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蛋白激酶 Cepsilon 通过 bad 磷酸化和调节 TNFalpha/JNK 通路调节前列腺癌细胞的存活。

Regulation of prostate cancer cell survival by protein kinase Cepsilon involves bad phosphorylation and modulation of the TNFalpha/JNK pathway.

机构信息

Department of Pharmacology, University of Pennsylvania School of Medicine, Philadelphia, Pennsylvania 19104-6160, USA.

出版信息

J Biol Chem. 2010 Aug 20;285(34):26033-40. doi: 10.1074/jbc.M110.128371. Epub 2010 Jun 21.

DOI:10.1074/jbc.M110.128371
PMID:20566643
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2924002/
Abstract

Protein kinase Cepsilon (PKCepsilon), a diacyglycerol- and phorbol ester-responsive serine-threonine kinase, has been implicated in mitogenic and survival control, and it is markedly overexpressed in human tumors, including in prostate cancer. Although prostate cancer cells undergo apoptosis in response to phorbol ester stimulation via PKCdelta-mediated release of death factors, the involvement of PKCepsilon in this response is not known. PKCepsilon depletion by RNAi or expression of a dominant negative kinase-dead PKCepsilon mutant potentiated the apoptotic response of PMA and sensitized LNCaP cells to the death receptor ligand TNFalpha. On the other hand, overexpression of PKCepsilon by adenoviral means protected LNCaP cells against apoptotic stimuli. Interestingly, PKCepsilon RNAi depletion significantly enhanced the release of TNFalpha in response to PMA and greatly potentiated JNK activation by this cytokine. Further mechanistic analysis revealed that PMA fails to promote phosphorylation of Bad in Ser(112) in PKCepsilon-depleted LNCaP cells, whereas PKCepsilon overexpression greatly enhanced Bad phosphorylation. This effect was independent of Akt, ERK, or p90Rsk, well established kinases for Ser(112) in Bad. Moreover, expression of a S112A-Bad mutant potentiated PMA-induced apoptosis. Finally, we found that upon activation PKCepsilon accumulated in mitochondrial fractions in LNCaP cells and that Bad was a substrate of PKCepsilon in vitro. Our results established that PKCepsilon modulates survival in prostate cancer cells via multiple pathways.

摘要

蛋白激酶 C ɛ(PKCɛ)是一种二酰基甘油和佛波酯反应性丝氨酸/苏氨酸激酶,已被牵涉到有丝分裂和存活控制中,并且在包括前列腺癌在内的人类肿瘤中明显过表达。尽管前列腺癌细胞通过 PKCδ介导的死亡因子释放对佛波酯刺激产生细胞凋亡,但 PKCɛ在该反应中的参与情况尚不清楚。通过 RNAi 耗竭 PKCɛ或表达显性失活激酶的 PKCɛ突变体,增强了 PMA 诱导的前列腺癌细胞凋亡反应,并使 LNCaP 细胞对死亡受体配体 TNFα敏感。另一方面,通过腺病毒表达过表达 PKCɛ可保护 LNCaP 细胞免受凋亡刺激。有趣的是,PKCɛ RNAi 耗竭显著增强了 PMA 诱导的 TNFα释放,并大大增强了该细胞因子对 JNK 的激活作用。进一步的机制分析表明,在 PKCɛ耗竭的 LNCaP 细胞中,PMA 不能促进 Bad 在 Ser(112)的磷酸化,而 PKCɛ过表达则大大增强了 Bad 的磷酸化。这种作用不依赖于 Akt、ERK 或 p90Rsk,这是 Bad 中 Ser(112)的公认激酶。此外,表达 S112A-Bad 突变体增强了 PMA 诱导的细胞凋亡。最后,我们发现 PKCɛ在 LNCaP 细胞中激活后积聚在线粒体部分,并且 Bad 是 PKCɛ在体外的底物。我们的结果表明,PKCɛ通过多种途径调节前列腺癌细胞的存活。

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Protein kinase Cepsilon interacts with signal transducers and activators of transcription 3 (Stat3), phosphorylates Stat3Ser727, and regulates its constitutive activation in prostate cancer.蛋白激酶Cε与信号转导及转录激活因子3(Stat3)相互作用,使Stat3的Ser727位点磷酸化,并调节其在前列腺癌中的组成性激活。
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A protein kinase Cepsilon-anti-apoptotic kinase signaling complex protects human vascular endothelial cells against apoptosis through induction of Bcl-2.一种蛋白激酶Cε-抗凋亡激酶信号复合物通过诱导Bcl-2表达保护人血管内皮细胞免受凋亡。
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Protein kinase Cepsilon makes the life and death decision.蛋白激酶Cε决定生死。
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