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Tanning Beds, Sunlamps, and Risk of Cutaneous Malignant Melanoma

¹ Cancer Control Research Program, British Columbia Cancer Agency; ² Department of Health Care and Epidemiology and ³ Division of Dermatology, Faculty of Medicine, University of British Columbia, Vancouver, Canada; and ⁴ School of Computing Sciences, Simon Fraser University, Burnaby, Canada

Requests for reprints: Richard P. Gallagher, Cancer Control Research Program, British Columbia Cancer Agency, 600 West 10th Avenue, Vancouver, BC, Canada V5Z 4E6. Phone: 604-877-6000; Fax: 604-877-1868. E-mail: richardg{at}bccancer.bc.ca

	Abstract

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Background: A number of studies have been conducted evaluating the risk of cutaneous malignant melanoma after exposure to sunlamps and/or sunbeds. The proportion of subjects in the individual studies who have reported exposure has, in general, been modest, and the resulting risk estimates for melanoma have been unstable with wide 95% confidence intervals (95% CI). The inconclusive results seen in individual studies have resulted in confusion as to the carcinogenicity of these devices.

Methods: We conducted a systematic review and meta-analysis of these studies. A review of the literature from Jan 1, 1984 to April 2004 using MEDLINE identified 12 case-control studies and 1 cohort study which quantitatively evaluated the use of sunlamps and/or sunbeds and subsequent melanoma. After applying exclusion/inclusion criteria, 9 case-control and 1 cohort study provided data for the analysis. Summary odds ratios (OR) and 95% CIs for sunlamp/sunbed use and subsequent melanoma were calculated using a random-effect model.

Results: Ten studies provided data for assessment of melanoma risk among subjects who reported "ever" being exposed compared with those "never" exposed. A positive association was found between exposure and risk (summary OR, 1.25; 95% CI, 1.05-1.49). Significant heterogeneity between studies was present. Evaluation of the metrics "first exposure as a young adult" (5 studies) and "longest duration or highest frequency of exposure" (6 studies) also yielded significantly elevated risk estimates (summary OR, 1.69; 95% CI, 1.32-2.18, and 1.61; 95% CI, 1.21-2.12, respectively, with no heterogeneity in either analysis).

Conclusions: Results indicate a significantly increased risk of cutaneous melanoma subsequent to sunbed/sunlamp exposure.

	Introduction

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There is good experimental and epidemiologic evidence that UV radiation exposure (mainly from sunlight) is causally related to all forms of human skin cancer including cutaneous malignant melanoma (1). Melanoma incidence has most strongly and consistently been associated with reported "intermittent sun exposure" mostly accrued through recreational activities. A quantitative review of studies of sun exposure and melanoma found a positive association between intermittent exposure and risk of cutaneous malignant melanoma in 21 (statistically significant in 16) of 23 studies included in the analysis (2).

Because by its nature, exposure to artificial UV radiation through sunlamp and sunbed use is intermittent in character, there has been consistent concern over the past 15 years that use of such devices for recreational tanning may increase risk of melanoma (3). In addition, data from surveys conducted in Europe (4, 5) and North America (6) indicate that sunbeds are now being used by a significant proportion of the population, particularly young people.

A series of epidemiologic investigations have attempted to determine the nature of this putative association. However, analysis of sunlamp/sunbed use has been hampered by small numbers of exposed subjects in individual studies. In order to evaluate the strength and consistency of association between use of these devices and melanoma, we have conducted a systematic review and meta-analysis.

	Materials and Methods

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To identify relevant studies of sunbeds/sunlamps and melanoma, we conducted a MEDLINE database search for the years 1984 to 2004, using the terms "melanoma (etiology, epidemiology) and sunbeds, sunlamps, and solarium" as keywords. We also selected all review articles in English on UV radiation, tanning devices, solaria, and melanoma, and scrutinized these to locate articles with data on sunlamp and sunbed use missed by the MEDLINE search. We did not attempt to locate unpublished data. We chose 1984 as the year of start of our search as that year saw the first publications from large-scale epidemiologic studies of melanoma and UV exposure with good control for potential phenotype confounders. The search yielded a total of 11 case-control studies reporting risk estimates for melanoma subsequent to sunbed/sunlamp use (7-18). In addition, one cohort study was found which reported on usage among Norwegian and Swedish women (19).

