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首页> 外文期刊>American Journal of Physiology >Caspase activity during cell stasis: avoidance of apoptosis in an invertebrate extremophile, Artemia franciscana.
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Caspase activity during cell stasis: avoidance of apoptosis in an invertebrate extremophile, Artemia franciscana.

机译:细胞停滞期间的半胱天冬酶活性:避免无脊椎动物极端分子法国蒿中的凋亡。

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Evaluation of apoptotic processes downstream of the mitochondrion reveals caspase-9- and low levels of caspase-3-like activities in partly purified extracts of Artemia franciscana embryos. However, in contrast to experiments with extracts of human hepatoma cells, cytochrome c fails to activate caspase-3 or -9 in extracts from A. franciscana. Furthermore, caspase-9 activity is sensitive to exogenous calcium. The addition of 5 mM calcium leads to a 4.86 +/- 0.19 fold (SD) (n = 3) increase in activity, which is fully prevented with 150 mM KCl. As with mammalian systems, high ATP (>1.25 mM) suppresses caspase activity in A. franciscana extracts. A strong inhibition of caspase-9 activity was also found by GTP. Comparison of GTP-induced inhibition of caspase-9 at 0 and 2.5 mM MgCl(2) indicates that free (nonchelated) GTP is likely to be the inhibitory form. The strongest inhibition among all nucleotides tested was with ADP. Inhibition by ADP in the presence of Mg(2+) is 60-fold greater in diapause embryos than in postdiapause embryos. Because ADP does not change appreciably in concentration between the two physiological states, it is likely that this differential sensitivity to Mg(2+)-ADP is important in avoiding caspase activation during diapause. Finally, mixtures of nucleotides that mimic physiological concentrations in postdiapause and diapause states underscore the depressive action of these regulators on caspase-9 during diapause. Our biochemical characterization of caspase-like activity in A. franciscana extracts reveals that multiple mechanisms are in place to reduce the probability of apoptosis under conditions of energy limitation in this embryo.
机译:线粒体下游的凋亡过程的评估揭示了半精制法国苦蒿胚的提取物中的caspase-9和低水平的caspase-3样活性。但是,与人肝癌细胞提取物进行的实验相反,细胞色素c不能激活方酸曲霉提取物中的caspase-3或-9。此外,caspase-9活性对外源钙敏感。添加5 mM钙可导致活性增加4.86 +/- 0.19倍(SD)(n = 3),而150 mM KCl则可完全防止这种情况。与哺乳动物系统一样,较高的ATP(> 1.25 mM)会抑制方酸曲霉提取物中的caspase活性。 GTP还发现了对caspase-9活性的强烈抑制。比较GTP诱导的caspase-9在0和2.5 mM MgCl(2)的抑制作用表明,游离的(非螯合的)GTP可能是抑制形式。在所有测试的核苷酸中,最强的抑制作用是使用ADP。在滞育胚胎中,在存在Mg(2+)的情况下,ADP的抑制作用比滞育后胚胎的抑制作用大60倍。由于ADP不会在两种生理状态之间的浓度发生明显变化,因此对Mg(2 +)-ADP的这种差异敏感性很可能对避免滞育期间胱天蛋白酶的活化很重要。最后,在滞后和滞育状态下模拟生理浓度的核苷酸混合物突显了滞育期间这些调节剂对caspase-9的抑制作用。我们在方球菌提取物中半胱天冬酶样活性的生化特征表明,存在多种机制可以降低这种胚胎在能量受限条件下凋亡的可能性。

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