ARTICLE
Auteur(s) : Hiroshi Hara, Teruhiko Makino, Osamu
Norisugi, Yukie Asano, Megumi Furuichi, Tadamichi Shimizu
Department of Dermatology, Graduate School of Medicine
and Pharmaceutical Sciences, University of Toyama,
Sugitani 2630, Toyama 930-0194, Japan
Bowen's disease (BD) is an in situ type of squamous cell
carcinoma occurring in the skin and mucocutaneous regions. Several
types of human papillomavirus (HPV) have recently been identified
in BD lesions. Most HPV-positive lesions in BD are localized in
either the genital region or distal extremities, and HPV type
16 is frequently detected [1, 2]. This report describes the
detection of HPV types 33 and 56 in BD which occurred on
the sole.
A 60-year-old Japanese male presented with a skin ulcer on his
left sole, which had been present for about 1 year. Physical
examination revealed a 12×12 mm skin ulcer with an irregular
edge on his left sole (figure 1A). The
peripheral skin was thoroughly wet. A few erythematous and
hyperkeratotic lesions were observed around the ulcer. This patient
had no genital lesions associated with HPV infection. The blood
test findings, including SCC antigen, were all within normal
ranges. The histological findings from the lesions showed an
irregular thickening of the epidermis with hyperkeratosis and
dyskeratotic cells (figure 1B). The
epidermis contained a lot of atypical cells, including clumping
cells (figure 1C). The
papillary dermis was not involved in the malignant process. These
findings were diagnostic for BD. The tumor was thereafter totally
excised. Polymerase chain reaction (PCR) amplification for the DNA
of HPV types 6, 11, 16, 18, 30, 31, 33, 35, 39, 45, 51, 52, 56, 58,
59 and 66 was performed, as previously reported [3]. As a
result, both HPV types 33 and 56 were detected from the
lesion tissue.
BD is one of the most common pre-malignant conditions of the
skin. Trauma, exposure to ultraviolet light, and the intake of
arsenic have all been cited as causative factors. Recently, HPV
infection has been implicated as another causal agent of BD. Based
on risk for cancer, HPVs have been divided into two major groups.
The high-risk group includes HPV types 16, 18, 31, 33, 35, 39, 45,
51, 52, 56 and 58, which are often detected in either
intraepithelial carcinoma or invasive carcinoma. The low-risk group
includes HPV types 6, 11, 42, 43 and 44. Oncoprotein E7 binds
to and inactivates Retinoblastoma protein (Rb) in high-risk types
of HPV infection, and consequently the expression of
p16INK4a is upregulated [4]. Therefore, dysregulation of
the Rb/p16INK4a pathway might be associated with the
pathogenesis of BD related to HPV infection. Both HPV types
33 and 56 were first detected in uterine cervical
carcinoma and are thought to have an oncogenic potential. These
HPVs have also been identified from extragenital BD lesions [5, 6].
Although multiple-type HPV is occasionally detected in single
lesions of both cervical carcinoma and BD, the combination of HPV
types 33 and 56 has never been reported in BD to date.
Therefore, this is the first paper to detect the two types of HPV,
namely, HPV types 33 and 56, from extragenital BD.
Acknowledgements
Financial support: none. Conflict of interest: none.
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