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Cell division cycle‐associated protein 1 as a new melanoma‐associated antigen
Authors:Aki Tokuzumi  Satoshi Fukushima  Azusa Miyashita  Satoshi Nakahara  Yosuke Kubo  Junji Yamashita  Miho Harada  Kayo Nakamura  Ikko Kajihara  Masatoshi Jinnin  Hironobu Ihn
Affiliation:Department of Dermatology and Plastic Surgery, Faculty of Life Sciences, Kumamoto University, Kumamoto, Japan
Abstract:Immune checkpoint inhibitors have increased the median survival of melanoma patients. To improve their effects, antigen‐specific therapies utilizing melanoma‐associated antigens should be developed. Cell division cycle‐associated protein 1 (CDCA1), which has a specific function at the kinetochores for stabilizing microtubule attachment, is overexpressed in various cancers. CDCA1, which is a member of cancer–testis antigens, does not show detectable expression levels in normal tissues. Quantitative reverse transcription polymerase chain reaction and immunoblotting analyses revealed that CDCA1 was expressed in all of the tested melanoma cell lines, 74% of primary melanomas, 64% of metastatic melanomas and 25% of nevi. An immunohistochemical analysis and a Cox proportional hazards model showed that CDCA1 could be a prognostic marker in malignant melanoma (MM) patients. CDCA1‐specific siRNA inhibited the cell proliferation of SKMEL2 and WM115 cells, but did not reduce the migration or invasion activity. These results suggest that CDCA1 may be a new therapeutic target of melanoma.
Keywords:cancer–  testis antigen  cell division cycle‐associated protein 1  immunotherapy  melanoma  NDC80 kinetochore complex component
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