Original Research

Physician Skin Examinations for Melanoma Screening

Cutis. 2015 September;96(3):175-182

References

1. American Cancer Society. Cancer Facts & Figures 2015. Atlanta, GA: American Cancer Society; 2015. http:  //www.cancer.org/Research/CancerFactsStatistics/cancer  factsfigures2015/cancer-facts-and-figures-2015. Accessed July 6, 2015.

2. Guy G Jr, Ekwueme D, Tangka F, et al. Melanoma treatment costs: a systematic review of the literature, 1990-2011. Am J Prev. 2012;43:537-545.

3. Margolis D, Halpern A, Rebbeck T, et al.  Validation of a melanoma prognostic model. Arch  Dermatol. 1998;134:1597-1601.

4. Wolff T, Tai E, Miller T. Screening for skin cancer: an update of the evidence for the U.S. Preventative Services Task Force. Ann Intern Med. 2009;150:194-198.

5. American Academy of Dermatology. Melanoma  Monday. http://www.aad.org/spot-skin-cancer  /community-programs-events/melanoma-monday. Accessed August 19, 2015.

6. Higgins JPT, Green S, eds. Cochrane Handbook for  Systematic Reviews of Interventions Version 5.1.0 [updated March 2011]. The Cochrane Collaboration, 2011. http:  //www.cochrane-handbook.org. Updated March 2011. Accessed November 10, 2014.

7. Viswanathan M, Berkman N. Development of the RTI item bank on risk of bias and precision of observational studies. J Clin Epidemiol. 2012;65:163-178.

8. Moher D, Liberati A, Tetzlaff J, et al; PRISMA group. Preferred reporting items for systematic reviews and  meta-analyses: the PRISMA statement [published online ahead of print July 23, 2009]. J Clin Epidemiol. 2009;62:1006-1012.

9. Berwick M, Armstrong B, Ben-Porat L. Sun exposure  and mortality from melanoma. J Natl Cancer Inst. 2005;97:195-199.

10. Berwick M, Begg C, Fine J, et al. Screening for cutaneous melanoma by skin self-examination. J Natl Cancer Inst. 1996;88:17-23.

11. Aitken J, Elwood J, Lowe J, et al. A randomised trial of population screening for melanoma. J Med Screen. 2002;9:33-37.

12. Schneider J, Moore D, Mendelsohn M. Screening program reduced melanoma mortality at the Lawrence Livermore National Laboratory, 1984 to 1996. J Am Acad Dermatol. 2008;58:741-749.

13. Expert Health Data Programming Inc. Health data  software and health statistics. Available from: http:  //www.ehdp.com. Accessed April 1, 2001. Cited by: Schneider J, Moore D, Mendelsohn M. Screening program reduced melanoma mortality at the Lawrence  Livermore National Laboratory, 1984 to 1996. J Am Acad Dermatol. 2008;58:741-749.

14. Aitken J, Elwood M, Baade P, et al. Clinical whole-body skin examination reduces the incidence of thick melanomas. Int J Cancer. 2010;126:450-458.

15. Katalinic A, Waldmann A, Weinstock M, et al. Does skin cancer screening save lives? an observational study comparing trends in melanoma mortality in regions with and without screening. Cancer. 2012;118:5395-5402.

16. Aitken J, Janda M, Elwood M, et al. Clinical outcomes from skin screening clinics within a community-based melanoma screening program. J Am Acad Dermatol. 2006;54:105-114.

17. Coory M, Baade P, Aitken JF, et al. Trends for in-situ and invasive melanoma in Queensland, Australia, 1982 to 2002. Cancer Causes Control. 2006;17:21-27.

18. Mayer JE, Swetter SM, Fu T, et al. Screening, early detection, education, and trends for melanoma: current status (2007-2013) and future directions: part II. screening, education, and future directions. J Am Acad Dermatol. 2014;71:611.e1-611.e10; quiz, 621-622.

19. Curiel-Lewandrowski C, Chen S, Swetter S, et al. Screening and prevention measures for melanoma: is there a survival advantage? Curr Oncol Rep. 2012;14:458-467.

