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New insights into rosacea pathophysiology: A review of recent findings

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TLDR
This review discusses some of the recent findings and aims to build unifying hypotheses for a modern understanding of rosacea pathophysiology, which is severely hampered by the complex activation of the innate and adaptive immune systems, enhanced neuroimmune communication, profound blood vessel and lymphatic vessel changes, and activation of almost every resident cell in the skin.
Abstract
Rosacea is a common, chronic inflammatory skin disease of poorly understood origin. Based on its clinical features (flushing, chronic inflammation, fibrosis) and trigger factors, a complex pathobiology involving different regulatory systems can be anticipated. Although a wealth of research has shed new light over recent years on its pathophysiology, the precise interplay of the various dysregulated systems (immune, vascular, nervous) is still poorly understood. Most authors agree on 4 major clinical subtypes of rosacea: erythematotelangiectatic rosacea, papulopustular rosacea, phymatous rosacea, and ocular rosacea. Still, it needs to be elucidated whether these subtypes develop in a consecutive serial fashion or if any subtypes may occur individually as part of a syndrome. Because rosacea often affects multiple family members, a genetic component is also suspected, but the genetic basis of rosacea remains unclear. During disease manifestation and early stage, the innate immune system and neurovascular dysregulation seem to be driving forces in rosacea pathophysiology. Dissection of major players for disease progression and in advanced stages is severely hampered by the complex activation of the innate and adaptive immune systems, enhanced neuroimmune communication, profound blood vessel and possibly lymphatic vessel changes, and activation of almost every resident cell in the skin. This review discusses some of the recent findings and aims to build unifying hypotheses for a modern understanding of rosacea pathophysiology.

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Roles of Mas-related G protein–coupled receptor X2 on mast cell–mediated host defense, pseudoallergic drug reactions, and chronic inflammatory diseases

TL;DR: It is proposed that host defense peptides that kill microbes directly and activate MCs through MRGPRX2 could serve as novel GPCR targets to modulate host defense against microbial infection.
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Interventions for rosacea.

TL;DR: Two topical treatments, metronidazole and azelaic acid, were shown to be more effective than placebo in papulopustular rosacea (moderate quality evidence for metRONidazoles and high for azelaoic acid) and pooled data from physician assessments in three trials demonstrated that metronIDazole was more effective compared to placebo.
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Assessment of the Genetic Basis of Rosacea by Genome-Wide Association Study

TL;DR: Collection of gene variants identified in this genome-wide association study support the concept of a genetic component for rosacea, and provide candidate targets for future studies to better understand and treatrosacea.
Journal ArticleDOI

Rosacea: Epidemiology, pathogenesis, and treatment

TL;DR: Because of the diverse presentations of rosacea, approaches to treatment must be individualized based on the disease severity, quality-of-life implications, comorbidities, trigger factors, and the patient's commitment to therapy.
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