Somatic mutations in CCK2R alter receptor activity that promote oncogenic phenotypes

WillardM.D.; LajinessM.E.; WulurI.H.; FengB.; SwearingenM.L.; UhlikM.T.; KinzlerK.W.; VelculescuV.E.; Sj?blomT.; MarkowitzS.D.; PowellS.M.; VogelsteinB.; BarberT.D.

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Somatic mutations in CCK2R alter receptor activity that promote oncogenic phenotypes

机译：CCK2R中的体细胞突变改变受体活性，从而促进致癌表型。

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The roles of cholecystokinin 2 receptor (CCK2R) in numerous physiologic processes in the gastrointestinal tract and central nervous system are 'well documented. There has been some evidence that CCK2R alterations play a role in cancers, but the functional significance of these alterations for tumorigenesis is unknown. We have identified six mutations in CCK2R among a panel of 140 colorectal cancers and 44 gastric cancers. We show that these mutations increase receptor activity, activate multiple downstream signaling pathways, increase cell migration, and promote angiogenesis. Our findings suggest that somatic mutations in CCK2R may promote tumorigenesis through deregulated receptor activity and highlight the importance of evaluating CCK2R inhibitors to block both the normal and mutant forms of the receptor.

机译：胆囊收缩素2受体（CCK2R）在胃肠道和中枢神经系统的许多生理过程中的作用已得到充分证明。有证据表明CCK2R改变在癌症中起作用，但是这些改变对肿瘤发生的功能意义尚不清楚。我们已经在一组140个大肠癌和44个胃癌中鉴定出CCK2R的六个突变。我们表明这些突变增加受体活性，激活多个下游信号通路，增加细胞迁移，并促进血管生成。我们的发现表明，CCK2R中的体细胞突变可通过受体活性失调促进肿瘤发生，并强调评估CCK2R抑制剂以阻断正常和突变形式受体的重要性。

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《Molecular cancer research: MCR》 |2012年第6期|共11页
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WillardM.D.; LajinessM.E.; WulurI.H.; FengB.; SwearingenM.L.; UhlikM.T.; KinzlerK.W.; VelculescuV.E.; Sj?blomT.; MarkowitzS.D.; PowellS.M.; VogelsteinB.; BarberT.D.;
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正文语种 eng
中图分类肿瘤学;
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1. Somatic mutations in CCK2R alter receptor activity that promote oncogenic phenotypes [J] . WillardM.D., LajinessM.E., WulurI.H., Molecular cancer research: MCR . 2012,第6期

机译：CCK2R中的体细胞突变改变受体活性，从而促进致癌表型。
2. Shared sporadic and somatic thyrotropin receptor mutations display more active in vitro activities than familial thyrotropin receptor mutations. [J] . Lueblinghoff J, Eszlinger M, Jaeschke H, Thyroid: official journal of the American Thyroid Association . 2011,第3期

机译：共享的散发性和体细胞促甲状腺激素受体突变比家族性促甲状腺激素受体突变显示出更活跃的体外活性。
3. Oncogenic mutations counteract intrinsic disorder in the EGFR kinase and promote receptor dimerization [J] . Shan Y., Eastwood M.P., Zhang X., Cell . 2012,第4期

机译：致癌突变可抵消EGFR激酶中的固有疾病并促进受体二聚化
4. GERMLINE AND SOMATIC MUTATIONS OF APC GENE AND THE GENOTYPE-PHENOTYPE ANALYSIS IN FAP AND SPORADIC COLORECTAL CANCERS [C] . Xiaorong Liu, Department of Genetics, Xiangnian Shan, 第四届国际后基因组生命科学技术学术论坛 . 2006

机译：FAP和散发性大肠癌中APC基因的种系和体细胞突变以及基因型-表型分析
5. Mutational analysis of the E5 protein of human papillomavirus type 16 to analyze the role of interaction with the 16-kDa subunit of the vacuolar H(+)-ATPase in inhibiting activity of this complex and altering metabolism of the epidermal growth factor receptor. [D] . Adam, Jamie L. 2000

机译：人类乳头瘤病毒16型E5蛋白的突变分析，以分析与液泡H（+）-ATPase的16-kDa亚基相互作用在抑制该复合物活性和改变表皮生长因子受体代谢中的作用。
6. Somatic Mutations in CCK2R Alter Receptor Activity that Promote Oncogenic Phenotypes [O] . Melinda D. Willard, Mary E. Lajiness, Isabella H. Wulur, -1

机译：在CCK2R阿尔特受体活性的体细胞突变促进致癌表型
7. Somatic Mutations in CCK2R Alter Receptor Activity that Promote Oncogenic Phenotypes [O] . Melinda D. Willard, Mary E. Lajiness, Isabella H. Wulur, 2012

机译：CCK2R中的体细胞突变改变促进致癌表型的受体活性
8. Ethyl Methanesulfonate-Induced Mutations of Major Genes for Quantitative Phenotypes: Mutant Alleles for Altered Activity of Brain or Liver Enzymes in C57BL/6J Mice and Their Inheritance Across Several Generations [R] . McGarrity, L. J. 1984

机译：甲基磺酸乙酯诱导的定量表型主要基因突变：C57BL / 6J小鼠脑或肝酶改变活性的突变等位基因及其在几代中的遗传

Somatic mutations in CCK2R alter receptor activity that promote oncogenic phenotypes

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