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通过原位杂交在大鼠辐射诱导的皮肤癌中检测到的癌基因扩增。

Oncogene amplification detected by in situ hybridization in radiation-induced skin cancers in rats.

作者信息

Jin Y, Burns F J, Garte S J

机构信息

New York University Medical Center, Department of Environmental Medicine, New York 10016.

出版信息

Radiat Res. 1992 Nov;132(2):193-9.

PMID:1438701
Abstract

Amplification of the c-myc oncogene has been detected by Southern blotting in the DNA of radiation-induced skin cancers in the rat. In the current work the localization of oncogene amplification within specific cells in the different cancers and in multiple biopsies of the same cancer was studied by in situ hybridization. The amount of amplification was measured by counting grains on tissue sections hybridized in situ to biotin-labeled human c-myc third exon, rat v-H-ras, and rat v-Ki-ras probes. The in situ estimates of c-myc amplification were generally correlated with previous findings using the Southern blot method, but within each cancer only a fraction of cells exhibited amplification. Multiple biopsies of a squamous carcinoma showed amplification of v-H-ras and c-myc but not v-Ki-ras during tumor growth, but none of these oncogenes were amplified during tumor regression. The c-myc-positive cells were distributed uniformly within the cancers and exhibited a more uniform nuclear structure in comparison to the more vacuolated c-myc-negative cells. A high [3H]thymidine labeling index was found in irradiated epidermal cells on Day 7 after exposure, and yet no evidence of c-myc oncogene amplification was found in situ. No c-myc amplification was found in unirradiated normal epidermis or in irradiated epidermal cells in the vicinity of radiation-induced cancers. The data indicate that c-myc amplification is cell-specific within radiation-induced carcinomas and does not occur in epidermal cells proliferating in response to radiation exposure.

摘要

通过Southern印迹法已在大鼠辐射诱导的皮肤癌DNA中检测到c-myc癌基因的扩增。在当前工作中,通过原位杂交研究了癌基因扩增在不同癌症的特定细胞内以及同一癌症的多次活检组织中的定位。通过对与生物素标记的人c-myc第三外显子、大鼠v-H-ras和大鼠v-Ki-ras探针原位杂交的组织切片上的银粒进行计数来测量扩增量。c-myc扩增的原位估计通常与先前使用Southern印迹法的结果相关,但在每个癌症中只有一小部分细胞表现出扩增。鳞状细胞癌的多次活检显示,在肿瘤生长期间v-H-ras和c-myc扩增,但v-Ki-ras未扩增,而在肿瘤消退期间这些癌基因均未扩增。c-myc阳性细胞在癌症中均匀分布,与液泡化程度更高的c-myc阴性细胞相比,其核结构更均匀。在照射后第7天,照射的表皮细胞中发现高[3H]胸苷标记指数,但原位未发现c-myc癌基因扩增的证据。在未照射的正常表皮或辐射诱导癌症附近的照射表皮细胞中未发现c-myc扩增。数据表明,c-myc扩增在辐射诱导的癌中具有细胞特异性,并且不会在因辐射暴露而增殖的表皮细胞中发生。

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