Selection of Studies
All case-control studies of cutaneous malignant melanoma that reported on use of sunlamps, sunbeds, or both were initially considered for the analysis. For inclusion, we required that numbers (or percentages) of exposed cases and controls were presented in the study, and odds ratios (ORs) with 95% confidence intervals (95% CI) were available, evaluating at least "ever" versus "never" use of these devices. Because of these requirements, two earlier studies were omitted; one due to missing CIs (7) and the other due to missing data on numbers of exposed cases and controls (8). A study by MacKie et al. (10) was also omitted because it was not possible from the information presented to determine accurately the proportions or numbers of cases and controls exposed. All other studies were included in the analysis.

In order to attempt to make the analysis reflect, as far as possible, recreational rather than medical use of sunlamps/sunbeds, we did not include studies of psoralen and UVA radiation therapy [e.g., that of Stern et al. (20)]. Where studies provided separate estimates of risk for medical and nonmedical use, the estimates for nonmedical use were used. Where separate estimates were not given, the overall ORs and CIs were used. Whenever possible, ORs adjusted for phenotype factors (hair, skin, eye color, phototype, number of nevi, etc.) and sun exposure were used in preference to crude or unadjust ed values. The studies of Swerdlow et al. (13) and Osterlind et al. (9) present risk estimates as crude ORs unadjusted for phenotype factors. Swerdlow⁵ indicated the "ever versus never exposed" value was adjusted only for age, sex, and region of residence. In the case of the study by Walter et al. (14), risk estimates were calculated as crude and adjusted ORs, and because the two analyses gave "essentially the same effect" (p.236), the authors presented the unadjusted values. Thus, the Walter estimates can be expected to closely approximate adjusted values.

A number of the studies presented data which allowed us to evaluate whether initial exposure to sunbeds/sunlamps occurring earlier in life "as a young adult" conferred a different risk than if exposure began closer to the time of the study. A total of five studies contributed to this analysis and, with the exception of the study of Walter et al. (14), the estimates used were the adjusted values.

Finally, a number of studies attempted to determine whether a dose-response gradient with exposure was seen. We produced summary ORs comparing melanoma risk between subjects with the longest duration or highest frequency of exposure and subjects never exposed. Six studies provided data for this analysis.

Two of the authors (R.P.G. and T.K.L.) examined each of the studies independently to determine which risk estimate was the best indicator of "first exposure as a young adult" and which was the best for "longest duration or highest frequency of use," and after a discussion concerning one study, agreed on the measures considered to be most appropriate.

Summary ORs and 95% CIs were calculated for the three measures of sunlamp/sunbed exposure noted above using the method of DerSimonian and Laird (21). The Q statistics was used as a test for heterogeneity among the original study estimates (22). Published gender-specific ORs (14) or period-specific ORs (15) were treated as separate entries or "studies" in the meta-analysis. Sensitivity analyses were conducted by recalculating summary ORs after eliminating specific studies.

	Results

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A total of 10 published articles (with 12 ORs) were used in assessing the relationship between ever versus never use of sunlamp/sunbed and melanoma (Table 1). The summary OR showed a modest elevated risk (OR, 1.25; 95% CI, 1.05-1.49). Positive associations were see n in 8 of 10 individual studies, although only 4 risk estimates were statistically significant. One of the studies (9) showed an inverse association. There was significant heterogeneity (Q = 28.9; P = 0.0024) likely due to the studies being conducted over a long period of time with different designs. Also, one study (9) showed results markedly different from the others. Recalculation excluding the Osterlind study substantially reduced but did not eliminate the heterogeneity, and had only a slight effect on the summary OR. Excluding both the Osterlind study and the Swerdlow study (not adjusted for phenotype factors) again had essentially no effect (OR, 1.24; 95% CI, 1.09-1.41). The cohort study of Veierod et al. (19) used "never/rarely" as the index in assessing exposure. We included this measure in the analysis as combining these two groups as the index should give a conservative estimate of risk among users. Excluding the Veierod study made little difference to the summary OR (OR, 1.21; 95% CI, 1.02-1.44).

