Clobetasol is a topical, synthetic fluorinated corticosteroid. Clobetasol is used to relieve the inflammatory and pruritic manifestations of moderate to severe corticosteroid-responsive dermatoses and psoriasis. Clobetasol is one of the most potent topical corticosteroids, and is usually recommended for short-term or cyclic therapy only. Very high potency topical corticosteroids are used as an alternative to systemic therapy for localized conditions. Long-term use can lead to systemic side effects, including hypothalamic-pituitary-adrenal (HPA) axis suppression. Clobetasol was first approved by the FDA in 1985.
General Administration Information
For storage information, see the specific product information within the How Supplied section.
-Best results are obtained when topical corticosteroids of adequate strength are used for specified lengths of time. Patients who fail to respond to clobetasol treatment after 1 to 4 weeks should be re-evaluated.
-Discontinue once control of the treated condition has been achieved. Intermittent application may need to be continued to maintain remission or control of the condition in some cases. Some authorities recommend cyclic applications (i.e., 2 weeks of clobetasol treatment followed by 1 week of lubrication only) for chronic conditions like psoriasis. The lowest effective maintenance application should be used. Other options include changing to a less potent topical corticosteroid for maintenance and control of inflammation and symptoms.
Route-Specific Administration
Topical Administration
-For topical dermatologic use only. Not for ophthalmic, oral, or intravaginal use. Generally not recommended for use on the face or intertriginous areas.
-Restrict application to the active lesions or affected areas and try to avoid normal surrounding skin.
-Do not use clobetasol propionate preparations with occlusive dressings. Instruct patients not to bandage, cover, or wrap area in any way that may be occlusive.
Cream/Ointment/Lotion Formulations
Cream, emollient cream, gel, or ointment:
-Wash hands before and after application. Use gloves if required by universal precautions. Apply sparingly in a thin film and rub gently into affected area.
-The amount of cream or ointment needed to cover a certain area can be calculated. A 1 g application of cream covers 100 cm2 of skin. The entire skin surface of the average size adult will be covered by 30 g of topical steroid cream.
Other Topical Formulations
Scalp solution:
-Wash hands before and after application. Use gloves if required by universal precautions. Apply sparingly in a thin film to the affected areas of the scalp; rub in gently and completely.
Topical foam:
-Olux foam
--Prior to first application, break the tiny plastic piece at the base of the can's rim by gently pushing back (away from the piece) on the nozzle.
-Invert the can and push the button to dispense a small amount of foam into the cap of the can, or directly on the affected skin area, taking care to avoid contact with the eyes. The amount should be no more than 1 and a half capfuls (approximately the size of a golf ball). Dispensing directly onto hands is not recommended, as the foam will begin to melt immediately upon contact with warm skin. If your fingers are warm, rinse them in cold water first. Be sure to dry them thoroughly before handling the foam. If the can seems warm or the foam seems runny, run the can under cold water.
-Using your fingertips, gently massage a thin layer of foam into affected areas until the foam disappears. If applying to the scalp, move the hair away from the affected area so that the foam can be applied directly to the affected areas. Repeat until the affected areas are treated.
-Wash hands after application. Patients should wash their hands after application unless the foam is being used to treat the hands.
-Throw away any of the unused medicine that was dispensed out of the can.
-This product is flammable; avoid heat, flame, or smoking during and immediately following application of the foam.
-Tovet foam
--Prior to first application, break the tiny plastic piece at the base of the can's rim by gently pushing back (away from the piece) on the nozzle.
-Shake well prior to each use.
-Invert the can and press the nozzle.
-Press down on the actuator to dispense a small amount of the foam into the palm of the hand.
-Apply a thin layer to the affected area and rub in gently until foam disappears. Use gloves if required by universal precautions.
-Wash hands after application. Patients should wash their hands after application unless the foam is being used to treat the hands.
-Throw away any of the unused medicine that was dispensed out of the can.
-This product is flammable; avoid heat, flame, or smoking during and immediately following application of the foam.
Topical spray:
-Wash hands before and after treatment. Spray directly onto the affected skin areas; rub in gently but completely.
