool

Lexicomp

Mon

Monitoring

ECG Baseline; repeat if dose >150 mg/day or symptoms
Routine Assess QRS duration and QTc interval before initiating antidepressant doses. TCAs widen QRS via sodium channel blockade; QRS >100 ms warrants caution. Not required for low-dose insomnia use.
Blood Pressure Baseline; weekly for first month, then periodically
Routine Orthostatic measurements (lying and standing) recommended, especially in elderly and patients on antihypertensives. Alpha-1 blockade causes postural hypotension.
Weight & BMI Baseline, then every 3 months
Routine H1 blockade contributes to weight gain. Address early with dietary counselling if a rising trend is identified.
Mental State Every visit for first 3 months, then periodically
Routine Screen for suicidality, especially in patients under 25. Also monitor for manic switching in patients with undiagnosed bipolar disorder.
Doxepin Plasma Level If poor response, suspected toxicity, or CYP2D6 PM
Trigger-Based Therapeutic range (doxepin + nordoxepin combined): 50–250 ng/mL for depression. Wide interpatient variability in metabolism makes TDM particularly useful.
Sodium If symptoms of SIADH (confusion, nausea, headache)
Trigger-Based SIADH is a rare postmarketing adverse reaction. Check sodium in elderly patients on diuretics or with unexplained confusion.
Intraocular Pressure If eye pain or visual disturbance
Trigger-Based Mydriatic effect may precipitate angle-closure glaucoma in patients with anatomically narrow angles. Contraindicated in glaucoma.

Contraindications & Cautions

Absolute Contraindications

Hypersensitivity to doxepin or other dibenzoxepines (cross-reactivity possible)
Glaucoma (all forms per current FDA labelling)
Current or past urinary retention
Concurrent MAOI use or use within 14 days of stopping an MAOI (including linezolid and IV methylene blue)

Relative Contraindications (Specialist Input Recommended)

Severe cardiovascular disease — recent myocardial infarction, heart failure, conduction abnormalities; TCA cardiotoxicity risk
Elderly patients with dementia or delirium risk — anticholinergic burden may precipitate or worsen cognitive impairment; Beers Criteria lists doxepin as potentially inappropriate for those ≥65
Bipolar disorder (unscreened) — risk of manic switching; screen before initiation
Severe hepatic impairment — doxepin undergoes extensive hepatic metabolism; anticipate elevated plasma levels
Pregnancy — risk of neonatal adaptation syndrome (respiratory distress, feeding difficulty, irritability) with third-trimester exposure; risk-benefit discussion essential

Use with Caution

Seizure history — doxepin may lower seizure threshold
Prostatic hypertrophy — anticholinergic effects may worsen urinary symptoms
Obstructive sleep apnoea — Silenor not recommended in severe OSA due to respiratory drive suppression potential
CYP2D6 / CYP2C19 poor metabolisers — increased exposure; consider dose reduction and TDM
Patients at risk of suicide — prescribe the smallest feasible quantity to reduce overdose risk; TCA overdose has a narrow toxic-to-therapeutic ratio

FDA Boxed Warning Suicidal Thoughts and Behaviours

Antidepressants, including doxepin, increase the risk of suicidal thoughts and behaviour in paediatric and young adult patients (under 25 years) in short-term studies. In pooled analyses of approximately 77,000 adults and 4,500 paediatric patients across antidepressant classes, the risk was 14 additional patients per 1,000 treated in those under 18, and 5 additional per 1,000 in those aged 18–24. All antidepressant-treated patients should be monitored for clinical worsening and emergence of suicidal thoughts, especially during the initial months of therapy and at dose changes. Doxepin is not approved for use in paediatric patients.

Patient Counselling

Purpose of Therapy

Doxepin is prescribed to treat depression, help maintain sleep, or relieve persistent itching, depending on the dose and formulation. At higher doses it adjusts brain chemistry to improve mood over several weeks, while at very low doses it primarily promotes sleep by blocking wakefulness signals. It is important for patients to understand that the antidepressant effect takes 2–4 weeks to become apparent, and treatment should not be stopped abruptly.

How to Take

For depression: doxepin can be taken once at bedtime or in divided doses through the day; taking the full dose at bedtime takes advantage of its sedating properties. For insomnia (Silenor): take within 30 minutes of bedtime on an empty stomach; do not eat within 3 hours before the dose. For the oral solution: measure with the supplied calibrated dropper and dilute in 120 mL of water, milk, or compatible fruit juice immediately before drinking. Topical cream should be applied in a thin layer and spaced at least 3–4 hours apart.

Drowsiness & Sedation

Tell patient Drowsiness is common and usually most pronounced in the first 1–2 weeks, then improves. Taking the medication at bedtime can help. Avoid driving or operating machinery until you know how doxepin affects you.

Call prescriber If daytime drowsiness persists beyond 2–3 weeks and is affecting daily function, or if you experience confusion or disorientation.

Dry Mouth & Constipation

Tell patient These are common anticholinergic effects. Sip water frequently, use sugar-free gum or lozenges, maintain good dental hygiene to prevent caries. Increase fibre and fluid intake for constipation.

Call prescriber If constipation is severe or accompanied by abdominal pain, or if you develop difficulty urinating.

Dizziness & Falls

Tell patient Stand up slowly from sitting or lying positions, particularly in the first few weeks of treatment. This reduces the chance of lightheadedness from blood pressure changes.

Call prescriber If you faint or feel close to fainting, or if dizziness is persistent and severe.

