Clobetasol Propionate: Comprehensive Drug Monograph

Pharmacokinetic Profile

Systemic Absorption

Low from intact skin; increased by inflammation, occlusion, barrier disruption

HPA Suppression Threshold

As low as 2 g/day (ointment)

Metabolism

Hepatic (corticosteroid pathways); not fully characterized

Protein Binding

Varies (as with systemic corticosteroids)

Elimination

Renal and biliary

Clinical Information

Drug Class

Topical corticosteroid — super-high potency (Class I)

Available Forms

Cream, Ointment, Gel, Foam, Lotion, Solution, Shampoo, Spray (all 0.05%)

Route

Topical

Max Duration

2 consecutive weeks (4 weeks for some formulations in psoriasis)

Max Weekly Dose

50 g (or 50 mL) per week

Renal Adjustment

Not required (minimal systemic absorption)

Hepatic Adjustment

Not required (minimal systemic absorption)

Pregnancy

Use only if benefit outweighs risk; teratogenic in animals

Lactation

Caution; not known if excreted in breast milk

Pediatric Use

Not recommended <12 years (most formulations)

Schedule

Rx only

Generic Available

Yes

Indications

Indication	Approved Population	Therapy Type	Status
Corticosteroid-responsive dermatoses (inflammatory and pruritic manifestations)	≥12 years (cream/ointment/gel/solution)	Short-term topical monotherapy	FDA Approved
Moderate to severe plaque-type psoriasis	≥16 years (emollient cream); ≥18 years (spray/lotion)	Short-term topical monotherapy	FDA Approved
Moderate to severe atopic dermatitis (short-term relief)	≥12 years	Short-term topical monotherapy	FDA Approved
Scalp dermatoses (psoriasis, seborrheic dermatitis of scalp)	≥12 years (solution); ≥18 years (shampoo)	Short-term topical monotherapy	FDA Approved

Clobetasol propionate is the most potent topical corticosteroid available, classified as super-high potency (US Class I / WHO Group IV). It is indicated for short-term treatment of moderate to severe inflammatory dermatoses that have not responded to less potent agents. Due to its potency and risk of hypothalamic-pituitary-adrenal (HPA) axis suppression, clobetasol propionate is intended as a second-line or rescue therapy, not a first-choice topical steroid. Treatment should be limited to the minimum duration necessary to achieve control, generally no more than 2 consecutive weeks for most formulations.

Off-Label Uses

Vulvar lichen sclerosus — Evidence quality: High. Clobetasol propionate 0.05% ointment is considered first-line therapy for vulvar lichen sclerosus per multiple international guidelines, though the specific formulation is not separately FDA-approved for this indication.

Alopecia areata — Evidence quality: Moderate. Used as initial topical therapy for limited patchy alopecia areata to induce regrowth.

Oral lichen planus — Evidence quality: Moderate. Topical clobetasol in an adhesive paste vehicle is commonly used for symptomatic erosive oral lichen planus.

Vitiligo (adjunctive) — Evidence quality: Low-Moderate. Used off-label to repigment limited vitiligo patches, particularly on the face and neck.

Cutaneous graft-versus-host disease — Evidence quality: Moderate. First-line topical therapy for acute and chronic cutaneous GVHD.

Dose

Dosing

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Severe plaque psoriasis — localized (≤20% BSA)	Thin film BID to affected areas	Thin film BID	50 g/week; max 2–4 weeks	Step down to lower-potency steroid once control achieved Clobex lotion/spray may be used up to 4 weeks for psoriasis per labelling
Severe eczema / Atopic dermatitis flare — short-term rescue	Thin film BID to affected areas	Thin film BID; taper or step down within 2 weeks	50 g/week; max 2 weeks	Not for maintenance; switch to mid-potency steroid or calcineurin inhibitor after flare control Avoid face, groin, axillae
Scalp psoriasis or severe scalp dermatoses	Solution or shampoo: apply to dry scalp BID (solution) or daily (shampoo)	Same frequency; 15 min contact for shampoo	50 mL/week; max 2–4 weeks	Shampoo: apply to dry scalp, lather after 15 min, rinse Clobex shampoo HPA suppression: 5/12 adolescents at 4 weeks
Vulvar lichen sclerosus — induction (off-label)	Ointment: fingertip unit once daily at bedtime	Once daily for 4–12 weeks, then taper	Per clinical response	Taper to 2–3 times/week for maintenance; long-term use accepted under specialist supervision Off-label but guideline-supported as first-line by BAD, ISSVD
Localized alopecia areata (off-label)	Thin film BID to affected scalp patches	BID for up to 12 weeks	Limited to patches; not for total scalp	Under occlusion (e.g., shower cap overnight) may increase efficacy but also increases HPA risk Monitor for scalp atrophy and telangiectasia