Topical shampoo:
-Wash hands before and after treatment. Do not wet hair prior to use. Apply directly to the affected area of the scalp. Rub in gently; leave on the scalp for 15 minutes. Instruct patients not to cover their head while the shampoo is on the scalp. After 15 minutes, add water, lather and rinse completely.
Extemporaneous Compounding-Topical
Dental topical preparation for application to oral vesiculoerosive disease:
-NOTE: Clobetasol is not approved by the FDA for dental administration.
-An extemporaneous preparation of clobetasol for buccal or oral mucous membrane application can be compounded by combining clobetasol propionate ointment in a 1:1 ratio with a plasticized hydrocarbon gel (Orabase-plain). No stability data are currently available.
When used for recommended treatment periods of 14 days or less, clobetasol topical preparations are usually well tolerated. The most frequently reported adverse reactions to clobetasol therapy are local in nature and include burning sensations, pruritus, and skin irritation. Burning and stinging sensations are more common with gel, emollient cream, and topical scalp foam/solution preparations of clobetasol and occur in 2-10% of patients. Other local adverse reactions reported in less than 2% of patients treated with clobetasol include acneiform rash, transient erythema, folliculitis, miliaria, perioral dermatitis, secondary infection, skin atrophy, skin hypopigmentation, skin peeling or cracking, xerosis, hypertrichosis, telangiectasia, and striae. Purpura and maculopapular rash may also occur. Additional adverse reactions related to scalp application of clobetasol include alopecia, vesicular rash, ocular irritation, and headache in roughly 0.3% of patients. Headache may be a clinical sign of elevated intracranial pressure. Adverse dermatologic effects are more likely to occur in intertriginous and facial areas, and tend to be more severe with fluorinated topical corticosteroids like clobetasol. Adverse dermatologic side effects of clobetasol are also more frequent with concurrent use of occlusive dressings. Some dermatologic effects, such as skin atrophy and striae, occur even with intermittent applications of high-potency topical corticosteroids, and may be permanent with prolonged treatment. If irritation develops, discontinue topical corticosteroids and institute appropriate therapy. The anti-inflammatory activity of topical corticosteroids may mask manifestations of infection. In the presence of dermatological infections, institute the use of an appropriate antifungal or antibacterial agent. If a favorable response does not promptly occur, discontinue the corticosteroid until the infection has been adequately controlled.
Signs and symptoms of corticosteroid withdrawal may occur with clobetasol dose reduction or discontinuation, and supplemental systemic corticosteroids may be needed. For example, disease flare may occur and HPA axis suppression may be present.
Systemic absorption of topical corticosteroids such as clobetasol can produce reversible hypothalamic-pituitary-adrenal (HPA) suppression with possible adrenocortical insufficiency after treatment discontinuation. In some patients, systemic absorption can produce manifestations of Cushing's syndrome, hypertension, hyperglycemia, and glycosuria. Percutaneous absorption of clobetasol is dependent on many factors including the vehicle, the integrity of the epidermal barrier, duration of use, and use of an occlusive dressing. Children may be more susceptible to systemic toxicity from equivalent doses due to their larger skin surface to body mass ratios. HPA axis suppression and increased intracranial pressure have been reported in children receiving topical corticosteroids. Manifestations of adrenocortical insufficiency in children include linear growth inhibition, delayed weight gain, low plasma cortisol concentrations, and absence of response to ACTH stimulation. Clinical signs of increased intracranial pressure include bulging fontanelles, headaches, and bilateral papilledema (i.e., pseudotumor cerebri). Clobetasol is a very-high-potency corticosteroid, and the risk of HPA axis suppression is greater than with other topical corticosteroids. However, the risk appears to be dose related. It is estimated that after 1 week of use of clobetasol at a dose of 3.5 grams twice daily (i.e., a 50-gram tube of clobetasol per week) over a 30% body surface area, 75% of adult patients will experience some degree of HPA axis suppression. In contrast, only 10% of adult patients using the equivalent of one 15-gram tube of clobetasol per week will have HPA axis suppression. One 4-week study of clobetasol emollient cream used in doses of 0.4-0.5 g twice daily in adult patients with plaque-type psoriasis resulted in no significant effects on serum cortisol concentrations or tolerability. Periodically evaluate patients applying clobetasol to a large surface area or to areas under occlusion for evidence of HPA axis suppression (using the ACTH stimulation test and urinary free cortisol test). To minimize risk of HPA axis suppression, discontinue therapy when control is achieved. If no improvement is seen within 2 weeks, reassessment of diagnosis may be necessary. If HPA axis suppression is noted, an attempt should be made to withdraw the drug, reduce the frequency of application, or substitute a less potent corticosteroid. Recovery of HPA axis function is generally prompt and complete upon discontinuation of the topical corticosteroid.
