Guanfacine: Comprehensive Drug Monograph

Pharmacokinetic Profile

Half-Life (XR)

~14 h children;
~18 h adolescents/adults

Metabolism

Hepatic; CYP3A4/5 (oxidation to 3-hydroxy-guanfacine)

Protein Binding

64–72% (mainly albumin)

Bioavailability

XR is ~58% relative to IR (lower C_max, lower AUC)

Volume of Distribution

6.3 L/kg (IV); apparent oral V_d higher in children

Clinical Information

Drug Class

Selective α_2A-agonist (centrally acting)

Available Doses

IR: 1, 2 mg
XR: 1, 2, 3, 4 mg

Route

Oral, once daily

Renal Adjustment

Dose reduction may be required in significant impairment

Hepatic Adjustment

Dose reduction may be required in significant impairment

Pregnancy

No adequate human studies; use only if benefit justifies risk

Lactation

Limited data; observe nursing infant for sedation

Schedule / Legal Status

Not controlled (Rx only)

Generic Available

Yes (IR and XR)

Indications

Indication	Approved Population	Therapy Type	Status
Attention-deficit/hyperactivity disorder (ADHD) — extended-release (Intuniv)	Children and adolescents 6–17 years	Monotherapy or adjunctive to stimulants	FDA Approved
Hypertension — immediate-release (Tenex)	Adults	Monotherapy or with a thiazide diuretic	FDA Approved
ADHD in adults	Adults ≥18 years	Monotherapy or adjunctive (typically with stimulant)	Off-Label
Tourette syndrome & chronic tic disorders	Children and adolescents	Monotherapy	Off-Label

The extended-release formulation (Intuniv) was FDA-approved in 2009 for pediatric ADHD and is one of two non-stimulant medications, alongside atomoxetine, with a specific FDA indication in this population (clonidine extended-release is also approved). Its non-stimulant profile, lack of abuse potential, and complementary mechanism to stimulants make it useful in patients with comorbid tic disorders, anxiety, or sleep disturbance, and in families concerned about controlled-substance prescribing. The immediate-release formulation (Tenex) retains an antihypertensive indication but is not recommended as first-line therapy for hypertension in current guidelines.

Common Off-Label Uses

Tourette syndrome & chronic tic disorders — supported by the AAN 2019 practice guideline as a treatment option for tics; randomized data show modest reduction. Evidence quality: moderate.

Anxiety, hyperarousal and irritability in autism spectrum disorder — small randomized and open-label studies suggest symptomatic benefit. Evidence quality: low.

PTSD-related nightmares and hyperarousal — small studies and case series; benefit less consistent than for prazosin. Evidence quality: low.

Adult ADHD adjunctive therapy — commonly prescribed as add-on to stimulants for residual symptoms; meta-analyses suggest moderate effect. Evidence quality: moderate.

Opioid withdrawal symptom control — clonidine has the larger evidence base in this setting; comparative data for guanfacine are limited. Evidence quality: very low.

Dose

Dosing

The two formulations are not interchangeable on a milligram-for-milligram basis. The extended-release tablet (Intuniv) is dosed once daily for ADHD, in the morning or evening, and titrated weekly. The immediate-release tablet (Tenex) is typically dosed at bedtime for hypertension to minimize daytime sedation. The recommended target weight-based range for Intuniv is 0.05–0.12 mg/kg/day.