Clinical Pearl: The “Weekend Pulse” Strategy

For chronic conditions requiring intermittent super-potent steroid use, some dermatologists employ a “weekend pulse” or “proactive” approach: after achieving initial control with daily clobetasol propionate (max 2 weeks), the patient transitions to applying clobetasol propionate only on 2 consecutive days per week (e.g., Saturday and Sunday) to previously affected areas. This approach reduces cumulative exposure and HPA axis risk while preventing flares. On the remaining days, a lower-potency steroid or emollient is used. This strategy has the strongest evidence base in psoriasis and lichen sclerosus maintenance.

Pharmacology

Mechanism of Action

Clobetasol propionate is a synthetic fluorinated corticosteroid and a prednisolone analog with exceptionally high glucocorticoid receptor affinity and minimal mineralocorticoid activity. Like all topical corticosteroids, it exerts its effects by binding to intracellular glucocorticoid receptors, forming a receptor-ligand complex that translocates to the nucleus and modulates gene transcription. This produces a broad spectrum of anti-inflammatory, immunosuppressive, antiproliferative, and vasoconstrictive effects in the skin.

Specifically, clobetasol propionate inhibits the release of arachidonic acid from cell membranes by inducing lipocortin (annexin A1), which inhibits phospholipase A2. This reduces the production of prostaglandins, leukotrienes, and other inflammatory mediators. It suppresses the transcription of pro-inflammatory cytokines (including IL-1, IL-6, TNF-alpha) by inhibiting NF-kappa B signaling. It reduces mast cell density and eosinophil activation, decreases capillary permeability (producing vasoconstriction and reduced edema), and inhibits keratinocyte proliferation. The combined anti-inflammatory, immunosuppressive, and antimitotic effects make it highly effective for recalcitrant inflammatory dermatoses, but also underlie its potential for skin atrophy and systemic side effects when used excessively.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Percutaneous; minimal from intact skin. Mean peak plasma ~0.63 ng/mL (healthy skin, 0.05% ointment); ~2.3–4.6 ng/mL (psoriasis/eczema). Increased by inflammation, broken barrier, occlusion, and larger treatment area.	Diseased skin absorbs significantly more drug, increasing systemic risk. Limiting BSA and duration is critical. HPA suppression documented at doses as low as 2 g/day.
Distribution	Bound to plasma proteins in varying degrees (as with systemic corticosteroids). Concentrates in the epidermis and dermis at the application site.	Local concentration drives therapeutic effect; systemic distribution is undesirable and dose-limiting.
Metabolism	Once absorbed, follows systemic corticosteroid metabolic pathways; metabolized primarily in the liver. Specific metabolic pathways for clobetasol propionate have not been fully characterized.	Hepatic impairment could theoretically slow clearance of absorbed drug, but this is not clinically relevant at standard topical doses.
Elimination	Excreted by kidneys (urine) and in bile. Absorbed drug is cleared through standard corticosteroid elimination pathways.	No dose adjustment needed for renal or hepatic impairment when used topically within labeled parameters.

Side Effects

Adverse effects with clobetasol propionate are predominantly local and relate to its potency. Systemic effects are possible with excessive use. Rates below are from the FDA-approved prescribing information for the emollient cream 0.05% and lotion 0.05% clinical trials.