Case reports describe the development of extensive visual impairment in patients secondary to the onset of glaucoma or ocular hypertension during the use of potent topical corticosteroids to treat severe atopic eczema of the face. Such adverse effects, if they occur, could lead to blindness. Cataracts have also been reported, usually with large doses or therapy greater than 6 months. The use of topical corticosteroids may also increase the risk of posterior subcapsular cataracts and retinopathy (central serous chorioretinopathy). Clobetasol is generally not recommended for application to the face. Any patient who develops changes in vision while applying clobetasol to the scalp or other areas should be evaluated for ocular hypertension. Low potency corticosteroids (e.g., hydrocortisone, dexamethasone) have been reported to be safer for short-term use around the eye area.
In general, excessive use of corticosteroids can lead to impaired wound healing. Since clobetasol is a topical corticosteroid, it should not be applied directly on or near healing wounds. A propensity for skin ulcer may develop in patients with markedly impaired circulation who use topical corticosteroids.
Tolerance may occur with the prolonged use of topical corticosteroids. Tolerance is usually described as a decreased acute vasoconstrictive response to the agent after a period of days to weeks. This may explain the dramatic responses noted initially by patients early in topical corticosteroid treatment and an apparent diminished response with time. Tolerance is reversible and may be attenuated by interrupted or cyclic schedules of application (e.g., clobetasol is given twice daily for 2-3 weeks, followed by a 1-week intermission).
Allergic contact dermatitis with corticosteroids such as clobetasol is usually diagnosed by observing a failure to heal. Appropriate diagnostic patch testing may help with the diagnosis.
Clobetasol is contraindicated in any patient with a history of corticosteroid hypersensitivity and hypersensitivity to clobetasol or any ingredients in the preparation. Although true corticosteroid hypersensitivity is rare, patients who have demonstrated a prior hypersensitivity reaction to clobetasol should not receive any form of clobetasol. It is possible, though also rare, that such patients will display cross-hypersensitivity to other corticosteroids. It is advisable that patients who have a hypersensitivity reaction to any corticosteroid undergo skin testing, which, although not a conclusive predictor, may help to determine if hypersensitivity to another corticosteroid exists. Such patients should be carefully monitored during and following the administration of any corticosteroid.
Systemic absorption of topical corticosteroids has produced reversible hypothalamic-pituitary-adrenal (HPA) suppression and/or manifestations of Cushing's syndrome in some patients. Clobetasol propionate has been shown to suppress the HPA axis at doses as low as 2 g/day. Conditions which increase systemic absorption include application of high-potency corticosteroids, use over large surface areas, prolonged use, use in areas where the epidermal barrier is disrupted (i.e., skin abrasion), use in pediatric patients, use in patients with hepatic disease, and the use of an occlusive dressing. Clobetasol propionate preparations should not be used with occlusive dressings. Patients receiving large doses of a potent topical corticosteroid like clobetasol should be evaluated periodically for evidence of HPA axis suppression and manifestations of Cushing's syndrome. If these effects are noted, an attempt should be made to withdraw the drug, to reduce the frequency of application, or to substitute a less potent corticosteroid. Recovery of HPA axis function is generally prompt and complete upon discontinuation. Infrequently, signs and symptoms of withdrawal may occur, requiring supplemental systemic corticosteroids. It is recommended that the administration of clobetasol creams, ointments, gels, or topical solutions be limited to no more than 14 days duration, in order to limit the risk of systemic effects. Clobetasol propionate emollient creams may be administered for up to 4 weeks duration if applied to no more than 5-10% of body surface area. The total weekly dose limit of 50 g or 50 mL of a 0.05% preparation should not be exceeded for any clobetasol preparation.