Mood Changes & Suicidality

Tell patient In the first weeks of treatment, some people may experience worsening mood, agitation, irritability, or new thoughts of self-harm. This risk is higher in those under 25. Family members or carers should also be alert to behavioural changes.

Call prescriber Immediately if you or those close to you notice worsening depression, new or increasing thoughts of self-harm, or unusual changes in behaviour.

Weight Gain

Tell patient Some patients experience increased appetite and gradual weight gain. Maintain a balanced diet and regular physical activity. Report significant changes early so the treatment plan can be adjusted.

Call prescriber If weight gain exceeds 5% of baseline body weight or is causing distress affecting treatment adherence.

Stopping Treatment

Tell patient Do not stop doxepin suddenly at antidepressant doses. A gradual dose reduction over several weeks is recommended to avoid discontinuation symptoms such as nausea, headache, and sleep disturbance. Low-dose insomnia formulations (3–6 mg) can be stopped without tapering.

Call prescriber If you experience uncomfortable withdrawal symptoms despite gradual dose reduction, or if depressive symptoms return.

Alcohol & Other Sedatives

Tell patient Avoid alcohol while taking doxepin as it amplifies drowsiness and impairs coordination. Inform your prescriber of all other sedating medications you take, including over-the-counter sleep aids and antihistamines.

Call prescriber If you are prescribed a new medication by another clinician, to check for interactions.

Ref

Sources

Regulatory (PI / SmPC)

Sinequan (doxepin hydrochloride) capsules and oral solution — Full Prescribing Information. Pfizer Inc. Revised July 2025. FDA Label Primary source for approved indications, dosing, adverse reactions, contraindications, and drug interactions at antidepressant doses.
Silenor (doxepin) tablets — Full Prescribing Information. Currax Pharmaceuticals LLC. FDA Label Source for low-dose insomnia indication, safety data at 3–6 mg, pharmacokinetic parameters, and elderly dosing.
Zonalon (doxepin hydrochloride) cream 5% — Full Prescribing Information. Mylan Pharmaceuticals. FDA Label Source for topical formulation indications, dosing, and systemic absorption data in pruritic dermatoses.

Key Clinical Trials

Roth T, Rogowski R, Hull S, et al. Efficacy and safety of doxepin 1 mg, 3 mg, and 6 mg in adults with primary insomnia. Sleep. 2007;30(11):1555–1561. DOI Pivotal randomised placebo-controlled trial establishing efficacy of ultra-low-dose doxepin for sleep maintenance in adults.
Krystal AD, Durrence HH, Scharf M, et al. Efficacy and safety of doxepin 1 mg and 3 mg in a 12-week sleep laboratory and outpatient trial of elderly subjects with chronic primary insomnia. Sleep. 2010;33(11):1553–1561. DOI Long-term trial in elderly demonstrating sustained efficacy of low-dose doxepin without anticholinergic side effects.
Greene SL, Reed CE, Schroeter AL. Double-blind crossover study comparing doxepin with diphenhydramine for the treatment of chronic urticaria. J Am Acad Dermatol. 1985;12(4):669–675. DOI Landmark study showing doxepin 10 mg TID was superior to diphenhydramine for chronic idiopathic urticaria.

Guidelines

Sateia MJ, Buysse DJ, Krystal AD, et al. Clinical practice guideline for the pharmacologic treatment of chronic insomnia in adults: an American Academy of Sleep Medicine clinical practice guideline. J Clin Sleep Med. 2017;13(2):307–349. DOI AASM guideline recommending low-dose doxepin for sleep maintenance insomnia based on available evidence.
Bernstein JA, Lang DM, Khan DA, et al. The diagnosis and management of acute and chronic urticaria: 2014 update. J Allergy Clin Immunol. 2014;133(5):1270–1277. DOI AAAAI/ACAAI joint consensus listing doxepin as a treatment option for refractory chronic urticaria.

Mechanistic / Basic Science

Gillman PK. Tricyclic antidepressant pharmacology and therapeutic drug interactions updated. Br J Pharmacol. 2007;151(6):737–748. DOI Comprehensive review of TCA receptor pharmacology including doxepin’s uniquely potent H1 antagonism.
Richelson E. Pharmacology of antidepressants. Mayo Clin Proc. 2001;76(5):511–527. DOI Provides receptor binding affinity data for TCAs, documenting doxepin’s exceptionally high H1 affinity.

Pharmacokinetics / Special Populations

Yan JH, Hubbard JW, McKay G, Korchinski ED, Midha KK. Absolute bioavailability and stereoselective pharmacokinetics of doxepin. Xenobiotica. 2002;32(7):615–623. DOI Definitive crossover PK study establishing absolute oral bioavailability and stereoselectivity of doxepin isomers.
Kirchheiner J, Meineke I, Müller G, Roots I, Brockmöller J. Contributions of CYP2D6, CYP2C9 and CYP2C19 to the biotransformation of E- and Z-doxepin in healthy volunteers. Pharmacogenetics. 2002;12(7):571–580. DOI Genotype-phenotype study characterising the influence of CYP polymorphisms on doxepin metabolism and supporting pharmacogenomic dose adjustment.
Almasi A, Patel P, Meza CE. Doxepin. In: StatPearls [Internet]. Treasure Island, FL: StatPearls Publishing; updated February 14, 2024. NCBI Bookshelf Peer-reviewed clinical summary covering indications, dosing, pharmacokinetics, adverse effects, and interprofessional considerations.