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Familial melanoma
Author(s) -
NEWTON J.A.
Publication year - 1993
Publication title -
clinical and experimental dermatology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.587
H-Index - 78
eISSN - 1365-2230
pISSN - 0307-6938
DOI - 10.1111/j.1365-2230.1993.tb00956.x
Subject(s) - medicine , dermatology , melanoma , cancer research
Summary The presence of large numbers of moles, atypical in appearance and distribution typifies the atypical mole syndrome. The syndrome may occur in one individual alone or in an autosomal‐dominant fashion in his/her family. The presence of this phenotype indicates an increased risk of melanoma, although the risk varies according to the presence or absence of a family history. The classification devised by Kraemer et al. 1 works well in estimating the risk of melanomas but is, as yet, not fully evaluated. The diagnosis of the syndrome is essentially clinical, necessitating the consideration of various aspects of phenotype such as total mole count, distribution, clinical appearance of the moles, the age of onset, site, and number of melanomas. It is always helpful to screen first‐degree and second‐degree relatives if there is a family history of moleyness or melanoma. Small numbers of clinically and, sometimes histologically dysplastic naevi may occur in normal individuals. The vast majority of these probably regress as do totally banal naevi, although a low percentage will result in a melanoma. 2 Those patients should be questioned to establish the existence of a family history of increased numbers of moles and melanoma. They should also be thoroughly examined for the presence of other signs of the syndrome: increased total mole count, iris freckles etc. In the absence of either a family history or these additional clinical features it is unlikely that these individuals have‘the syndrome'. Common sense advice about sun avoidance and self‐examination should be given. It is important to distinguish this from the atypical mole syndrome (AMS). Many authors are unhappy about the use of the term‘dysplastic naevus syndrome’for this condition, partly because the histological appearances of the atypical naevi are not dysplastic in the true sense of the word. 3 There has also been considerable uncase amongst pathologists about the implications of reporting a naevus as‘dysplastic’. The situation may be improved if it is recognized that dysplastic naevi can occur normally in the general population and that what is important is the recognition of the full phenotype and family history. Some patients from melanoma families do not have‘classically dysplastic’naevi. It is , therefore, probably better to abandon the term dysplastic naevus syndrome in favour of‘atypical mole syndrome’.