大肠高、中分化腺癌临床特点、遗传不稳定性、TP53与KRAS基因突变的差异比较

Comparison on Clinicopathological Features, Genetic Instability, TP53 and KRAS Gene Mutations between Well and Moderately Differentiated Colorectal Adenocarcinoma

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摘要目的:近年来大肠中分化腺癌检出比例有所增高。本研究旨在探讨大肠中分化腺癌临床病理学及分子遗传学特征。方法:回顾过去30年1073例大肠癌的病理分型,比较其中328例高、中分化腺癌临床病理学特点。激光细胞学扫描技术,双荧光高分辨率微卫星不稳定性技术评价129例大肠癌遗传不稳定性特点,TP53、KRAS基因突变采用直接测序法检测。结果:由1979年始每10年为1组,至2008年计3组。中分化腺癌所占比例分别为37%、38%及55%。其中的328例大肠癌高、中分化腺癌病理学研究表明,中分化者较高分化者病期晚、浸润深、淋巴结转移率高、静脉侵袭阳性率高。对74例高分化腺癌与55例中分化腺癌的分子遗传学研究表明,高、中分化腺癌的DNA倍体与微卫星不稳定性情况无显著性差异,TP53与KRAS基因突变频率也无显著差异。但TP53的移码突变仅在高分化腺癌中检出(4例,P<0.05)。KRAS的颠换突变在高分化癌中检出5例(23%),在中分化癌中检出12例(57%),差异有显著性意义(P<0.05)。结论:高、中分化腺癌在临床病理学特征方面存在明显差异。大肠中分化腺癌较高分化腺癌生物学行为差,发现时病期较晚,治疗随访中需要引起足够重视。两种病理学类型的肿瘤遗传不稳定性急基因突变频率等背景相似,但基因突变谱的差别提示两种腺癌的发生背景的不同。 Objective： This study is to evaluate the differences of clinicopathological and genetic features between well and moderately differentiated colorectal adenocarcinoma. Methods： A total of 1073 colorectal carcinoma cases were retrospectively reviewed to show the ratio of well and moderately differentiated adenocarcinoma in a timely fashion. The clinicopathological features of 328 well or moderately differentiated adenocarcinoma cases were evaluated. In 129 cases, Laser Scanning Cytomertery was used to assess DNA ploidy, the microsatellite instability status were studied by High Resolution Fluorescent Microsatellite Analysis assay. Mutation hotspots of TP53 and KRAS genes were directly sequenced. Results： The ratio of moderate differentiated adenocarcinoma in all pathology types was increased in the recent decade. Comparing with well differentiated adenocarcinoma, the moderately differentiated carcinoma showed more invasive characteristics, such as late stage, deeper infiltration, higher lymphatic metastatic rate, stronger vein invasion （P〈0.05）. The genetic instability patterns reflected by DNA aneuploidy or microsatellite instability of the well and moderately differentiated carcinoma were similar. The mutation rates of TP53 and KRAS genes were similar. However, frameshift mutation of TP53 was detected only in well differentiated adenocarcinoma; the frequency of trasversion mutations of KRAS were significantly higher in moderately differentiated adenocarcinoma. Conclusions：TRAIL and docetaxel have synergistlic killing effects on nasopharyngeal carcinoma CNE2 cells, which has a promising prospect in the treatment ofnasopharyngeal carcinoma.

作者赵岩郑志超挂地吉弘冲英次张涛张剑军赵宜良前原喜彦

机构地区辽宁省肿瘤医院第三外科九州大学大学院医学研究院消化器综合外科

出处《现代生物医学进展》 CAS 2010年第6期1061-1064,共4页 Progress in Modern Biomedicine

关键词大肠癌高分化腺癌中分化腺癌遗传不稳定性突变 Colorectal neoplasms Moderately differentiated adenocarcinoma Well differentiated adenocarcinoma Genetic Instabil-ity Mutation

分类号 R735.34 [医药卫生—肿瘤]

