Calcipotriene: Complete Drug Monograph

Pharmacokinetic Profile

Systemic Absorption

~6% (±3%) on psoriatic plaques; ~5% on normal skin

Metabolism

Rapidly converted to inactive metabolites within 24 h (similar to natural vitamin D)

Protein Binding

Bound to specific vitamin D-binding plasma proteins

Calcaemic Potency

<1% that of calcitriol (~200-fold less calcaemic)

Elimination

Hepatic recycling; excreted in bile (similar to calcitriol)

Clinical Information

Drug Class

Topical Vitamin D3 Analogue

Available Formulations

Cream 0.005%, Ointment 0.005%, Foam 0.005%, Scalp Solution 0.005%

Route

Topical only (not for ophthalmic, oral, or intravaginal use)

Renal Adjustment

No formal adjustment; caution with extensive use due to hypercalcaemia risk

Hepatic Adjustment

No formal adjustment

Pregnancy

No adequate human data; animal studies show minor skeletal abnormalities at high doses

Lactation

Low systemic absorption; likely low levels in breast milk; use with caution

Schedule / Legal Status

Prescription only (not a controlled substance)

Generic Available

Yes (cream, ointment; foam as Sorilux)

Black Box Warning

Calcipotriene Indications

Indication	Approved Population	Therapy Type	Status
Plaque psoriasis (body)	Adults (cream, ointment); adults and children ≥4 years (foam)	Monotherapy or adjunctive with topical corticosteroids / phototherapy	FDA Approved
Plaque psoriasis (scalp)	Adults (scalp solution); adults and children ≥4 years (foam)	Monotherapy or adjunctive	FDA Approved

Calcipotriene was the first topical vitamin D analogue approved for psoriasis (1993 in the US) and remains a cornerstone of topical psoriasis management. It is positioned as first-line topical therapy either alone or in combination with topical corticosteroids for mild-to-moderate plaque psoriasis. The combination product calcipotriene/betamethasone dipropionate (Taclonex, Enstilar) is frequently prescribed for enhanced efficacy. Clinical improvement is typically detectable within 2 weeks, with efficacy demonstrated at 8 weeks in pivotal trials. Guidelines support long-term use of topical vitamin D analogues for up to 52 weeks.

Off-Label Uses

Vitiligo: Used in combination with phototherapy to promote repigmentation. Evidence quality: moderate (small controlled trials).

Morphoea (localised scleroderma): Some case series report benefit. Evidence quality: low.

Ichthyosis and other keratinisation disorders: Limited evidence from case reports. Evidence quality: very low.

Dose

Calcipotriene Dosing

Dosing by Formulation

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Plaque psoriasis (body) — cream	Thin layer BID	Thin layer BID	100 g/week	Rub in gently and completely; safety demonstrated for 8 weeks Avoid application to face (FDA PI)
Plaque psoriasis (body) — ointment	Thin layer QD–BID	Thin layer QD–BID	100 g/week	Once-daily dosing may have similar efficacy to twice daily (FDA PI); ointment may be slightly more effective than cream Avoid face; improvement in ~2 weeks
Scalp psoriasis — solution	Apply to lesions BID	Apply to lesions BID	100 g/week	Comb hair to remove scaly debris first; part hair and apply directly to lesions Avoid spreading to forehead; safety demonstrated for 8 weeks
Plaque psoriasis (body and scalp) — foam (Sorilux)	Thin layer BID	Thin layer BID	100 g/week	Shake well; dispense into palm; rub until foam disappears Approved for ≥4 years; flammable propellant — avoid fire/flame
Combination with topical corticosteroid (sequential or alternating)	Varies by regimen	Calcipotriene BID weekdays; corticosteroid BID weekends (one approach)	100 g/week calcipotriene	Multiple regimens used: sequential, weekend/weekday, or AM/PM split Reduces corticosteroid exposure while maintaining efficacy; up to 52 weeks per guidelines
Paediatric use (≥4 years) — foam only	Thin layer BID	Thin layer BID	100 g/week/m² BSA	Higher ratio of skin surface area to body mass increases systemic absorption risk Cream and ointment: paediatric safety not established per Dovonex PI

Clinical Pearl: Weekly Application Limits

To minimise the risk of hypercalcaemia, total weekly application should not exceed 100 g (some sources recommend a daily maximum of 15 g). The 100 g/week limit applies across all formulations. When calcipotriene is used in combination with the fixed-dose calcipotriene/betamethasone dipropionate product, the total calcipotriene exposure from both products must be considered. Patients should not apply calcipotriene to more than approximately 30–40% of body surface area.

