Dysplastic naevi with moderate to severe histological dysplasia: A risk factor for melanoma

A. R. Shors; S. Kim; E. White; Z. Argenyi; R. L. Barnhill; P. Duray; L. Erickson; J. Guitart; M. G. Horenstein; L. Lowe; J. Messina; M. S. Rabkin; B. Schmidt; C. R. Shea; M. J. Trotter; M. W. Piepkorn

doi:10.1111/j.1365-2133.2006.07466.x

Dysplastic naevi with moderate to severe histological dysplasia: A risk factor for melanoma

A. R. Shors, S. Kim, E. White, Z. Argenyi, R. L. Barnhill, P. Duray, L. Erickson, J. Guitart, M. G. Horenstein, L. Lowe, J. Messina, M. S. Rabkin, B. Schmidt, C. R. Shea, M. J. Trotter, M. W. Piepkorn

Laboratory Medicine and Pathology

Research output: Contribution to journal › Article › peer-review

52 Scopus citations

Abstract

Background: The risk of malignant melanoma associated with histologically dysplastic naevi (HDN) has not been defined. While clinically atypical naevi appear to confer an independent risk of melanoma, no study has evaluated the extent to which HDN are predictive of melanoma. Objectives: To estimate the risk of melanoma associated with HDN. Secondarily, the risk associated with number of naevi and large naevi is estimated. Methods: We enrolled 80 patients with newly diagnosed melanoma along with 80 spousal controls. After obtaining information on melanoma risk factors and performing a complete cutaneous examination, the most clinically atypical naevus was biopsied in both cases and controls. Histological dysplasia was then assessed independently by 13 dermatopathologists (0, no dysplasia; 1, mild dysplasia; 2, moderate dysplasia; 3, severe dysplasia). The dermatopathologists were blinded as to whether the naevi were from melanoma subjects or controls. Multivariate analyses were performed to determine if there was an independent association between the degree of histological dysplasia in naevi and a personal history of melanoma. Results: In persons with naevi receiving an average score of > 1 (i.e. naevi considered to have greater than mild histological dysplasia), there was an increased risk of melanoma [odds ratio (OR) 2.60, 95% confidence interval (CI) 0.99-6.86] which persisted after adjustment for confounders (OR 3.99, 95% CI 1.02-15.71). Very few dermatopathologists reliably graded naevi of subjects with melanoma as being more dysplastic than naevi of control subjects. Among the entire group, the interobserver reliability associated with grading histological dysplasia in naevi was poor (weighted kappa 0.28). Conclusions: HDN do appear to confer an independent risk of melanoma. However, this result may add more to our biological understanding of melanoma risk than to clinical assessment of risk, because HDN assessed by a single pathologist generally cannot be used to assess risk of melanoma. Future studies should be directed at establishing reproducible, predictive criteria for grading naevi.

Original language	English (US)
Pages (from-to)	988-993
Number of pages	6
Journal	British Journal of Dermatology
Volume	155
Issue number	5
DOIs	https://doi.org/10.1111/j.1365-2133.2006.07466.x
State	Published - Nov 2006

Keywords

Atypical naevi
Case-control
Dysplastic naevi
Melanoma

ASJC Scopus subject areas

Dermatology

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10.1111/j.1365-2133.2006.07466.x

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Shors, A. R., Kim, S., White, E., Argenyi, Z., Barnhill, R. L., Duray, P., Erickson, L., Guitart, J., Horenstein, M. G., Lowe, L., Messina, J., Rabkin, M. S., Schmidt, B., Shea, C. R., Trotter, M. J., & Piepkorn, M. W. (2006). Dysplastic naevi with moderate to severe histological dysplasia: A risk factor for melanoma. British Journal of Dermatology, 155(5), 988-993. https://doi.org/10.1111/j.1365-2133.2006.07466.x

Shors, AR, Kim, S, White, E, Argenyi, Z, Barnhill, RL, Duray, P, Erickson, L, Guitart, J, Horenstein, MG, Lowe, L, Messina, J, Rabkin, MS, Schmidt, B, Shea, CR, Trotter, MJ & Piepkorn, MW 2006, 'Dysplastic naevi with moderate to severe histological dysplasia: A risk factor for melanoma', British Journal of Dermatology, vol. 155, no. 5, pp. 988-993. https://doi.org/10.1111/j.1365-2133.2006.07466.x

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title = "Dysplastic naevi with moderate to severe histological dysplasia: A risk factor for melanoma",

abstract = "Background: The risk of malignant melanoma associated with histologically dysplastic naevi (HDN) has not been defined. While clinically atypical naevi appear to confer an independent risk of melanoma, no study has evaluated the extent to which HDN are predictive of melanoma. Objectives: To estimate the risk of melanoma associated with HDN. Secondarily, the risk associated with number of naevi and large naevi is estimated. Methods: We enrolled 80 patients with newly diagnosed melanoma along with 80 spousal controls. After obtaining information on melanoma risk factors and performing a complete cutaneous examination, the most clinically atypical naevus was biopsied in both cases and controls. Histological dysplasia was then assessed independently by 13 dermatopathologists (0, no dysplasia; 1, mild dysplasia; 2, moderate dysplasia; 3, severe dysplasia). The dermatopathologists were blinded as to whether the naevi were from melanoma subjects or controls. Multivariate analyses were performed to determine if there was an independent association between the degree of histological dysplasia in naevi and a personal history of melanoma. Results: In persons with naevi receiving an average score of > 1 (i.e. naevi considered to have greater than mild histological dysplasia), there was an increased risk of melanoma [odds ratio (OR) 2.60, 95% confidence interval (CI) 0.99-6.86] which persisted after adjustment for confounders (OR 3.99, 95% CI 1.02-15.71). Very few dermatopathologists reliably graded naevi of subjects with melanoma as being more dysplastic than naevi of control subjects. Among the entire group, the interobserver reliability associated with grading histological dysplasia in naevi was poor (weighted kappa 0.28). Conclusions: HDN do appear to confer an independent risk of melanoma. However, this result may add more to our biological understanding of melanoma risk than to clinical assessment of risk, because HDN assessed by a single pathologist generally cannot be used to assess risk of melanoma. Future studies should be directed at establishing reproducible, predictive criteria for grading naevi.",

