SOCS-1 inhibition of type I interferon limits<i>Staphylococcus aureus</i>skin host defense

Klopsfenstein, Nathan; Brandt, Stephanie; Castellanos, Sydney; Serezani, C. Henrique

doi:10.1101/2020.09.28.317107

Cited by 1 publication

(1 citation statement)

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“…These cytokines may enhance skin immune responses against S. aureus, influencing bacterial loads. 28 Opposingly, chronic exposure to interferons disrupts the skin barrier, increasing staphylococcal colonization. 29,30 These divergent effects of interferons may account for the different outcomes regarding skin Staphylococcus spp.…”

Section: Discussionmentioning

confidence: 99%

Recombinant human interferon‐α14 for the treatment of canine allergic pruritic disease in eight dogs

Beirão

Taraciuk

Trentin

et al. 2021

Veterinary Record Open

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Background Allergic pruritic diseases are increasingly common in dogs. This group of conditions hampers life quality as pruritus progressively interferes with normal behaviours. Therefore, new treatment modalities for canine allergic pruritic diseases are necessary. While novel drugs have recently reached the market, there is still the need for other therapeutic approaches. Some dogs are refractory even to the newer compounds, and cost is also an important issue for these. Older therapeutic modalities are only moderately successful or have considerable secondary effects, as is the case with glucocorticoids. Objectives Report on the use of recombinant human interferon‐α14 (rhIFN‐α14) for the treatment of canine allergic pruritus. Following the experience with a similar compound in the Japanese market, it was expected that rhIFN‐α14 could alter the Th1/Th2 disbalance that drives these diseases. Methods Here, we present an uncontrolled trial in which eight dogs with clinical diagnosis of allergic pruritus were treated with rhIFN‐α14, either orally or via subcutaneous injections. Skin condition, microbiota and anti‐interferon antibody levels were assessed. Results The parenteral use of interferon induced hypersensitivity in two of the three dogs in which it was used. The oral administration was consistently safe and could reduce signs of the allergic condition in three of the five treated animals. Treatment also altered the skin microbiota, as verified by next‐generation sequencing. Conclusion The present results indicate that rhIFN‐α14 is a viable candidate for the treatment of canine allergic pruritus. Future controlled studies are needed, and the oral route is indicated for further trials.

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Section: Discussionmentioning

confidence: 99%