Prevalence of Merkel Cell Polyomavirus in Primary Eyelid Merkel Cell Carcinomas and Association With Clinicopathological Features - 13/04/23
, AOI SUKEDA 2, YOSHINARI YAMAMOTO 2, SHIN-ICHIRO OHNO 3, KEISUKE GOTO 2, MASAHIKO KURODA 3, TOSHITAKA NAGAO 2, HIROSHI GOTO 1Highlights |
• | Merkel cell polyomavirus (MCPyV) infection is a critical risk factor for the development of Merkel cell carcinoma (MCC). |
• | A high prevalence of MCPyV infection is found in cutaneous MCC, but the situation in eyelid MCC is unknown. |
• | MCPyV antigens were detected in tumor tissues of all 10 patients with eyelid MCC, using PCR and immunohistochemistry with monoclonal antibodies CM2B4 and Ab3. |
• | MCPyV status in MCC is useful for the diagnosis and choice of therapy for eyelid MCC and provides insights for understanding the pathophysiology of this tumor. |
Graphical abstract |
Résumé |
Purpose |
Merkel cell polyomavirus (MCPyV) infection is a known to be a critical risk factor for the development of Merkel cell carcinoma (MCC). Various reports on cutaneous MCC have shown that the differences in clinicohistopathological characteristics depend on the presence of MCPyV, but the situation in eyelid MCC is unknown. This study aimed to assess the prevalence of MCPyV in patients with eyelid MCC and examine the clinicohistopathological characteristics of MCPyV-associated eyelid MCC.
Design |
Retrospective observational case series with laboratory investigations.
Methods |
Ten patients treated for eyelid MCC were included. Histopathological characteristics were examined by immunohistochemical staining using 12 antibodies. MCPyV infection was evaluated by PCR using primer sets targeting large T antigens of the MCPyV genome and by immunohistochemical staining using CM2B4 and Ab3 monoclonal antibodies. The MCPyV viral load was also quantified by PCR using 3 primer sets.
Results |
All patients (4 males and 6 females) were Japanese with mean age of 79 (range: 63 to 87) years. One patient died due to distant metastasis 8 months after surgery for MCC. Immunohistochemical studies showed typical MCC findings in all cases, including CK20 and neuroendocrine marker positivity. PCR and immunohistochemistry with CM2B4 and Ab3 detected MCPyV antigen in all tumors. Quantitative PCR using sT, LT4, and TAg primers yielded 0.94, 1.72, and 1.05 copies per cell, respectively.
Conclusion |
Clinical and histopathological characteristics of 10 patients with eyelid MCC were elucidated. MCPyV infection was detected in all eyelids. These results provide insight for understanding the tumorigenesis of eyelid MCC.
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Vol 249
P. 49-56 - mai 2023 Retour au numéro
Article précédent
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