≥10%Very Common

Adverse Effect	Incidence	Clinical Note
HPA axis suppression (with extended use or large BSA)	25% (1 week, ≥30% BSA); up to 80% (4 weeks lotion)	Dose-, duration-, area-, and occlusion-dependent; generally reversible on discontinuation; most potent predictor of systemic risk

1–10%Common

Adverse Effect	Incidence	Clinical Note
Burning / Stinging at application site	~5%	Most common reported adverse reaction in clinical trials; transient; usually self-limiting
Pruritus	<2%	Paradoxical in some patients; may indicate developing sensitization
Erythema at application site	<2%	Distinct from the treated condition; may indicate irritant or allergic contact dermatitis to the vehicle
Skin atrophy	<2% (short courses); higher with prolonged use	Thinning of the epidermis and dermis; can become irreversible with extended use; particularly problematic on the face and flexures
Telangiectasia	<2%	Dilated superficial blood vessels; may be irreversible; risk increases with duration and use on the face
Folliculitis / Acneiform eruptions	<2%	Steroid folliculitis; more likely under occlusion or on trunk
Cracking and fissuring of the skin	<2%	Especially on fingers, palms, and soles with excessive use

SeriousSerious (Regardless of Frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Cushing’s syndrome (iatrogenic)	Rare (reported in infants and adults)	Weeks to months of overuse	Discontinue clobetasol; endocrinology referral; gradual taper to avoid adrenal crisis; may require systemic steroid replacement
Adrenal crisis (on abrupt withdrawal after prolonged use)	Rare	Within days of abrupt discontinuation	Emergency systemic corticosteroid replacement; never abruptly stop after prolonged use on large areas
Glaucoma / Increased intraocular pressure	Rare; risk with periocular use	Weeks to months	Avoid application near eyes; ophthalmology referral if visual symptoms develop; measure IOP
Posterior subcapsular cataracts	Rare; with prolonged periocular use	Months of use near eyes	Ophthalmology referral; avoid periocular application
Irreversible skin atrophy and striae	Uncommon with short courses; risk increases with duration	Weeks to months of continuous use	Discontinue use; striae are permanent; counsel patient that atrophy may partially recover over months
Allergic contact dermatitis (to vehicle or clobetasol itself)	Rare	Days to weeks	Suspect if condition worsens despite treatment; patch testing; switch vehicle or class

DiscontinuationDiscontinuation Considerations

Planned discontinuation

At 2 weeks (labeled max)

Approach: Step down to mid-potency steroid or calcineurin inhibitor; do not stop abruptly after prolonged or extensive use.

Rebound flare risk

Moderate to High

Risk factors: Abrupt discontinuation, psoriasis, prolonged use. Rebound may be more severe than the original condition, particularly in psoriasis.

Managing the Step-Down: Avoiding Rebound and Withdrawal

Abrupt discontinuation of clobetasol propionate after extended use (beyond 2 weeks or on large body surface areas) can precipitate rebound flaring of the underlying condition, and in severe cases, symptoms of adrenal insufficiency. The recommended approach is a gradual step-down: (1) reduce frequency from twice daily to once daily for 1 week; (2) alternate with a mid-potency steroid (e.g., triamcinolone 0.1%) for another 1–2 weeks; (3) transition to maintenance with a low-potency steroid or non-steroidal agent (tacrolimus, pimecrolimus). In psoriasis, abrupt cessation of potent topical steroids has been associated with pustular flares.

Int

Drug Interactions

Clobetasol propionate has minimal systemic absorption under normal use conditions, making pharmacokinetic drug interactions unlikely. The clinically relevant interactions are pharmacodynamic, primarily related to additive immunosuppressive or skin-thinning effects.

ModerateOther Topical Corticosteroids (concomitant use)

MechanismAdditive HPA axis suppression from combined corticosteroid exposure

EffectIncreased risk of systemic corticosteroid effects, including adrenal suppression and Cushing’s syndrome

ManagementDo not use clobetasol propionate concurrently with other topical corticosteroid products; use one potency-appropriate agent at a time

FDA PI

ModerateSystemic Corticosteroids

MechanismAdditive HPA axis suppression from topical + systemic corticosteroid exposure

EffectCompounded risk of adrenal suppression, hyperglycemia, osteoporosis, and immunosuppression

ManagementUse with caution; minimize topical steroid exposure if systemic steroids are required; monitor for signs of excessive steroid effect

Clinical consensus

ModerateCYP3A4 Inhibitors (ritonavir, itraconazole, cobicistat)

