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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Effect of apocalmodulin on recombinant human brain glutamic acid decarboxylase.
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Effect of apocalmodulin on recombinant human brain glutamic acid decarboxylase.

机译:载脂蛋白调节蛋白对重组人脑谷氨酸脱羧酶的影响。

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In this work, we report that the recombinant glutathione S-transferase (GST)-human L-glutamic acid decarboxylase (HGAD) isoforms, 65-kDa L-glutamic acid decarboxylase (GAD) (GST-HGAD65) fusion protein or free truncated HGAD65, were activated by apocalmodulin (ApoCaM) to an extent of 60%. Both truncated forms of GAD67 (tGAD67), HGAD67(Delta1-70) and HGAD67(Delta1-90), were markedly activated by ApoCaM to an extent of 141 and 85%, respectively, while GST-HGAD67 was not significantly affected. The activation appears to be due to an increase of GAD affinity for its cofactor, pyridoxal phosphate (PLP). This conclusion is based on the following observations. Firstly, the V(max) of GAD was increased when ApoCaM was present whereas the affinity for the substrate, glutamate, was not affected. Secondly, the affinity of GAD for PLP was increased in the presence of ApoCaM. Thirdly, results from calmodulin-agarose affinity column chromatography studies indicated a direct interaction or binding between ApoCaM and GAD. Fourthly, ApoCaM was found to be copurified with GAD65/GAD67 by anti-GAD65/67 immunoaffinity column using rat brain extract. Hence, it is proposed that a conformational change is induced when ApoCaM interacts with GAD65 or tGAD67, resulting in an increase of GAD affinity for PLP and the activation of GAD. The physiological significance of the interaction between GAD and ApoCaM is discussed.
机译:在这项工作中,我们报告了重组的谷胱甘肽S-转移酶(GST)-人L-谷氨酸脱羧酶(HGAD)亚型,65 kDa L-谷氨酸脱羧酶(GAD)(GST-HGAD65)融合蛋白或游离的截短的HGAD65被Apocalmodulin(ApoCaM)激活的程度为60%。截短形式的GAD67(tGAD67),HGAD67(Delta1-70)和HGAD67(Delta1-90)两种形式均被ApoCaM分别激活至141和85%的程度,而GST-HGAD67并未受到明显影响。激活似乎是由于GAD对其辅因子磷酸吡ido醛(PLP)的亲和力增加所致。该结论基于以下观察。首先,当存在ApoCaM时,GAD的V(max)增加,而对底物谷氨酸的亲和力却没有受到影响。其次,在ApoCaM存在下,GAD对PLP的亲和力增加。第三,钙调蛋白-琼脂糖亲和柱色谱研究的结果表明ApoCaM和GAD之间存在直接的相互作用或结合。第四,使用大鼠脑提取物通过抗GAD65 / 67免疫亲和柱,发现ApoCaM与GAD65 / GAD67共纯化。因此,提出了当ApoCaM与GAD65或tGAD67相互作用时引起构象变化,导致GAD对PLP的亲和力增加和GAD的活化。讨论了GAD与ApoCaM之间相互作用的生理意义。

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