Dermatology: Practical and Conceptual


Observation  |  Dermatol Pract Concept 2016;6(4):10 43

DERMATOLOGY PRACTICAL & CONCEPTUAL
www.derm101.com

Early diagnosis of genital mucosal melanoma: 
how good are our dermoscopic criteria?

Tova Rogers, MFA1, Melissa Pulitzer, MD2, Maria L. Marino, MD1, Ashfaq A. Marghoob, MD1, 
Oliver Zivanovic, MD3, Michael A. Marchetti, MD1

1 Dermatology Service, Memorial Sloan Kettering Cancer Center, New York, NY, USA

2 Pathology Service, Memorial Sloan Kettering Cancer Center, New York, NY, USA

3 Gynecology Service, Department of Surgery, Memorial Sloan Kettering Cancer Center, New York, NY, USA

Key words: melanoma, genital, mucosal melanoma, dermoscopy

Citation: Rogers T, Pulitzer M, Marino M, Marghoob A, Zivanovic O, Marchetti M. Early diagnosis of genital mucosal melanoma: how 
good are our dermoscopic criteria? Dermatol Pract Concept 2016;6(4):10. doi: 10.5826/dpc.0604a10

Received: April 28, 2016; Accepted: July 25, 2016; Published: October 31, 2016

Copyright: ©2016 Rogers. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which 
permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Funding: None.

Competing interests: The authors have no conflicts of interest to disclose.

All authors have contributed significantly to this publication.

Corresponding author: Michael A. Marchetti, MD, Dermatology Service, Department of Medicine, Memorial Sloan Kettering Cancer 
Center, 16 E 60th Street, New York 10065, USA. Tel. 646-888-6016; Fax: 646-888-6478. Email: marchetm@mskcc.org

Background: There are limited studies on the dermoscopic features of mucosal melanoma, particu-
larly early-stage lesions. Described criteria include the presence of blue, gray, or white colors, with a 
reported sensitivity of 100%. It is unclear if these features will aid in the detection of early mucosal 
melanoma or improve diagnostic accuracy compared to naked-eye examination alone.

Case: An Asian female in her fifties was referred for evaluation of an asymptomatic, irregularly pig-
mented patch of the clitoral hood and labia minora of unknown duration. Her past medical history 
was notable for Stage IV non-small cell lung cancer. She denied a personal or family history of skin 
cancer. Dermoscopic evaluation of the vulvar lesion revealed heterogeneous brown and black pigmen-
tation mostly composed of thick lines. There were no other colors or structures present. As the dif-
ferential diagnosis included vulvar melanosis and mucosal melanoma, the patient was recommended 
to undergo biopsy, which was delayed due to complications from her underlying lung cancer. Repeat 
dermoscopic imaging performed three months later revealed significant changes concerning for mela-
noma, including increase in size, asymmetric darkening, and the appearance of structureless areas and 
central blue and pink colors. Histopathological examination of a biopsy and subsequent resection 
confirmed the diagnosis of melanoma in situ.

Conclusion: Previously described dermoscopic features for mucosal melanoma may not have high 
sensitivity for early melanomas. Additional studies are needed to define the dermoscopic character-
istics of mucosal melanomas that aid in early detection. Health care providers should have a low 
threshold for biopsy of mucosal lesions that show any clinical or dermoscopic features of melanoma, 
especially in older women.

ABSTRACT

mailto:marchetm@mskcc.org


44 Observation  |  Dermatol Pract Concept 2016;6(4):10

On examination, a 12 x 13 mm, irregular, dark brown-

black patch was noted on her clitoral hood and labia minora 

(Figure 1). Ill-defined, patchy, light brown pigmentation on 

bilateral labia minora was also observed. There was no lymph-

adenopathy on palpation of the inguinal and femoral nodal 

basins. Dermoscopic evaluation of the lesion was performed 

using polarized contact dermoscopy with ultrasound gel and 

a polyvinyl chloride barrier. It revealed heterogeneous brown 

and black pigmentation composed of thick lines without 

other structures (Figure 2a). There was no evidence of blue, 

gray, or white colors or other dermoscopic features reported 

to be specific for the diagnosis of melanoma. The differential 

included mucosal melanosis and melanoma. Given the atypical 

clinical appearance of a large, asymmetric, pigmented macule 

with color variegation, a biopsy was recommended but was 

delayed due to complications from the patient’s underlying 

malignancy. On follow-up examination three months later, 

repeat dermoscopic imaging with polarized contact dermos-

copy using ultrasound gel and a polyvinyl chloride barrier 

revealed significant changes concerning for melanoma, includ-

ing increase in size, asymmetric darkening, and the appearance 

of structureless areas and central blue and pink colors (Figure 

2b). Histopathological examination of an incisional biopsy and 

subsequent excision revealed melanoma in situ with a charac-

teristic proliferation of enlarged, poorly nested and confluent, 

severely atypical melanocytes. Other notable histopathologic 

findings included skipping foci of heavily pigmented dermal 

melanophages, variable lichenoid inflammatory infiltrate, and 

marked vascular ectasia and congestion (Figure 3).

Case report

An Asian female in her fifties was referred for evaluation of an 

asymptomatic, pigmented vulvar lesion of unknown duration. 

She denied a personal or family history of skin cancer. Her 

past medical history was notable for Stage IV non-small cell 

lung cancer diagnosed nine months prior and managed with 

surgery and oral erlotinib.

