PI 3-kinases: hidden potentials revealed.

Vogt PK; Bader AG; Kang S

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PI 3-kinases: hidden potentials revealed.

机译：PI 3-激酶：揭示了潜在的潜力。

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The potential oncogenicity of PI 3-kinases is revealed by two principal mechanisms: mutations causing gain of function and overexpression of wild-type proteins. Cancer-specific mutations in PIK3CA, the gene coding for the catalytic subunit p110alpha of PI 3-kinase, are oncogenic in the animal. These mutations are therefore significant determinants of the oncogenic cellular phenotype in human tumors and are appropriate and promising targets for small molecule inhibitors. Overexpression of wild-type p110beta, gamma and delta induces oncogenic transformation in cell culture. Although these non-alpha isoforms of PI 3-kinase have not been found mutated in human cancer, deregulated expression could contribute to cellular oncogenic properties and deserves increased attention.

机译：PI 3-激酶的潜在致癌性通过两个主要机制揭示：引起功能获得的突变和野生型蛋白的过表达。 PIK3CA中的癌症特异性突变是PI 3激酶的催化亚基p110alpha编码的基因，在动物中是致癌的。因此，这些突变是人肿瘤中致癌细胞表型的重要决定因素，并且是小分子抑制剂的合适且有希望的靶标。野生型p110beta，γ和δ的过表达诱导细胞培养中的致癌转化。尽管尚未在人类癌症中发现PI 3-激酶的这些非α同工型，但表达失调可能有助于细胞致癌，并应引起更多关注。

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《Cell cycle》 |2006年第9期|共4页
作者
Vogt PK; Bader AG; Kang S;
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正文语种 eng
中图分类细胞生物学;
关键词
1-Phosphatidylinositol 3-Kinase; Cell Transformation; Neoplastic; Neoplasms; 1-磷脂酰肌醇3-激酶; 细胞转化; 肿瘤; 肿瘤;

机译：1-Phosphatidylinositol 3-Kinase;Cell Transformation;Neoplastic;Neoplasms;1-磷脂酰肌醇3-激酶;细胞转化;肿瘤;肿瘤;

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1. PI 3-kinases: hidden potentials revealed. [J] . Vogt PK, Bader AG, Kang S Cell cycle . 2006,第9期

机译：PI 3-激酶：揭示了潜在的潜力。
2. Lower Phosphoinositide 3-Kinase (PI 3-kinase) Activity and Differential Expression Levels of Selective Catalytic and Regulatory PI 3-Kinase Subunit Isoforms in Prefrontal Cortex and Hippocampus of Suicide Subjects [J] . Yogesh Dwivedi, Hooriyah S Rizavi, Tara Teppen, Neuropsychopharmacology . 2008,第10期

机译：自杀对象前额叶皮层和海马中较低的磷酸肌醇3-激酶（PI 3-激酶）活性和选择性催化和调节PI 3-激酶亚基亚型的差异表达水平
3. Diverse mechanisms activate the PI 3-kinase/mTOR pathway in melanomas: implications for the use of PI 3-kinase inhibitors to overcome resistance to inhibitors of BRAF and MEK [J] . Khanh B. Tran, Sharada Kolekar, Anower Jabed, BMC Cancer . 2021,第1期

机译：多种机制激活黑素瘤中的PI 3-激酶/ mTOR途径：对使用PI 3-激酶抑制剂的影响克服BRAF和MEK抑制剂的抗性
4. PI 3-kinase, Akt/PKB and Ras signalling pathways involved in the control of cell survival [C] . Julian Downward NATO Advanced Study Institute on Molecular Mechanisms of Signal Transduction . 2000

机译：PI 3-激酶，AKT / PKB和RAS信号传导途径涉及细胞存活的控制
5. Inositol (1,4,5) trisphosphate 3-kinase B (ItpkB) is central to thymic development by regulating Phosphoinositide 3-kinase (PI3K) downstream of mild and strong TCR signals. [D] . Sternberg, Luise. 2013

机译：肌醇（1,4,5）三磷酸3激酶B（ItpkB）通过调节轻度和强TCR信号下游的磷酸肌醇3激酶（PI3K）对胸腺发育至关重要。
6. Phosphatidylinositol (PI) 3-kinase and PI 4-kinase binding to the CD4-p56lck complex: the p56lck SH3 domain binds to PI 3-kinase but not PI 4-kinase. [O] . K V Prasad, R Kapeller, O Janssen, 1993

机译：磷脂酰肌醇（PI）3-激酶和PI 4-激酶与CD4-p56lck复合物结合：p56lck SH3域与PI 3-激酶结合但与PI 4-激酶结合。
7. PI 3-Kinases: Hidden Potentials Revealed [O] . Peter K. Vogt, Andreas G. Bader, Sohye Kang 2006

机译：PI 3-Kinases：隐藏的潜力揭示了

PI 3-kinases: hidden potentials revealed.

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