Skin care research: Pathophysiology of photoaging of human skin: focus on neutrophils.

Intelligent anti-aging skin care based on independent research

Lose wrinkles, keep your bank account!

Skin Care 101

Skin Care Basics

Skin Protection

Skin Biology

Biology of Aging

Ingredient Guide

Skin & Nutrition

Skin Conditions

Anti-Aging Treatments

Topical Actives

Wrinkle Fillers

Noninvasive

Invasive

Skin Care Smarts

Smart Choices

Best Practices

Find Good Skin Doc

Quick Tips

Freebie Finder

Reviews & Research

Product Reviews

Provider Reviews

Skin Care Research

Clinical Trials

How-To Infopacks

Skin Rejuvenation

DIY Skin Care

Skin & Nutrition

Eye Skin Care

Longevity In a Pill

Community & Misc

Forums

Polls & Surveys

News and Updates

Search

-- advertisements --

You are here: Skin Care Research >

Pathophysiology of photoaging of human skin: focus on neutrophils.

Author: Rijken F, Kiekens RC, van den Worm E, Lee PL, van Weelden H, Bruijnzeel PL

Author affiliation: Department of Dermatology, G.02.124, University Medical Centre Utrecht, Heidelberglaan 100, 3584, CX, Utrecht, The Netherlands. F.Rijken@azu.nl

Publication date & source: 2006.02, Photochem Photobiol Sci., 5(2):184-9. Epub 2006 Jan 3.

Publication type: Review

UV-induced skin damage is the result of a complex cascade of events. Many studies have focused on the skin effects induced by UV-B or UV-A separately. Recently a UV-source that emits UV-B and UV-A together in a ratio comparable to daily sunlight has been introduced: i.e. solar simulated radiation (SSR). By exposing human skin type I-III to erythematogenic doses of UV (> or =1 MED) emitted by a SSR source we have noticed that: (a) neutrophils are initially the main infiltrating cell type in the dermis and (b) these infiltrating cells are the a key source of in vivo enzymatically [corrected] active enzymes such as elastase, [corrected] matrix metallo proteinases-1 and -9 (MMPs-1 and -9). These enzymes are relevant to the process of photoaging, as they break down the extracellular matrix. Keratinocytes and fibroblasts also produce matrix degrading enzymes, but to a lesser extent. Our results indicate a primary role for infiltrating neutrophils in the initial steps of photoaging. This is further supported by the observation that after exposure of skin type VI to physical doses of SSR, equivalent to those used for skin types I-III, no neutrophils and neutrophil-derived enzymatic activity were observed, explaining why skin type VI is [corrected] less susceptible to photoaging than skin types [corrected] I-III. Statement: Although most of the data, referred to, have been published, the current perspective in which they are put together is completely novel and has not been published elsewhere.

Indexes of Skin Care Research Abstracts
by Subject Category	Most Recent

-- advertisements --