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黑色素瘤不同肿瘤进展阶段中N-和K-ras突变的分析。

Analysis of N- and K-ras mutations in the distinctive tumor progression phases of melanoma.

作者信息

Demunter A, Stas M, Degreef H, De Wolf-Peeters C, van den Oord J J

机构信息

Department of Pathology, Laboratory of Morphology and Molecular Pathology, University Hospitals, Katholieke Universiteit Leuven, Leuven, Belgium.

出版信息

J Invest Dermatol. 2001 Dec;117(6):1483-9. doi: 10.1046/j.0022-202x.2001.01601.x.

Abstract

Mutations in the ras genes are key events in the process of carcinogenesis; in particular, point mutations in codon 61 of exon 2 of the N-ras gene occur frequently in cutaneous melanoma. To investigate whether these mutations occur in early or late tumor progression phases, we searched for point mutations in the N- and K-ras genes in 69 primary cutaneous melanoma, 35 metastases, and seven nevocellular nevi in association with cutaneous melanoma. Lesions were microdissected in order to procure pure tumor samples from the distinctive growth phases of the cutaneous melanoma; the very sensitive denaturing gradient gel electrophoresis technique was used to visualize the mutations, and was followed by sequencing. Point mutations in the N-ras gene but not in the K-ras gene were detected on denaturing gradient gel electrophoresis. Twenty-three primary (33%) and nine metastatic (26%) melanomas showed bandshifts for N-ras. In the majority of cases, mutations occurring in early growth phases (i.e., the "intraepidermal" radial growth phase), were preserved in later growth phases (i.e., the invasive radial growth phase, vertical growth phase, and metastatic phase), which proves the clonal relationship between the successive growth phases. In three cases, however, the mutations differed between the distinctive growth phases within the same cutaneous melanoma, due to the occurrence of an additional mutation (especially in codon 61) in a later tumor progression phase. Our approach also permitted us to analyze the mutational status of nevi, associated with cutaneous melanoma. Six out of seven associated nevi carried the same sequence (mutated or wild-type) as the primary cutaneous melanoma, whereas in one case the sequence for N-ras differed between the primary melanoma and the associated nevus. In conclusion, this approach allowed us to demonstrate the clonal relationship between subsequent growth phases of melanoma and associated nevi; our results suggest that N-ras exon 1 mutations preferentially occur during early stages of tumor progression and hence may be involved in melanoma initiation, whereas those in N-ras exon 2 are found preferentially during later stages and hence are more probably involved in metastatic spread of cutaneous melanoma.

摘要

ras基因的突变是致癌过程中的关键事件;特别是,N-ras基因第2外显子密码子61的点突变在皮肤黑色素瘤中频繁发生。为了研究这些突变发生在肿瘤进展的早期还是晚期,我们在69例原发性皮肤黑色素瘤、35例转移瘤和7例与皮肤黑色素瘤相关的痣细胞痣中寻找N-和K-ras基因的点突变。对病变进行显微切割,以便从皮肤黑色素瘤的不同生长阶段获取纯肿瘤样本;使用非常灵敏的变性梯度凝胶电泳技术来观察突变,随后进行测序。在变性梯度凝胶电泳上检测到N-ras基因的点突变,但未检测到K-ras基因的点突变。23例原发性(33%)和9例转移性(26%)黑色素瘤显示N-ras有带移。在大多数情况下,发生在早期生长阶段(即“表皮内”放射状生长阶段)的突变在后期生长阶段(即侵袭性放射状生长阶段、垂直生长阶段和转移阶段)得以保留,这证明了连续生长阶段之间的克隆关系。然而,在3例病例中,同一皮肤黑色素瘤不同生长阶段的突变有所不同,这是由于在肿瘤进展后期出现了额外的突变(特别是密码子61)。我们的方法还使我们能够分析与皮肤黑色素瘤相关的痣的突变状态。7例相关痣中有6例与原发性皮肤黑色素瘤具有相同的序列(突变型或野生型),而在1例病例中,原发性黑色素瘤和相关痣的N-ras序列不同。总之,这种方法使我们能够证明黑色素瘤及其相关痣后续生长阶段之间的克隆关系;我们的结果表明,N-ras外显子1突变优先发生在肿瘤进展的早期阶段,因此可能参与黑色素瘤的起始,而N-ras外显子2的突变则优先出现在后期阶段,因此更可能参与皮肤黑色素瘤的转移扩散。

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