Differential induction of autophagy in caspase-3/7 down-regulating and Bcl-2 overexpressing recombinant CHO cells subjected to sodium butyrate treatment.

Lee JS; Kim YJ; Kim CL; Lee GM

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Differential induction of autophagy in caspase-3/7 down-regulating and Bcl-2 overexpressing recombinant CHO cells subjected to sodium butyrate treatment.

机译：caspase-3 / 7下调和Bcl-2过表达的重组CHO细胞在丁酸钠处理中自噬的差异诱导。

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Previous research showed that co-down-regulation of caspase-3/7 in rCHO cells, unlike Bcl-2 overexpression, did not effectively block apoptotic cell death induced by 3mM sodium butyrate (NaBu). Here, it is found that the control of autophagy is also related to this different response to NaBu treatment. With NaBu treatment, co-down-regulation of caspase-3/7 enhanced autophagy induction, whereas Bcl-2 overexpression delayed onset of autophagy induction in a Beclin-1 independent manner. The blockage of autophagy showed a detrimental effect on cell viability even in the Bcl-2 overexpressing cells, which suggests the importance of autophagy control for successful anti-cell death engineering of rCHO cells

机译：先前的研究表明，与Bcl-2过表达不同，rCHO细胞中caspase-3 / 7的共下调不能有效阻断3mM丁酸钠（NaBu）诱导的凋亡细胞死亡。在这里，发现自噬的控制也与对NaBu处理的这种不同反应有关。用NaBu处理，共下调caspase-3 / 7增强自噬诱导，而Bcl-2过表达以Beclin-1独立的方式延迟自噬诱导的开始。自噬的阻断甚至在Bcl-2过表达的细胞中也显示出对细胞活力的有害影响，这表明自噬控制对于成功地对rCHO细胞进行抗细胞死亡工程改造的重要性

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《Journal of Biotechnology》 |2012年第1期|共8页
作者
Lee JS; Kim YJ; Kim CL; Lee GM;
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正文语种 eng
中图分类生物工程学（生物技术）;
关键词
Autophagy; Caspase-3/7; Bcl-2; Sodium butyrate; CHO cells; Beclin-1;

机译：自噬;Caspase-3 / 7;Bcl-2;丁酸钠;CHO细胞;Beclin-1;

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1. Differential induction of autophagy in caspase-3/7 down-regulating and Bcl-2 overexpressing recombinant CHO cells subjected to sodium butyrate treatment. [J] . Lee JS, Kim YJ, Kim CL, Journal of Biotechnology . 2012,第1期

机译：caspase-3 / 7下调和Bcl-2过表达的重组CHO细胞在丁酸钠处理中自噬的差异诱导。
2. Diallyl Disulfide Induces Caspase-Dependent Apoptosis via Mitochondria-Mediated Intrinsic Pathway in B16F-10 Melanoma Cells by Up-Regulating P53, Caspase-3 and Down-Regulating Pro-Inflammatory Cytokines and Nuclear Factor- xbeta-Mediated Bcl-2 Activation [J] . P. Pratheeshkumar, P. Thejass, amp, Journal of environmental pathology, toxicology and oncology: official organ of the International Society for Environmental Toxicology and Cancer . 2010,第2期

机译：二烯丙基二硫通过上调P53，Caspase-3和下调促炎性细胞因子及核因子-xbeta介导的Bcl-2激活，通过线粒体介导的B16F-10黑色素瘤细胞内源性途径诱导Caspase依赖性凋亡。
3. MSCs modifies the proliferation of leukemia MOLT-4 cells and induces their apoptosis through up-regulating Bax, caspase-3, and-8, and down-regulating Bcl-2 expression [J] . Mohaddeseh Rahbaran, Sadegh Shojaei Baghini, Mahsa Mardasi, Annals of Cancer Research and Therapy . 2021,第1期

机译：MSCS改变白血病Molt-4细胞的增殖，并通过上调节Bax，Caspase-3和-8和下调Bcl-2表达诱导它们的细胞凋亡
4. Influence of Down-regulation of Caspase-3 and CASPASE-7 by Sirnas on Sodium Butyrate-induced Apoptotic Cell Death of Chinese Hamster Ovary Cells Producing Thrombopoietin [C] . Yun Hee Sung, Soon Hye Park, Sung Hyun Kim, General Meeting of European Society of Animal Cell Technology . 2007

机译：SIRNA对丁酸钠诱导血小板诱导素诱导胁迫诱导诱导诱导诱导血管生成素的凋亡细胞死亡的影响
5. Modulation of heparan sulfate biosynthesis by sodium butyrate in recombinant CHO cells [O] . Payel Datta, Bo Yang, Robert J. Linhardt, 2015

机译：丁酸钠对重组CHO细胞中硫酸乙酰肝素生物合成的调控
6. bcl-2 and bak may play a pivotal role in sodium butyrate-induced apoptosis in colonic epithelial cells; however overexpression of bcl-2 does not protect against bak-mediated apoptosis [O] . Angela Hague, G. Darío Díaz, Diane J. Hicks, 1997

机译：Bcl-2和Bak可能在结肠上皮细胞中诱导丁酸钠诱导的凋亡中发挥枢轴作用;然而，Bcl-2的过度表达不保护Bak介导的凋亡

Differential induction of autophagy in caspase-3/7 down-regulating and Bcl-2 overexpressing recombinant CHO cells subjected to sodium butyrate treatment.

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