keywords = "Atypical naevi, Case-control, Dysplastic naevi, Melanoma",

author = "Shors, {A. R.} and S. Kim and E. White and Z. Argenyi and Barnhill, {R. L.} and P. Duray and L. Erickson and J. Guitart and Horenstein, {M. G.} and L. Lowe and J. Messina and Rabkin, {M. S.} and B. Schmidt and Shea, {C. R.} and Trotter, {M. J.} and Piepkorn, {M. W.}",

year = "2006",

month = nov,

doi = "10.1111/j.1365-2133.2006.07466.x",

language = "English (US)",

volume = "155",

pages = "988--993",

journal = "British Journal of Dermatology",

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TY - JOUR

T1 - Dysplastic naevi with moderate to severe histological dysplasia

T2 - A risk factor for melanoma

AU - Shors, A. R.

AU - Kim, S.

AU - White, E.

AU - Argenyi, Z.

AU - Barnhill, R. L.

AU - Duray, P.

AU - Erickson, L.

AU - Guitart, J.

AU - Horenstein, M. G.

AU - Lowe, L.

AU - Messina, J.

AU - Rabkin, M. S.

AU - Schmidt, B.

AU - Shea, C. R.

AU - Trotter, M. J.

AU - Piepkorn, M. W.

PY - 2006/11

Y1 - 2006/11

N2 - Background: The risk of malignant melanoma associated with histologically dysplastic naevi (HDN) has not been defined. While clinically atypical naevi appear to confer an independent risk of melanoma, no study has evaluated the extent to which HDN are predictive of melanoma. Objectives: To estimate the risk of melanoma associated with HDN. Secondarily, the risk associated with number of naevi and large naevi is estimated. Methods: We enrolled 80 patients with newly diagnosed melanoma along with 80 spousal controls. After obtaining information on melanoma risk factors and performing a complete cutaneous examination, the most clinically atypical naevus was biopsied in both cases and controls. Histological dysplasia was then assessed independently by 13 dermatopathologists (0, no dysplasia; 1, mild dysplasia; 2, moderate dysplasia; 3, severe dysplasia). The dermatopathologists were blinded as to whether the naevi were from melanoma subjects or controls. Multivariate analyses were performed to determine if there was an independent association between the degree of histological dysplasia in naevi and a personal history of melanoma. Results: In persons with naevi receiving an average score of > 1 (i.e. naevi considered to have greater than mild histological dysplasia), there was an increased risk of melanoma [odds ratio (OR) 2.60, 95% confidence interval (CI) 0.99-6.86] which persisted after adjustment for confounders (OR 3.99, 95% CI 1.02-15.71). Very few dermatopathologists reliably graded naevi of subjects with melanoma as being more dysplastic than naevi of control subjects. Among the entire group, the interobserver reliability associated with grading histological dysplasia in naevi was poor (weighted kappa 0.28). Conclusions: HDN do appear to confer an independent risk of melanoma. However, this result may add more to our biological understanding of melanoma risk than to clinical assessment of risk, because HDN assessed by a single pathologist generally cannot be used to assess risk of melanoma. Future studies should be directed at establishing reproducible, predictive criteria for grading naevi.

AB - Background: The risk of malignant melanoma associated with histologically dysplastic naevi (HDN) has not been defined. While clinically atypical naevi appear to confer an independent risk of melanoma, no study has evaluated the extent to which HDN are predictive of melanoma. Objectives: To estimate the risk of melanoma associated with HDN. Secondarily, the risk associated with number of naevi and large naevi is estimated. Methods: We enrolled 80 patients with newly diagnosed melanoma along with 80 spousal controls. After obtaining information on melanoma risk factors and performing a complete cutaneous examination, the most clinically atypical naevus was biopsied in both cases and controls. Histological dysplasia was then assessed independently by 13 dermatopathologists (0, no dysplasia; 1, mild dysplasia; 2, moderate dysplasia; 3, severe dysplasia). The dermatopathologists were blinded as to whether the naevi were from melanoma subjects or controls. Multivariate analyses were performed to determine if there was an independent association between the degree of histological dysplasia in naevi and a personal history of melanoma. Results: In persons with naevi receiving an average score of > 1 (i.e. naevi considered to have greater than mild histological dysplasia), there was an increased risk of melanoma [odds ratio (OR) 2.60, 95% confidence interval (CI) 0.99-6.86] which persisted after adjustment for confounders (OR 3.99, 95% CI 1.02-15.71). Very few dermatopathologists reliably graded naevi of subjects with melanoma as being more dysplastic than naevi of control subjects. Among the entire group, the interobserver reliability associated with grading histological dysplasia in naevi was poor (weighted kappa 0.28). Conclusions: HDN do appear to confer an independent risk of melanoma. However, this result may add more to our biological understanding of melanoma risk than to clinical assessment of risk, because HDN assessed by a single pathologist generally cannot be used to assess risk of melanoma. Future studies should be directed at establishing reproducible, predictive criteria for grading naevi.

KW - Atypical naevi

KW - Case-control

KW - Dysplastic naevi

KW - Melanoma

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Dysplastic naevi with moderate to severe histological dysplasia: A risk factor for melanoma

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