Exploring the effects of sun exposure using explant skin.

Enjoyment of sunshine is a quintessential aspect of the human experience. Exposure provides a myriad of health benefits, from fostering essential vitamin synthesis to enhancing overall mental well-being. However, and especially with record daily temperatures recently occurring, it is equally vital to recognise the potential risks associated with extended sun exposure, particularly the adverse effects on the skin. Here, we examine how the use of explant skin models, specifically our patented TenSkin™ platform, may be used to evaluate not only the efficacy of sunscreens, but also to explore the underlying biological processes that arise as a result of exposure to the sun. The aim is to use such models to assess the best strategies for preserving skin integrity by understanding the mechanisms by which sun exposure affects us from the molecular level up and how most effectively to prevent the negative effects.

Energy from the sun has effectively nurtured life on Earth, and as such the biological evolution of species has emerged in a symbiotic relationship with natural sunlight. The interesting article by Mead [1] offers a fabulous and detailed overview of the effects of sunlight on humans, the extent and significance of which cannot be overstated. When the skin is exposed to sunlight, it initiates a chain of events culminating in the synthesis of vitamin D: an invaluable nutrient that is instrumental in maintaining strong bones, bolstering the immune system, and enhancing overall well-being. Furthermore, the sun’s radiance is known to stimulate the release of serotonin, a neurotransmitter linked to mood regulation. However, these benefits are counterbalanced by the potential risks associated with excessive exposure to the sun.

Prolonged and unprotected exposure to ultraviolet (UV) radiation can result in DNA damage, leading to a myriad of skin issues, including sunburn, premature aging, and an escalated susceptibility to skin cancer. It is evident that prudent sun exposure practices are essential for reaping its rewards while minimising its detrimental effects.

Among the notable consequences of sun exposure is its role in the aging process. Photoaging, a distinctive form of skin aging induced by chronic UV radiation exposure, leads to the degradation of collagen and elastin fibers, pivotal components responsible for skin elasticity and firmness. The outcome is a visible manifestation of fine lines, wrinkles, changes in pigmentation, and sagging skin. Notably, many of these aging effects are intrinsically linked to DNA damage. UV radiation induces mutations in the DNA of skin cells, disrupting their normal function and contributing to the breakdown of vital structural proteins. By examining the correlation between photoaging and DNA damage, we gain a deeper understanding of the importance of effective sun protection strategies.

Sunscreens stand as a formidable defense against the harmful impacts of UV radiation on the skin. Categorised into two main types, reflective and absorbing, sunscreens function as barriers to protect the skin from the full brunt of UV radiation. Reflective sunscreens harness the properties of minerals like zinc oxide and titanium dioxide to physically deflect and scatter UV rays. Absorbing sunscreens, on the other hand, employ organic compounds to absorb UV radiation, which is then converted to heat energy, which can lead to additional compounding effects [2,3].

The efficacy of these sunscreens in preventing DNA damage can be meticulously scrutinised using explant skin models.

Several pivotal studies have harnessed explant skin models to unravel the intricate relationship between sunscreens and DNA damage:

Full thickness ex vivo skin explant studies are clearly evidencing a previously unveiled level of understanding in skin physiology when compared to other models including animal skin, reconstituted human skin or other cultures [4]. However, the majority primarily utilise skin from middle-aged Caucasian female (Fitzpatrick type I-II) donors. This limits the generalisation of the findings to the wider population. Greater donor variation becomes increasingly important when it is appreciated that significant differences exist in the extracellular matrix when comparing explants from younger and older donors or between males and females [4,5], as well as the response to the sun in Fitzpatrick skin types III-VI. It has been estimated that skin with a naturally darker pigment can remain in the sun 4-6x longer before reaching an excessive dose of UV rays [6].

The duality of sun exposure, offering both essential benefits and potential risks, underscores the necessity of strategic sun protection. Explant skin models, through their intricate replication of human skin, have emerged as indispensable tools for dissecting the intricate interplay between sunscreens and DNA damage. Reflective sunscreens, enriched with zinc oxide and titanium dioxide, demonstrate considerable promise in thwarting DNA damage. Moreover, the unwavering commitment to consistent sunscreen application, coupled with innovative formulations like nanoparticle-based sunscreens, amplifies the protective shield against the ravages of UV radiation.

In conclusion, prudent scheduling of outdoor activities and the planned use of protective clothing and sunscreen when needed ensures that our time in the sunshine is very much about ‘laughter all the while’ and ‘more happiness’ while ensuring that we minimise the worries about the consequences that may unfold in our tomorrows. ‘Make me happy through the years, never bring me any tears’! Just like Morecambe and Wise said we should!

With apologies to younger readers who may not be familiar with the iconic comedy duo of Brtish TV in the late 1960s, 1970s and early 80s. Ask your parents!

And the lyrics are……

“Bring me laughter all the while
In this world where we live there should be more happiness
So much joy you can give to each brand new bright tomorrow
Make me happy through the years never bring me any tears”

Dr Paul Campbell October 2023

References

1.      Mead, M.N. (2008) ‘Benefits of sunlight: A bright spot for human health’, Environmental Health Perspectives, 116(4). doi:10.1289/ehp.116-a160.

2.      Calapre, L. et al. (2016) ‘Heat-mediated reduction of apoptosis in UVB-damaged keratinocytes in vitro and in human skin ex vivo’, BMC Dermatology, 16(1). doi:10.1186/s12895-016-0043-4.

3.      Calapre, L. et al. (2017) ‘SIRT1 activation mediates heat-induced survival of UVB damaged keratinocytes’, BMC Dermatology, 17(1). doi:10.1186/s12895-017-0060-y.

4.      Neil, J.E., Brown, M.B. and Williams, A.C. (2020) ‘Human skin explant model for the investigation of topical therapeutics’, Scientific Reports, 10(1). doi:10.1038/s41598-020-78292-4.

5.      Solé-Boldo, L. et al. (2020) ‘Single-cell transcriptomes of the human skin reveal age-related loss of fibroblast priming’, Communications Biology, 3(1). doi:10.1038/s42003-020-0922-4.

6.      Abadie, S., Bedos, P. and Rouquette, J. (2019) ‘A human skin model to evaluate the protective effect of compounds against UVA damage’, International Journal of Cosmetic Science, 41(6), pp. 594–603. doi:10.1111/ics.12579.