Pharmacology

Mechanism of Action

Calcipotriene is a synthetic analogue of calcitriol (1,25-dihydroxyvitamin D3) that binds with comparable affinity to the intracellular vitamin D receptor (VDR) in keratinocytes. Upon binding, the VDR forms a heterodimer with the retinoid X receptor (RXR), and this complex translocates to the nucleus where it binds to vitamin D response elements (VDREs) in target gene promoters. This transcriptional regulation produces two key therapeutic effects: inhibition of keratinocyte proliferation and promotion of keratinocyte differentiation, thereby normalising the accelerated epidermal turnover characteristic of psoriasis and restoring the granular layer. Calcipotriene also modulates immune function by reducing CD8+ and IL-17+ T cell activity and dampening inflammatory cytokine signalling. Critically, calcipotriene retains the antiproliferative and pro-differentiating effects of calcitriol while being approximately 200 times less potent in regulating calcium metabolism, making it suitable for topical use with a substantially lower risk of hypercalcaemia.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	~6% (±3% SD) absorbed systemically from psoriatic skin; ~5% (±2.6% SD) from normal skin (radiolabelled ointment studies)	Low systemic absorption limits risk of hypercalcaemia at recommended doses; plasma levels typically below limit of quantification (10 pg/mL)
Distribution	Bound to specific vitamin D plasma transport proteins; disposition similar to endogenous vitamin D	Follows natural vitamin D handling pathways; minimal systemic accumulation expected
Metabolism	Rapidly converted to inactive metabolites within 24 h of application; metabolic pathway parallels natural calcitriol; recycled via liver	Primary metabolites are much less potent than parent compound; rapid inactivation provides safety margin
Elimination	Excreted in bile (similar to calcitriol); exact renal/faecal proportions not characterised for topical use	Follows endogenous vitamin D3 elimination; short effective half-life limits systemic exposure

Side Effects

Side effect data are derived from controlled clinical trials reported in the FDA prescribing information for Dovonex (cream, ointment, scalp solution) and Sorilux (foam). Adverse effects are predominantly local skin reactions at the application site. Calcipotriene has no boxed warning and carries a favourable systemic safety profile owing to its low percutaneous absorption.

≥10% Very Common

Adverse Effect	Incidence	Clinical Note
Burning, stinging, tingling (scalp solution)	~23%	Transient; most common with scalp solution; usually resolves within minutes of application
Burning, itching, skin irritation (cream/ointment)	10–15%	Lesional and perilesional; dose-dependent; may improve with continued use or formulation switch
Rash (scalp solution)	~11%	Localised to application area; assess for allergic contact dermatitis if persistent

1–10% Common

Adverse Effect	Incidence	Clinical Note
Erythema	1–10%	Localised redness at application site; usually mild
Dry skin / peeling	1–10%	Perilesional dryness; manage with concurrent emollients
Dermatitis / worsening of psoriasis	1–10%	Includes worsening of existing plaques and development of facial/scalp psoriasis; discontinue if significant worsening
Pruritus	1–10%	Localised to treated areas; differentiate from underlying psoriasis itch

Serious Serious Adverse Effects (Regardless of Frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Hypercalcaemia	<1% (with excessive use)	Days to weeks with overuse	Discontinue until serum calcium normalises; reversible on cessation; associated with use exceeding 100 g/week
Allergic contact dermatitis	Rare	Days to weeks after initiation	Discontinue; confirm with diagnostic patch testing (FDA PI); reported specifically with cream formulation

Discontinuation Discontinuation Rates

Long-Term AE Incidence (Open-Label, up to 1 year)

~25% experienced skin irritation

Context: In open-label extension studies (>400 patients), skin irritation occurred in ~25% and worsening psoriasis in ~10% over up to 1 year of use. Specific discontinuation rates are not reported in the FDA PI. Notably, ~50% of patients no longer required calcipotriene by week 16 due to satisfactory results.

Controlled Trials (8 weeks)

Low

Discontinuation due to adverse events was uncommon in the 8-week controlled trial period. Most local reactions were mild and self-limiting. The FDA PI does not provide a specific percentage for treatment discontinuation due to AEs.

Managing Local Irritation

Perilesional irritation is the most common reason patients discontinue calcipotriene. Strategies to improve tolerability include switching formulations (the cream is generally better tolerated than the ointment for some patients), reducing application frequency to once daily, applying an emollient barrier to perilesional skin before calcipotriene, and ensuring the product is not applied to the face or intertriginous areas (though some studies suggest cautious off-label facial use). Patients experiencing persistent irritation may benefit from transitioning to a fixed-dose combination with betamethasone dipropionate, which provides anti-inflammatory protection and reduces irritation.

Int

Drug Interactions

Calcipotriene has minimal systemic absorption and no known clinically significant drug-drug interactions based on formal pharmacokinetic studies. The primary interaction concern is additive effects on calcium metabolism when combined with other vitamin D-related products. The FDA PI does not list any specific drug interaction contraindications.