20. Terushkin V, Halpern A. Melanoma early detection. Hematol Oncol Clin North Am. 2009;23:481-500.

21. Geller A, Greinert R, Sinclair C, et al. A nationwide population-based skin cancer screening in Germany: proceedings of the first meeting of the International Task Force on Skin Cancer Screening and Prevention  (September 24 and 25, 2009) [published online ahead of print April 8, 2010]. Cancer Epidemiol. 2010;34:355-358.

22. Kornek T, Schafer I, Reusch M, et al. Routine skin cancer screening in Germany: four years of experience from  the dermatologists’ perspective. Dermatology. 2012;225:289-293.

23. De Giorgi V, Grazzini M, Rossari S, et al. Is skin  self-examination for cutaneous melanoma detection still adequate? a retrospective study. Dermatology. 2012;225:31-36.

24. Swetter S, Johnson T, Miller D, et al. Melanoma in middle-aged and older men: a multi-institutional survey study of factors related to tumor thickness. Arch Dermatol. 2009;145:397-404.

25. Kantor J, Kantor D. Routine dermatologist-performed  full-body skin examination and early melanoma detection. Arch Dermatol. 2009;145:873-876.

26. Kovalyshyn I, Dusza S, Siamas K, et al. The impact of physician screening on melanoma detection. Arch Dermatol. 2011;147:1269-1275.

27. Pollitt R, Clarke C, Shema S, et al. California  Medicaid enrollment and melanoma stage at diagnosis: a population-based study. Am J Prev Med. 2008;35:7-13.

28. Roetzheim R, Lee J, Ferrante J, et al. The influence of dermatologist and primary care physician visits on melanoma outcomes among Medicare beneficiaries. J Am Board Fam Med. 2013;26:637-647.

29. Durbec F, Vitry F, Granel-Brocard F, et al. The role of circumstances of diagnosis and access to dermatological care in early diagnosis of cutaneous melanoma: a population-based study in France. Arch Dermatol. 2010;146:240-246.

30. Lakhani N, Saraiya M, Thompson T, et al. Total body skin examination for skin cancer screening among U.S. adults from 2000 to 2010. Prev Med. 2014;61:75-80.

31. Oliveria SA, Heneghan MK, Cushman LF, et al. Skin cancer screening by dermatologists, family practitioners, and internists: barriers and facilitating factors. Arch Dermatol. 2011;147:39-44.

32. Bigby M. Why the evidence for skin cancer screening is insufficient: lessons from prostate cancer screening. Arch Dermatol. 2010;146:322-324.

Results

A total of 705 titles were screened, 98 abstracts were assessed for eligibility, 42 full-text reviews were carried out, and 5 eligible studies were identified (Figure 1). Five observational studies were included in the final review. A summary of the results is presented in Table 1.

Included studies were assessed for several types of biases, including selection bias, attrition bias, detection bias, performance bias, and response bias. The judgments were given for each domain (Table 2). There was heterogeneity in study design, reporting of total-body skin examination methods, and reporting of outcomes among all 5 studies. All 5 studies were assessed as having a medium risk of bias.

Physician Skin Examination Impact

One article by Berwick et al⁹ reanalyzed data from a 1996 study¹⁰ and provided no significant evidence regarding the benefits of PSEs in the reduction of melanoma mortality. Data for 650 patients with newly diagnosed melanomas were obtained from the Connecticut Tumor Registry, a site for the National Cancer Institute’s Surveillance, Epidemiology, and End Results (SEER) program, along with 549 age- and sex-frequency matched controls from the general population.¹⁰ Participants were followed biannually for a mean of 5.4 years. Of the original 650 case patients, 122 were excluded from the study with reasons provided. Physician skin examination was defined as a positive response to the following questionnaire item: “[Before your recent biopsy] did the doctor examine your skin during any of your visits?”⁹ Data analysis showed no significant association between PSE and death from melanoma. Upon univariate analysis, the hazard ratio for physician screening was 0.7 (95% confidence interval [CI], 0.4-1.3).⁹

