Altered expression of stromal interaction molecule(STIM)-calcium release-activated calcium channel protein(ORAI) and inositol1,4,5-trisphosphate receptors(IP_3Rs)in cancer:will they become a new battlefield for oncotherapy?

The stromal interaction molecule(STIM)-calcium release-activated calcium channel protein(ORAI) and inositol1,4,5-trisphosphate receptors(IP_3Rs) play pivotal roles in the modulation of Ca^(2+)-regulated pathways from gene transcription to cell apoptosis by driving calcium-dependent signaling processes.Increasing evidence has implicated the dysregulation of STIM-ORAI and IP_3Rs in tumorigenesis and tumor progression.By controlling the activities,structure,and/or expression levels of these Ca^(2+)-transporting proteins,malignant cancer cells can hijack them to drive essential biological functions for tumor development.However,the molecular mechanisms underlying the participation of STIM-ORAI and IP_3Rs in the biological behavior of cancer remain elusive.In this review,we summarize recent advances regarding STIM-ORAI and IP_3Rs and discuss how they promote cell proliferation,apoptosis evasion,and cell migration through temporal and spatial rearrangements in certain types of malignant cells.An understanding of the essential roles of STIM-ORAI and IP_3Rs may provide new pharmacologic targets that achieve a better therapeutic effect by inhibiting their actions in key intracellular signaling pathways.

IP_(3)R与RyR对新生大鼠心肌细胞钙振荡调控的研究

目的拟探讨新生期心肌细胞中肌浆网上两种主要的钙离子释放通道1,4,5-三磷酸肌醇受体(1,4,5-trisphosphate receptors,IP_(3)Rs)及雷诺丁受体(ryanodine receptors,RyRs)对细胞内钙振荡的调节作用。方法以体外培养原代新生SD大鼠心肌细胞为实验材料,通过钙离子指示剂fura-2荧光成像,分别利用IP_(3)Rs及RyRs通道的激动剂phenylephrine(PE)、caffeine,以及抑制剂2-APB和tetracaine作用于细胞,研究这两类通道对细胞内钙振荡信号的影响。结果培养的单层新生大鼠心肌细胞有自发的同步的钙振荡;PE处理使得钙振荡频率增加,而2-APB则抑制胞内钙振荡的频率,但它们对钙振荡幅度无明显影响;caffeine增加钙振荡频率但扰乱细胞跳动节律,而tetracaine则完全抑制心肌细胞的钙振荡信号,使细胞停止跳动。此外,应用PE分别作用于培养3 d、7 d及10 d的新生大鼠心肌细胞后,发现其对钙振荡频率的调增作用随培养时间增加而明显下降。结论新生大鼠心肌细胞内钙振荡频率主要受IP_(3)Rs调节,而RyRs是大量钙离子释放的主要通道,决定钙振荡的幅度。