ModerateOral Vitamin D Supplements / Calcium Supplements

MechanismAdditive effect on calcium metabolism from exogenous vitamin D and calcium sources

EffectIncreased risk of hypercalcaemia, particularly when calcipotriene is used on large body surface areas or exceeds recommended weekly limits

ManagementMonitor serum calcium if concurrent use with high-dose vitamin D or calcium supplementation; ensure weekly calcipotriene limits are observed

Clinical Practice

ModeratePhototherapy (UVB / PUVA)

MechanismIn animal studies, calcipotriene reduced the time for UVR to induce skin tumour formation (statistically significant in male mice)

EffectTheoretical increased photosensitivity risk; may enhance UVR-induced tumour promotion

ManagementSome clinicians advise applying calcipotriene after phototherapy sessions rather than before; counsel patients to avoid excessive natural or artificial UV exposure (FDA PI)

FDA PI (Animal Data)

MinorTopical Corticosteroids

MechanismComplementary mechanisms; no pharmacokinetic interaction

EffectSynergistic efficacy; corticosteroid may reduce calcipotriene-induced irritation

ManagementWidely used in combination; apply at different times of day or use fixed-dose combination product; no dose adjustment needed

Clinical Practice / Guidelines

MinorSalicylic Acid (topical)

MechanismSalicylic acid may inactivate calcipotriene due to pH-related chemical instability

EffectReduced calcipotriene efficacy if applied simultaneously

ManagementAvoid simultaneous application; if both needed, apply at different times of day or use salicylic acid as a descaling pre-treatment before calcipotriene

Clinical Practice

Mon

Monitoring

Serum Calcium If using extensively or on large BSA
Trigger-based Not routinely required for standard use. Check if applying to >30% BSA, using >100 g/week, or if symptoms of hypercalcaemia develop (nausea, increased thirst, confusion, fatigue). Discontinue until calcium normalises if elevated. Elevations are transient and reversible.
Local Skin Reactions Each follow-up visit
Routine Assess for burning, irritation, erythema, and perilesional dermatitis. Worsening of psoriasis (including new facial or scalp involvement) occurred in 1–10% of patients. Consider allergic contact dermatitis if irritation is disproportionate; patch testing may be warranted (cream formulation).
Treatment Response 2 weeks; then 8 weeks
Routine Initial improvement expected within 2 weeks. Formal efficacy assessment at 8 weeks (controlled trial endpoint). If no improvement at 8 weeks, reconsider treatment plan. In open-label studies, ~50% of patients achieved satisfactory response by 16 weeks and no longer required treatment.
Paediatric Growth Periodically for long-term paediatric use
Trigger-based Children have a higher skin surface area to body mass ratio, increasing risk of systemic absorption. Monitor calcium and growth parameters in children receiving prolonged treatment.

Contraindications & Cautions

Absolute Contraindications

Hypercalcaemia—calcipotriene may further elevate serum calcium
Evidence of vitamin D toxicity
Hypersensitivity to calcipotriene or any component of the formulation

Relative Contraindications (Specialist Input Recommended)

Application to the face—not recommended per FDA PI due to increased irritation risk; some studies support cautious off-label facial use in selected patients
Extensive body surface area involvement (>30–40% BSA)—increased risk of systemic absorption and hypercalcaemia

Use with Caution

Paediatric patients—higher skin-surface-area-to-mass ratio increases systemic absorption risk; foam approved ≥4 years, cream/ointment safety not established in children per Dovonex PI
Elderly patients (≥65 years)—statistically more severe skin-related adverse events observed with ointment in patients over 65 compared to younger adults (FDA PI)
Concurrent UV exposure—animal data suggest calcipotriene may enhance UVR-induced skin tumour formation; counsel patients to limit sun exposure and avoid tanning beds
Concurrent high-dose vitamin D or calcium supplementation—monitor serum calcium
Foam formulation (Sorilux)—contains flammable propellant; avoid fire, flame, and smoking during and immediately after application

Patient Counselling

Purpose of Therapy

Calcipotriene is a topical form of vitamin D that is applied directly to psoriasis plaques. It works by slowing the rapid growth of skin cells and encouraging them to mature normally, which reduces the thickness, scaling, and redness of psoriasis patches. It is not a steroid and can be used long-term as part of your psoriasis management plan.

How to Use

Apply a thin layer to the affected areas only and rub in gently and completely. Wash your hands thoroughly after application unless your hands are the treated area. Avoid getting the medication on your face, in your eyes, or on areas of skin without psoriasis. For scalp treatment, comb hair first to remove loose scales, then part hair and apply directly to the affected area. Improvement usually begins within 2 weeks, but it may take up to 8 weeks to see full benefit.

Skin Irritation

Tell patientMild burning, stinging, or irritation at the application site is common, especially in the first few weeks. This usually improves with continued use. Applying a plain moisturiser to the surrounding healthy skin before calcipotriene may help reduce perilesional irritation.