The SCREEN (Skin Cancer Research to Provide Evidence for Effectiveness of Screening in Northern Germany) project, which was undertaken in Schleswig-Holstein, Germany, is the world’s largest systematic population-based skin cancer screening program.¹⁵ The participation rate was  19% (N=360,288) of the eligible population (citizens aged ≥20 years with statutory health insurance). Screening was a 2-step process performed by trained physicians: initial general practitioner whole-body skin examination followed by referral to a dermatologist for evaluation of suspicious skin findings. Five years after the SCREEN program was conducted, melanoma mortality declined by 47% per 100,000 men and by 49% per 100,000 women. The annual percentage change in the most recent 10-year period (2000-2009) was 7.5% (95% CI, –14.0 to –0.5; P<.05) for men and 7.1% for women (95% CI,  –10.5 to –2.9; P<.05). Simultaneously, the melanoma mortality rates in the 4 unscreened adjacent regions and the rest of Germany were stable, significantly (P<.05) different from the decline in mortality observed in Schleswig-Holstein.¹⁵

A community-based, prospective cohort study investigated the impact of an employee melanoma screening program at the Lawrence Livermore National Laboratory (Livermore, California) (1984-1996) demonstrated an impact on melanoma thickness and mortality rates.¹² The cohort (approximately 5100 participants) was followed over 3 phases of surveillance: (1) preawareness (1969-1975), (2) early awareness of increased melanoma risk (1976-1984), and (3) screening program (1984-1996). The screening program encouraged employees to self-examine their skin for “suggestive lesions”; if a suggestive lesion was found, a full-body skin examination was performed by a physician. After being evaluated, participants with melanoma, dysplastic nevi, 50 or more moles, or a family history of melanoma were offered a periodic full-body examination every 3 to 24 months, often with  full-body photography and dermoscopy. Physician skin screening resulted in a reduction in crude incidence of thicker melanomas (defined as  >0.75 mm) during the 3 study phases. Compared with the early-awareness period (phase 2), a 69% reduction in the diagnosis of thick melanomas was reported in the screening program period (phase 3)(P=.0001). During the screening period, no eligible melanoma deaths occurred in the study population, whereas the expected number of deaths was 3.39 (P=.034) based on observed melanoma mortality in 5 San Francisco/Oakland Bay–area counties in California as reported to the SEER program from 1984 to 1996.¹²

The strongest evidence for reduced thickness of melanomas detected via PSEs was reported in a  population-based, case-control study by Aitken et al¹⁴ of all residents in Queensland, Australia, aged 20 to 75 years with a histologically confirmed first primary invasive cutaneous melanoma diagnosed between January 2000 and December 2003. Whole-body PSE in the 3 years before diagnosis was inversely associated with tumor thickness at diagnosis (χ²=44.37; P<.001), including a 14% lower risk of diagnosis of a thick melanoma (>0.75 mm)(odds ratio [OR], 0.86;  95% CI, 0.75-0.98) and a 40% lower risk of diagnosis of a melanoma that was 3 mm or larger (OR, 0.60;  95% CI, 0.43-0.83). The investigators applied melanoma thickness-specific survival estimates to the thickness distribution of the screened and unscreened cases in their sample to estimate melanoma deaths within 5 and 10 years of diagnosis. Compared to the unscreened cases, they estimated that the screened cases would have 26% fewer melanoma deaths within 5 years of diagnosis and  23% fewer deaths within 10 years.¹⁴

References

2. Guy G Jr, Ekwueme D, Tangka F, et al. Melanoma treatment costs: a systematic review of the literature, 1990-2011. Am J Prev. 2012;43:537-545.

3. Margolis D, Halpern A, Rebbeck T, et al.  Validation of a melanoma prognostic model. Arch  Dermatol. 1998;134:1597-1601.

4. Wolff T, Tai E, Miller T. Screening for skin cancer: an update of the evidence for the U.S. Preventative Services Task Force. Ann Intern Med. 2009;150:194-198.

5. American Academy of Dermatology. Melanoma  Monday. http://www.aad.org/spot-skin-cancer  /community-programs-events/melanoma-monday. Accessed August 19, 2015.

6. Higgins JPT, Green S, eds. Cochrane Handbook for  Systematic Reviews of Interventions Version 5.1.0 [updated March 2011]. The Cochrane Collaboration, 2011. http:  //www.cochrane-handbook.org. Updated March 2011. Accessed November 10, 2014.