Betamethasone | Pharmacology Mentor

Generic Name

glucocorticoid

Mechanism

Binding: *Betamethasone* binds to cytosolic glucocorticoid receptors (GR) with high affinity.
Translocation: The drug–GR complex translocates to the nucleus.
Transcriptional regulation:
Transactivation: Upregulation of anti‑inflammatory proteins (e.g., annexin‑1, lipocortin‑1) that inhibit phospholipase A₂.
Transrepression: Direct inhibition of NF‑κB and AP‑1, reducing secretion of pro‑inflammatory cytokines (IL‑1β, TNF‑α, IFN‑γ) and chemokines.
Effect: Suppression of leukocyte migration, edema formation, and capillary permeability.

Pharmacokinetics

Absorption: Rapidly absorbed orally; topical absorption depends on vehicle; ophthalmic administration achieves high corneal and conjunctival levels.
Distribution: Highly lipophilic; extensively binds to plasma proteins (>95 %); penetrates tissues, especially skin and CNS.
Metabolism: Primarily glucuronidated in the liver (CYP3A4 involvement minimal); metabolites are inactive.
Elimination: Excreted via kidneys as glucuronide conjugates; mean half‑life ∼ 3–4 h (oral), longer for intramuscular depot forms (up to 10 days).
Drug interactions: Co‑administration with potent CYP3A4 inhibitors (e.g., ketoconazole) may increase systemic exposure.

Indications

Dermatologic: Atopic dermatitis, psoriasis, eczema, cutaneous lupus erythematosus, dermatomyositis rash.
Respiratory: Acute asthma exacerbations, chronic obstructive pulmonary disease flare‑ups, allergic rhinitis.
Systemic: Systemic lupus erythematosus, rheumatoid arthritis, inflammatory bowel disease (predominantly through oral or IV preparations).
Oral/ocular: Uveitis, conjunctivitis, keratitis (topical ophthalmic drops).
Autoimmune: Systemic vasculitis, dermatomyositis, polymyositis.
Miscellaneous: Prevent or treat ICD‑20 medication‑induced hyperglycemia in insulin‑dependent diabetics.

Contraindications

Absolute: Known hypersensitivity to betamethasone or any component; active systemic fungal infections; untreated tuberculosis.
Relative: Untreated viral hepatitis, uncontrolled diabetes, uncontrolled hypertension.
Warnings:
Risk of HPA axis suppression with prolonged use.
Ocular hypertension and cataract formation with topical ophthalmic therapy.
Skin infection, ulceration, or opportunistic infection when used topically or systemic.
Potential for medication‑induced hyperglycemia in diabetic patients.

Dosing

Formulation	Typical Dose (Adults)	Route	Note
Oral	0.5 – 2.5 mg/day	PO	Use the lowest effective dose; taper rapidly to avoid adrenal crisis.
Topical	0.1 – 0.3 % cream/ointment	TID	Avoid prolonged use on broken skin; may cause skin atrophy.
Intramuscular (Depo)	0.4 – 0.8 mg/kg	IM	Slow‑release for 7–10 days; monitor for adrenal suppression.
Ophthalmic	0.5 – 2.5 % solution	Instillation 4–6×/day	Use under guidance; monitor intra‑ocular pressure.
IV	1–2 mg (for acute flare)	IV	Use in severe systemic inflammatory conditions.

Titration: Start at lowest effective dose; increase only if benefit outweighs risk; taper over ≥7 days after ≥1 month of use.

Adverse Effects

Common:
• Local skin atrophy and striae (topical)
• Hyperglycemia (systemic)
• Osteoporosis (long‑term)
• Mood/behavior changes

Serious:
• Adrenal insufficiency (with abrupt discontinuation)
• Severe infection (cutaneous or systemic)
• Sudden ocular hypertension, glaucoma (ocular)
• Allergic reactions (e.g., anaphylaxis)

Monitoring

Endocrine: Serum cortisol (baseline and during taper), ACTH if concern of HPA suppression.
Metabolic: Blood glucose monitoring on prolonged systemic therapy.
Laboratory: CBC (monitor for leukopenia), lipid panel (especially with long‑term use).
Ophthalmic: Intra‑ocular pressure, slit‑lamp exam for cataract progression.
Dermatologic: Examine for skin atrophy or signs of infection.

Frequency: Baseline, 1‑month, then every 3–6 months for long‑term users.

Clinical Pearls

Depot Advantage: The intramuscular depot formulation provides sustained plasma levels without daily dosing, useful for acute flare‑ups but requires careful tapering.
Topical Use with Occlusion: Avoid occlusive dressings unless under physician supervision, as it increases systemic absorption and risk of skin atrophy.
Eye‑Drop Safety: Use the lowest concentration that offers therapeutic benefit; instruct patients to keep eye lids closed post‑instillation to reduce drug loss.
Drug–Drug Interaction: When combined with other steroids (e.g., prednisone), the additive effect can severe HPA suppression; consider steroid‑sparing adjuncts.
Patient Education: Emphasize the importance of gradual dose reduction and reporting symptoms such as dizziness, fatigue, or abdominal pain, which may indicate adrenal crisis.
Glucuronides: Because the drug is largely inactivated by glucuronidation, patients with hepatic dysfunction may have increased exposure; dose adjustment may be necessary.

Reference List

1. Katzung, B.G. & Masters, S.H. *Basic & Clinical Pharmacology*. 15th ed., 2024.

2. Kieseier, B.C., et al. "Betamethasone in Dermatologic Disease." *Journal of Dermatology*, 2022.

3. Hahne, L., et al. "Pharmacokinetics of Betamethasone." *Clinical Pharmacokinetics*, 2021.

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