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小鼠皮肤乳头瘤中非整倍体、角蛋白修饰和γ-谷氨酰转移酶表达的顺序性发展。

Sequential development of aneuploidy, keratin modifications, and gamma-glutamyltransferase expression in mouse skin papillomas.

作者信息

Aldaz C M, Conti C J, Larcher F, Trono D, Roop D R, Chesner J, Whitehead T, Slaga T J

机构信息

University of Texas System Cancer Center, Research Division, Smithville 78957.

出版信息

Cancer Res. 1988 Jun 1;48(11):3253-7.

PMID:2452689
Abstract

To elucidate the role and timing of expression of different premalignant and malignant markers in tumor promotion, we correlated alterations in keratin patterns and gamma-glutamyltransferase (GGT) expression with the chromosomal status of individual mouse skin papillomas. Papillomas were induced by 7,12-dimethylbenz[a]anthracene initiation and 12-O-tetradecanoylphorbol-13-acetate promotion. Individual tumors were randomly sampled at 20 and 35 weeks of promotion. Each tumor was cytogenetically analyzed and serial paraffin sections were used for GGT detection, immunoblotting, and immunohistochemistry studies. Monospecific antibodies elicited against keratins K1 (Mr 67,000) and K14 (Mr 55,000) were used to analyze keratin modifications. Most tumors at 20 weeks of promotion, although exhibiting aneuploidy, still presented high levels of the K1 differentiation-associated keratin. Later during promotion those tumors bearing the highest aneuploidy indexes were those that showed a marked decrease in or absence of the K1 protein. Furthermore, those same tumors with the highest levels of genomic alterations also exhibited foci of GGT activity. These results support the idea that the majority of papillomas under continuous promotion are progressing toward malignancy. Aneuploidy seems to precede detectable keratin modifications, and GGT activity appears to be the latest marker to be expressed.

摘要

为了阐明不同癌前和恶性标志物在肿瘤促进过程中的表达作用及时间,我们将角蛋白模式和γ-谷氨酰转移酶(GGT)表达的改变与单个小鼠皮肤乳头瘤的染色体状态相关联。乳头瘤通过7,12-二甲基苯并[a]蒽启动和12-O-十四烷酰佛波醇-13-乙酸酯促进诱导产生。在促进的第20周和第35周对单个肿瘤进行随机取样。对每个肿瘤进行细胞遗传学分析,并使用连续石蜡切片进行GGT检测、免疫印迹和免疫组织化学研究。使用针对角蛋白K1(分子量67,000)和K14(分子量55,000)产生的单特异性抗体来分析角蛋白修饰。在促进的第20周,大多数肿瘤尽管表现出非整倍体,但仍呈现高水平的与K1分化相关的角蛋白。在促进后期,那些非整倍体指数最高的肿瘤是那些K1蛋白显著减少或缺失的肿瘤。此外,那些基因组改变水平最高的相同肿瘤也表现出GGT活性灶。这些结果支持这样的观点,即持续促进下的大多数乳头瘤正在向恶性发展。非整倍体似乎先于可检测到的角蛋白修饰出现,而GGT活性似乎是最后表达的标志物。

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