Targeting mitotic exit leads to tumor regression in vivo: Modulation by Cdk1, Mastl, and the PP2A/B55alpha,delta phosphatase.

Manchado E; Guillamot M; de Carcer G; Eguren M; Trickey M; Garcia Higuera I; Moreno S; Yamano H; Canamero M; Malumbres M

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Targeting mitotic exit leads to tumor regression in vivo: Modulation by Cdk1, Mastl, and the PP2A/B55alpha,delta phosphatase.

机译：靶向有丝分裂退出导致体内肿瘤消退：由Cdk1，Mastl和PP2A / B55alpha，δ磷酸酶调节。

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Targeting mitotic exit has been recently proposed as a relevant therapeutic approach against cancer. By using genetically engineered mice, we show that the APC/C cofactor Cdc20 is essential for anaphase onset in vivo in embryonic or adult cells, including progenitor/stem cells. Ablation of Cdc20 results in efficient regression of aggressive tumors, whereas current mitotic drugs display limited effects. Yet, Cdc20 null cells can exit from mitosis upon inactivation of Cdk1 and the kinase Mastl (Greatwall). This mitotic exit depends on the activity of PP2A phosphatase complexes containing B55alpha or B55delta regulatory subunits. These data illustrate the relevance of critical players of mitotic exit in mammals and their implications in the balance between cell death and mitotic exit in tumor cells.

机译：最近提出了靶向有丝分裂出口作为针对癌症的相关治疗方法。通过使用基因工程小鼠，我们显示APC / C辅因子Cdc20对于胚胎或成年细胞（包括祖细胞/干细胞）体内体内后期后期发作是必不可少的。 Cdc20的消融导致侵袭性肿瘤的有效消退，而目前的有丝分裂药物显示有限的作用。然而，在Cdk1和激酶Mastl（Greatwall）失活后，Cdc20空细胞可以退出有丝分裂。这种有丝分裂退出取决于包含B55alpha或B55delta调节亚基的PP2A磷酸酶复合物的活性。这些数据说明了哺乳动物中有丝分裂退出的关键参与者的相关性及其对肿瘤细胞中细胞死亡和有丝分裂退出之间平衡的影响。

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《Cancer Cell》 |2010年第6期|共14页
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Manchado E; Guillamot M; de Carcer G; Eguren M; Trickey M; Garcia Higuera I; Moreno S; Yamano H; Canamero M; Malumbres M;
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正文语种 eng
中图分类肿瘤学;
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入库时间 2022-08-18 09:16:22

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1. Targeting mitotic exit leads to tumor regression in vivo: Modulation by Cdk1, Mastl, and the PP2A/B55alpha,delta phosphatase. [J] . Manchado E, Guillamot M, de Carcer G, Cancer Cell . 2010,第6期

机译：靶向有丝分裂退出导致体内肿瘤消退：由Cdk1，Mastl和PP2A / B55alpha，δ磷酸酶调节。
2. Targeting mitotic exit in solid tumors [J] . Christine Greil, Ralph W?sch, Julia Felthaus, American Journal of Cancer Research . 2021,第7期

机译：靶向实体瘤中的丝分裂出口
3. Tumor regression and modulation of gene expression via tumor-targeted tocotrienol niosomes [J] . Tan Doryn Meam-Yee, Fu Ju-Yen, Wong Fu-Shun, Nanomedicine . 2017,第20期

机译：肿瘤回归和基因表达的调节通过肿瘤靶向TOCOTRINOR NIOSOMES
4. Regulation of mitotic entry and exit by the interaction of PP2A:B56delta and Cdc25C. [D] . Forester, Craig Michael. 2007

机译：PP2A：B56delta和Cdc25C的相互作用调节有丝分裂的进入和退出。
5. Control of mitotic exit by PP2A regulation of Cdc25C and Cdk1 [O] . Craig M. Forester, Jessica Maddox, Justin V. Louis, 2007

机译：通过PP2A调节Cdc25C和Cdk1来控制有丝分裂出口
6. Targeting mitotic exit leads to tumor regression in vivo: Modulation by Cdk1, Mastl, and the PP2A/B55α,δ phosphatase [O] . Manchado, Eusebio, Guillamot, María, García-Higuera, Irene, 2012

机译：靶向有丝分裂出口可导致体内肿瘤消退：Cdk1，Mastl和PP2A /B55α，δ磷酸酶的调控

Targeting mitotic exit leads to tumor regression in vivo: Modulation by Cdk1, Mastl, and the PP2A/B55alpha,delta phosphatase.

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