Abstract
Background
Numerous epidemiologic studies and a few systematic reviews have investigated the association between occupational solar exposure and basal cell carcinoma (BCC). However, previous reviews have several deficits with regard to included and excluded studies/risk estimates and the assessment of risk of selection bias (RoSB). Our aim was to review epidemiologic studies with a focus on these deficits and to use meta-(regression) analyses to summarize risk estimates.
Methods
We systematically searched PubMed (including MEDLINE) and Embase for epidemiologic studies. Study evaluation considered four main aspects of risk of bias assessments, i.e. Selection of subjects (selection bias); Exposure variables; Outcome variables; Data analysis.
Results
Of 56 identified references, 32 were used for meta-(regression) analyses. The overall pooled risk estimate for BCC comparing high/present vs. low/absent occupational solar exposure was 1.20 (95% CI 1.02–1.43); among studies without major deficits regarding data analysis, it was 1.10 (95% CI 0.91–1.33). Studies with low and high RoSB had pooled risk estimates of 0.83 (95% CI 0.73–0.93) and 1.95 (95% CI 1.42–2.67), respectively. The definitions of exposure and outcome variables were not correlated with study risk estimates. Studies with low RoSB in populations with the same latitude or lower than Germany had a pooled risk estimate of 1.01 (95% CI 0.88–1.15).
Conclusion
Due to the different associations between occupational solar exposure and BCC among studies with low and high RoSB, we reason that the current epidemiologic evidence base does not permit the conclusion that regular outdoor workers have an increased risk of BCC.
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Introduction
Natural ultraviolet (UV) light is an important risk factor for skin cancer. However, the exposure patterns that are associated with increased risks of the different skin cancer types seem to be different. Malignant melanoma is associated with intermittent exposure during recreation, particularly in childhood and adolescence. Similarly, basal cell carcinoma (BCC) seems to be foremost associated with intermittent exposure, whereas squamous cell carcinoma (SCC) is associated with total or occupational exposure [1].
Numerous epidemiologic studies have been conducted on the question whether occupational solar exposure increases BCC risk, and three systematic reviews are available [2,3,4]. However, only one review investigated risk estimates in dependence on risk of bias (RoB) of the underlying studies [4], focusing on BCC and SCC together. In any case, all three reviews missed important issues in their performed RoB assessments with respect to selection bias.
In occupational epidemiology, potential risk factors are usually related to blue-collar or manual workers. However, such workers that in general have a comparably low socio-economic status (SES) take part in epidemiologic studies comparably infrequent [5, 6]. In case-control studies, this concerns foremost the control group [6]. In the event of low participation rates, a biased risk estimate of the exposure-disease association can result [7]. Furthermore, selection bias can also result when the source of control participants does not represent the general population. Some studies on occupational solar exposure and BCC recruited controls from patients with non-malignant dermatologic conditions or attending skin cancer screening. However, subjects with low SES, blue-collar or outdoor jobs report non-malignant dermatologic conditions or the consultation of dermatologists and the utilization of skin cancer screening comparably infrequent [8,9,10,11].
A second concern applies to the type of exposure variables. All previous systematic reviews used some risk estimates from original studies that do not refer to usual outdoor work but to a rather intermittent type of exposure in subjects that help their relatives in farming during summer. Furthermore, they partly used risk estimates for very specific agricultural job subgroups with increased risks, while not considering the picture for agricultural jobs overall [2, 3].
Thirdly, all previous reviews missed relevant literature. For example, one review restricted studies to those that were conducted in only one country [3], while another review excluded some studies that compared specific single outdoor jobs with all other jobs/the general population [4]. For the third review, it seems that the search string used for PubMed (including MEDLINE) was rather insensitive, with only 189 hits received [2].
Our aim was to review epidemiologic studies on regular occupational solar exposure and BCC and to use meta-(regression) analyses to summarize study risk estimates. We ran a new literature search to ensure identification of relevant studies. We summarized study risk estimates depending on various aspects regarding RoB, considering selection of subjects (selection bias), exposure variables, outcome variables, and data analysis.