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
ADHD — children 6–12 yr (XR / Intuniv) — monotherapy	1 mg PO once daily	1–4 mg/day	4 mg/day	Titrate by no more than 1 mg/week; weight-based target 0.05–0.12 mg/kg/day Doses above 4 mg/day have not been evaluated in this age group
ADHD — adolescents 13–17 yr (XR / Intuniv) — monotherapy	1 mg PO once daily	1–7 mg/day	7 mg/day	Titrate by no more than 1 mg/week; many adolescents respond at 4–7 mg/day Doses above 7 mg/day have not been evaluated
ADHD — adjunctive to a stimulant (XR / Intuniv)	1 mg PO once daily	1–4 mg/day	4 mg/day	Same titration cadence as monotherapy; monitor for additive bradycardia/hypotension Doses above 4 mg/day have not been studied in adjunctive trials
Hypertension — adults (IR / Tenex)	1 mg PO at bedtime	1–3 mg HS	3 mg/day	If inadequate after 3–4 weeks, increase to 2 mg, then 3 mg Doses >3 mg/day add little benefit and worsen adverse effects
Tourette syndrome / chronic tic disorder (off-label, pediatric)	0.5–1 mg/day	1–4 mg/day divided	~4 mg/day	IR formulation often used in 2–3 divided doses; titrate slowly over 4–6 weeks Tic response is gradual; reassess at 8–12 weeks
Switching between IR and XR	Discontinue current formulation and titrate the new one starting at 1 mg/day			Do not substitute mg-for-mg — XR has lower C_max and AUC than the same IR dose Follow standard XR titration schedule when switching

Dose Adjustments in Special Populations

Population	Recommendation	Rationale
Hepatic impairment (clinically significant)	Consider dose reduction	Approximately 50% of clearance is hepatic via CYP3A4/5
Renal impairment (clinically significant)	Consider dose reduction	Approximately 50% of guanfacine is excreted unchanged in urine
Strong or moderate CYP3A4 inhibitor co-administration	Reduce Intuniv dose to 50% of target	Inhibitors substantially raise guanfacine plasma exposure
Strong or moderate CYP3A4 inducer co-administration	Consider titrating up to 2× the target dose over 1–2 weeks	Inducers can substantially lower guanfacine exposure and reduce efficacy
Elderly (HTN indication)	Start 1 mg HS; titrate cautiously	Higher risk of orthostasis, falls, and bradycardia

Discontinuation

Guanfacine should not be stopped abruptly. The Intuniv label specifies that the total daily dose should be tapered in decrements of no more than 1 mg every 3–7 days to minimize the risk of rebound hypertension. The risk is greater at higher doses, with concomitant stimulant use, and after prolonged therapy.

Clinical Pearl — Administration of Extended-Release Tablets

Intuniv tablets must be swallowed whole — never crushed, chewed, or split — because disrupting the matrix accelerates release and produces immediate-release pharmacokinetics with risk of hypotension and sedation. Co-administration with a high-fat meal increases C_max by approximately 75% and AUC by approximately 40%, so high-fat meals should be avoided. After two or more consecutive missed doses, consider re-titrating based on tolerability.

Pharmacology

Mechanism of Action

Guanfacine is a selective post-synaptic α_2A-adrenergic receptor agonist with substantially greater affinity (reported as 15–20 fold) for the α_2A subtype than for α_2B or α_2C subtypes — the feature that distinguishes it pharmacologically from clonidine and explains its more favourable sedation and cardiovascular profile. In the prefrontal cortex, α_2A activation on pyramidal neurons is hypothesized to strengthen functional network connectivity and improve working memory and behavioural inhibition; this central action is believed to underlie its therapeutic effect in ADHD. Peripherally, agonism at brainstem α₂ receptors reduces sympathetic outflow, producing a fall in peripheral vascular resistance, heart rate, and blood pressure that accounts for both its antihypertensive effect and its principal cardiovascular adverse effects. Unlike stimulants, guanfacine is not a CNS stimulant, has no abuse potential, and does not increase synaptic dopamine or noradrenaline in the striatum.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Readily absorbed; T_max ~5 h (XR, paediatric); 4–8 h (XR, adults); 1–4 h (IR). High-fat meal raises C_max ~75% and AUC ~40% (XR)	Take XR consistently; avoid high-fat meals to prevent peak-related toxicity
Distribution	V_d 6.3 L/kg (after IV dosing); apparent oral V_d higher in paediatric patients (~24 L/kg in children, ~20 L/kg in adolescents); protein binding 64–72% (chiefly albumin)	Wide tissue distribution; protein binding low enough that displacement interactions are clinically minor
Metabolism	Hepatic via CYP3A4 (and CYP3A5); main metabolite 3-hydroxy-guanfacine (and its glucuronide and sulfate conjugates)	Susceptible to CYP3A4 inhibitors and inducers; dose adjustment required (see Interactions)
Elimination	~50% excreted unchanged in urine; remainder as metabolites; t_½ ~14 h in children, ~18 h in adolescents and adults (range reported 10–30 h)	Once-daily XR dosing supported by long half-life; clearance reduced in significant renal or hepatic impairment