Figure 2. Polarized contact dermoscopic images of vulvar melanoma in situ. (a) Baseline dermoscopic image showed heterogeneous and 

asymmetric brown and black pigmentation composed of thick lines. (b) Repeat dermoscopic imaging three months later showed increase in 

size, asymmetric and multifocal darkening, and the appearance of structureless areas and central blue and pink colors. [Copyright: ©2016 

Rogers.]

Figure 1. Clinical appearance of vulvar melanoma in situ showed 

12 x 13 mm asymmetric patch with color variegation on the clitoral 

hood and labia minora. [Copyright: ©2016 Rogers.]



Observation  |  Dermatol Pract Concept 2016;6(4):10 45

Clinically, VM can present as flat or raised lesions with 

irregular borders and are often greater than 7 mm in size 

[7]. A majority of VM are pigmented, however, amelanotic 

VM accounts for 4% to 27% of cases [2,4]. Late symptoms 

include bleeding and pruritus, while many lesions, especially 

early lesions, can be asymptomatic [2]. Most VM are diag-

nosed at locally advanced stages. A 2015 study that included 

63 cases of VM demonstrated a median Breslow thickness at 

presentation of 3.3 mm (range: 0-20mm) [1]. Regional nodal 

disease is not uncommon at presentation [4].

The most common histological subtypes of VM are super-

ficial spreading and nodular [1,8]. Compared to cutaneous 

melanoma, VM show distinct genetic mutations. A 2014 

study evaluating the genetic profiles of VM found KIT muta-

tions in 18% of cases (7/39) and NRAS mutations in 12% of 

cases (5/42). No mutations in BRAF (0/39) or EGFR (0/30) 

were found [9]. The overall prognosis of VM is worse than 

that for cutaneous melanoma, with 61% versus 91% five-

year melanoma-specific survival rates, respectively [8]. It is 

Conclusion

Vulvar melanoma (VM) accounts for 1% to 3% of all mela-

nomas arising in women [1]. It most frequently occurs in the 

fifth or sixth decade of life, suggesting that clinicians should 

have a heighted suspicion for melanoma when evaluating pig-

mented mucosal lesions in older women [2-4]. The incidence is 

slightly higher in Caucasians compared to Hispanics, Asians, 

Blacks, and American-Indians [5]. Risk factors include chronic 

inflammation, such as that associated with lichen sclerosis 

[6]. The differential diagnosis of pigmented vulvar lesions 

includes vulvar nevi and vulvar melanosis (also referred to as 

vulvar lentiginosis or vulvar melanotic macule), particularly 

in younger individuals. Vulvar nevi tend to present clinically 

as evenly pigmented papules or macules with regular borders. 

Their colors range from red to dark brown-black and they 

typically measure less than 1 cm. Vulvar melanosis is char-

acterized by single or multiple, irregularly pigmented, tan to 

black macules or patches with uneven borders [6].

Figure 3. Histopathology of vulvar melanoma in situ. (a) Photomicrograph of initial biopsy specimen showing a broad, asymmetric, junc-

tional melanocytic proliferation with variable epidermal acanthosis and dermal clusters of heavily pigmented melanophages (hematoxylin-

eosin stain, original magnification x100). (b, c, d) Images of excised specimen showing confluent, severely atypical melanocytes with pag-

etoid spread (b), hematoxylin-eosin stain, original magnification x400), areas with lichenoid lymphoid infiltrates and melanophages (c), 

hematoxylin-eosin stain, original magnification x200), and the intersection of congested and ectatic vasculature with dermal melanophages 

and junctional melanoma (d), hematoxylin-eosin stain, original magnification x200). [Copyright: ©2016 Rogers.]



46 Observation  |  Dermatol Pract Concept 2016;6(4):10

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unclear if the poorer prognosis associated with VM is due to 

later detection or more aggressive biological behavior [10].

Dermoscopic features of VM have been described. Blum 

et al evaluated 11 cases of VM, 10 of which were invasive, 

and found that the presence of blue, gray, or white colors 

with or without structureless areas had 100% sensitivity for 

melanoma [11]. de Giorgio et al described a case of superficial 

spreading melanoma of the vulva with a Breslow depth of 0.5 

mm that presented with a blue-gray area and whitish veil [12]. 

Lin et al evaluated the dermoscopic features of 40 pigmented 

mucosal lesions in Japanese patients, including 8 melanomas, 

2 of which were vulvar. They found that 6 of the 8 melanomas 

(75%), including both vulvar lesions, had multicomponent 

patterns. The vulvar lesions also had multiple colors and 

blue-white veils [13]. These findings are in contrast to the 

described dermoscopic features of vulvar melanosis, which 

include a ring-like pattern, a homogeneous or structureless 

pattern, a reticular pattern, and a globular pattern [14-16]. 

A limitation of the studies evaluating the dermoscopic mor-

phologies of mucosal melanoma is that the studied lesions 

were clinically detected and often of an advanced stage; it 

is therefore unknown if the application of these criteria will 

aid in the detection of early mucosal melanomas. Consistent 

with this limitation, Betti et al described a case of melanoma 

in situ on the glans penis with an irregular pigment network 

but no other worrisome features [17].

In order to not miss an opportunity for early detection of 

mucosal melanoma, health care providers should have a low 

threshold for biopsy of lesions that demonstrate any clinical 

or dermoscopic features concerning for melanoma. This is 

especially true for older patients. Larger studies are needed 

to more rigorously define clinical and dermoscopic criteria 

that accurately distinguish early mucosal melanomas from 

benign skin lesions.

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https://www.ncbi.nlm.nih.gov/pubmed/15274702
https://www.ncbi.nlm.nih.gov/pubmed/20846309