Topical corticosteroids, including clobetasol, should be used with caution in patients with diabetes mellitus. Exacerbation of diabetes may occur with systemic absorption of the topical corticosteroid. Use of topical corticosteroids may further delay healing of skin ulcers in diabetic patients.
Efficacy and adverse reaction data in the pediatric population are limited for topical clobetasol; therefore use in neonates, infants, or children under 12 years of age is not recommended. Children and infants may absorb proportionally larger amounts of topical corticosteroids due to a larger skin surface area to body weight ratio, and therefore are more susceptible to developing systemic toxicity, especially with very-high-potency products. Hypothalamic-pituitary-adrenal (HPA) axis suppression, Cushing's syndrome, growth inhibition (linear growth retardation and delayed weight gain), and increased intracranial pressure have been reported in children receiving topical corticosteroids. Administration of topical corticosteroids to children should be limited to the least amount compatible with an effective therapeutic regimen. Clobetasol is not approved to treat diaper dermatitis. If children are being treated in the diaper area, tight-fitting diapers or plastic pants should be avoided as these garments may act as an occlusive dressing and increase systemic absorption of the drug.
Clobetasol should be used during pregnancy only if the potential benefit justifies the potential risk to the fetus. Topical corticosteroids, including clobetasol, should not be used in large amounts, on large areas, or for prolonged periods of time in pregnant women. Guidelines recommend mild to moderate potency agents over potent corticosteroids, which should be used in short durations. Fetal growth restriction and a significantly increased risk of low birthweight has been reported with use of potent or very potent topical corticosteroids during the third trimester, particularly when using more than 300 grams. There are no adequate and well-controlled studies of teratogenic effects from topical application of clobetasol in pregnant women. Corticosteroids have been shown to be teratogenic after dermal, oral, and subcutaneous administration in animal studies. Clobetasol has greater potency, and thus greater teratogenic potential, than other topical corticosteroids. After subcutaneous clobetasol propionate administration to pregnant mice and rabbits, increased malformations, such as cleft palate and skeletal abnormalities, were observed.
It is not known whether topical administration of clobetasol could result in sufficient systemic absorption to produce detectable quantities in breast milk to cause issues during breast-feeding; the manufacturers recommend to use with caution. However, most dermatologists stress that topical corticosteroids can be safely used during lactation. If applied topically, care should be used to ensure the infant will not come into direct contact with the area of application, such as the breast. Increased blood pressure has been reported in an infant whose mother applied a high potency topical corticosteroid ointment directly to the nipples. Consider the benefits of breast-feeding, the risk of potential infant drug exposure, and the risk of an untreated or inadequately treated condition. If a breast-feeding infant experiences an adverse effect related to a maternally ingested drug, healthcare providers are encouraged to report the adverse effect to the FDA.
The normal inflammatory response to local infections can be masked by clobetasol. Application of topical corticosteroids to areas of infection, including tuberculosis of the skin, dermatologic fungal infection, and cutaneous or systemic viral infection (e.g., herpes infection, measles, varicella), should be initiated or continued only if the appropriate anti-infective treatment is instituted. If the infection does not respond to the antimicrobial therapy, the concurrent use of the topical corticosteroid should be discontinued until the infection is controlled. Topical corticosteroids may delay the healing of non-infected wounds, such as venous stasis ulcers. Use clobetasol preparations with caution in patients with markedly impaired circulation or peripheral vascular disease; skin ulceration has been reported in these patients following topical corticosteroid use.
As with other potent fluorinated topical corticosteroids, clobetasol should not be used to treat acne vulgaris, acne rosacea, or perioral dermatitis as clobetasol may aggravate these conditions. Clobetasol preparations should not be applied to the face, groin, vagina, or axillae. Care should be taken to avoid use around the eyes; ocular exposure should be avoided. If unintended contact happens, the patient should rinse the exposed area well with water. Visual impairment, ocular hypertension and cataracts have been reported with ocular exposure to other high potency topical corticosteroids. Preexisting glaucoma may be aggravated if clobetasol is used in the periorbital area. Advise patients to report any visual symptoms and consider referral to an ophthalmologist for evaluation.