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1赵岩,张涛,郑志超,张剑军,赵宜良,前原喜彦.直结肠癌BUBR1的过度表达与TP53突变及微卫星状态关系提示其过度表达与染色体不稳定表型有关(英文)[J].现代生物医学进展,2008,8(8):1401-1405. 被引量：1

二级参考文献22

1Lengauer C, Kinzler KW, Vogelstein B. Genetic instability in colorectal cancers [J]. Nature, 1997, 386( 6625 ): 623-627.
2Lengauer C, Kinzler KW, Vogelstein B. Genetic instabilities in human cancers [J]. Nature, 1998, 396(6712): 643-649.
3Bharadwaj R, Yu H. The spindle checkpoint, aneuploidy, and cancer [J]. Oneogene, 2004, 23( 11 ): 2016-2027.
4Lampson MA, Kapoor TM. The human mitotic checkpoint protein BubRl regulates chromosome-spindle attachments [J]. Nat Cell Biol, 2005, 7(1 ): 93-98.
5Chen R-H, BubR1 is essential for kinetochore localization of other spindle checkpoint proteins and its phosphorylation requires Madl [J].J. Cell Biol., 2002, 158(3): 487-496.
6Shin H-J, Baek K-H, Jeon A-H, et al. Dual roles of human BubR1, a mitotic checkpoint kinase, in the monitoring of chromosomal instability [J]. Cancer Cell, 2003, 4 (6): 483-497.
7Fang Y, Liu T, Wang X, et al. BubR1 is involved in regulation of DNA damage responses [J]. Oncogene, 2006, 25(25 ): 3598-3605.
8Hanks S, Coleman K, Reid S, et al. Constitutional aneuploidy and cancer predisposition caused by biallelic mutations in BUB1B [J]. Nat Genet, 2004, 36 ( 11 ): 1159-1161.
9Matsuura S, Matsumoto Y, Morishima K-i, et al. Monoallelic BUB1B mutations and defective mitotic-spindle checkpoint in seven families with premature chromatid separation (PCS) syndrome [J]. American Journal of Medical Genetics, 2006, 140A(4): 358-367.
10Yamamoto Y, Matsuyama H, Chochi Y, et al., Overexpression of BUBR1 is associated with chromosomal instability in bladder cancer [J]. Cancer Genet Cytogenet, 2007, 174( 1 ): 42-47.

1丁秀杰,张睿.CD44基因在结肠癌组织中的表达及其意义[J].现代肿瘤医学,2014,22(6):1363-1365. 被引量：6
2卞美璐,连利娟.妇科肿瘤遗传研究进展[J].国外医学（妇产科学分册）,1990,17(1):1-3. 被引量：3
3刘庆庚.恶性肿瘤遗传因素探讨[J].锦州医学院学报,1992,13(5):73-73.
4孙洁宁,陈仁彪.肿瘤遗传基础研究的进展[J].上海第二医科大学学报,1992,12(3):263-269.
5罗学宏,王骏.防范大肠癌筛查是关键[J].家庭医学（上半月）,2015,30(10):21-21. 被引量：1
6巫协宁.胰腺癌和壶腹癌的分子机制[J].国外医学（消化系疾病分册）,1997,17(4):225-228.
7肖文华,刘为纹,吕有勇,李诤.肝细胞癌抑癌基因p53突变[J].新消化病学杂志,1997,5(9):573-574. 被引量：10
8王凤军,鲁明良.直肠癌静脉侵袭的临床研究[J].中国肛肠病杂志,1998,18(6):10-12.
9王凤军,董新舒,赵家宏,罗开秀,罗绪珍,唐桂春.直肠癌静脉侵袭的临床病理学研究[J].实用肿瘤学杂志,1996,10(1):18-20. 被引量：4
10郑鑫,郑华川,赵恩宏,肖丽君,赵爽,杨宗伟.CD147在胃肠道癌中的表达及意义[J].承德医学院学报,2014,31(3):187-189. 被引量：2

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大肠高、中分化腺癌临床特点、遗传不稳定性、TP53与KRAS基因突变的差异比较

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