AI Article Synopsis
- IL-17A is known to play a significant role in immune-mediated inflammatory diseases, while the function of IL-17F, which shares some similarity with IL-17A, is not well understood, though combining the inhibition of both shows potential benefits in treating psoriasis.
- In this study, researchers investigated how IL-17A and IL-17F are regulated in psoriatic disease using various advanced techniques, including RNA sequencing and a new cytokine-capture method.
- The findings highlight that IL-17F is expressed more than IL-17A in psoriatic conditions, with differing cell populations responsible for each isoform and their expression influenced by both inflammatory signals and medications, suggesting a need to target both IL-
Article Abstract
Background: IL-17A plays a pivotal pathogenic role in several immune-mediated inflammatory diseases. Despite sharing 50% sequence homology with IL-17A, the role of IL-17F remains less clear. Clinical findings suggest that dual inhibition of IL-17A and IL-17F in psoriatic disease is more efficacious than IL-17A inhibition alone, positing a pathogenic role for IL-17F.
Objective: We characterized the regulation of IL-17A and IL-17F in psoriatic disease.
Methods: Using both in vitro systems and lesional skin tissue from patients, we interrogated the chromosomal, transcriptional, and protein expression landscape of IL-17A and IL-17F T17 cells. Alongside established assays such as single-cell RNA sequencing, we developed a novel cytokine-capture technique that was combined with chromatin immunoprecipitation sequencing and RNA sequencing.
Results: We confirm a preferential elevation of IL-17F over IL-17A in psoriatic disease and show that expression of each isoform predominantly occurs in distinct cell populations. The expression of both IL-17A and IL-17F exhibited a high degree of plasticity, with the balance between the 2 isoforms influenced by proinflammatory signaling and by anti-inflammatory drugs such as methylprednisolone. This plasticity was reflected in a broad H3K4me3 region at the IL17A-F locus, while opposing effects of STAT5/IL-2 signaling were observed for each of the 2 genes. Functionally, higher IL17F expression was linked to greater cell proliferation.
Conclusion: There are key differences in the regulation of IL-17A and IL-17F in psoriatic disease, leading to distinct inflammatory cell populations. As such, we propose that both IL-17A and IL-17F neutralization may be required to maximally inhibit IL-17-driven pathology.
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| http://dx.doi.org/10.1016/j.jaci.2023.03.035 | DOI Listing |
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