Topical corticosteroids should be used for brief periods, or under close medical supervision in patients with evidence of pre-existing skin atrophy. Geriatric patients may be more likely to have preexisting skin atrophy secondary to aging. Purpura and skin lacerations that may raise the skin and subcutaneous tissue from deep fascia may be more likely to occur with the use of topical corticosteroids in geriatric patients. Topical clobetasol clinical trials included insufficient numbers of elderly patients to do a separate analysis of efficacy and safety in this population. Based on available data, no dosage adjustments are required for elderly patients receiving topical clobetasol. Use of lower potency topical corticosteroids also may be necessary in some patients.
The foam formulation of clobetasol is flammable. Avoid use near a fire or flame, including tobacco smoking during or immediately after application.
For the treatment of corticosteroid-responsive dermatoses, including atopic dermatitis, graft-versus-host disease (GVHD), localized vitiligo, eczema, phimosis, lichen planus, and localized bullous pemphigoid:
-for the general treatment of corticosteroid-responsive dermatoses:
Topical dosage (cream, gel, foam, or ointment):
Adults: Apply a thin layer topically to the affected skin area(s) 2 times daily. Max: 50 g/week. If no improvement within 2 weeks, reassess diagnosis.
Children and Adolescents 12 to 17 years: Apply a thin layer topically to the affected skin area(s) 2 times daily. Max: 50 g/week. If no improvement within 2 weeks, reassess diagnosis.
Topical dosage (lotion):
Adults: Apply a thin layer topically to the affected skin area(s) 2 times daily. Max: 50 g/week. If no improvement within 2 weeks, reassess diagnosis.
Topical dosage (solution):
Adults: Apply a thin layer topically to the affected scalp area(s) 2 times daily. Max: 50 mL/week. If no improvement within 2 weeks, reassess diagnosis.
Children and Adolescents 12 to 17 years: Apply a thin layer topically to the affected scalp area(s) 2 times daily. Max: 50 mL/week. If no improvement within 2 weeks, reassess diagnosis.
-for the treatment of atopic dermatitis:
Topical dosage (cream, gel, foam, or ointment):
Adults: Apply a thin layer topically to the affected skin area(s) 2 times daily until symptoms resolve. Max: 50 g/week. If no improvement within 2 weeks, reassess diagnosis. Proactive, intermittent application of topical corticosteroids 1 to 2 times weekly to areas that commonly flare is recommended to help prevent relapses.
Children and Adolescents 12 to 17 years: Apply a thin layer topically to the affected skin area(s) 2 times daily until symptoms resolve. Max: 50 g/week. If no improvement within 2 weeks, reassess diagnosis. Proactive, intermittent application of topical corticosteroids 1 to 2 times weekly to areas that commonly flare is recommended to help prevent relapses.
Topical dosage (lotion):
Adults: Apply a thin layer topically to the affected skin area(s) 2 times daily until symptoms resolve. Max: 50 g/week. If no improvement within 2 weeks, reassess diagnosis. Proactive, intermittent application of topical corticosteroids 1 to 2 times weekly to areas that commonly flare is recommended to help prevent relapses.
Topical dosage (solution):
Adults: Apply a thin layer topically to the affected scalp area(s) 2 times daily until symptoms resolve. Max: 50 mL/week. If no improvement within 2 weeks, reassess diagnosis. Proactive, intermittent application of topical corticosteroids 1 to 2 times weekly to areas that commonly flare is recommended to help prevent relapses.
Children and Adolescents 12 to 17 years: Apply a thin layer topically to the affected scalp area(s) 2 times daily until symptoms resolve. Max: 50 mL/week. If no improvement within 2 weeks, reassess diagnosis. Proactive, intermittent application of topical corticosteroids 1 to 2 times weekly to areas that commonly flare is recommended to help prevent relapses.
-for the treatment of GVHD:
Topical dosage (cream, gel, foam, or ointment):
Adults: Apply a thin layer topically to the affected skin area(s) 2 times daily. May be used under occlusion for palms of hand and soles of feet to enhance efficacy. Max: 50 g/week.
Children and Adolescents 12 to 17 years: Apply a thin layer topically to the affected skin area(s) 2 times daily. May be used under occlusion for palms of hand and soles of feet to enhance efficacy. Max: 50 g/week.