Call prescriberIf burning or irritation is severe, worsens over time, or if you notice a new rash, swelling, or blistering in the treated area (which may indicate an allergic reaction).

Application Limits

Tell patientDo not use more than your prescriber recommends. Using too much of this medication can raise calcium levels in your blood, which can cause symptoms such as unusual tiredness, nausea, increased thirst, or confusion. Do not exceed 100 grams (approximately two standard tubes) per week.

Call prescriberIf you experience increased thirst, frequent urination, nausea, loss of appetite, confusion, or unusual fatigue, as these may indicate high calcium levels.

Sun Exposure

Tell patientThis medication may make your skin more sensitive to sunlight. Avoid excessive sun exposure and tanning beds. Use sunscreen (SPF 30 or higher) and wear protective clothing on treated areas when outdoors.

Call prescriberIf you develop an unexpected sunburn or rash on treated areas after sun exposure.

Foam Flammability (Sorilux)

Tell patientIf using the foam formulation, the propellant is flammable. Do not smoke, use open flames, or go near sources of heat until the foam has completely dried on your skin. Do not puncture the canister or expose it to temperatures above 49°C (120°F).

Call prescriberNot applicable—this is a standing safety precaution for every application.

Ref

Sources

Regulatory (PI / SmPC)

LEO Pharma / Glenmark Pharmaceuticals. Dovonex (calcipotriene) ointment and cream 0.005%. Full prescribing information. Revised 2025. accessdata.fda.govPrimary source for dosing, adverse reaction rates (10–15% irritation for cream/ointment), absorption data (6%), and contraindications.
Dovonex (calcipotriene) scalp solution 0.005%. Prescribing information. accessdata.fda.govSource for scalp solution adverse reaction rates (23% burning/stinging, 11% rash) and geriatric data.
Mayne Pharma. Sorilux (calcipotriene) foam 0.005%. Full prescribing information. rxlist.comSource for foam-specific data including paediatric approval (≥4 years), pharmacokinetics (plasma levels below LOQ), and flammability warnings.

Key Clinical Trials

Kragballe K. Treatment of psoriasis with calcipotriol and other vitamin D analogues. J Am Acad Dermatol. 1992;27(6 Pt 1):1001–1008. doi:10.1016/0190-9622(92)70302-vLandmark early trial establishing calcipotriol efficacy and the ~200-fold reduced calcaemic potency relative to calcitriol.
Lebwohl M, Siskin SB, Epinette W, et al. A multicenter trial of calcipotriene ointment and halobetasol propionate ointment compared with either agent alone for the treatment of psoriasis. J Am Acad Dermatol. 1996;35(2 Pt 1):268–269. doi:10.1016/S0190-9622(96)90344-4Demonstrated superiority of calcipotriene-corticosteroid combination over either agent alone, establishing the rationale for combination therapy.
Sorilux foam phase III trials. Two identical randomised double-blind vehicle-controlled 8-week studies (n = 659). Data summarised in Sorilux PI. Established efficacy of calcipotriene foam in plaque psoriasis (ISGA 0/1 response) and confirmed safety in adolescents and adults.

Guidelines

Menter A, Korman NJ, Elmets CA, et al. Guidelines of care for the management of psoriasis and psoriatic arthritis: Section 3. Guidelines of care for the management and treatment of psoriasis with topical therapies. J Am Acad Dermatol. 2009;60(4):643–659. doi:10.1016/j.jaad.2008.12.032AAD guideline positioning calcipotriene as first-line topical therapy for mild-to-moderate psoriasis, with long-term use recommendations up to 52 weeks.
Elmets CA, Korman NJ, Prater EF, et al. Joint AAD-NPF guidelines of care for the management and treatment of psoriasis with topical therapy and the use of retinoids and phototherapy. J Am Acad Dermatol. 2021;84(6):1551–1569. doi:10.1016/j.jaad.2021.02.071Updated AAD-NPF guideline addressing combination vitamin D analogue and corticosteroid regimens for long-term management.

Mechanistic / Basic Science

Bikle DD. Vitamin D regulated keratinocyte differentiation. J Cell Biochem. 2004;92(3):436–444. doi:10.1002/jcb.20095Detailed review of VDR-mediated keratinocyte differentiation pathways explaining the antiproliferative mechanism relevant to calcipotriene.

Pharmacokinetics / Special Populations

Calcipotriene therapeutic cheat sheet. Next Steps in Dermatology. 2024. nextstepsinderm.comClinical summary confirming 100 g/week and 15 g/day maximum dosing limits and formulation-specific considerations.
DailyMed. Calcipotriene ointment USP 0.005%. National Library of Medicine. dailymed.nlm.nih.govStructured FDA label for generic calcipotriene ointment providing absorption data, open-label extension safety findings, and formulation details.

Dovonex (Calcipotriene)