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视网膜杆状细胞外段盘状膜ADP - 核糖基环化酶的催化特性

Catalytic properties of the retinal rod outer segment disk ADP-ribosyl cyclase.

作者信息

Fabiano Andrea, Panfoli Isabella, Calzia Daniela, Bruschi Maurizio, Ravera Silvia, Bachi Angela, Cattaneo Angela, Morelli Alessandro, Candiano Giovanni

机构信息

Department of Biology, University of Genoa, Genova, Italy.

出版信息

Vis Neurosci. 2011 Mar;28(2):121-8. doi: 10.1017/S0952523810000404. Epub 2011 Jan 27.

Abstract

Cyclic ADP-ribose (cADPR) is a second messenger modulating intracellular calcium levels. We have previously described a cADPR-dependent calcium signaling pathway in bovine rod outer segments (ROS), where calcium ions play a pivotal role. ROS ADP-ribosyl cyclase (ADPR-cyclase) was localized in the membrane fraction. In the present work, we examined the properties of the disk ADPR-cyclase through the production of cyclic GDP-ribose from the NAD(+) analogue NGD(+). The enzyme displayed an estimated K(m) for NGD(+) of 12.5 ± 0.3 μM, a V(max) of 26.50 ± 0.70 pmol cyclic GDP-ribose synthesized/min/mg, and optimal pH of 6.5. The effect of divalent cations (Zn(2+), Cu(2+), and Ca(2+)) was also tested. Micromolar Zn(2+) and Cu(2+) inhibited the disk ADPR-cyclase activity (half maximal inhibitory concentration, IC50=1.1 and 3.6 μM, respectively). By contrast, Ca(2+) ions had no effect. Interestingly, the properties of the intracellular membrane-associated ROS disk ADPR-cyclase are more similar to those of the ADPR-cyclase found in CD38-deficient mouse brain, than to those of CD38 or CD157. The novel intracellular mammalian ADPR-cyclase would elicit Ca(2+) release from the disks at various rates in response to change in free Ca(2+) concentrations, caused by light versus dark adaptation, in fact there was no difference in disk ADPR-cyclase activity in light or dark conditions. Data suggest that disk ADPR-cyclase may be a potential target of retinal toxicity of Zn(2+) and may shed light to the role of Cu(2+) and Zn(2+) deficiency in retina.

摘要

环磷酸腺苷核糖(cADPR)是一种调节细胞内钙水平的第二信使。我们之前曾描述过牛视杆细胞外段(ROS(ROS中一种依赖cADPR的钙信号通路,其中钙离子起着关键作用。ROS腺苷二磷酸核糖基环化酶(ADPR-环化酶)定位于膜部分。在本研究中,我们通过从NAD(+)类似物NGD(+)生成环磷酸鸟苷核糖来研究盘状ADPR-环化酶的特性。该酶对NGD(+)的估计米氏常数K(m)为12.5±0.3μM,最大反应速度V(max)为26.50±0.70 pmol环磷酸鸟苷核糖合成/分钟/毫克,最适pH为6.5。还测试了二价阳离子(Zn(2+)、Cu(2+)和Ca(2+))的作用。微摩尔浓度的Zn(2+)和Cu(2+)抑制盘状ADPR-环化酶活性(半数最大抑制浓度,IC50分别为1.1和3.6μM)。相比之下,Ca(2+)离子没有影响。有趣的是,细胞内膜相关的ROS盘状ADPR-环化酶的特性与在CD38缺陷小鼠脑中发现的ADPR-环化酶更相似,而与CD38或CD157的特性不同。这种新型的细胞内哺乳动物ADPR-环化酶会根据明暗适应引起的游离Ca(2+)浓度变化,以不同速率引发盘状物释放Ca(2+),实际上在明或暗条件下盘状ADPR-环化酶活性没有差异。数据表明盘状ADPR-环化酶可能是Zn(2+)视网膜毒性的潜在靶点,并且可能有助于阐明Cu(2+)和Zn(2+)缺乏在视网膜中的作用。

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