Side Effects

The adverse-effect profile is dominated by sedation, fatigue, and cardiovascular effects (hypotension, bradycardia). Most adverse effects are dose-related, attenuate over the first weeks of therapy, and respond to slower titration. Frequencies below are taken from the Intuniv FDA prescribing information (fixed-dose paediatric monotherapy Studies 1 and 2; n=513 on Intuniv vs n=149 placebo) and the Tenex FDA prescribing information for adult hypertension. In the Intuniv tables the term “somnolence” encompasses somnolence, sedation, and hypersomnia, and the term “hypotension” encompasses hypotension and orthostatic and diastolic/systolic blood-pressure decreases.

≥10% Very Common

Adverse Effect	Incidence	Clinical Note
Somnolence (umbrella: somnolence/sedation/hypersomnia) — Intuniv paediatric	38%	Versus 11% placebo in fixed-dose trials; rises with dose (28% at 1 mg, 51% at 4 mg). Peaks early in therapy and usually attenuates
Headache — Intuniv paediatric	23%	Versus 19% placebo; usually mild and transient
Fatigue — Intuniv paediatric	14%	Versus 3% placebo; distinct from sedation; can persist beyond initial weeks
Abdominal pain (umbrella term) — Intuniv paediatric	11%	Versus 9% placebo; rises with dose. Take with light food if tolerated
Dry mouth — Tenex IR adult HTN	up to 47%	Dose-dependent; far more frequent with IR formulation in adults than with XR in paediatric trials
Constipation — Tenex IR adult HTN	up to 16%	Dose-related; address with hydration, fibre, and osmotic laxatives if needed
Somnolence — Tenex IR adult HTN	up to 10–21%	Bedtime dosing minimizes daytime impact
Fatigue — Tenex IR adult HTN	~12%	Similar pattern to paediatric population; usually improves with continued therapy

1–10% Common

Adverse Effect	Incidence	Clinical Note
Hypotension (umbrella term) — Intuniv paediatric	7%	Versus 3% placebo; orthostatic hypotension reported in ~1%. Check seated and standing BP at each dose increase
Lethargy — Intuniv paediatric	6%	Versus 3% placebo; overlaps with somnolence; consider dose reduction if functioning declines
Dizziness — Intuniv paediatric	6%	Often orthostatic; counsel on slow positional changes
Nausea — Intuniv paediatric	6%	Generally improves with continued therapy
Decreased appetite — Intuniv paediatric	6%	Less appetite suppression than stimulants; track weight in children
Irritability — Intuniv paediatric	6%	Distinguish from underlying ADHD/mood symptoms; reassess if worsening
Dry mouth — Intuniv paediatric	4%	Less prominent than with the IR formulation in adults
Constipation — Intuniv paediatric	3%	Hydration and fibre usually sufficient
Insomnia (umbrella term) — Intuniv paediatric	~2–13%	Range across trials; paradoxical despite sedation; review dose timing
Bradycardia — Intuniv paediatric	2–5%	Document baseline HR; symptomatic bradycardia warrants dose review
Nightmare/abnormal dreams — Intuniv paediatric	2%	Rises with dose; usually self-limiting
Enuresis (umbrella term) — Intuniv paediatric	2%	Includes nocturia and urinary incontinence; rare in adults
First-degree AV block — Intuniv paediatric	<2%	Listed as <2% adverse reaction in fixed-dose trials
Asthenia — Tenex IR adult HTN	~6%	Generalized weakness; distinguish from sedation
Impotence — Tenex IR adult HTN	listed as ≤3%	Reported as a reason for dropout in adult trials; usually reversible on discontinuation

