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Rosacea pathogenesis and therapeutics: current treatments and a look at future targets. | LitMetric

AI Article Synopsis

  • Rosacea is a chronic skin condition that causes both health issues and economic strain due to treatment costs and loss of productivity.
  • The disease involves multiple symptoms and has complex causes, including skin barrier dysfunction, immune system responses, and neurovascular factors.
  • Ongoing research is focused on understanding its mechanisms better and exploring new treatments targeting pathways like JAK/STAT inhibitors and other novel molecular targets to improve patient outcomes.

Article Abstract

Rosacea is a chronic inflammatory skin condition associated with a significant health and economic burden from costs and loss of productivity due to seeking medical treatment. The disease encompasses multiple phenotypic manifestations involving a complex and multi-variate pathogenesis. Although the pathophysiology of rosacea is not completely understood, ongoing research is continually elucidating its mechanisms. In this review, current concepts of rosacea pathogenesis will be addressed which involve skin barrier and permeability dysfunction, the innate and adaptive immune systems, and the neurovascular system. More specifically, the cathelicidin pathway, transient potential receptor channels, mast cells, and the NLRP3 inflammasome pathway are various targets of current pharmacologic regimens. Future therapies may seek different mechanisms to act on current treatment targets, like the potential use of JAK/STAT inhibitors in ameliorating skin barrier dysfunction or TLR antagonists in alleviating cathelicidin mediated inflammation. Other potential treatments aim for entirely different molecular targets such as microvesicle particle mediated local and systemic inflammation. Ultimately rosacea is associated with a significant health and economic burden which warrants deeper research into its pathogenesis and resultant new treatment discovery.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10773789PMC
http://dx.doi.org/10.3389/fmed.2023.1292722DOI Listing

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