MechanismReduced hepatic clearance of any systemically absorbed clobetasol propionate

EffectTheoretically increased systemic exposure to clobetasol and risk of HPA suppression or Cushing-like effects

ManagementUse clobetasol on the smallest area for the shortest duration possible; consider a less potent steroid alternative; this interaction is most relevant when clobetasol is applied to large BSA or under occlusion

Class effect / Lexicomp

MinorTopical Retinoids (tretinoin, adapalene, tazarotene)

MechanismRetinoids thin the stratum corneum, potentially increasing percutaneous absorption of clobetasol

EffectIncreased local and potentially systemic clobetasol exposure; increased skin irritation

ManagementIf used together, apply at different times of day (e.g., clobetasol in the morning, retinoid in the evening); monitor for excessive irritation or atrophy

Clinical consensus

Mon

Monitoring

Routine laboratory monitoring is not required for short courses (≤2 weeks) on limited body surface area. However, when clobetasol propionate is used on larger areas, for longer durations, or in vulnerable populations, HPA axis evaluation should be considered.

HPA Axis FunctionIf use exceeds 2 weeks or >20% BSA
Trigger-BasedACTH stimulation test (cosyntropin test), morning plasma cortisol, or urinary free cortisol. Clobetasol has been shown to suppress the HPA axis at doses as low as 2 g/day. In clinical studies, 25% of patients with ≥30% BSA involvement developed adrenal suppression after just 1 week. Recovery is generally prompt upon discontinuation.
Skin Integrity AssessmentEvery visit during treatment
RoutineInspect for signs of skin atrophy (thinning, visible blood vessels, shiny appearance), striae, telangiectasia, and steroid rosacea. These may develop within weeks of use, particularly on the face and flexural areas. Some changes (striae, telangiectasia) may be irreversible.
Treatment DurationEvery visit
RoutineConfirm the patient is not exceeding 2 consecutive weeks of use (4 weeks for specific psoriasis formulations). Verify total weekly application does not exceed 50 g. Patients frequently self-extend potent steroid use beyond the prescribed duration.
Growth Velocity (pediatric)If used in adolescents 12–17 years
Trigger-BasedChildren are more susceptible to systemic absorption due to higher body surface area to body mass ratio. Monitor height velocity if clobetasol use is prolonged or recurrent. Use is not recommended under age 12.
Ocular SymptomsEvery visit if applied to face or near eyes
Trigger-BasedAsk about visual changes, pain, or blurred vision. Topical corticosteroid use near the eyes carries risk of glaucoma, increased IOP, and posterior subcapsular cataracts. Refer to ophthalmology if symptoms occur.
Signs of Secondary InfectionEvery visit
RoutineCorticosteroids suppress local immune defenses. Monitor for signs of bacterial, fungal, or viral superinfection (e.g., worsening despite treatment, impetiginization, tinea incognito, herpes simplex flare). Treat infection before continuing clobetasol.

Contraindications & Cautions

Absolute Contraindications

Hypersensitivity to clobetasol propionate, other corticosteroids, or any component of the formulation.
Primary skin infections — Untreated bacterial, viral (including herpes simplex, varicella), or fungal infections of the skin. Corticosteroids mask infection and promote spread.

Relative Contraindications (Specialist Input Recommended)

Rosacea and perioral dermatitis — Clobetasol propionate should not be used to treat these conditions; it causes exacerbation and dependence.
Application to the face, groin, or axillae — The labelling explicitly states these areas should be avoided due to enhanced absorption and risk of atrophy and striae. If required in these areas, use the lowest potency for the shortest time.
Pregnancy — Clobetasol propionate is teratogenic in animals (cleft palate, skeletal abnormalities in mice at subcutaneous doses as low as 0.03 mg/kg). No adequate human data. Use only if the potential benefit justifies the potential risk to the fetus.

Use with Caution

Pediatric patients <12 years — Not recommended due to higher systemic absorption risk from greater BSA-to-mass ratio. Children have developed HPA axis suppression, Cushing’s syndrome, and growth retardation from topical clobetasol.
Occlusive dressings — Substantially increase percutaneous absorption; should not be used unless specifically directed by the prescriber for recalcitrant disease, with close monitoring.
Pre-existing skin atrophy — The Clobex spray and lotion labelling specifically state: do not use if atrophy is present at the treatment site.
Lactation — Unknown whether clobetasol propionate is excreted in breast milk. Use on the smallest area for the shortest duration; avoid application to the breast.
Patients planning surgery — Inform the surgical team if using clobetasol propionate, as HPA axis suppression may affect the stress response to surgery.

