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具有非息肉样生长特征的结直肠癌的病理特征和基因改变

Pathological features and genetic alterations in colorectal carcinomas with characteristics of nonpolypoid growth.

作者信息

Kaneko K, Kurahashi T, Makino R, Konishi K, Ito H, Katagiri A, Kumekawa Y, Hirayama Y, Yoneyama K, Kushima M, Kusano M, Tajiri H, Rembacken B J, Mitamura K, Imawari M

机构信息

Second Department of Internal Medicine, Showa University School of Medicine, Tokyo, Japan.

出版信息

Br J Cancer. 2004 Jul 19;91(2):312-8. doi: 10.1038/sj.bjc.6601965.

Abstract

We sought to clarify pathological features and genetic alterations in colorectal carcinomas with characteristics of nonpolypoid growth. Colorectal carcinomas resected at Showa University Hospital in Tokyo included 86 with characteristics of polypoid growth (PG) and 21 with those of nonpolypoid growth (NPG). Mutations of APC, Ki-ras, and p53 genes, as well as microsatellite instability (MSI), were analysed using fluorescence-based polymerase chain reaction-single-strand conformation polymorphism (PCR-SSCP). Carcinomas with an NPG pattern were smaller than PG tumours (P<0.0001). Carcinomas with a PG pattern were more likely to harbour Ki-ras mutations (36%) than NPG tumours (0%; P<0.0001). Mutation types in the APC gene differed significantly between PG and NPG carcinomas (P=0.0189), including frameshift mutations in 66% of PG carcinomas but no NPG carcinomas. Presence of a p53 mutation at a 'hot spot' also was more likely in PG carcinomas (37%) than in NPG carcinomas (0%; P=0.0124). No significant difference in presence of MSI was evident between carcinomas with PG and NPG patterns. In conclusion, significant genetic differences were evident between carcinomas with PG and NPG patterns. Genetic changes in NPG carcinomas differed from those of the conventional adenoma-carcinoma sequence. Assuming that some nonpolypoid growth lesions transform rapidly into advanced carcinomas, 20% of all colorectal carcinomas may progress in this manner.

摘要

我们试图阐明具有非息肉样生长特征的结直肠癌的病理特征和基因改变。东京昭和大学医院切除的结直肠癌中,86例具有息肉样生长(PG)特征,21例具有非息肉样生长(NPG)特征。使用基于荧光的聚合酶链反应-单链构象多态性(PCR-SSCP)分析APC、Ki-ras和p53基因的突变以及微卫星不稳定性(MSI)。具有NPG模式的癌肿比PG肿瘤小(P<0.0001)。具有PG模式的癌肿比NPG肿瘤更易发生Ki-ras突变(36%对0%;P<0.0001)。PG和NPG癌肿之间APC基因的突变类型有显著差异(P=0.0189),包括66%的PG癌肿有移码突变,而NPG癌肿无此突变。PG癌肿中“热点”处p53突变的发生率也高于NPG癌肿(37%对0%;P=0.0124)。PG和NPG模式的癌肿之间MSI的存在无显著差异。总之,PG和NPG模式的癌肿之间存在明显的基因差异。NPG癌肿的基因变化不同于传统腺瘤-癌序列的变化。假设一些非息肉样生长病变迅速转变为进展期癌肿,那么所有结直肠癌中可能有20%以这种方式进展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0d45/2409809/0de46ce8989b/91-6601965f1.jpg

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