Extra c-myc oncogene copies in high risk cutaneous malignant melanoma and melanoma metastases

黑色素瘤 癌症研究 等色体 荧光原位杂交 生物 癌基因 基因座(遗传学) 基因 结节性黑色素瘤 基因复制 染色体 病理 分子生物学 细胞周期 医学 核型 遗传学
作者
G Kraehn,Jochen Utikal,Martin Udart,K.M. Greulich,G. Bezold,Peter Kaskel,Ulrike Leiter,R. U. Peter
出处
期刊:British Journal of Cancer [Springer Nature]
卷期号:84 (1): 72-79 被引量:129
标识
DOI:10.1054/bjoc.2000.1535
摘要

Amplification and overexpression of the c-myc gene have been associated with neoplastic transformation in a plethora of malignant tumours. We applied interphase fluorescence in situ hybridization (FISH) with a locus-specific probe for the c-myc gene (8q24) in combination with a corresponding chromosome 8 alpha-satellite probe to evaluate genetic alterations in 8 primary melanomas and 33 advanced melanomas and compared it to 12 melanocytic nevi, 7 safety margins and 2 cases of normal skin. Additionally, in metaphase spreads of 7 melanoma cell lines a whole chromosome 8 paint probe was used. We investigated the functionality of the c-myc gene by detecting c-myc RNA expression with RT-PCR and c-myc protein by immunohistochemistry. 4/8 primary melanomas and 11/33 melanoma metastases showed additional c-myc signals relative to the centromere of chromosome 8 copy number. None of the nevi, safety margins or normal skin samples demonstrated this gain. In 2/7 melanoma cell lines (C32 and WM 266-4) isochromosome 8q formation with a relative gain of c-myc copies and a loss of 8p was observed. The highest c-myc gene expression compared to GAPDH was found in melanoma metastases (17.5%). Nevi (6.6%) and primary melanomas (5.0%) expressed the c-myc gene on a lower level. 72.7% of the patients with c-myc extra copies had visceral melanoma metastases (UICC IV), patients without c-myc gain in 35.0% only. The collective with additional c-myc copies also expressed the gene on a significantly higher level. These results indicate that a c-myc gain in relation to the centromere 8 copy number might be associated with advanced cutaneous melanoma.

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