Abstract
Rosacea is a common chronic inflammatory skin disease of the central facial skin and is of unknown origin. Currently, two classifications of rosacea exist that are based on either “preformed” clinical subtypes (erythematotelangiectatic, papulopustular, phymatous, and ocular) or patient-tailored analysis of the presented rosacea phenotype. Rosacea etiology and pathophysiology are poorly understood. However, recent findings indicate that genetic and environmental components can trigger rosacea initiation and aggravation by dysregulation of the innate and adaptive immune system. Trigger factors also lead to the release of various mediators such as keratinocytes (for example, cathelicidin, vascular endothelial growth factor, and endothelin-1), endothelial cells (nitric oxide), mast cells (cathelicidin and matrix metalloproteinases), macrophages (interferon-gamma, tumor necrosis factor, matrix metalloproteinases, and interleukin-26), and T helper type 1 (T H1) and T H17 cells. Additionally, trigger factors can directly communicate to the cutaneous nervous system and, by neurovascular and neuro-immune active neuropeptides, lead to the manifestation of rosacea lesions. Here, we aim to summarize the recent advances that preceded the new rosacea classification and address a symptom-based approach in the management of patients with rosacea.
Highlights
Rosacea is a common chronic inflammatory skin disease of the central facial skin and is of unknown origin
This review aims to summarize the recent developments in our understanding of rosacea’s pathophysiology that preceded the release of the modified rosacea classification and to illustrate the therapeutic management of individual rosacea patients on the basis of their symptoms
Rhinophyma nearly exclusively presents in the male gender, flushing and erythema often are the first disease signs in younger ages, and telangiectasias make up first rosacea lesions in older ages
Summary
Halioua B, Cribier B, Frey M, et al.: Feelings of stigmatization in patients with rosacea. Haber R, El Gemayel M: Comorbidities in rosacea: A systematic review and update. Egeberg A, Hansen PR, Gislason GH, et al.: Patients with rosacea have increased risk of dementia. Holmes AD, Spoendlin J, Chien AL, et al.: Evidence-based update on rosacea comorbidities and their common physiologic pathways. Buhl T, Sulk M, Nowak P, et al.: Molecular and Morphological Characterization of Inflammatory Infiltrate in Rosacea Reveals Activation of Th1/Th17 Pathways. Kistowska M, Meier B, Proust T, et al.: Propionibacterium acnes promotes Th17 and Th17/Th1 responses in acne patients.
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