ARTICLE
Auteur(s) : Retno DANARTI, Arne KÖNIG, Rudolf HAPPLE
Department of Dermatology, Philipp University,
Deutschhausstrasse 9, D‐35033, Marburg, Germany
Reprints: R. Happle Fax: (+ 49)‐6421‐2862902 E‐mail:
happlemailer.uni‐marburg.de
Article accepted on 11\06\2003
Key words: The large congenital melanocytic nevus
(LCMN) is a disfiguring lesion covering extensive areas of the body
surface. Its incidence is approximately 1 in 20,000 live
births [1, 2]. Clinically, LCMN is characterized by one or more
large round or irregularly shaped patches presenting at birth and
commonly involving the trunk without any midline separation [3].
Often there are satellite lesions of a similar appearance in the
periphery of the main lesion, or additional small nevi may be
scattered over the entire skin surface [4]. Some proposed size
criteria defining LCMN include those greater than 2 percent of
the body surface area [5], nevi greater than 20 cm at their
largest diameter [6], and nevi that cannot be excised in a single
procedure [7]. The large nevi involving the head and neck may be
considered as indicative of leptomeningeal involvement [8]. A
precise risk of neurocutaneous melanosis for patients with LCMN is
not known. A variety of abnormalities have been reported in
association with LCMN, such as spina bifida occulta, hypertrophy of
cranial bones, prognathism, high arched palate, scoliosis [9],
atrophy of the involved limb [1, 10, 11], and cutis marmorata [12].
The impact of LCMN is serious because of a frequently associated
leptomeningeal melanocytosis; a high risk of malignant
transformation; a congenital esthetic problem with undesirable
psychological reactions; and because it is difficult to treat [8].
The risk of malignant transformation of large congenital
melanocytic nevi is increased although exact percentages are
elusive. Quaba and Wallace calculated the risk of melanoma to be
8.52 percent during the first 15 years of life [5]. A
longitudinal study of a large series of patients with LCMN reported
a lifetime incidence of malignant transformation of 4 to
6 percent [13]. As reviewed by Kaplan [14] and Kopf et
al. [6], other authors reported the incidence of malignant
melanoma developing from large congenital nevi to be 2\110 (2%)
[15], 5\82 (6%) [16], 4\40 (10%) [9], 6\56 (11%) [17], or 17\55
(31%) [6, 8, 14]. Most cases of LCMN, including neurocutaneous
melanosis, are sporadic [8, 18‐20]. On the other hand, when
studying the literature on LCMN we found 14 familial cases,
raising the question of a role of genetic factors.
Methods and results
A literature review revealed 7 familial cases of large
congenital melanocytic nevi and 7 reports on large congenital
melanocytic nevi with a family history of congenital medium
size\small nevi. They are presented in Table
I and Table II. In several of
these patients, satellite lesions or disseminated small nevi were
likewise present. A neurological involvement was reported in none
of these families.
Table I. Familial occurrence of large
congenital melanocytic nevi
| Authors and year of publication |
Sex |
Location of nevi |
Family members with
congenital large nevi |
| Gould and Pyle, 1897 [31] |
M |
Trunk |
Sister (neck and entire back) |
| Sachs, 1912 [32] |
M |
Trunk, forearms |
Brother and sister (trunk, forearms) |
| Beck, 1927 [33] |
M |
¿ |
Grandmother |
| Bhatavadekar, 1933 [34] |
M |
Trunk |
Grandfather |
| Voigtländer and Jung, 1974 [35] |
F |
Abdomen, lower back, buttocks, left thigh |
Brother* (right wrist) |
| Hecht, 1981 [36] |
M |
Scalp |
Paternal male cousin (scalp) |
| Duchesne, 1984 [37] |
F |
Abdomen, lower back, buttocks, thigh |
Paternal uncle (trunk)
|
* In addition, the mother had multiple small melanocytic nevi
involving her trunk and limbs.
.
Table II. Large congenital melanocytic nevi
with a family history of congenital medium‐size\small nevi
| Authors and year of publication |
Sex |
Location of large congenital nevi |
Family members with congenital medium\small nevi |
| Spitzer, 1905 [38] |
M |
¿ |
Brother (scalp)
Sister (back) |
| Pickrell and Clay, 1944 [39] |
M |
Left thigh and upper part
of the left lower leg |
Father (buttock) |
| Russel and Reyes, 1959 [40] |
F |
Entire back |
Mother (scattered small nevi
over the bodies)
Siblings (scattered small nevi
over the bodies) |
Goodman et al., 1971 [23]
Family A |
F |
Abdomen, lower back,
buttocks, thigh |
Father (face, trunk)
Brother (face, thigh) |
| Family B |
M |
Anterior chest, shoulders, entire back |
Mother (face, shoulder)
Brother (trunk) |
| Family C |
M |
Occipital region, neck, left buttock |
Mother (trunk, face)
Maternal grandmother (trunk) |
Groh and Schnyder, 1984 [41]
Case 2 |
M |
Trunk |
Mother (neck)
Cousin (neck)
|
.