Topical dosage (lotion):
Adults: Apply a thin layer topically to the affected skin area(s) 2 times daily. May be used under occlusion for palms of hand and soles of feet to enhance efficacy. Max: 50 g/week.
Topical dosage (solution):
Adults: Apply a thin layer topically to the affected scalp area(s) 2 times daily. Max: 50 mL/week.
Children and Adolescents 12 to 17 years: Apply a thin layer topically to the affected scalp area(s) 2 times daily. Max: 50 mL/week.
For the treatment of vulvar lichen sclerosus*:
Topical dosage (cream):
Adult females: Apply a thin layer to the affected vulvar, labial, and perineal areas twice daily, once in the morning and once at night. Treatment must be limited to 2 consecutive weeks, and amounts greater than 50 g per week should not be used. In a retrospective, uncontrolled analysis of 36 women with biopsy-proven lichen sclerosis, the initial clobetasol treatment course provided remission of symptoms in 77% of patients, and 47% noted an improvement in tissue appearance at one year of follow-up. The authors noted that intermittent clobetasol applications may be needed to maintain results.
Topical dosage (Ointment):
Adult Females: Apply a thin layer to affected vulvar areas for 3 months- use once daily for the first month, then on alternate days for the second month, and then twice weekly for the third month. This regimen has been studied and is strongly recommended by the British Association of Dermatologists. Another regimen that has been shown to be effective is clobetasol applied once daily for 3 months; if symptoms resolved in less than 3 months, the ointment was applied twice weekly for the remainder of the treatment period.
For the alternative treatment of vision-threatening periocular capillary hemangioma* in infancy and early childhood:
Topical dosage (cream):
Children and Infants: Limited reports have used topical clobetasol propionate cream as an alternative to intralesional corticosteroid injections. Treatment was prescribed with 0.05% clobetasol propionate cream applied to the area twice daily for 2 weeks, followed by a 1-week intermission. The cycle was repeated as needed. The 3 cases responded within 4 months to the topical treatment. Children were closely monitored for adrenal suppression. Clobetasol application was reserved for instances in which the risks of the disease (e.g., permanent visual loss) to the infant or the young child outweighed the potential risks of clobetasol treatment. Because the involution of the hemangioma occurs at a slower rate than would intralesional injection, topical clobetasol would not be appropriate in instances of acute, severe visual axis occlusion.
For the treatment of psoriasis:
Topical dosage (non-emollient cream, foam, gel, or ointment):
Adults: Apply a thin layer topically to the affected skin area(s) twice daily. Max: 50 g/week. Treatment beyond 2 consecutive weeks is not recommended. The duration of the therapy depends on factors such as the topical corticosteroid potency, disease severity and anatomic location, and age. After improvement, may consider transitioning to lower-potency corticosteroid, using intermittent therapy, and combining treatment with noncorticosteroidal agents. Taper by reducing use to every other day, then twice weekly, then discontinue if adequate control is maintained. Guidelines recommend class 1 to 5 topical corticosteroids for up to 4 weeks for plaque psoriasis not involving intertriginous areas and class 1 to 7 topical corticosteroids for a minimum of up to 4 weeks for scalp psoriasis. Use of topical corticosteroids for more than 12 weeks may be considered under careful supervision.
Children and Adolescent 12 to 17 years: Apply a thin layer topically to the affected skin area(s) twice daily. Max: 50 g/week. Treatment beyond 2 consecutive weeks is not recommended. Guidelines recommend topical corticosteroids as monotherapy for short-term treatment of localized psoriasis.
Topical dosage (emollient cream):
Adults: Apply a thin layer topically to the affected skin area(s) twice daily. Max: 50 g/week. Treatment beyond 4 consecutive weeks is not recommended. The duration of the therapy depends on factors such as the topical corticosteroid potency, disease severity and anatomic location, and age. After improvement, may consider transitioning to lower-potency corticosteroid, using intermittent therapy, and combining treatment with noncorticosteroidal agents. Taper by reducing use to every other day, then twice weekly, then discontinue if adequate control is maintained. Guidelines recommend class 1 to 5 topical corticosteroids for up to 4 weeks for plaque psoriasis not involving intertriginous areas and class 1 to 7 topical corticosteroids for a minimum of up to 4 weeks for scalp psoriasis. Use of topical corticosteroids for more than 12 weeks may be considered under careful supervision.
