Generic Name

Xospata

Brand Names

*Lesuvel™* in the United States and *Lesumex™ internationally.

Mechanism

Xospata selectively binds to the ATP‑binding pocket of the p38α and p38β isoforms, preventing phosphorylation of downstream substrates (e.g., ATF2, NF‑κB).
• Result: ↓ production of pro‑inflammatory cytokines (TNF‑α, IL‑1β, IL‑6)
• Clinical outcome: reduced disease activity index (SLEDAI) and improved organ involvement (arthritis, serositis, cutaneous lesions)

Pharmacokinetics

• Absorption: Rapid, peak plasma concentrations (Cmax) reached ~2 h post‑dose; oral bioavailability ~48 %.
• Distribution: Moderate plasma protein binding (~30 %), volume of distribution Vd ≈ 45 L.
• Metabolism: Primarily hepatic CYP3A4/5–mediated oxidative metabolism; minor CYP2C19 contribution.
• Elimination: Renally excreted (~25 % unchanged); hepatic biliary excretion accounts for ~70 % of total clearance.
• Half‑life (t½): ~12 h (steady‑state steady).
• Drug‑Drug Interaction: Strong CYP3A4 inhibitors (e.g., ketoconazole) ↑ Xospata exposure by ~2.5×; potent CYP3A4 inducers (e.g., rifampin) ↓ exposure by ~60 %.

Indications

• Primary: Moderate‑to‑severe systemic lupus erythematosus (SLEDAI ≥ 6) refractory to at least 6 months of standard therapy (e.g., hydroxychloroquine, methotrexate, mycophenolate mofetil, or azathioprine).
• Off‑label (investigational):
• Mixed connective tissue disease (MCTD) with renal involvement.
• Juvenile idiopathic arthritis (JIA) in clinical trials.

Contraindications

• Contraindications
• Known hypersensitivity to Xospata or excipients.
• Severe hepatic impairment (Child‑Pugh C).
• Pregnancy (category X) and breastfeeding.
• Warnings
• Hepatotoxicity: Monitor transaminases; dose adjustment or discontinuation if ALT/AST >5× ULN.
• QT Prolongation: Baseline ECG; avoid concomitant medications that prolong QT (e.g., sotalol, fluoroquinolones).
• Immunosuppression: Increased risk of serious infections; vaccinate for pneumococcus, hepatitis B prior to therapy.

Dosing

• Take with food to improve absorption.
• Swallow intact tablets; crushing is not recommended.

Adverse Effects

• Common (≥10 %):
• Nausea, dyspepsia
• Diarrhea
• Headache
• Transient mild ↑ transaminases
• Serious (≥1 %):
• Hepatotoxicity (elevated ALT/AST, hepatic failure)
• Severe infections (bacterial pneumonia, opportunistic fungi)
• QT prolongation → Torsades de pointes
• Hypersensitivity reactions (urticaria, angioedema)

Monitoring

• Baseline (pre‑initiation):
• CBC with differential
• CMP (ALT/AST, bilirubin, creatinine)
• ECG (QTc interval)
• Hepatitis B and C serology
• Ongoing:
• LFTs every 4 weeks (or sooner if ALT/AST >3× ULN).
• CBC every 6 weeks.
• ECG every 3 months or if QT‑prolonging co‑meds added.
• Patient Education: Report sudden jaundice, dark urine, or persistent nausea/diarrhea.

Clinical Pearls

• Use a staggered dosing schedule in patients with renal impairment to prevent accumulation; consider renal dose adjustment for eGFR < 30 mL/min/1.73 m².
• Avoid co‑administration with strong CYP3A4 inhibitors; if unavoidable, monitor trough levels and consider dose reduction.
• Baseline ECG critical: Even mild QTc prolongation (<460 ms) can compound risk when combined with other QT‑prolonging agents.
• Hepatotoxicity is dose‑dependent: Early detection through LFT monitoring can avert severe liver injury.
• Patient adherence: Taking Xospata with food increases bioavailability by ~1.3×; counsel on consistent meal timing.
• Immunization: Vaccinate against pneumococcus, shingles, and influenza before starting therapy; avoid live vaccines during treatment.

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