BH3 mimetic-elicited Ca2+ signals in pancreatic acinar cells are dependent on Bax and can be reduced by Ca2+-like peptides

Pawel E Ferdek; Monika A Jakubowska; Polina Nicolaou; Julia V Gerasimenko; Oleg V Gerasimenko; Ole H Petersen

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BH3 mimetic-elicited Ca2+ signals in pancreatic acinar cells are dependent on Bax and can be reduced by Ca2+-like peptides

机译：BH3在胰腺缩醛细胞中的敏捷CA 2 + 信号依赖于Bax，可以通过Ca 2 + / sup> -like pertike肽减少

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BH3 mimetics are small-molecule inhibitors of B-cell lymphoma-2 (Bcl-2) and Bcl-xL, which disrupt the heterodimerisation of anti- and pro-apoptotic Bcl-2 family members sensitising cells to apoptotic death. These compounds have been developed as anti-cancer agents to counteract increased levels of Bcl-2 proteins often present in cancer cells. Application of a chemotherapeutic drug supported with a BH3 mimetic has the potential to overcome drug resistance in cancers overexpressing anti-apoptotic Bcl-2 proteins and thus increase the success rate of the treatment. We have previously shown that the BH3 mimetics, BH3I-2′ and HA14-1, induce Ca2+ release from intracellular stores followed by a sustained elevation of the cytosolic Ca2+ concentration. Here we demonstrate that loss of Bax, but not Bcl-2 or Bak, inhibits this sustained Ca2+ elevation. What is more, in the absence of Bax, thapsigargin-elicited responses were decreased; and in two-photon-permeabilised bax ?/? cells, Ca2+ loss from the ER was reduced compared to WT cells. The Ca2+-like peptides, CALP-1 and CALP-3, which activate EF hand motifs of Ca2+-binding proteins, significantly reduced excessive Ca2+ signals and necrosis caused by two BH3 mimetics: BH3I-2′ and gossypol. In the presence of CALP-1, cell death was shifted from necrotic towards apoptotic, whereas CALP-3 increased the proportion of live cells. Importantly, neither of the CALPs markedly affected physiological Ca2+ signals elicited by ACh, or cholecystokinin. In conclusion, the reduction in passive ER Ca2+ leak in bax ?/? cells as well as the fact that BH3 mimetics trigger substantial Ca2+ signals by liberating Bax, indicate that Bax may regulate Ca2+ leak channels in the ER. This study also demonstrates proof-of-principle that pre-activation of EF hand Ca2+-binding sites by CALPs can be used to ameliorate excessive Ca2+ signals caused by BH3 mimetics and shift necrotic death towards apoptosis.

机译：BH3模拟物是B细胞淋巴瘤-2（BCL-2）和BCL-XL的小分子抑制剂，其破坏抗凋亡的BCL-2家族成员敏化细胞的抗凋亡和凋亡死亡的异单异化。这些化合物已被发展为抗癌剂，以抵消通常存在于癌细胞中的Bcl-2蛋白水平。支持BH3模拟物的化学治疗药物的应用具有克服过表达抗凋亡Bcl-2蛋白的癌症的耐药性，从而增加了治疗的成功率。我们之前已经表明，BH3模拟物，BH3I-2'和HA14-1，从细胞内储存释放，然后持续升高胞质CA 2 + 浓度。在这里，我们证明了丢失的BAX，但不是BCL-2或BAK，抑制了这种持续的CA ^{2 + 高度。更重要的是，在没有BAX的情况下，尾骨引发的反应减少;在双光子透透过的Bax α/α/α/θs中，与wt细胞相比，从ER的损失降低。 Ca 2 + -like肽，calp-1和calp-3，其激活Ca 2 + - 困难蛋白的EF手动术，显着减少了过量的Ca 2 + 由两个BH3模拟物引起的信号和坏死：BH3I-2'和Gossypol。在CALP-1的存在下，细胞死亡从坏死朝向凋亡转移，而CALP-3增加了活细胞的比例。重要的是，CALPS都不明显受ACH，或胆囊蛋白引发的生理CA ^{2 + 信号。总之，在BAX α/α/α/α/α/α/α/α/α/α/α/α/α/α/α/α/α/α/α/α/α/η的泄漏以及BH3模拟物触发大量CA 2 + /通过解放BAX来表示信号，表明BAX可以调节ER中的泄漏通道。本研究还证明了原理上，CA ^{2 + 耦合位点的原则上的原理原则上可用于改善过多的CA ^{2 + 信号BH3模拟物和将坏死性移植到细胞凋亡中。}}}}

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《Cell death & disease.》 |2017年第3期|共页
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Pawel E Ferdek; Monika A Jakubowska; Polina Nicolaou; Julia V Gerasimenko; Oleg V Gerasimenko; Ole H Petersen;
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1. Glucagon-like Peptide 1 Receptor Signaling in Acinar Cells Causes Growth-Dependent Release of Pancreatic Enzymes [J] . Nicolai J. Wewer Albrechtsen, Reidar Albrechtsen, Lasse Bremholm, Cell Reports . 2016,第11期

机译：胰高血糖素样肽1受体信号在腺泡细胞中导致生长依赖的胰腺酶释放。
2. Role of Regulators of G-Protein Signaling 4 in Ca2+ Signaling in Mouse Pancreatic Acinar Cells [J] . Park Soonhong, Lee Syng-Ill, Shin Dong Min The Korean Journal of Physiology & Pharmacology . 2011,第6期

机译：G蛋白信号传导调节剂4在小鼠胰腺腺泡细胞Ca2 +信号传导中的作用
3. Heterogeneity of cannabinoid ligand-induced modulations in intracellular Ca2+ signals of mouse pancreatic acinar cells in vitro [J] . Kun-kun Xia, Jian-xin Shen, Ze-bing Huang, 中国药理学报：英文版 . 2019,第003期

机译：大麻素配体诱导的小鼠胰腺腺泡细胞胞内Ca2 +信号调控的异质性
4. CCK regulation of monitor peptide pene expression in pancreatic acinar AR42J cells. [C] . TOSHI KINOUCHI, SATOSHI TSUZUKI, CHIEKO MINAMI, Joint International Meeting of the Japanese Association for Animal Cell Technolog and and European Society for Animal Cell Technology . 1999

机译：CCK肽肽在胰腺AR42J细胞中监测肽PENE表达的调节。
5. BH3 peptides induce mitochondrial fission and cell death in the absence of BAX and BAK. [D] . Shroff, Emelyn Helen. 2009

机译：在没有BAX和BAK的情况下，BH3肽诱导线粒体分裂和细胞死亡。
6. BH3 mimetic-elicited Ca2+ signals in pancreatic acinar cells are dependent on Bax and can be reduced by Ca2+-like peptides [O] . Pawel E Ferdek, Monika A Jakubowska, Polina Nicolaou, 1996

机译：BH3模拟物在胰腺腺泡细胞中引起的Ca2 +信号依赖于Bax，并且可以被类似Ca2 +的肽所减少
7. BH3 mimetic-elicited Ca2+ signals in pancreatic acinar cells are dependent on Bax and can be reduced by Ca2+-like peptides [O] . Ferdek Pawel, Jakubowska Monika, Polina Nicolaou, 2017

机译：BH3模拟物在胰腺腺泡细胞中引起的Ca2 +信号依赖于Bax，并且可以被类似Ca2 +的肽所减少

BH3 mimetic-elicited Ca2+ signals in pancreatic acinar cells are dependent on Bax and can be reduced by Ca2+-like peptides

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