Skin care research: Ultraviolet radiation exposure accelerates the accumulation of the aging-dependent T414G mitochondrial DNA mutation in human skin.

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 >

Ultraviolet radiation exposure accelerates the accumulation of the aging-dependent T414G mitochondrial DNA mutation in human skin.

Author: Birket MJ, Birch-Machin MA

Author affiliation: Dermatological Sciences, Institute of Cellular Medicine, School of Clinical and Laboratory Sciences, The Medical School, University of Newcastle upon Tyne, Newcastle upon Tyne NE2 4HH, UK.

Publication date & source: 2007.08, Aging Cell., 6(4):557-64. Epub 2007 Jun 18.

Publication type: Research Support, Non-U.S. Gov't

The accumulation of mitochondrial DNA (mtDNA) mutations has been proposed as an underlying cause of the aging process. Such mutations are thought to be generated principally through mechanisms involving oxidative stress. Skin is frequently exposed to a potent mutagen in the form of ultraviolet (UV) radiation and mtDNA deletion mutations have previously been shown to accumulate with photoaging. Here we report that the age-related T414G point mutation originally identified in skin fibroblasts from donors over 65 years also accumulates with age in skin tissue. Moreover, there is a significantly greater incidence of this mutation in skin from sun-exposed sites (chi(2)= 6.8, P < 0.01). Identification and quantification of the T414G mutation in dermal skin tissue from 108 donors ranging from 8 to 97 years demonstrated both increased occurrence with photoaging as well as an increase in the proportion of molecules affected. In addition, we have discovered frequent genetic linkage between a common photoaging-associated mtDNA deletion and the T414G mutation. This linkage indicates that mtDNA mutations such as these are unlikely to be distributed equally across the mtDNA population within the skin tissue, increasing their likelihood of exerting focal effects at the cellular level. Taken together, these data significantly contribute to our understanding of the DNA damaging effects of UV exposure and how resultant mutations may ultimately contribute towards premature aging.

Indexes of Skin Care Research Abstracts
by Subject Category	Most Recent

-- advertisements --