Materials and methods
Scope of the review
This review was not pre-registered. It has evolved as part of our routine work that encompassed reviewing the evidence on occupational solar exposure and BCC risk. We started by reviewing systematic reviews but noted that these had important deficits (see Introduction). Our focus was to elaborate on these deficits and to review epidemiologic studies considering these deficits.
Literature search
We searched PubMed (including MEDLINE) in October 2021 and Embase in November 2021, adapting the search string proposed by [2] in order to increase sensitivity (Online Resource 1). In accordance with [2], studies in which the exposure was defined as work in any or a specific outdoor job or related sun/UV exposure were eligible. References were screened according to the PECOS scheme (Online Resource 2). We also inspected systematic reviews [2,3,4] and reference lists of original studies. Studies with full texts other than English or German were translated with DeepL (https://www.deepl.com/translator) or Google Translator (https://translate.google.com).
Evaluation of studies
The evaluation of studies centred on four main aspects that are usually addressed in RoB assessments (e.g. [12]), i.e. (1) Selection of subjects (selection bias); (2) Exposure variables; (3) Outcome variables; (4) Data analysis.
Selection of subjects (selection bias)
As pointed out in the Introduction, the frequent, comparably low attendance of subjects with low SES or manual/blue-collar jobs in control groups is associated with selection bias in occupational case-control studies. In cohort studies, selection bias during follow up can occur when continued participation is a common effect of exposure and outcome [7, 13]. Moreover, selection bias can result if exposure information is missing selectively or if study groups do not stem from the same base population. In case-control studies, the latter can particularly be assumed if sources of controls do not represent the general population.
Based on available RoB assessment instruments (e.g. [12]) and the information given above, we developed a simple scheme and allocated a high RoSB when.
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in case-control studies, participation rates were unknown or < 50%Footnote 1 in cases and/or controls
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in cohort studies, loss to follow-up was ≥ 50%.
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the availability of exposure information was < 50% among designated study participants.
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study groups did not represent the same base population; for case-control studies this was assumed for mainly dermatologic controls or other sources of controls that do presumably not represent the general population.
Exposure variables
WHO/ILO working group [4] excluded studies that compared specific single outdoor jobs with all other jobs/the general population. Their argument was that, in such studies, exposure reference groups also contain outdoor workers and, thus, risk estimates are underestimated. In contrast, we did not exclude such studies and aimed to evaluate whether their risk estimates differ from the estimates of other studies. We further assessed whether studies defined quantitative exposure variables, including cumulative or mean estimates of exposure, or not. Finally, these two aspects were combined, differentiating between studies with quantitative exposure variables that do not compare single outdoor jobs with all other jobs/the general population and all other studies.
Outcome variables
For all included studies, histological verification of the outcome can be assumed (based on pathology, medical or cancer registry records). We evaluated whether risk estimates differed between studies that involved only cases with first ever BCC and studies that potentially included cases with subsequent BCC. In the event of subsequent BCC diagnoses, risk estimates are potentially biased as the exposure period extends until after the first diagnosis. Moreover, cases possibly change their behaviour after an initial diagnosis.
Data analysis
As a minimum requirement, risk estimates should be controlled for age, sex, and study centre (if applicable) in a statistical (regression) model of the exposure-disease association. We also looked for other model-misspecifications, e.g. the inclusion of potentially highly correlated variables in the same regression model.
Meta-(regression) analyses
Random-effects meta-(regression) analyses were carried out with Stata 17 [14]. Certain details are described in Online Resource 3 (e.g. reasons for excluded studies; detailed approach of selection of risk estimates). Very briefly, risk estimates for occupational solar exposure due to overall outdoor work were preferred. Otherwise, in accordance with [2], risk estimates for specific single occupations were used. However, we used only risk estimates for agricultural jobs as these were evaluated in all studies on specific occupations that were eligible for our meta-analysis and as these entail many outdoor workers. This approach ensures a certain homogeneity with regard to the index exposure among the studies on specific occupations/jobs.
