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Functional interactions among STIM1, Orai1 and TRPC1 on the activation of SOCs in HL-7702 cells

机译:STIM1,Orai1和TRPC1之间的功能相互作用对HL-7702细胞中SOC的激活

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STTM1, Orai 1 and TRPC1 are all reported to be important for store-operated Ca~(2+) entry (SOCE) in diverse cells. However, there is no evidence for the functional interaction of the three proteins in SOCE in human liver cells. The objective of this study is to determine whether they are involved in SOCE in normal human liver cells. Liposomal transfection method was used to increase expression levels of the three proteins in HL-7702 cells, a normal human liver cell line. Western blot and single cell RT-PCR were applied to evaluate transfection effectiveness. Changes in store-operated current (I_(SOC)) and SOCE were investigated using whole-cell patch-clamp recording and calcium imaging. I_(SOC) is detected in HL-7702 cells and it is inhibited either by 2-Aminoethoxydiphenyl borate (2-APB) or La~(3+) . Overexpression of STIM1 or Orai1 alone did not induce any change in Isoc- TRPC1-transfection, however, caused approximate 2.5-fold increase in Isoc- A large increase (>10-fold) in I_(SOC) emerged when both STIM1 and Orai1 were co-transfected into HL-7702 cells. Co-overexpression of STIM1 + TRPC1 also caused >10-fold increase in I_(SOC) and addition of Orai1 did not cause any further increase. In HL-7702 cells, TRPC1 and Orai1 take part in SOCE independently of each other. Functional interactions of STIM1 and Orai1 or TRPC1 contribute to Isoc activation.
机译:据报道,STTM1,Orai 1和TRPC1对于在不同细胞中的存储操作性Ca〜(2+)进入(SOCE)都是重要的。但是,尚无证据表明人肝细胞中SOCE中这三种蛋白的功能相互作用。这项研究的目的是确定它们是否参与正常人肝细胞中的SOCE。脂质体转染法用于增加正常人肝细胞系HL-7702细胞中这三种蛋白质的表达水平。 Western blot和单细胞RT-PCR用于评估转染效果。使用全细胞膜片钳记录和钙成像研究了存储操作电流(I_(SOC))和SOCE的变化。在HL-7702细胞中检测到I_(SOC),并被2-氨基乙氧基二苯基硼酸酯(2-APB)或La〜(3+)抑制。仅STIM1或Orai1的过表达并没有引起Isoc-TRPC1转染的任何变化,但是,导致Isoc大约增加了2.5倍-当STIM1和Orai1都被抑制时,I_(SOC)出现了大的增加(> 10倍)。共转染到HL-7702细胞中。 STIM1 + TRPC1的共过表达也导致I_(SOC)的增加> 10倍,添加Orai1并没有引起任何进一步的增加。在HL-7702细胞中,TRPC1和Orai1彼此独立地参与了SOCE。 STIM1和Orai1或TRPC1的功能相互作用有助于Isoc激活。

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