Serious Regardless of Frequency

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Syncope	~1% (paediatric, mostly long-term open-label)	During titration or with dehydration/heat	Withhold dose; assess vitals; reduce dose or alternative; counsel on hydration
Symptomatic hypotension / orthostasis	Uncommon	Days to weeks; greater on dose increases	Reduce or hold dose; review concomitant antihypertensives
Symptomatic bradycardia	Rare	Variable; risk increases with sympatholytic co-medication	ECG; cardiology referral; discontinue if persistent symptoms
Atrioventricular block (worsening of pre-existing or new)	Rare	Any time; greater risk with concomitant sympatholytic drugs	ECG; cardiology evaluation; usually requires discontinuation
Rebound hypertension on abrupt discontinuation (with reports of hypertensive encephalopathy)	Class effect; rare with proper taper (postmarketing)	Within days of stopping; greater risk at higher doses and with stimulant co-use	Reinitiate guanfacine and taper slowly; daily BP monitoring; emergency care if encephalopathic features
Hypersensitivity reactions (rash, exfoliative dermatitis, pruritus)	Rare	Any time	Discontinue; supportive care; future use contraindicated
Hallucinations	Postmarketing reports; very rare	Variable	Discontinue; psychiatric evaluation

Discontinuation Treatment Cessation Rates

Paediatric (XR / Intuniv) — monotherapy

12% vs 4% placebo

Top reasons: somnolence/sedation (6%), fatigue (2%); hypotension, headache, and dizziness each ~1%. Discontinuation rises with dose (3% at 1 mg, 18% at 4 mg).

Paediatric (XR / Intuniv) — adjunctive to stimulant

3% vs 1% placebo

Top reasons: no specific adverse reaction reached the ≥2% threshold for discontinuation in this study.

Reason for Discontinuation	Incidence (Paediatric XR, Fixed-Dose Monotherapy)	Context
Somnolence / sedation / hypersomnia	6% (vs 1% placebo)	Most common cause overall; rises with dose (3% at 1 mg, 11% at 4 mg)
Fatigue	2% (vs 0% placebo)	Persistent fatigue beyond 4 weeks should prompt dose review
Hypotension	~1%	Met the ≥2% threshold in some dose groups but not across all doses combined
Headache	~1%	Less commonly the lone reason for stopping
Dizziness	~1%	Usually orthostatic in nature

Managing Sedation — The Most Common Limiting Effect

Sedation peaks early in titration and is the leading cause of discontinuation. Strategies that improve tolerability without giving up therapeutic benefit: (1) advance dose by 1 mg only every 1–2 weeks rather than weekly in sensitive patients; (2) shift the dose to bedtime if morning sedation predominates; (3) reassess concurrent CNS depressants such as antihistamines, anticonvulsants, or sleep aids. Most cases improve substantially over weeks of continued therapy.

Int

Drug Interactions

Guanfacine is a CYP3A4 substrate, so the most clinically meaningful interactions involve strong and moderate CYP3A4 inhibitors and inducers. Pharmacodynamic interactions — additive sedation with CNS depressants and additive hypotension and bradycardia with cardiovascular drugs — are also frequent in real-world practice. Guanfacine does not significantly affect the pharmacokinetics of methylphenidate or lisdexamfetamine.

