Hec1 overexpression hyperactivates the mitotic checkpoint and induces tumor formation in vivo

机译：Hec1过表达在体内过度激活有丝分裂检查点并诱导肿瘤形成

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摘要

Hec1 (Highly Expressed in Cancer 1) is one of four proteins of the outer kinetochore Ndc80 complex involved in the dynamic interface between centromeres and spindle microtubules. Its overexpression is seen in a variety of human tumors and correlates with tumor grade and prognosis. We show here that the overexpression of Hec1 in an inducible mouse model results in mitotic checkpoint hyperactivation. As previously observed with overexpression of the Mad2 gene, hyperactivation of the mitotic checkpoint leads to aneuploidy in vitro and is sufficient to generate tumors in vivo that harbor significant levels of aneuploidy. These results underscore the role of chromosomal instability as a result of mitotic checkpoint hyperactivation in the initiation of tumorigenesis.

机译：Hec1（在癌症1中高度表达）是外部着丝粒Ndc80复合体的四种蛋白质之一，其参与着丝粒和纺锤体微管之间的动态界面。在多种人类肿瘤中均可见其过度表达，并与肿瘤的分级和预后相关。我们在这里显示，Hec1在诱导型小鼠模型中的过表达导致有丝分裂检查点过度激活。如先前在Mad2基因的过表达中观察到的，有丝分裂检查点的过度活化导致体外非整倍性，并且足以在体内产生具有显着水平的非整倍性的肿瘤。这些结果强调了有丝分裂检查点过度活化导致的染色体不稳定在肿瘤发生中的作用。

著录项

期刊名称 Proceedings of the National Academy of Sciences of the United States of America
作者
Elena Diaz-Rodríguez; Rocio Sotillo; Juan-Manuel Schvartzman; Robert Benezra;
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作者单位

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年(卷),期 2008(105),43
年度 2008
页码 16719–16724
总页数 6
原文格式 PDF
正文语种
中图分类
关键词
aneuploidy cancer chromosome instability;

机译：非整倍性;癌症;染色体不稳定;

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专利

1. Hec1 Overexpression Hyperactivates The Mitotic Checkpoint And Induces Tumor Formation In Vivo [J] . Elena Diaz-Rodriguez, Rocio Sotillo, Juan-Manuel Schvartzman, Proceedings of the National Academy of Sciences of the United States of America . 2008,第43期

机译：Hec1过表达可激活有丝分裂检查点并体内诱导肿瘤形成
2. Expression analysis of mitotic spindle checkpoint genes in breast carcinoma: role of NDC80/HEC1 in early breast tumorigenicity, and a two-gene signature for aneuploidy [J] . Ivan Bièche, Sophie Vacher, Fran?ois Lallemand, Molecular Cancer . 2011,第1期

机译：乳腺癌中有丝分裂纺锤体检查点基因的表达分析：NDC80 / HEC1在早期乳腺癌致瘤性中的作用以及非整倍性的两个基因标记
3. Overexpression of the dynein light chain km23-1 in human ovarian carcinoma cells inhibits tumor formation in vivo and causes mitotic delay at prometaphase/metaphase. [J] . Pulipati NR, Jin Q, Liu X, International Journal of Cancer =: Journal International du Cancer . 2011,第3期

机译：动力蛋白轻链km23-1在人卵巢癌细胞中的过度表达抑制了体内肿瘤的形成，并导致前中期/中期的有丝分裂延迟。
4. SET/I2PP2A Overexpression in a Normal Oral Keratinocyte (NOK-SI) Cell Lineage Induces Cell Transformation with Tumorigenic Phenotype [C] . Lays Martin Sobral, Ricardo Coletta, Carlos Curti, Molecular Medicine TRI-CON. . 2014

机译：在正常口腔角质形成细胞（NOK-Si）细胞谱系中设置/ I2PP2A过表达诱导致瘤表型细胞转化
5. Alternative receptor tyrosine kinase signalling in mammary tumors induced by transgenic IGF-IR overexpression. [D] . Campbell, Craig Ian. 2011

机译：转基因IGF-IR过表达诱导的乳腺肿瘤中的替代受体酪氨酸激酶信号传导。
6. Expression analysis of mitotic spindle checkpoint genes in breast carcinoma: role of NDC80/HEC1 in early breast tumorigenicity and a two-gene signature for aneuploidy [O] . Ivan Bièche, Sophie Vacher, François Lallemand, 2011

机译：乳腺癌中有丝分裂纺锤体检查点基因的表达分析：NDC80 / HEC1在早期乳腺癌致瘤性中的作用以及非整倍性的两个基因标记
7. Hec1 overexpression hyperactivates the mitotic checkpoint and induces tumor formation in vivo [O] . Diaz-Rodríguez, Elena, Sotillo, Rocio, Schvartzman, Juan-Manuel, 2008

机译：Hec1过表达在体内过度激活有丝分裂检查点并诱导肿瘤形成

Hec1 overexpression hyperactivates the mitotic checkpoint and induces tumor formation in vivo

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