Virus Dataset Sample Info

> Dataset: 23322199 Search Result


Summary
Item Summary
Project 23322199
Virus Name MCV
Sample Number 20
Disease Non-small cell lung cancer (NSCLC)
Country Japan

Sample
ID Sample ID Age Gender Origin Detail
1 SCC3 73 F Japan View
2 SCC15a 78 M Japan View
3 SCC17 74 M Japan View
4 SCC21 71 M Japan View
5 SCC22 73 M Japan View
6 SCC23 71 M Japan View
7 SCC24 69 M Japan View
8 SCC27 75 F Japan View
9 SCC32 83 M Japan View
10 AC7 78 M Japan View
11 AC8 59 M Japan View
12 AC15 70 F Japan View
13 AC16 74 F Japan View
14 AC34 73 M Japan View
15 AC35 71 F Japan View
16 AC37 67 M Japan View
17 AC39 66 F Japan View
18 AC43b 81 F Japan View
19 LCNEC27 79 M Japan View
20 PL2 68 M Japan View

Literature
Item Summary
PMID 23322199
Title Detection of Merkel Cell Polyomavirus With a Tumour-Specific Signature in Non-Small Cell Lung Cancer
Abstract Background: We searched for a viral aetiology for non-small cell lung cancer (NSCLC), focusing on Merkel cell polyomavirus (MCPyV). Methods: We analysed 112 Japanese cases of NSCLC for the presence of the MCPyV genome and the expressions of RNA transcripts and MCPyV-encoded antigen. We also conducted the first analysis of the molecular features of MCPyV in lung cancers. Results: PCR revealed that 9 out of 32 squamous cell carcinomas (SCCs), 9 out of 45 adenocarcinomas (ACs), 1 out of 32 large-cell carcinomas, and 1 out of 3 pleomorphic carcinomas were positive for MCPyV DNA. Some MCPyV DNA-positive cancers expressed large T antigen (LT) RNA transcripts. Immunohistochemistry showed that MCPyV LT antigen was expressed in the tumour cells. The viral integration sites were identified in one SCC and one AC. One had both episomal and integrated/truncated forms. The other carried an integrated MCPyV genome with frameshift mutations in the LT gene. Conclusion: We have demonstrated the expression of a viral oncoprotein, the presence of integrated MCPyV, and a truncated LT gene with a preserved retinoblastoma tumour-suppressor protein-binding domain in NSCLCs. Although the viral prevalence was low, the tumour-specific molecular signatures support the possibility that MCPyV is partly associated with the pathogenesis of NSCLC in a subset of patients.