C-myc oncogene expression in human melanoma and its relationship with tumour antigenicity
被引:25
作者:
Grover, R
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机构:MT VERNON HOSP,DEPT HISTOPATHOL,NORTHWOOD HA6 2RN,MIDDLESEX,ENGLAND
Grover, R
Ross, DA
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机构:MT VERNON HOSP,DEPT HISTOPATHOL,NORTHWOOD HA6 2RN,MIDDLESEX,ENGLAND
Ross, DA
Richman, PI
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机构:MT VERNON HOSP,DEPT HISTOPATHOL,NORTHWOOD HA6 2RN,MIDDLESEX,ENGLAND
Richman, PI
Robinson, B
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机构:MT VERNON HOSP,DEPT HISTOPATHOL,NORTHWOOD HA6 2RN,MIDDLESEX,ENGLAND
Robinson, B
Wilson, GD
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机构:MT VERNON HOSP,DEPT HISTOPATHOL,NORTHWOOD HA6 2RN,MIDDLESEX,ENGLAND
Wilson, GD
机构:
[1] MT VERNON HOSP,DEPT HISTOPATHOL,NORTHWOOD HA6 2RN,MIDDLESEX,ENGLAND
[2] MT VERNON HOSP,CRC,GRAY LAB,NORTHWOOD HA6 2RN,MIDDLESEX,ENGLAND
来源:
EUROPEAN JOURNAL OF SURGICAL ONCOLOGY
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1996年
/
22卷
/
04期
关键词:
melanoma;
antigen;
oncogene;
D O I:
10.1016/S0748-7983(96)90154-7
中图分类号:
R73 [肿瘤学];
学科分类号:
100214 ;
摘要:
Melanoma produces specific tumour antigens which are capable of eliciting an immune response. However, this tumour evades the immune system, in part, by downregulation of class I HLA antigens on the cell surface,, which are required for T cell recognition. It has been suggested that the oncogene c-myc may have a role in effecting this change in vitro, however, the relationship between oncoprotein level and tumour antigenicity has not been established in human tumours. This study measured c-myc oncoprotein in 94 melanoma specimens (46 primary tumours and 48 regional metastases) using flow cytometry and evaluated class I HLA expression with immunohistochemistry. C-myc expression was found in 91 tumours (96%) with higher expression in metastases than primary melanomas (P<0.005). Class I HLA expression was found to show great variation although metastases showed less antigenicity than primary tumours (P<0.01). Analysis of the relationship between these two parameters revealed a highly significant correlation in both primary (P<0.01) and metastatic disease (P<0.01), with high oncoprotein being associated with down regulation of cell surface antigens. Knowledge of the control of tumour antigenicity is likely to provide an objective platform for the development of new strategies for immunotherapy.