AI Article Synopsis

  • The study investigates the connection between nasal carriage of Staphylococcus aureus (S. aureus) and flare-ups in patients with hidradenitis suppurativa (HS) undergoing treatment with adalimumab (ADA), the only FDA-approved biologic for HS.
  • Among 39 patients, those who experienced flare-ups had a higher incidence of nasal S. aureus carriage compared to those with a successful treatment response, indicating a potential link between the bacteria and treatment failure.
  • The findings suggest that S. aureus may contribute to the deterioration of response to ADA in HS patients, and further studies are needed to validate these results on a larger scale.

Article Abstract

Background: Several patients with hidradenitis suppurativa (HS) present flare-ups during treatment with adalimumab (ADA), the cause of which is not clear. ADA is the only FDA-approved biologic for the therapy of moderate-to-severe HS. A previous study of our group has shown that Staphylococcus aureus stimulation of whole blood affects the production of human β-defensin 2 and modulates HS severity. It is, therefore, hypothesized, that carriage of S. aureus may drive HS flare-ups.

Objective: To explore the association between carriage of S. aureus and loss of response to ADA.

Patients And Methods: Among patients with moderate-to-severe HS without carriage of S. aureus at start of treatment with ADA, we investigated for carriage of S. aureus from the nares when flare-ups occurred. Flare-ups were pre-defined as at least 25% increase of inflammatory lesions (sum of inflammatory nodules and abscesses) from baseline. Samplings were also done after completion of 12 weeks of ADA treatment from all patients who did not present flare-ups. Clinical response to ADA was assessed by the HS Clinical Response score (HiSCR).

Results: Thirty-nine patients were studied; 24 with Hurley II stage HS and 15 with Hurley III stage HS. Twenty-nine patients achieved HiSCR after 12 weeks of treatment without any flare-ups; 10 patients had flare-ups and failed HiSCR. Three (10.3%) and 5 (50%) patients, respectively, had nasal carriage of S. aureus (odds ratio 8.67; 95% CI 1.54-48.49; p = 0.014). Among 32 patients reaching follow-up week 48, 20 patients achieved HiSCR and 12 had flare-ups leading to ADA failure; 2 (10%) and 5 (41.7%) patients, respectively, had positive culture for S. aureus (odds ratio 6.42; 95% CI 1.00-41.20; p = 0.05).

Conclusion: Nasal carriage of S. aureus may be associated with loss of response to ADA. Findings need confirmation in larger series of patients.

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Source
http://dx.doi.org/10.1159/000512617DOI Listing

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