Major Strong & moderate CYP3A4 inhibitors (ketoconazole, itraconazole, ritonavir, clarithromycin)

MechanismInhibition of guanfacine’s primary metabolic pathway

EffectIncreased plasma exposure; greater risk of sedation, hypotension, syncope

ManagementReduce Intuniv dose to 50% of target when initiating or continuing the inhibitor; restore dose when inhibitor is stopped

FDA PI

Major Strong & moderate CYP3A4 inducers (rifampin, phenytoin, carbamazepine, St John’s wort)

MechanismAccelerated CYP3A4-mediated metabolism

EffectReduced guanfacine concentration; loss of clinical effect

ManagementConsider titrating Intuniv up to 2× the target dose over 1–2 weeks; halve the dose again over 1–2 weeks when the inducer is stopped

FDA PI

Major Other antihypertensives & sympatholytic drugs

MechanismAdditive blood-pressure lowering and AV-nodal slowing

EffectSymptomatic hypotension, syncope, bradycardia, falls

ManagementStagger initiation; check seated and standing BP and HR within 1–2 weeks; counsel on orthostatic precautions

FDA PI

Major Beta-blockers (especially when discontinuing guanfacine)

MechanismUnopposed alpha-mediated vasoconstriction during α₂-agonist withdrawal

EffectSevere rebound hypertension if guanfacine is stopped while a beta-blocker continues (class effect with α₂-agonists)

ManagementDiscontinue the beta-blocker first when possible; otherwise taper guanfacine very slowly with daily BP checks

Lexicomp

Moderate Valproic acid

MechanismPossible mutual pharmacokinetic interference; valproate concentrations may rise

EffectPossible elevated valproate levels and increased adverse effects

ManagementMonitor valproate levels and signs of toxicity if combination is used

FDA PI

Moderate CNS depressants (alcohol, benzodiazepines, opioids, sedating antihistamines)

MechanismPharmacodynamic synergy on central depression

EffectPronounced sedation, impaired alertness, increased fall risk

ManagementCounsel on driving; minimize concurrent sedating drugs; avoid alcohol

FDA PI

Moderate Stimulants (methylphenidate, amphetamines)

MechanismPharmacodynamic; opposing cardiovascular effects

EffectNo clinically significant pharmacokinetic interaction with methylphenidate or lisdexamfetamine; combination generally well tolerated

ManagementCombination is FDA-approved for ADHD; monitor HR and BP at each visit; greater attention to rebound risk if stopping guanfacine while continuing stimulant

FDA PI

Moderate Tricyclic antidepressants (e.g., amitriptyline, imipramine)

MechanismTCAs antagonize central α₂-receptors

EffectMay reduce antihypertensive and ADHD efficacy of guanfacine

ManagementReassess clinical response; consider non-TCA alternative if possible

Lexicomp

Minor Grapefruit juice

MechanismIntestinal CYP3A4 inhibition

EffectModest increase in guanfacine concentration possible

ManagementCounsel patients to avoid large daily quantities

Lexicomp

Minor High-fat meals (XR formulation)

MechanismEffect on extended-release matrix kinetics

EffectC_max rises ~75% and AUC ~40%; increased peak-related adverse effects

ManagementAvoid taking with high-fat meals; consistent timing relative to food

FDA PI

Mon

Monitoring

The Intuniv prescribing information specifies measuring heart rate and blood pressure prior to initiation, following dose increases, and periodically while on therapy. Paediatric patients on chronic therapy additionally need growth and behavioural surveillance.

Blood pressure Baseline; after each dose change; periodically thereafter
Routine Document seated and standing values during titration. Symptomatic orthostasis or significant decline below age-appropriate norms warrants pause and reassessment.
Heart rate Baseline; after each dose change; periodically thereafter
Routine A resting HR below age-appropriate norms or symptomatic bradycardia should prompt dose review.
Cardiac history & ECG Baseline cardiac history at initiation; ECG if risk factors
Trigger-based Indicated when there is a personal or family history of structural heart disease, sudden cardiac death, arrhythmia, or use of other sympatholytic or AV-nodal-blocking agents.
Sedation & alertness Each visit during titration and first weeks
Routine Use parent or teacher report or self-rating in adolescents. Persistent functional sedation beyond several weeks warrants dose reduction.
ADHD response Baseline; reassess at 4–6 weeks; then every 3–6 mo
Routine Validated rating scales (Vanderbilt, SNAP-IV, ADHD-RS) at home and school improve sensitivity to change.
Growth (paediatric) Periodically (e.g., every 6 mo)
Routine Plot weight and height percentiles. Long-term Intuniv data show normal growth trajectories, but ongoing surveillance is reasonable.
Mood & behaviour Each visit, especially during titration
Routine Ask about mood change, irritability, and unusual experiences. Hallucinations have been reported postmarketing.
Renal function If CKD risk; if signs of accumulation
Trigger-based About half of guanfacine is excreted unchanged in urine. Routine monitoring in healthy patients is not required.
Hepatic function If clinical suspicion or hepatotoxic co-medication
Trigger-based No routine LFT screening required for guanfacine alone.
Adherence & taper plan Each visit; explicitly before any planned discontinuation
Routine Confirm taper plan in writing. Children with vomiting illnesses are at particular risk for unintentional rebound hypertension.

