Paradoxical reactions during treatment with biological agents may be defined as an appearance or exacerbation of a pathological condition that usually responds to this class of drug. Typical examples of paradoxical adverse effect are, among others, palmoplantar pustular and psoriasiform reactions or HS, in patients during a treatment of rheumatoid arthitis or IBD mainly. A few reports have been described an exacerbation of psoriasis1, palmoplantar pustular, or pustular psoriasis eruption with secukinumab. Marasca et al. highlights the immunological comperformed to evaluate its efficacy and safety in moderate-to-severe HS, which will presumably be completed on January 2019. Hidradenitis suppurativa has also been reported to be paradoxically induced in patients treated with TNFα blockers, such infliximab or adalimumab (Delobeau et al., 2016). In a recently published series of 25 cases (Faivre et al., 2016), complete resolution of paradoxical hidradenitis suppurativa occurred after treatment discontinuation or switching to another biological agent, whereas reintroduction of the same biological agent resulted in relapse in all cases. Few reports have been published in order to communicate a good response to secukinumab in patients diagnosed of HS (with or without overlap psoriasis) (Thorlacius, Theut Riis, & Jemec, 2018). Nevertheless, secukinumab can also be the trigger of a paradoxical HS, as the case reported. Marasca (Marasca et al., 2019) highlights the immunological complexity that may surround autoinflammatory diseases showing the potential double pathophysiological face of secukinumab in HS, describing a case of secukinumab-induced HS and a case of HS provoked by adalimumab treatment and controlled with secukinumab therapy. The activation of interferon type I or IL-1β, and others local cytokine balance modifications, may explain the occurrence of paradoxical HS. This hypothesis is mainly focused on treatments based on TNF blockers. A possible explanation would be an increasing of the concentration of TNF-alpha, IL-26, IL-29, and IFN-γ produced by T-cells, accompanied by the increasing of IL-12 and IL-23 produced by dendritic cells. The possible magnification of ICAM-1 and TGF-B signaling, would trigger hyperproliferative keratinocytes, and as a result, HS lesions. Real world evidence and results from randomized clinical trials with secukinumab for HS, will shed light on the real and main role that anti-IL-17 drugs play in this complex disease. From clinical and immunological HS context, new therapeutic frontiers will be opened providing useful information to improve the knowledge of the immunological pathways that cause it. ORCID Francisco J. Navarro-Triviño https://orcid.org/0000-0002-5454-3671Ricardo Ruiz-Villaverde https://orcid.org/0000-0002-0381-6174