	Discussion

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Results of the analysis are, of course, dependent on the choice of measures selected from each study. The overall measure, ever versus never use, is fairly clear-cut, with the caveat that we selected the risk estimate and CIs noted "for tanning purposes" rather than total use wherever possible. Recalculation of summary ORs using values for total sunbed/sunlamp usage rather than use for tanning purposes indicated that our decision did not affect the conclusions reached. The measures used to assess first exposure as a young adult were subject to more judgment. The case-control studies defined a young adult in different ways, with first exposure ages ranging from "less than 25" to "less than 39 years." For the women's prospective cohort study (19), we defined first exposure as a young adult to be women who used sunbeds for the first time at ages 10 to 19. As this cohort was comprised of women who were recruited in 1991 to 1992 at ages 30 to 50, early exposure would have occurred before 1980.

The longest duration or highest frequency of use analysis combined what we considered to be the best measure of cumulative sunbed/sunlamp exposure available within each study. The intention of this analysis was to compare risk estimates in subjects with maximal cumulative usage to that in subjects "ever exposed" and those "never exposed." This would enable us to determine whether there was a suggestion of a gradient of risk from none to maximal use. Of course those subjects most heavily exposed will also be included in the ever exposed category, so the OR differences seen between the levels of exposure are not independent.

The published articles covered a time period of nearly 20 years. During this time the UV emissions of artificial tanning devices changed in character. Sunlamps used up to the late 1970s were usually used in the home setting (except for medical use) and emitted primarily UVB (sometimes with a small component of UVC). In the early 1980s, two major changes took place. Indoor tanning began to be done largely in commercial salons rather than at home, and salons began to use UVA lamps. Thus, the character of the exposure changed and because of this there is some question whether results from the early studies (9, 13, 14) can be legitimately combined with those of more recent studies. We suggest that combining the results of the studies is appropriate, as there is no convincing human data demonstrating that UVB is more or less strongly related to melanoma than UVA. In fact, there is some evidence that melanocytes exposed in vivo to either UVA or to UVB show similar levels of thymine dimer formation (23). In addition, studies have shown that UVA as well as UVB impairs antioxidant function and promotes reactive oxygen species, events known to be involved in cutaneous carcinogenesis (24-27). Finally, the risk estimates from later studies, taken together, do not differ in character from those seen in the earlier investigations.

Finally, whereas we have used risk estimates adjusted for phenotype factors and, when possible, for sun exposure, it is unlikely that the studies have achieved complete control for these potential confounders. If individuals who use artificial tanning devices are more likely to suntan, as many suspect, then some of the elevated risk seen might be due to recreational sun tanning.

Our results, however, suggest that any exposure to artificial tanning devices modestly, but significantly, increases risk of cutaneous melanoma; however, caution is needed as it is possible that there is unpublished (or unanalyzed) data on sunbed or sunlamp use in existence from previously conducted etiologic studies of melanoma. The subgroup analysis of risk among those exposed "early in adult life" suggests a risk estimate slightly higher than that seen in the ever versus never analysis. We take this to indicate that risk increases with adequate lag time (>10 years) after commencement of exposure. However, as noted above, this lag time is potentially confounded by the change in tanning device emissions from UVB to UVA in the early 1980s. The latter interpretation, however, seems unlikely as risk estimates for exposure during the period when UVA was emitted by sunbeds (17) are similar to those seen during earlier periods.

Summary ORs for those with the longest duration or highest frequency of use suggest a higher risk of melanoma among those most heavily exposed than among those ever exposed. Confidence intervals of the two estimates do overlap, however, it does give some indication that a dose-response effect might be found to be present if exposure data were more effectively captured.