Contraindications & Cautions

Absolute Contraindications

History of hypersensitivity to guanfacine, its inactive ingredients, or other products containing guanfacine. Rash and pruritus have been reported and exfoliative dermatitis has been described with the immediate-release product.

Relative Contraindications — Specialist Input Recommended

Pre-existing heart block, sinus node dysfunction, or significant baseline bradycardia — cardiology input before initiation, given potential to worsen these.
History of syncope or conditions predisposing to syncope (orthostatic hypotension, dehydration).
Recent myocardial infarction or unstable cardiovascular disease.
Cerebrovascular disease — risk of cerebral hypoperfusion with abrupt BP lowering.
Severe hepatic impairment — reduced clearance; consider dose reduction with specialist input.
Severe renal impairment — consider dose reduction with specialist input.
Concurrent strong or moderate CYP3A4 inhibitors that cannot be substituted — reduce Intuniv to 50% of target dose and monitor closely.

Use with Caution

Elderly patients — higher orthostatic hypotension and fall risk.
Patients on multiple antihypertensives or other sympatholytic drugs — additive effects on BP, HR, and AV conduction likely.
Pregnancy — no adequate, well-controlled human studies; use only if benefit justifies fetal risk.
Lactation — observe nursing infants for sedation and somnolence.
Operating heavy machinery or driving — particularly during titration.
Children with intercurrent vomiting illness — missed doses can lead to rebound hypertension.
Concurrent alcohol or other CNS depressants — advise patients to avoid.

FDA Class-Wide Regulatory Warning Risk of Rebound Hypertension on Abrupt Discontinuation

The Intuniv prescribing information warns that abrupt discontinuation can lead to clinically significant and persistent rebound hypertension above baseline levels and increases in heart rate. Hypertensive encephalopathy has been reported in association with rebound hypertension with both Intuniv and immediate-release guanfacine, particularly with high-dose therapy and concomitant stimulant use. Children commonly have gastrointestinal illnesses that lead to vomiting and inability to take medications, placing them at particular risk.

To minimize this risk, the total daily dose should be tapered in decrements of no more than 1 mg every 3–7 days. Blood pressure and heart rate should be monitored when reducing the dose or discontinuing therapy. This is a class effect shared with other centrally acting α₂-agonists such as clonidine.

Patient Counselling

Purpose of Therapy

For ADHD, guanfacine works differently from stimulants. It activates a specific receptor in the front of the brain that supports focus, attention, and impulse control, often with additional benefit for irritability or sleep. It is not a stimulant, has no abuse potential, and benefit usually emerges over 2–4 weeks once the effective dose is reached, rather than within hours like stimulants. For hypertension, guanfacine reduces blood pressure by lowering the signal from the brain that tells blood vessels to constrict.

How to Take

The extended-release tablet is taken once daily at the same time each day, in the morning or evening. It must be swallowed whole and never crushed, chewed, or split. Avoid taking it with a high-fat meal because this can cause too much medicine to be released at once. The immediate-release tablet for blood pressure is usually taken at bedtime to reduce daytime drowsiness. If two or more doses are missed in a row, the prescriber may need to re-titrate the dose. Never double up on a missed dose.