FDA Class-Wide Safety Advisory — Super-Potent Topical Corticosteroids HPA Axis Suppression and Duration Limitation

Clobetasol propionate is a super-high potency topical corticosteroid that has been shown to suppress the HPA axis at doses as low as 2 g per day. Patients receiving super-potent corticosteroids should not be treated for more than 2 consecutive weeks at a time, and only small areas should be treated at any one time, due to the increased risk of HPA axis suppression. Cushing’s syndrome has been reported in both infants and adults following prolonged use. If HPA axis suppression is noted, the drug should be withdrawn gradually, the frequency of application reduced, or a less potent corticosteroid substituted. Recovery of HPA axis function is generally prompt upon discontinuation.

Patient Counselling

Purpose of Therapy

Clobetasol propionate is a very strong prescription steroid cream/ointment used to reduce redness, itching, swelling, and discomfort caused by skin conditions that have not responded to milder treatments. It is intended for short-term use only — typically no more than 2 weeks — and should not be used as a long-term moisturizer or maintenance therapy.

How to Take

Apply a thin layer to the affected skin area only, twice a day, and rub in gently. Do not apply to healthy skin, and do not use more than prescribed. Wash your hands after applying, unless the hands are the area being treated. Do not cover the treated area with bandages or tight dressings unless directed by your prescriber.

Duration and Quantity Limits

Tell patientUse clobetasol propionate for no longer than 2 weeks at a time unless your prescriber specifically instructs otherwise. Do not use more than 50 grams (approximately one large tube) per week. Using too much or for too long can cause serious side effects including thinning of the skin and hormonal problems.

Call prescriberIf your condition has not improved after 2 weeks of treatment, or if it worsens.

Areas to Avoid

Tell patientDo not apply clobetasol propionate to the face, underarms, or groin area unless specifically directed by your prescriber. The skin in these areas is thinner and more vulnerable to side effects like thinning, stretch marks, and visible blood vessels. Avoid getting the medication in your eyes.

Call prescriberIf you accidentally get clobetasol in your eyes and experience pain, blurred vision, or other visual changes.

Skin Changes to Watch For

Tell patientWatch for thinning of the skin (it may appear shiny or develop visible blood vessels), stretch marks, or easy bruising in the treated areas. These can be signs of excessive steroid use and may be permanent in some cases.

Call prescriberIf you notice skin thinning, stretch marks, or persistent redness that was not present before starting treatment.

Stopping Treatment

Tell patientDo not stop using clobetasol propionate abruptly if you have been using it for more than 2 weeks or on large areas of your body. Your prescriber may instruct you to gradually reduce the frequency of application to prevent your skin condition from flaring back worse than before.

Call prescriberIf you experience a significant worsening of your skin condition after stopping treatment, or if you develop extreme fatigue, dizziness, or weakness after stopping (which could indicate hormonal effects).

Infection Risk

Tell patientClobetasol propionate reduces your skin’s immune defenses. If you develop signs of a skin infection (increased redness, warmth, pus, crusting, or a painful cold sore) in the treated area, stop using the cream and contact your prescriber. Do not use clobetasol on skin that is already infected.

Call prescriberPromptly if signs of infection appear in or near the treated area.

Surgery or Medical Procedures

Tell patientInform any doctor or surgeon that you are using clobetasol propionate if you are having surgery or a medical procedure. The medication can affect your body’s response to stress.

Call prescriberBefore any planned surgery to discuss whether a steroid stress dose is needed.