If there is a causal relationship between sunlamp/sunbed exposure and melanoma, the public health question is asked: how important is the risk? It is not possible with the data available to answer this question with any certainty. However, a large number of epidemiologic studies have been conducted on the relationship between solar UV exposure and melanoma, and these have been summarized quantitatively by Nelemans et al. (28) and Elwood and Jopson (2). Combining the highest reported levels of "intermittent" exposure produced a summary OR for all studies of 1.71 (95% CI, 1.54-1.90) in the Elwood study, and 1.57 (95% CI, 1.29-1.91) for population-based studies in the Nelemans investigation. These values are similar to that seen for longest duration or highest frequency of use of sunlamps/sunbeds in the present study. Although caution is required due to the possibility of confounding by inadequate control for concurrent sun exposure, the results suggest that artificial UV may be a significant contributor to risk among those with substantial exposure.

In summary, whereas it is not possible to determine accurately how much sunbed/sunlamp use contributes to individual risk of cutaneous malignant melanoma, it seems clear that any use of these devices elevates risk for cutaneous malignant melanoma. Furthermore, risk further increases with appropriate lag time, and frequency and duration of use seem likely to be positively related to the magnitude of the risk.

	Footnotes

 
Grant support: Michael Smith Foundation for Health Research Infrastructure award.

The costs of publication of this article were defrayed in part by the payment of page charges. This article must therefore be hereby marked advertisement in accordance with 18 U.S.C. Section 1734 solely to indicate this fact.

⁵ Personal communication (April 30, 2004).

Received 7/28/04; revised 10/14/04; accepted 10/27/04.

	References

Top Abstract Introduction Materials and Methods Results Discussion References

 