Drowsiness & Sedation

Tell patient Sedation is most prominent in the first weeks of therapy and usually improves substantially. Avoid driving, cycling, or operating machinery until you know how the medication affects you. Avoid alcohol, which makes drowsiness much worse.

Call prescriber If drowsiness is severe enough to interfere with school or work, persists beyond several weeks, or is associated with confusion or inability to wake normally.

Dizziness & Light-headedness

Tell patient Stand up slowly from sitting or lying down, especially in the morning. Stay well hydrated, particularly in hot weather or during exercise. Sit or lie down immediately if you feel light-headed.

Call prescriber If you faint or nearly faint, fall, or feel dizzy with chest pain or palpitations.

Heart Rate & Blood Pressure

Tell patient Guanfacine slows the heart rate and lowers blood pressure as part of how it works. Mild slowing is expected and not harmful in most people.

Call prescriber If you feel your heart racing, skipping beats, or beating very slowly; if you have chest pain, shortness of breath, or unusual fatigue.

Stopping the Medication

Tell patient Never stop guanfacine suddenly. Stopping abruptly can cause a sharp rise in blood pressure, headache, anxiety, and a fast heart rate, and rare but serious cases have included hypertensive encephalopathy. Always taper under your prescriber’s guidance, even if you feel well.

Call prescriber If you have missed two or more doses, develop severe headache, palpitations, or feel acutely unwell after stopping. Children with stomach bugs that prevent taking the medication need an early call.

Mood & Behaviour Changes

Tell patient Most people feel calmer on guanfacine. Less commonly, children may become more irritable, low in mood, or experience nightmares. Hallucinations have been reported very rarely.

Call prescriber For significant behavioural change, persistent low mood, or any unusual sensory experience such as hearing or seeing things that are not there.

Taking with Other Medications

Tell patient Inform every healthcare provider that you take guanfacine. Many cold and allergy medications, sleep aids, and antidepressants can add to its sedative or blood-pressure effects. Avoid grapefruit juice in large quantities. Always ask the pharmacist before starting an over-the-counter product.

Call prescriber Before starting any new prescription, especially antibiotics, antifungals, or seizure medications.

Dry Mouth & Constipation

Tell patient Drink water regularly, chew sugar-free gum, and use sugar-free lozenges for dry mouth. For constipation, increase fluids and fibre; an over-the-counter osmotic laxative may help if needed. These effects are more common with the immediate-release tablet used for blood pressure than with the extended-release form.

Call prescriber If constipation persists more than two weeks despite home measures, or if abdominal pain is severe.

Ref

Sources

Regulatory (PI / SmPC)

Intuniv (guanfacine) extended-release tablets — full prescribing information. U.S. Food and Drug Administration. Available at accessdata.fda.gov Primary source for ADHD dosing tables, pediatric trial adverse-event tables, CYP3A4 dose-adjustment guidance, and the rebound hypertension warning.
Tenex (guanfacine hydrochloride) immediate-release tablets — full prescribing information. U.S. Food and Drug Administration. Available at accessdata.fda.gov Primary source for adult hypertension dosing, the IR-formulation adverse-event profile (dry mouth, constipation, asthenia, impotence), and discontinuation/rebound warnings.
Intuniv Summary of Product Characteristics. European Medicines Agency. Available at ema.europa.eu European regulatory perspective; aligns with the FDA label on dosing and adverse events.