Adolescent 16 to 17 years: Apply a thin layer topically to the affected skin area(s) twice daily. Max: 50 g/week. Treatment beyond 4 consecutive weeks is not recommended. Guidelines recommend topical corticosteroids as monotherapy for short-term treatment of localized psoriasis.
Topical dosage (spray solution):
Adults: Spray directly onto the affected skin area(s) twice daily. Max: 50 g/week. Limit treatment beyond 2 weeks to localized lesions of moderate to severe plaque psoriasis that have not sufficiently improved after the initial 2 weeks of treatment. The duration of the therapy depends on factors such as the topical corticosteroid potency, disease severity and anatomic location, and age. After improvement, may consider transitioning to lower-potency corticosteroid, using intermittent therapy, and combining treatment with noncorticosteroidal agents. Taper by reducing use to every other day, then twice weekly, then discontinue if adequate control is maintained. Guidelines recommend class 1 to 5 topical corticosteroids for up to 4 weeks for plaque psoriasis not involving intertriginous areas and class 1 to 7 topical corticosteroids for a minimum of up to 4 weeks for scalp psoriasis. Use of topical corticosteroids for more than 12 weeks may be considered under careful supervision.
Topical dosage (lotion):
Adults: Apply a thin layer topically to the affected skin area(s) twice daily. Max: 50 g/week. Limit treatment beyond 2 weeks to localized lesions (less than 10% of body surface area) of moderate to severe plaque psoriasis that have not sufficiently improved after the initial 2 weeks of treatment. The duration of the therapy depends on factors such as the topical corticosteroid potency, disease severity and anatomic location, and age. After improvement, may consider transitioning to lower-potency corticosteroid, using intermittent therapy, and combining treatment with noncorticosteroidal agents. Taper by reducing use to every other day, then twice weekly, then discontinue if adequate control is maintained. Guidelines recommend class 1 to 5 topical corticosteroids for up to 4 weeks for plaque psoriasis not involving intertriginous areas and class 1 to 7 topical corticosteroids for a minimum of up to 4 weeks for scalp psoriasis. Use of topical corticosteroids for more than 12 weeks may be considered under careful supervision.
Topical dosage (scalp solution):
Adults: Apply topically to the psoriatic scalp area(s) twice daily. Max: 50 g/week. Limit treatment to 2 consecutive weeks. The duration of the therapy depends on factors such as the topical corticosteroid potency, disease severity and anatomic location, and age. After improvement, may consider transitioning to lower-potency corticosteroid, using intermittent therapy, and combining treatment with noncorticosteroidal agents. Taper by reducing use to every other day, then twice weekly, then discontinue if adequate control is maintained. Guidelines recommend class 1 to 7 topical corticosteroids for a minimum of up to 4 weeks for scalp psoriasis. Use of topical corticosteroids for more than 12 weeks may be considered under careful supervision.
Children and Adolescent 12 to 17 years: Apply topically to the psoriatic scalp area(s) twice daily. Max: 50 g/week. Limit treatment to 2 consecutive weeks. Guidelines recommend topical corticosteroids as monotherapy for short-term treatment of localized psoriasis.
Topical dosage (shampoo):
Adults: Apply topically to the psoriatic scalp area(s) once daily. Leave in place for 15 minutes, then lather and rinse. Max: 50 g/week. Limit treatment to 4 consecutive weeks. The duration of the therapy depends on factors such as the topical corticosteroid potency, disease severity and anatomic location, and age. After improvement, may consider transitioning to lower-potency corticosteroid, using intermittent therapy, and combining treatment with noncorticosteroidal agents. Taper by reducing use to every other day, then twice weekly, then discontinue if adequate control is maintained. Guidelines recommend class 1 to 7 topical corticosteroids for a minimum of up to 4 weeks for scalp psoriasis. Use of topical corticosteroids for more than 12 weeks may be considered under careful supervision.
