Zauber Peter, Marotta Stephen P, Sabbath-Solitare Marlene
Department of Medicine, Saint Barnabas Medical Center 100 Old Short Hills Road, Livingston, NJ 07039, USA.
Department of Pathology, Saint Barnabas Medical Center 100 Old Short Hills Road, Livingston, NJ 07039, USA.
Int J Mol Epidemiol Genet. 2016 Mar 23;7(1):24-31. eCollection 2016.
Mutations of the gene GNAS have been shown to activate the adenylate cyclase gene and lead to constitutive cAMP signaling. Several preliminary reports have suggested a role for GNAS gene mutations during colorectal carcinogenesis, particularly mucinous carcinomas. The aim of this study was to clarify the incidence of GNAS mutations in adenomas (tubular, tubulovillous, and villous), carcinomas with residual adenoma, and carcinomas, and to relate these findings to mutations of the KRAS gene and to the mucinous status of the tumors. We used standard PCR techniques and direct gene sequencing to evaluate tumors for gene mutations. No GNAS mutations were identified in 25 tubular adenomas, but were present in 6.4% of tubulovillous adenomas and 11.2% of villous adenomas. A GNAS mutation was found in 9.7% of the benign portion of carcinoma with residual adenoma, but in none of 86 carcinomas. A similar trend was seen for KRAS mutation across the five groups of tumors. GNAS mutations may function as an important driver mutation during certain phases of colorectal carcinogenesis, but may then be lost once the biological advantage gained by the mutated gene is no longer necessary to sustain or advance tumor development.
已证实基因GNAS的突变可激活腺苷酸环化酶基因并导致组成性cAMP信号传导。一些初步报告表明GNAS基因突变在结直肠癌发生过程中发挥作用,尤其是在黏液腺癌中。本研究的目的是阐明GNAS突变在腺瘤(管状、管状绒毛状和绒毛状)、伴有残留腺瘤的癌以及癌中的发生率,并将这些发现与KRAS基因的突变以及肿瘤的黏液状态相关联。我们使用标准PCR技术和直接基因测序来评估肿瘤的基因突变情况。在25例管状腺瘤中未发现GNAS突变,但在6.4%的管状绒毛状腺瘤和11.2%的绒毛状腺瘤中存在该突变。在伴有残留腺瘤的癌的良性部分中,9.7%发现有GNAS突变,但在86例癌中均未发现。在五组肿瘤中,KRAS突变也呈现出类似趋势。GNAS突变可能在结直肠癌发生的某些阶段作为重要的驱动突变发挥作用,但一旦突变基因所获得的生物学优势不再是维持或促进肿瘤发展所必需的,该突变可能就会丢失。