Key Clinical Trials

Biederman J, Melmed RD, Patel A, et al. A randomized, double-blind, placebo-controlled study of guanfacine extended release in children and adolescents with attention-deficit/hyperactivity disorder. Pediatrics. 2008;121(1):e73–e84. doi:10.1542/peds.2006-3695 Pivotal pediatric monotherapy trial that established Intuniv efficacy and dose-response in ADHD.
Sallee FR, McGough J, Wigal T, et al. Guanfacine extended release in children and adolescents with attention-deficit/hyperactivity disorder: a placebo-controlled trial. J Am Acad Child Adolesc Psychiatry. 2009;48(2):155–165. doi:10.1097/CHI.0b013e318191769e Second pivotal trial confirming efficacy in 6–17-year-olds with detailed adverse-event characterization.
Wilens TE, Bukstein O, Brams M, et al. A controlled trial of extended-release guanfacine and psychostimulants for attention-deficit/hyperactivity disorder. J Am Acad Child Adolesc Psychiatry. 2012;51(1):74–85.e2. doi:10.1016/j.jaac.2011.10.012 Adjunctive-to-stimulant trial supporting combination-therapy approval.
Newcorn JH, Stein MA, Childress AC, et al. Randomized, double-blind trial of guanfacine extended release in children with attention-deficit/hyperactivity disorder: morning or evening administration. J Am Acad Child Adolesc Psychiatry. 2013;52(9):921–930. doi:10.1016/j.jaac.2013.06.006 Comparative timing study informing flexible morning vs evening administration schedules.

Guidelines

Wolraich ML, Hagan JF, Allan C, et al. Clinical practice guideline for the diagnosis, evaluation, and treatment of attention-deficit/hyperactivity disorder in children and adolescents. American Academy of Pediatrics. Pediatrics. 2019;144(4):e20192528. doi:10.1542/peds.2019-2528 Current AAP guideline addressing the place of guanfacine among non-stimulant options.
Pliszka S, AACAP Work Group on Quality Issues. Practice parameter for the assessment and treatment of children and adolescents with attention-deficit/hyperactivity disorder. J Am Acad Child Adolesc Psychiatry. 2007;46(7):894–921. doi:10.1097/chi.0b013e318054e724 AACAP framework for sequencing stimulants and α₂-agonists in pediatric ADHD.
Pringsheim T, Okun MS, Mller-Vahl K, et al. Practice guideline recommendations summary: treatment of tics in people with Tourette syndrome and chronic tic disorders. American Academy of Neurology. Neurology. 2019;92(19):896–906. doi:10.1212/WNL.0000000000007466 AAN guideline supporting α₂-agonists, including guanfacine, as treatment options for tics.
National Institute for Health and Care Excellence. Attention deficit hyperactivity disorder: diagnosis and management (NG87). London: NICE; updated 2019. Available at nice.org.uk UK guideline; positions guanfacine as a non-stimulant option after stimulants and atomoxetine.

Mechanistic / Basic Science

Arnsten AFT. The use of α_2A-adrenergic agonists for the treatment of attention-deficit/hyperactivity disorder. Expert Rev Neurother. 2010;10(10):1595–1605. doi:10.1586/ern.10.133 Authoritative mechanistic review on α_2A agonism in prefrontal cortex and ADHD.
Sorkin EM, Heel RC. Guanfacine: a review of its pharmacodynamic and pharmacokinetic properties, and therapeutic efficacy in the treatment of hypertension. Drugs. 1986;31(4):301–336. doi:10.2165/00003495-198631040-00003 Foundational pharmacology review covering the immediate-release formulation in hypertension.

Pharmacokinetics / Special Populations

Boellner SW, Pennick M, Fiske K, Lyne A, Shojaei A. Pharmacokinetics of a guanfacine extended-release formulation in children and adolescents with attention-deficit/hyperactivity disorder. Pharmacotherapy. 2007;27(9):1253–1262. doi:10.1592/phco.27.9.1253 Pediatric PK study supporting once-daily dosing and weight-based titration; source of paediatric vs adolescent half-life and apparent volume-of-distribution data cited above.
Swearingen D, Pennick M, Shojaei A, Lyne A, Fiske K. A phase I, randomized, open-label, crossover study of the single-dose pharmacokinetic properties of guanfacine extended-release 1-, 2-, and 4-mg tablets in healthy adults. Clin Ther. 2007;29(4):617–625. doi:10.1016/j.clinthera.2007.04.001 Adult PK comparison across XR strengths informing food-effect and bioavailability discussions.