Course of analyses
After a first meta-analysis (level 1), studies with deficits regarding data analysis (see Material and Methods) were excluded to remove possible data analysis-related bias ahead of further analyses. At level 2, several sub-analyses were conducted to investigate risk estimates with regard to: Selection of subjects (selection bias); Exposure variables; Outcome variables (see Material and Methods); Study type; Sex; Mean geographical latitude of studies (in analogy to [2]).
Results
Literature search
The literature search yielded 4039 hits, including 281 duplicates (Online Resource 4). Of 56 retained full texts, 32 were used for meta-(regression) analyses. The 24 excluded references are described in Online Resource 5, section A, together with one reference used in [2] that did not meet our selection criteria [15].
Evaluation of the literature
Table 1 visualizes the evaluation results of the studies that were included in the meta-(regression) analyses. Online Resource 6 explains the results in detail. A comprehensive overview of the studies is presented in Online Resource 7 (case-control studies) and Online Resource 8 (other study types).
Meta-(regression) analyses
The first meta-analysis yielded a pooled risk estimate of 1.20 (95% CI 1.02–1.43) (level 1) (Fig. 1). At level 2, the pooled risk estimate without studies with deficits regarding data analysis was 1.10 (95% CI 0.91–1.33). For studies with low and high RoSB, the pooled risk estimates were 0.83 (95% CI 0.73–0.93) and 1.95 (95% CI 1.42–2.67), respectively (Fig. 2). Among the 16 case-control studies only, almost identical results occurred (data not shown). A stratified analysis with these studies shows that with respect to the issues used to evaluate RoSB, similar patterns emerged as for RoSB overall (Online Resource 9). The pooled risk estimate among the five cohort studies (all with low RoSB) was 0.84 (95% CI 0.75–0.95). The definitions of exposure variables and the outcome were not correlated with risk estimates (Online Resource 10). This also held true among studies with low RoSB. In this subgroup, only latitude was related to the size of risk estimates (Table 2). Studies with populations north of Germany (> 50th latitude) showed a lower pooled risk estimate (0.73; 95% CI 0.63–0.84) than studies in populations ≤ 50th latitude (1.01; 95% CI 0.88–1.15).
Discussion
Selection of subjects (selection bias)
Our analyses indicate that studies with high RoSB overestimate underlying risk. Most of them are case-control studies with unknown or low participation rates, particularly among controls. Unfortunately, study reports do usually not contain information on the representativeness of the control group. Unless this is implemented, low or unknown participation rates should be treated with caution. The same is true for presumably unrepresentative sources of controls such as patients with minor dermatologic conditions. Most of the studies with high RoSB had more than one limitation that led to this characterization. Of course, if both a low participation and an ill-defined control group are present at the same time, it can hardly be evaluated whether one or the other or both lead to biased risk estimates.
Diagnostic/detection bias
BCC is a condition with a certain diagnostic bias. Data from a nationwide dermatopathology laboratory in Germany show the highest mean tumor depths in members of agricultural health and local public health insurances [49]. The latter involve more people that work in physically strenuous jobs and less people that work in offices compared to the general population [50]. These findings are in accordance with observations that a lower SES or outdoor work are inversely associated with the usage of skin cancer screening [10, 11] and initial dermatologist visits [9, 10]. Such a diagnostic bias putatively is also present in the reviewed epidemiologic studies. However, as it concerns almost all studies, its impact cannot be evaluated. Yet, an underestimation of risk might be limited. As BCC is a tumor that continuously infiltrates adjacent tissue, the diagnostic bias probably concerns mainly the time point a person seeks medical help but not if someone seeks medical help or not. The tendency for delayed diagnoses in outdoor workers might even lead to an overestimation of outdoor exposure and risk. Studies including medical examination and histological verification to record all BCC cases in populations, accounting for previously diagnosed BCC and tumor depth, would help to evaluate BCC risk without this bias. Among the studies in our review, one used medical surveys to identify BCC cases. It did not show a clearly increased risk in relation to outdoor work as compared to indoor work (RR = 1.25; 95% CI 0.88–1.78) [22]. We are not aware of further published studies on occupational solar exposure and BCC that actively used medical examinations to identify cases, including surveys. In case-control studies, the medical examination to identify unknown BCC cases in the control group and the knowledge of their occupational solar exposure would also help to quantify diagnostic bias.
