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多阶段甲状腺肿瘤发生过程中核癌基因的结构与表达

Structure and expression of nuclear oncogenes in multi-stage thyroid tumorigenesis.

作者信息

Wyllie F S, Lemoine N R, Williams E D, Wynford-Thomas D

机构信息

CRC Thyroid Tumour Biology Research Group, Department of Pathology, University of Wales College of Medicine, Cardiff, UK.

出版信息

Br J Cancer. 1989 Oct;60(4):561-5. doi: 10.1038/bjc.1989.313.

Abstract

We have investigated the possibility that structural alterations of the 'nuclear' oncogene family (c-myc, N-myc, L-myc, fos, myb and p53) leading to aberrant expression might, as in several other tumour types, play a role in the multi-stage development of tumorigenesis in the human thyroid follicular cell. Direct analysis of expression by slot and Northern blot RNA hybridisation showed that normal thyroid expresses surprisingly high levels of fos, and to a lesser extent c-myc, c-myc expression was markedly increased in all tumours, both benign and malignant, but no increase was seen in any other nuclear oncogene. fos expression was reduced specifically in one type of malignant tumour-follicular carcinoma-in inverse correlation with differentiation. Southern blot analysis showed no evidence of rearrangement or amplification of c-myc, or of any other 'nuclear' oncogene in any thyroid tumour. We conclude that there is no evidence that a primary abnormality of these genes plays a role in thyroid follicular cell tumorigenesis and suggest that the observed changes in expression can be adequately explained as secondary consequences of the tumour phenotype.

摘要

我们研究了“核”癌基因家族(c-myc、N-myc、L-myc、fos、myb和p53)的结构改变导致异常表达的可能性,这种异常表达可能像在其他几种肿瘤类型中一样,在人类甲状腺滤泡细胞肿瘤发生的多阶段发展中起作用。通过狭缝杂交和Northern印迹RNA杂交对表达进行的直接分析表明,正常甲状腺组织中fos的表达水平出奇地高,c-myc的表达水平相对较低。在所有肿瘤(包括良性和恶性肿瘤)中,c-myc的表达均显著增加,但在任何其他核癌基因中均未观察到增加。在一种恶性肿瘤——滤泡癌中,fos的表达特异性降低,且与分化呈负相关。Southern印迹分析表明,在任何甲状腺肿瘤中均未发现c-myc或任何其他“核”癌基因发生重排或扩增。我们得出结论,没有证据表明这些基因的原发性异常在甲状腺滤泡细胞肿瘤发生中起作用,并认为观察到的表达变化可以充分解释为肿瘤表型的继发性后果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bcf3/2247101/70d0628786e1/brjcancer00120-0060-a.jpg

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