Maximum Dosage Limits:
-Adults
50 mL/week scalp or topical solutions and shampoo; 59 mL/week spray solution; 50 g/week other topicals.
-Geriatric
50 mL/week scalp or topical solutions and shampoo; 59 mL/week spray solution; 50 g/week other topicals.
-Adolescents
>= 16 years: Safety and efficacy of lotion, shampoo, and spray solution have not been established; 50 g/week of other formulations.
13 to < 16 years: Safety and efficacy of emollient cream, lotion, shampoo, and spray solution have not been established; 50 g/week of other formulations.
-Children
>= 12 years: Safety and efficacy of emollient cream, lotion, shampoo, and spray solution have not been established; 50 g/week of other formulations.
< 12 years: Safety and efficacy have not been established.
-Infants
Safety and efficacy have not been established.
-Neonates
Safety and efficacy have not been established.
Patients with Hepatic Impairment Dosing
Specific guidelines for dosage adjustments in hepatic impairment are not available; it appears that no dosage adjustments are needed.
Patients with Renal Impairment Dosing
Specific guidelines for dosage adjustments in renal impairment are not available; it appears that no dosage adjustments are needed.
*non-FDA-approved indication
Deferasirox: (Moderate) Because gastric ulceration and GI bleeding have been reported in patients taking deferasirox, use caution when coadministering with other drugs known to increase the risk of peptic ulcers or gastric hemorrhage including corticosteroids.
Metyrapone: (Major) Medications which affect pituitary or adrenocortical function, including all corticosteroid therapy, should be discontinued prior to and during testing with metyrapone. Patients taking inadvertent doses of corticosteroids on the test day may exhibit abnormally high basal plasma cortisol levels and a decreased response to the test. Although systemic absorption of topical corticosteroids is minimal, temporary discontinuation of these products should be considered if possible to reduce the potential for interference with the test results.
Topical corticosteroids exhibit anti-inflammatory, antipruritic, and vasoconstrictive properties. At the cellular level, corticosteroids induce peptides called lipocortins. Lipocortins antagonize phospholipase A2 , an enzyme which causes the breakdown of leukocyte lysosomal membranes to release arachidonic acid. This action decreases the subsequent formation and release of endogenous inflammatory mediators including prostaglandins, kinins, histamine, liposomal enzymes and the complement system. Early anti-inflammatory effects of topical corticosteroids include the inhibition of macrophage and leukocyte movement and activity in the inflamed area by reversing vascular dilation and permeability. Later inflammatory processes such as capillary production, collagen deposition, keloid (scar) formation also are inhibited by corticosteroids. Clinically, these actions correspond to decreased edema, erythema, pruritus, plaque formation and scaling of the affected skin.
Clobetasol is administered topically to the skin as a cream, gel, ointment, or topical solution.
Because clobetasol is fluorinated and also contains a substituted 17-hydroxyl group, it is not metabolized in the skin. Repeated application results in a cumulative depot effect in the skin, which may lead to a prolonged duration of action and increased systemic absorption. Due to the fact that circulating levels are below the level of detection, the use of pharmacodynamic endpoints for assessing the systemic exposure of topical clobetasol is necessary. Once in the systemic circulation, clobetasol is metabolized in the liver, but systemic metabolism has not been fully quantified. Excretion of clobetasol propionate and its metabolites occurs via the urine and bile.
-Route-Specific Pharmacokinetics
Topical Route
The extent of percutaneous absorption of the topical corticosteroids is dependent on many factors, including the pharmaceutical vehicle and the integrity of the epidermis. Absorption after topical application of clobetasol is increased in areas that have skin damage, inflammation, or occlusion, or in areas where the stratum corneum is thin such as the eyelids, genitalia, axillae, and face. The use of occlusive dressings with the application of clobetasol enhances penetration into the skin, and may increase the chance of systemic absorption. Ointments have a hydrating effect, are lipophilic, and enhance the penetration of clobetasol into the skin. Clobetasol gels, foams, and solutions also have enhanced topical penetration versus cream preparations. Once absorbed, maximal vasoconstrictive effects of clobetasol occur within 1.5 hours of application. Anti-inflammatory effects are usually not seen for hours after clobetasol application, since the mechanism of action requires alterations in synthesis of proteins.