| Literature DB >> 28070504 |
D H González Maglio1, M L Paz1, J Leoni1.
Abstract
Sunlight, composed of different types of radiation, including ultraviolet wavelengths, is an essential source of light and warmth for life on earth but has strong negative effects on human health, such as promoting the malignant transformation of skin cells and suppressing the ability of the human immune system to efficiently detect and attack malignant cells. UV-induced immunosuppression has been extensively studied since it was first described by Dr. Kripke and Dr. Fisher in the late 1970s. However, skin exposure to sunlight has not only this and other unfavorable effects, for example, mutagenesis and carcinogenesis, but also a positive one: the induction of Vitamin D synthesis, which performs several roles within the immune system in addition to favoring bone homeostasis. The impact of low levels of UV exposure on the immune system has not been fully reported yet, but it bears interesting differences with the suppressive effect of high levels of UV radiation, as shown by some recent studies. The aim of this article is to put some ideas in perspective and pose some questions within the field of photoimmunology based on established and new information, which may lead to new experimental approaches and, eventually, to a better understanding of the effects of sunlight on the human immune system.Entities:
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Year: 2016 PMID: 28070504 PMCID: PMC5187459 DOI: 10.1155/2016/1934518
Source DB: PubMed Journal: Biomed Res Int Impact factor: 3.411
Summary of irradiation protocols producing UV-induced immunosuppression. The experimental design of all the papers cited in the table included the irradiation before the sensitization stage of the immune responses. CHS: contact hypersensitivity; DTH: delayed type hypersensitivity; Oxa: oxazolone; DNFB: 2,4-dinitrofluorobenzene; Ova: ovalbumin.
| Authors | UV source | UV dose employed | MED represented | Mice strain | Type of reaction (antigen) |
|---|---|---|---|---|---|
| Reeve et al. [ | UVA/UVB | 3 × 4500 mJ/cm2 (UVA); 3 × 252 mJ/cm2 (UVB) | 1 MED | C57BL/6 | CHS (Oxa) |
| Majewski et al. [ | UVR | 4 × 150 mJ/cm2 | Not expressed | C57BL/6 | CHS (DNFB) |
| Wang et al. [ | UVB | 3 × 45 mJ/cm2 | Not expressed | C57BL/6 | CHS (DNFB) |
| Schwarz et al. [ | UVB | 4 × 150 mJ/cm2 | Not expressed | C57BL/6 | CHS (DNFB) |
| Gorman et al. [ | 65% UVB | 400 and 800 mJ/cm2 | >1 MED | Balb/c and C57BL/6 | CHS (DNFB) |
| Zhang et al. [ | 45% UVB | 750 mJ/cm2 | Not expressed | C57BL/6 | CHS (DNFB) |
| Guéniche et al. [ | UVB + UVA | Not expressed | 2.5 MED | SKH:HR1 | CHS (DNFB) |
| Shreedhar et al. [ | 65% UVB | 1500 mJ/cm2 | Not expressed | C3H/HeN | DTH (alloantigen) |
| Li et al. [ | UVB | 200 mJ/cm2 | Not expressed | C57BL/6 | CHS (DNFB) |
| Rana et al. [ | UVB | 3 × 150 mJ/cm2 | 0.5 MED | C57BL/6 | DTH (Ova) |
| Dixon et al. [ | UVB and UVA | 3 × 400 mJ/cm2 (UVB) | 3 MED | SKH:HR1 | CHS (Oxa) |
Figure 1Sunlight effects on the skin and the immune system. The effects triggered by different wavebands of radiation are summarized, focusing on those effects described in the text. UCA: urocanic acid; ROS: reactive oxygen species; MMPs: matrix metalloproteases; MED: minimal erythema dose; DCs: dendritic cells; LNs: lymph nodes.