1. International Agency for Research on Cancer. IARC monographs on the evaluation of carcinogenic risk to humans. Vol 55. Solar and ultraviolet radiation. Lyon: IARC Press; 1992.
2. Elwood JM, Jopson J. Melanoma and sun exposure; an overview of published studies. Int J Cancer 1997;73:198–203.[CrossRef][Medline]
3. Young AR, Tanning devices-fast track to skin cancer? Pigment Cell Res 2004;17:2–9.[CrossRef][Medline]
4. Amir Z, Wright A, Kernohan E, Hart G. Attitudes, beliefs and behavior regarding the use of sunbeds among healthcare workers in Bradford. Eur J Cancer Care 2000;9:76–9.
5. Jerkegren E, Sandreiser L, Brandberg Y, Rosdahl I. Sun-related behavior and melanoma awareness among Swedish university students. Eur J Cancer Prev 1999;8:27–34.[CrossRef][Medline]
6. Geller AC, Colditz G, Oliveria S, et al.. Use of sunscreen, sunburning rates, and tanning bed use among more than 10000 US children and adolescents. Pediatrics 2002;109:1009–14.[Abstract/Free Full Text]
7. Gallagher RP, Elwood JM, Hill GB. Risk factors for cutaneous malignant melanoma: the western Canada melanoma study. Recent Results Cancer Res 1986;102:38–55.[Medline]
8. Holman CDJ, Armstrong BK, Heenan PJ, et al. The causes of malignant melanoma: results from the West Australian Lions melanoma research project. Recent Results Cancer Res 1986;102:18–37.[Medline]
9. Osterlind A, Tucker MA, Stone BJ, Jensen OM. The Danish case-control study of cutaneous malignant melanoma: II. Importance of UV light exposure. Int J Cancer 1988;42:319–24.[Medline]
10. MacKie RM, Freudenberger T, Aitchison TC. Personal risk-factor chart for cutaneous melanoma. Lancet 1989;2:487–90[CrossRef][Medline]
11. Garbe C, Weiss J, Kruger S, et al. The German Melanoma Registry and environmental risk factors implied. Recent Results Cancer Res 1993;128:69–89.[Medline]
12. Holly EA, Aston DA, Cress R, Ahn DK, Kristiansen JJ. Cutaneous melanoma in women I. Exposure to sunlight, ability to tan, and other risk factors related to ultraviolet light. Am J Epidemiol 1995;141:923–33.[Abstract/Free Full Text]
13. Swerdlow AJ, English JS, MacKie RM, et al. Fluorescent lights, ultraviolet lamps, and risk of cutaneous melanoma. BMJ 1988;297:647–50.
14. Walter SD, Marrett LD, From L, Hertzman C, Shannon HS, Roy P. The association of cutaeous malignant melanoma with use of sunbeds and sunlamps. Am J Epidemiol 1990;131:232–43.[Abstract/Free Full Text]
15. Autier P, Dore J-F, Lejeune F, et al. Cutaneous malignant melanoma and exposure to sunlamps and sunbeds: an EORTC multicentre case-control study in Belgium, France and Germany. Int J Cancer 1994;58:809–13.[Medline]
16. Westerdahl J, Olsson H, Masback A, et al. Use of sunbeds or sunlamps and malignant melanoma in Southern Sweden. Am J Epidemiol 1994;140:691–9.[Abstract/Free Full Text]
17. Westerdahl J, Ingvar C, Masback A, Jonsson N, Olsson H. Risk of cutaneous malignant melanoma in relation to use of sunbeds: further evidence for UV-A carcinogenicity. Br J Cancer 2000;82:1593–9.[CrossRef][Medline]
18. Chen Y-T, Dubrow R, Zheng T, Barnhill RL, Fine J, Berwick M. Sunlamp use and risk of cutaneous malignant melanoma: a population-based, case-control study in Connecticut USA. Int J Epidemiol 1998;27:758–65.[Abstract/Free Full Text]
19. Veierod MB, Weiderpass E, Thorn M, et al. A prospective study of pigmentation, sun exposure, and risk of cutaneous malignant melanoma in women. J Natl Cancer Inst 2003;95:1530–8.[Abstract/Free Full Text]
20. Stern RS, Nichols KT, Vakeva LH; for the PUVA Follow-up Study. Malignant melanoma in patients treated for psoriasis with methoxsalen (psoralen) and ultraviolet A radiation (PUVA). N Engl J Med 1997;336:1041–5.[Abstract/Free Full Text]
21. DerSimonian R, Laird N. Meta-analysis in clinical trials. Control Clin Trials 1986;7:177–88.[CrossRef][Medline]
22. Petitti DB. Meta-analysis, decision analysis, and cost effectiveness analysis: methods for quantitative medicine. New York: Oxford University Press; 1994.
23. Young AR, Potten CS, Nikaido O, et al. Human melanocytes and keratinocytes exposed to UVB or UVA in vivo show comparable levels of thymine dimers. J Invest Dermatol 1998;111:936–40.[CrossRef][Medline]
24. Fuchs J, Huflejt, Rothfuss LM, Wilson DS, Carcamo G, Packer L. Acute effects of near ultraviolet and visible light on the cutaneous antioxidant system. Photochem Photobiol 1989;50:739–44[Medline]
25. Fuchs J, Huflejt ME, Rothfuss LM, Wilson DS, Carcamo G, Packer L. Impairment of enzymatic and nonenzymatic antioxidants in skin by UVB irradiation. J Invest Dermatol 1989;93:769–73.[CrossRef][Medline]
26. Sander CS, Hamm F, Elsner P, Thiele JJ. Oxidative stress in malignant melanoma and non-melanoma skin cancer. Br J Dermatol 2003;148:913–22.[CrossRef][Medline]
27. Sander CS, Chang H, Hamm F, Elsner P, Thiele JJ. Role of oxidative stress and the antioxidant network in cutaneous carcinogenesis. Int J Dermatol 2004;43:326–35[CrossRef][Medline]
28. Nelemans PJ, Rampen FHJ, Ruiter DJ, Verbeek ALM. An addition to the controversy on sunlight exposure and melanoma risk. J Clin Epidemiol 1995;48:1331–42.[CrossRef][Medline]

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