AI Article Synopsis
- Omalizumab (OMA) is the first FDA-approved biological treatment for severe chronic spontaneous urticaria (CSU) and continues to be considered the safest option available.
- A study tracked 93 CSU patients over six years to evaluate how many could stop using OMA and whether certain biomarkers could predict this outcome.
- After six years, about 52% of the patients still required OMA therapy, and those who couldn't stop had significantly lower IgE levels and higher anti-TPO antibody positivity.
Article Abstract
Background: Omalizumab (OMA) was the first FDA-approved biological drug for severe chronic spontaneous urticaria (CSU), and until today is the only beneficial and truly safe one. The objectives were: To assess the prevalence of CSU patients in whom OMA cannot be stopped over time. We also asked if biomarkers (e.g., anti-TPO antibodies and total IgE) could assist in anticipating this issue.
Methods: We used our prospective registry of 93 patients, which included CSU disease duration, the onset of OMA treatment, Urticaria Activity Score (UAS7) during follow-up, co-morbidities, serum IgE levels and the presence of anti-TPO antibodies. Finally, we assessed the response to OMA during a period of six years.
Results: Out of the 93 treated CSU patients, OMA was stopped in ten patients after six months being defined as failures. In another ten patients, OMA was discontinued after 2-4 years of therapy, achieving a remission. Seventy-three patients are still treated between 2 and 6 years, having different degrees of response. Of these, in thirty-eight (52%) patients, we could not stop OMA even after six years due to CSU relapses. The prevalence of lower serum IgE levels and anti-TPO antibody positivity was significantly higher in CSU patients in whom OMA could not be stopped.
Conclusion: This is the first study where OMA-treated CSU patients were followed up to six years. In half of them, long-term therapy of six years is still required.
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|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11480063 | PMC |
| http://dx.doi.org/10.3389/falgy.2024.1464466 | DOI Listing |
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