How Does Mometasone Work in the Body

Chemical Composition & Molecular Structure

Mometasone furoate is a synthetic corticosteroid with the chemical name 9,21‑dichloro‑11β,17‑dihydroxy‑16α‑methylpregna‑1,4‑diene‑3,20‑dione 17‑(2‑furoate). Its molecular formula (free base) is C₂₇H₃₀Cl₂O₆ and molecular weight 521.4 g/mol. The drug is formulated as the monohydrate in a white, aqueous suspension for intranasal use.

Key Pharmaceutical Properties

Mechanism of Action: Mometasone Pathway

Mometasone exerts its therapeutic effect through genomic and non‑genomic pathways, ultimately dampening the allergic inflammatory cascade.

1. Glucocorticoid receptor binding: After diffusion into target cells (epithelial, eosinophils, mast cells), mometasone binds to cytoplasmic glucocorticoid receptors with high affinity. The drug‑receptor complex translocates to the nucleus.
2. Transrepression: In the nucleus, the complex interferes with transcription factors (NF‑κB, AP‑1), suppressing the expression of pro‑inflammatory cytokines (IL‑4, IL‑5, IL‑13), chemokines, and adhesion molecules.
3. Transactivation: It also increases transcription of anti‑inflammatory proteins (lipocortin‑1, IL‑10), further resolving inflammation.
4. Clinical correlates: Reduced eosinophil infiltration, decreased mucus secretion, and diminished nasal mucosa oedema lead to relief of sneezing, itching, rhinorrhoea, and congestion.

Absorption & Distribution (Pharmacokinetics)

Following intranasal administration, a fraction of the dose is retained in the nasal cavity; the remainder is swallowed. Systemic absorption from the nasal mucosa is minimal (<0.1% of nominal dose) due to low solubility and extensive first‑pass metabolism of the swallowed portion.

Metabolic Effects & Elimination

Metabolism: The small amount of mometasone that reaches the systemic circulation is rapidly metabolised in the liver, primarily by the CYP3A4 isoenzyme, to multiple hydroxylated metabolites. These metabolites are pharmacologically inactive.

Elimination: Over 90% of an absorbed dose is excreted via the bile into faeces; less than 1% appears in urine as unchanged drug or metabolites. The terminal half‑life after intravenous administration is approximately 5.8 hours, but this is not relevant for nasal therapy due to negligible systemic levels.

Clinical Efficacy in Rhinitis and Nasal Polyps

Allergic rhinitis (seasonal/perennial): Mometasone furoate nasal spray reduces nasal symptoms (sneezing, itching, rhinorrhoea, congestion) and ocular symptoms in many patients. Improvement begins within 12 hours after the first dose, but maximal benefit is achieved after 1‑2 weeks of regular use. It is licensed for adults and children ≥3 years (usual dose: one or two sprays per nostril once daily).

Nasal polyps: In adults (≥18 years), mometasone shrips existing polyps and prevents regrowth. The recommended starting dose is two sprays in each nostril once daily; if no response after 5‑6 weeks, it may be increased to twice daily. Regular use reduces nasal obstruction and improves quality of life.

• Onset for polyps: Symptom improvement may take several weeks; if no benefit after 5‑6 weeks of twice‑daily dosing, reassess treatment.
• Steroid‑sparing effect: Mometasone can reduce the need for oral corticosteroids in polyp patients.

Mometasone FAQs

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