Ref

Sources

Regulatory (PI / SmPC)

Clobetasol Propionate Cream, 0.05% (Emollient) — Full Prescribing Information. Sun Pharmaceutical Industries. DailyMedSource for emollient cream adverse reaction rates (burning/stinging 5%, pruritus/erythema/atrophy <2%), HPA suppression data (25% at 1 week with ≥30% BSA), and 50 g/week dosage limit.
Clobex (clobetasol propionate) Lotion, 0.05% — Full Prescribing Information. Galderma Laboratories. FDA Label (2012)Source for lotion-specific HPA suppression data (9/14 patients suppressed at 2 weeks; 8/10 at 4 weeks in psoriasis), clinical trial efficacy, and atopic dermatitis indication data.
Clobex (clobetasol propionate) Spray, 0.05% — Full Prescribing Information. Galderma Laboratories. FDA Label (2018)Source for spray formulation dosing in psoriasis (≤20% BSA), pregnancy/lactation data, and teratogenicity findings (umbilical hernia in rats at >12.5 mcg/kg/day SC).
Clobetasol Propionate Ointment, 0.05% — Full Prescribing Information. DailyMedSource for ointment-specific HPA axis suppression threshold (2 g/day), teratogenicity data (mice: cleft palate at 0.03 mg/kg SC; rabbits: 3–10 mcg/kg SC), and occlusive dressing warnings.

Key Clinical Trials & Reviews

Feldman SR. Relative potency of various topical corticosteroids. UpToDate. UpToDateComprehensive classification of topical corticosteroids by potency; positions clobetasol propionate as US Class I (super-high potency).
Torsekar RG, Koranne RV. Topical corticosteroid use and misuse: a clinical review. Indian J Dermatol. 2023;68(5):480-490.Review addressing duration limits, step-down strategies, and consequences of topical corticosteroid misuse including rebound flares and steroid-dependent dermatitis.
Chi CC, Kirtschig G, Baldo M, et al. Topical interventions for genital lichen sclerosus. Cochrane Database Syst Rev. 2011;(12):CD008240. DOI: 10.1002/14651858.CD008240.pub2Cochrane review establishing clobetasol propionate 0.05% ointment as first-line therapy for vulvar lichen sclerosus with high-quality evidence.

Guidelines

British Association of Dermatologists guidelines for the management of lichen sclerosus, 2018. Br J Dermatol. 2018;178(4):839-853. DOI: 10.1111/bjd.16241BAD guideline recommending clobetasol propionate 0.05% as first-line for vulvar lichen sclerosus with specific tapering protocols for long-term maintenance.
Eichenfield LF, Tom WL, Berger TG, et al. Guidelines of care for the management of atopic dermatitis: Section 2. Management and treatment of atopic dermatitis with topical therapies. J Am Acad Dermatol. 2014;71(1):116-132. DOI: 10.1016/j.jaad.2014.03.023AAD guideline on topical corticosteroid use in atopic dermatitis, including potency selection, duration limitations, and step-down strategies.

Mechanistic / Basic Science

Schoepe S, Schacke H, May E, Asadullah K. Glucocorticoid therapy-induced skin atrophy. Exp Dermatol. 2006;15(6):406-420. DOI: 10.1111/j.0906-6705.2006.00435.xDetailed review of the mechanisms underlying corticosteroid-induced skin atrophy, including collagen degradation and dermal thinning relevant to clobetasol’s adverse effect profile.
Hengge UR, Ruzicka T, Schwartz RA, Cork MJ. Adverse effects of topical glucocorticosteroids. J Am Acad Dermatol. 2006;54(1):1-15. DOI: 10.1016/j.jaad.2005.01.010Comprehensive review of local and systemic adverse effects of topical corticosteroids, including HPA suppression thresholds, skin atrophy mechanisms, and ocular complications.

Pharmacokinetics / Special Populations

Duong TV, et al. Characterizing local and systemic exposure to clobetasol propionate in healthy subjects and patients with atopic dermatitis. Br J Clin Pharmacol. 2025. DOI: 10.1002/bcp.70102PBPK modelling study demonstrating that systemic clobetasol exposure increases with impaired skin barrier and larger application area; supports 50 g/week max and ≤30% BSA recommendation.
Tadicherla S, Ross K, Shenefelt PD, Fenske NA. Topical corticosteroids in dermatology. J Drugs Dermatol. 2009;8(12):1093-1105. PubMed: 20027937Practical review of topical corticosteroid pharmacology, vehicle selection, and prescribing strategies including pulse and weekend protocols for super-potent steroids.