Exposure variables
Due to a possible underestimation of the exposure-disease association, WHO/ILO working group [4] excluded studies that compared specific single outdoor jobs with all other jobs/the general population. However, this does not seem justified. First, it impedes the evaluation of the impact of such studies on pooled risk estimates. Our analyses did not identify an impact. Secondly, exposure reference groups are seldom free of any exposure. For example, when quantitative exposure variables are categorized, the reference levels often include certain fractions of outdoor work as well.
With regard to studies on single outdoor occupations, we focused on agricultural jobs. This might have introduced some bias. However, in addition to our primary analyses on exposure variables, a secondary stratified analysis of studies on agricultural jobs and of studies on outdoor jobs in general did not show systematic differences of risk estimates either (data not shown).
Types of UV exposure and BCC
Our meta-analysis of studies with low RoSB yielded a summary risk estimate of 0.83 (95% CI 0.73–0.93). We would by no means interpret this inverse association as causal in the sense that the largest outdoor work exposure leads to the lowest risk of BCC. For example, personal protection measures and protective work conditions might have affected the result. However, regular outdoor workers also establish a continuous natural UV protection throughout the year at sun-exposed parts of the body and are, thus, putatively less sensitive to periods of intensive UV exposure than indoor workers. In fact, epidemiologic studies generally show that intermittent UV exposure is important for BCC occurrence [1]. Furthermore, it was shown that BCC incidence is highest in subjects with high SES [19, 25, 51,52,53] who work comparatively seldom in outdoor jobs.
Our review focused on regular outdoor occupations. We excluded studies that evaluated BCC risk of subjects with more intermittent and intense outdoor UV exposure. For instance, Vlajinac et al. [54] reported an increased risk of BCC in subjects that help their relatives in agriculture in summer, while regular farmers had no increased risk based on their Table 1. Additional studies should evaluate BCC risk in association with occupational exposure scenarios that encompass intermittent and intense outdoor UV exposure, such as in seasonal workers.
Data analysis
We did not evaluate risk estimates in dependence on adjustment for potential confounders such as SES, skin type or recreational UV exposure. In fact, whether such variables are confounders is study-specific and cannot be assumed in general. Unfortunately, study reports generally lack information to judge this. Future studies should take the aspect of confounding more into account. However, for studies with high RoSB, adjustment for SES is advisable to reduce selection bias. One of the studies with high RoSB adjusted for education, but probably only in dichotomous form [30]. A separate sensitivity analysis [48] of another study with high RoSB [23] yielded a 20% lower risk estimate with versus without adjustment for education.
Latitude of the study population
Our analyses showed a lower pooled risk estimate for studies with latitudes > 50° than for studies with latitudes ≤ 50°. This could have several reasons. In this review, studies in populations more in the north than Germany were exclusively based on exhaustive registries. This prevents potential bias that can occur in studies that actively recruit and interrogate participants. A second possible reason could be the weaker solar radiation more in the north as compared to other regions. However, the weaker radiation is accompanied by a generally lighter and more sensitive skin of the common, long-time resident population and, thus, might not be the main explanation.
Results of previous reviews as compared to our review
Previous meta-analyses resulted in pooled risk estimates of 1.43 (95% CI 1.23–1.66) [2] and 1.50 (95% CI 1.10–2.04) [4]. In comparison, our pooled estimate based on all studies was only 1.20 (95% CI 1.02–1.43). The main reasons for this difference were already mentioned in the Introduction.
