Hidradenitis Suppurativa Clinical Trial
Official title:
A Pilot Study to Examine Safety, Activity and Biomarkers in Participants With Hidradenitis Suppurativa Receiving a Previously Tested Subcutaneous Dose of Anti-IL-23 Monoclonal Antibody Guselkumab.
Hidradenitis Suppurativa (HS) is a severe, chronic debilitating disease with a variable and
incomplete response to current treatments. Existing immunological studies have found
dysregulation in the TH17:Treg axis with an increase in inflammatory mediators including
TNFalpha, IL-17 IL-23 (amongst others) in lesional skin. Multiple cell typesincluding CD4+
cells, dendritic cells and macrophages infiltrate active lesions of HS and produce this major
contribution from the Th17 axis.
One of the main barriers to the development of novel and effective treatments for HS is the
lack of biomarker(s) of disease activity, as well as our incomplete understanding of the
pathogenesis of this disease. Given the pronounced contribution of Th17 pathway (including
interleukin-23) in the inflammation in HS, further investigation into the role of this axis
in the pathogenicity of HS is essential. Guselkumab is a fully human interluekin-23
antagonist, FDA approved for the treatment of moderate to severe psoriasis in participants 18
years and over. Guselkumab is a novel potential therapy.
Hidradenitis Suppurativa (HS) is a severe, chronic debilitating disease with a variable and
incomplete response to current treatments. Existing immunological studies have found
dysregulation in the TH17:Treg axis with an increase in inflammatory mediators including
TNFalpha, IL-17 IL-23 (amongst others) in lesional skin. Multiple cell typesincluding CD4+
cells, dendritic cells and macrophages infiltrate active lesions of HS and produce this major
contribution from the Th17 axis.
One of the main barriers to the development of novel and effective treatments for HS is the
lack of biomarker(s) of disease activity, as well as our incomplete understanding of the
pathogenesis of this disease. Markers such as C- Reactive Protein, IL-6, soluble IL-2
receptor, S100A8/9, lipocalin-2 and the neutrophil/lymphocyte rati7 have been proposed as
potential biomarkers but lack high specificity and correlation with disease severity. Given
the pronounced contribution of Th17 pathway (including interleukin-23) in the inflammation in
HS, further investigation into the role of this axis in the pathogenicity of HS is essential.
Guselkumab is a fully human interluekin-23 antagonist, FDA approved for the treatment of
moderate to severe psoriasis in participants 18 years and over. Guselkumab is a novel
potential therapy.
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