Discussion
The vast majority of LCMN do not show familial occurrence [8,
18‐20]. In these congenital disorders, genetic mosaicism probably
originates virtually always from a postzygotic mutation, which
would explain why LCMN is usually sporadic [1]. One might
hypothesize that in a heterozygous individual, a somatic mutational
event may cause loss of the corresponding wild‐type allele (loss of
heterozygosity, LOH) at the LCMN locus, resulting in a cell that is
either homozygous or hemizygous for the LCMN gene.
In 1986, one of us provided a tentative explanation why several
disorders always occur sporadically, always show a mosaic pattern
with a highly variable arrangement, and virtually never involve the
entire integument [21]. The theory of an autosomal lethal gene
surviving by mosaicism was based on the assumption that the
presence of such mutation in a zygote would lead to death of the
embryo at an early stage of development. Cells bearing the mutation
can survive only in a mosaic state, in close proximity with normal
cells. In principle, an individual with a mosaic state of a lethal
gene cannot transmit the mutation to the next generation; if
transmitted, the zygote with the lethal mutation will die in utero.
According to this concept, the phenotype of LCMN should always
occur sporadically [22]. However, as an exception from this rule,
the possibility of paradominant inheritance may be considered in
familial cases of LCMN.
In reviewing the literature on LCMN we found several reports of
LCMN occurring in more than one member of a given family,
indicating the presence of some genetic factor. Goodman et
al. [23] have postulated that some cases of LCMN may be
genetically determined by an autosomal dominant gene with variable
expressivity. However, these rare familial cases do not display a
consistent Mendelian pattern of inheritance. The hypothesis of
autosomal dominant inheritance with variable expressivity [23]
cannot explain why this disease always occurs in a mosaic
pattern.
Cockayne [24] thought that such nevi are likely to be inheritable
but felt that their mode of inheritance is probably rather
complex.
Goodman et al. [23] postulated that some cases of giant
pigmented hairy nevus may be genetically determined by an
"autosomal dominant gene with variable expressivity".
Cantú et al. [25] discussed several hypotheses to explain
the discordant occurrence of giant pigmented nevus in monozygotic
twins: non‐penetrance of the gene in one parent and in the normal
twin; a gametic half‐chromatid mutation; and a postzygotic
double‐strand mutation occurring after the two‐cell stage
replications. They also discussed the possibility of an autosomal
recessive gene as the cause of giant pigmented nevus. A homozygous
individual would be expected to have the entire skin surface
affected; since no individual has been reported with such features,
the homozygous mutation would probably be lethal. However, a
heterozygous could have, by somatic recombination, a homozygous
cell line so that the giant pigmented nevus would become manifest
[25].
This mosaic arrangement may be best explained by paradominant
inheritance [26]. Individuals heterozygous for a paradominant
mutation are, as a rule, phenotypically normal and, therefore, the
gene can be transmitted without any clinical expression through
many generations. The trait only becomes manifest when a somatic
mutation occurs at an early stage of embryogenesis. This leads to a
clonal population of homozygous or hemizygous cells and creates a
mosaic phenotype.
This concept would explain why LCMN occurs virtually always
sporadically, and why the exceptional cases of familial aggregation
of this trait do not show any consistent Mendelian pattern
[26].
A list of phenotypes that may be explained by paradominant
inheritance now includes: (1) Becker nevus, (2) sebaceous nevus,
(3) speckled lentiginous nevus, (4) lateral telangiectatic nevus,
(5) Sturge‐Weber‐Klippel‐Trenaunay syndrome, (6) nevus anemicus,
(7) unilateral nevoid telangiectasia, (8) Proteus syndrome, (9)
Poland anomaly, (10) cutis marmorata telangiectatica congenita [3,
26‐30] and (11) LCMN.
The presence of congenital medium‐sized or small melanocytic nevi
in family members would reflect LOH occurring in a heterozygous
embryo at a later developmental stage.
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