Intrinsic and Extrinsic Risk Factors for Sagging Eyelids

• Autores: Leonie C. Jacobs, Fan Liu, Isabel Bleyen, David A. Gunn, Albert Hofman, Caroline C. W. Klaver, André G. Uitterlinden, H. A. Martino Neumann, Veronique Bataille, Timothy D. Spector, Manfred Kayser
• Localización: JAMA Dermatology, ISSN 2168-6068, Vol. 150, Nº. 8, 2014, págs. 836-843
• Idioma: inglés
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• Resumen

  • Importance Sagging eyelids, or dermatochalasis, are a frequent concern in older adults. It is considered a feature of skin aging, but risk factors other than aging are largely unknown.

    Objective To study nongenetic and genetic risk factors for sagging eyelids.

    Design Upper eyelid sagging was graded in 4 categories of severity using digital photographs. Dermatochalasis was defined as the eyelid hanging over the eyelashes. Age, sex, skin color, tanning ability, hormonal status in women, current smoking, body mass index, and sun protection behavior were analyzed in a multivariable multinomial logistic regression model. Genetic predisposition was assessed using heritability analysis and a genome-wide association study.

    Setting and Participants The study was performed in 2 independent population-based cohorts. The Rotterdam Study included older adults from one district in Rotterdam, the Netherlands, and the UK Adult Twin Registry (TwinsUK) included twins from all over the United Kingdom. Participants were 5578 unrelated Dutch Europeans (mean age, 67.1 years; 44.0% male) from the Rotterdam Study and 2186 twins (mean age, 53.1 years; 10.4% male) from the TwinsUK.

    Main Outcomes and Measures Sagging eyelid severity levels, ranging from 1 (normal control) to 4 (severe sagging).

    Results Among 5578 individuals from the Rotterdam Study, 17.8% showed dermatochalasis (moderate and severe sagging eyelids). Significant and independent risk factors for sagging eyelids included age, male sex, lighter skin color, and higher body mass index. In addition, current smoking was borderline significantly associated. Heritability of sagging eyelids was estimated to be 61% among 1052 twin pairs from the TwinsUK (15.6% showed dermatochalasis). A meta-analysis of genome-wide association study results from 5578 Rotterdam Study and 1053 TwinsUK participants showed a genome-wide significant recessive protective effect of the C allele of rs11876749 (P?=?1.7?×?10?8). This variant is located close to TGIF1 (an inducer of transforming growth factor ?), which is a known gene associated with skin aging.

    Conclusions and Relevance This is the first observational study to date demonstrating that other risk factors (male sex, genetic variants, lighter skin color, high body mass index, and possibly current smoking) in addition to aging are involved in the origin of sagging eyelids.