4.8 Article

Improved detection suggests all Merkel cell carcinomas harbor Merkel polyomavirus

Journal

JOURNAL OF CLINICAL INVESTIGATION
Volume 122, Issue 12, Pages 4645-4653

Publisher

AMER SOC CLINICAL INVESTIGATION INC
DOI: 10.1172/JCI64116

Keywords

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Funding

  1. Claudia Adams Barr Program in Innovative Basic Cancer Research at the Dana-Farber Cancer Institute
  2. DF/HCC Development Award
  3. Skin Cancer SPORE [P50 CA93683]
  4. Fundacion Caja Madrid, Spain
  5. Eilian Family Research Fund for Merkel Cell Carcinoma at the Dana-Farber Cancer Institute

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A human polyomavirus was recently discovered in Merkel cell carcinoma (MCC) specimens. The Merkel cell polyomavirus (MCPyV) genome undergoes clonal integration into the host cell chromosomes of MCC tumors and expresses small T antigen and truncated large T antigen. Previous studies have consistently reported that MCPyV can be detected in approximately 80% of all MCC tumors. We sought to increase the sensitivity of detection of MCPyV in MCC by developing antibodies capable of detecting large T antigen by immunohistochemistry. In addition, we expanded the repertoire of quantitative PCR primers specific for MCPyV to improve the detection of viral DNA in MCC. Here we report that a novel monoclonal antibody detected MCPyV large T antigen expression in 56 of 58 (97%) unique MCC tumors. PCR analysis specifically detected viral DNA in all 60 unique MCC tumors tested. We also detected inactivating point substitution mutations of TP53 in the two MCC specimens that lacked large T antigen expression and in only 1 of 56 tumors positive for large T antigen. These results indicate that MCPyV is present in MCC tumors more frequently than previously reported and that mutations in TP53 tend to occur in MCC tumors that fail to express MCPyV large T antigen.

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