Of the previous systematic reviews, only the review by WHO/ILO working group [4] evaluated study risk estimates in dependence on RoB. The analysis for non-melanoma skin cancer (NMSC, i.e. BCC and/or SCC) showed a lower pooled risk estimate for studies with only low RoB (1.11; 95% CI 0.86–1.43) as compared to studies with a high RoB in at least one of nine domains (1.98; 95% CI 1.44–2.72) (Fig. A7.8, page 180); most of the studies with low RoB also had a low RoSB according to our criteria. A stratification of the studies from WHO/ILO working group’s meta-analysis on BCC (Fig. A6.4, page 170) would result in a pooled risk estimate of 0.98 (95% CI 0.76–1.26) for studies with low RoB (acc. to Fig. 5, page 56) and, in addition, low RoSB according to our criteria [37, 42, 43, 45] (Online Resource 11). The studies with high RoB in any of the nine domains (acc. to Fig. 5, page 56) would yield a pooled risk estimate of 1.67 (95% CI 1.12–2.49). Despite the divergent results of their stratified analysis on NMSC risk, WHO/ILO working group [4] concluded a moderate quality of evidence for a positive association between occupational solar exposure and NMSC. In our view, this conclusion is not justified.
Further aspects
We did not formally investigate BCC risk related to occupational solar exposure separately for BCC at different anatomic locations, for different histologic BCC subtypes or for subjects with different skin sensitivity (skin type or tanning ability). Only few studies provided information on these questions, specifically few studies with adjustment for age and sex and with low RoSB [20, 28, 34, 36, 43, 45]. One study showed increased risks of BCC at the head/neck and of nodular BCC, especially in relation to shorter occupational solar exposure, but not of BCC at the trunk and of superficial BCC [20]. On the contrary, another study showed a positive association between occupational solar exposure and BCC at the trunk but not BCC at other locations [45]. Future studies should investigate these issues further.
Protection measures and work conditions might affect BCC risk in outdoor workers, e.g. clothes, headgear, sunscreen, sunglasses, working in shade/shading of workplaces, work breaks when UV index is highest, etc. We did not evaluate the influence of such measures on risk estimates. Indeed, this was usually not focused in the included original studies. In some studies, the exposure variables were weighted or the analyses were adjusted for some protection measures, usually clothes worn. Yet, no study stratified the analysis by protection measures/work conditions or conducted analyses using variables such as “work in intense sun” or “work in sun without protection”. Thus, present study results must be interpreted against the background of habitual work conditions and protection measures in the study populations.
Conclusion
We reason that the current epidemiologic evidence base does not permit the conclusion that regular outdoor workers have an increased risk of BCC. Studies with low risk of bias, particularly with low risk of selection bias, do not show a positive association between occupational solar exposure and BCC. Many of the available studies on natural UV radiation and BCC rather suggest that intensive UV exposure periods during spare time and sunburns (frequently defined as “intermittent” exposure) increase risk. Future studies should investigate if the frequent observation of a higher BCC risk in subjects with a comparably high SES can be explained by intermittent intense UV radiation exposure periods that lead to erythema and sunburns. Additionally, the influence of diagnostic/detection bias on risk estimates should be quantified.
Notes
There is no consensus on definitive critical proportions. Furthermore, a certain proportion of missing observations does not indicate selection bias, just as a certain proportion of available observations does not indicate the absence of selection bias. The differentiation of studies will be used in meta-(regression) analysis in order to assess whether systematic selection bias might be present or not.
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Acknowledgements
We sincerely thank Rebecca Wolf and Joanna Smolinska for their critical support with literature search and screening.
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Both authors (Andrea Wendt and Matthias Möhner) contributed to the conception and design of the review. Both authors extracted the information from the reviewed studies, evaluated the studies, performed the meta-(regression) analyses and interpreted the results. Andrea Wendt wrote the first draft of the manuscript and both authors commented on previous versions of the manuscript. Both authors read and approved the final manuscript. The authors take full responsibility for the methods, analyses, interpretations and conclusions in the present review. The presented ideas and opinions are exclusively those of the authors and do not necessarily reflect those of the authors’ affiliation.
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Wendt, A., Möhner, M. Occupational solar exposure and basal cell carcinoma. A review of the epidemiologic literature with meta-analysis focusing on particular methodological aspects. Eur J Epidemiol 39, 13–25 (2024). https://doi.org/10.1007/s10654-023-01061-w
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DOI: https://doi.org/10.1007/s10654-023-01061-w