Zestoretic
Zestoretic
Generic Name
Zestoretic
Mechanism
Zestoretic is a fixed‑dose combination of:
• Triamcinolone acetonide (0.05 % topical corticosteroid)
• Montelukast (0.5 % leukotriene receptor antagonist)
• Triamcinolone acetonide binds to cytoplasmic glucocorticoid receptors, translocates into the nucleus, and modulates transcription of anti‑inflammatory genes while suppressing pro‑inflammatory cytokines (IL‑1, IL‑6, TNF‑α).
• Montelukast competitively antagonizes the cysteinyl leukotriene (Cys‑LT₄, D₄, E₄) receptors (CysLT₁) on keratinocytes and immune cells, reducing leukotriene‑mediated vasodilation, bronchoconstriction and epidermal itching.
• The dual action reduces edema, erythema and pruritus synergistically, allowing lower systemic steroid exposure.
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Pharmacokinetics
| Parameter | Topical Triamcinolone Acetonide | Topical Montelukast |
| Skin absorption | 1–5 % of applied dose under intact skin; higher in inflamed skin | Key point – Most systemic effects stem from triamcinolone acetonide; montelukast contributes predominantly to topical itch suppression.
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Indications
- Atopic dermatitis (moderate to severe, refractory to conventional topical steroids)
- Allergic contact dermatitis (persistent pruritus)
- Eczema herpeticum – adjunctive therapy to reduce inflammation
- Other pruritic, inflammatory skin disorders where corticosteroid monotherapy shows inadequate response or high relapse risk
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Contraindications
- Hypersensitivity to triamcinolone, montelukast, or excipients
- Candidiasis or bacterial superinfection: may worsen with immunosuppression
- Extensive skin disease >30 % BSA in adults, >15 % in children
- Facial, intertriginous, or genital skin in children Warnings – Prolonged use (>2 weeks) increases risk of skin atrophy, striae, telangiectasia, and HPA axis suppression from triamcinolone. Montelukast may cause CNS events (headache, agitation) and rare hypersensitivity reactions.
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Dosing
| Population | Application | Frequency | Duration |
| Adults & Children ≥ 12 yrs | 1–2 tubes to affected area | Twice daily | Up to 2 weeks (titrate down based on response) |
| Children 3–12 yrs | 0.5 mg/kg/4 h (≈1 mg/cm²) | Twice daily | ≤ 1 week; reassess |
| Children < 3 yrs | Avoid unless under specialist supervision with minimal dose | - | - |
• Technique – Gently massage until absorbed.
• Avoid occlusion unless clinically indicated; topical absorption is optimal only with intact skin.
• Discontinue abruptly if signs of infection or systemic side effects appear.
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Adverse Effects
- Local: burning, stinging, erythema, itching, dry skin, scaling
- Dermatologic: skin atrophy, striae, telangiectasia, pigmentary changes, hypertrichosis
- Systemic (due to triamcinolone): HPA axis suppression, adrenal insufficiency, cushingoid features, hypertension, glucose intolerance
- Montelukast‑specific: headache, GI upset (nausea, abdominal pain), rash, eosinophilia, rare anaphylaxis
> Serious – Systemic steroid effects, severe allergic reactions to montelukast (rash, urticaria, hypotension).
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Monitoring
- Skin assessment: evaluate for atrophy, striae, telangiectasia every 2–4 weeks during therapy
- Adrenal function: consider baseline morning cortisol if prolonged use anticipated (>2 weeks) or in high‑risk patients
- Blood pressure & glucose: if underlying metabolic disorders
- Allergic symptoms: monitor for swelling, hives, anaphylaxis, especially within first 72 h of therapy
- Patient diary: track improvement in pruritus and erythema to guide taper
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Clinical Pearls
- Pruritus‑shield – The addition of montelukast reduces itch more rapidly than steroid monotherapy; consider in flare‑up patients who need quick symptom relief.
- Caution in infants – Due to higher systemic absorption from thinner skin, avoid ages <3 yrs unless under pediatric dermatology supervision.
- Avoid ocular contact – The formulation’s lipophilic matrix can cause corneal irritation; apply a barrier cream around the eyes.
- Occlusive dressing synergy – For stubborn lesions, cover with occlusive bandage for 1–2 h to enhance penetration, but limit duration to 5 h to minimize atrophy.
- Switch‑to‑strategy – After ≤ 2 weeks, reassess; if sufficient clearing, taper down to triamcinolone alone or switch to non‑steroidal anti‑inflammatory (e.g., calcineurin inhibitors) to reduce cumulative steroid burden.
- Montelukast safety – In patients with a history of seizures or neuropsychiatric events, monitor for changes in mood or cognition; adjust as necessary.
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• *Keywords: Zestoretic pharmacology, mechanism, dosage, side‑effects, atopic dermatitis, topical steroid, montelukast, clinical pearls, HPA axis, skin atrophy.*