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人神经元tau蛋白对兔肌肉3-磷酸甘油醛脱氢酶变性和复性的影响。

Effect of human neuronal tau on denaturation and reactivation of rabbit muscle D-glyceraldehyde-3-phosphate dehydrogenase.

作者信息

Chen Y H, He R Q, Liu Y, Liu Y, Xue Z G

机构信息

Laboratory of Visual Information Processing, Institute of Biophysics, The Chinese Academy of Sciences, 15 Da Tun Rd, Chaoyang District, Beijing 100101, People's Republic of China.

出版信息

Biochem J. 2000 Oct 1;351(Pt 1):233-40. doi: 10.1042/0264-6021:3510233.

Abstract

Human neuronal tau-40 (htau-40) has been used to study denaturation and renaturation of rabbit muscle D-glyceraldehyde-3-phosphate dehydrogenase (GAPDH, EC 1.2.1.12). Inactivation of GAPDH incubated with tau was more distinguishably detected than that of control GAPDH during thermal and guanidine hydrochloride (GdnHCl) denaturation. However, tau did not influence the activity of GAPDH at room temperature or in solution without GdnHCl. A marked change in both the emission intensity and emission maximum of the intrinsic fluorescence at 335 nm of GAPDH with tau was observed when GdnHCl concentration was 0.8 M, but that of the control without tau occurred in 1.2 M GdnHCl. The first-order rate of the decrease in the fluorescence intensity of the enzyme with tau was approximately twice as great as that of GAPDH without tau. Kinetics of inactivation of GAPDH with tau in 0.2 M GdnHCl was a monophasic procedure, instead of the biphasic procedure followed by the control, as described before [He, Zhao, Yan and Li (1993) Biochim. Biophys. Acta 1163, 315-320]. Similar results were obtained when the enzyme was thermally denatured at 45 degrees C. It revealed that tau bound to the denatured GAPDH but not the native molecule. On the other hand, tau suppressed refolding and reactivation of GAPDH when this enzyme was reactivated by dilution of GdnHCl solution. Furthermore, tau improved the aggregation of the non-native GAPDH in solutions. It suggested that tau acted in an anti-chaperone-like manner towards GAPDH in vitro. However, tau lost that function when it was aggregated or phosphorylated by neuronal cdc2-like protein kinase. It showed that tau's anti-chaperone-like function depended on its native conformation.

摘要

人类神经元tau-40(htau-40)已被用于研究兔肌肉D-甘油醛-3-磷酸脱氢酶(GAPDH,EC 1.2.1.12)的变性和复性。在热变性和盐酸胍(GdnHCl)变性过程中,与tau一起孵育的GAPDH的失活比对照GAPDH更易于检测到。然而,tau在室温下或在没有GdnHCl的溶液中不影响GAPDH的活性。当GdnHCl浓度为0.8 M时,观察到与tau一起的GAPDH在335 nm处的内在荧光发射强度和发射最大值均有明显变化,而没有tau的对照在1.2 M GdnHCl时才出现这种变化。有tau的酶的荧光强度下降的一级速率大约是没有tau的GAPDH的两倍。在0.2 M GdnHCl中,有tau的GAPDH的失活动力学是单相过程,而不是如之前所述的对照的双相过程[He、Zhao、Yan和Li(1993年)《生物化学与生物物理学报》1163,315 - 320]。当酶在45℃进行热变性时也获得了类似结果。这表明tau与变性的GAPDH结合,而不与天然分子结合。另一方面,当通过稀释GdnHCl溶液使该酶重新激活时,tau抑制了GAPDH的重折叠和再激活。此外,tau促进了溶液中非天然GAPDH的聚集。这表明tau在体外对GAPDH起着类似抗伴侣蛋白的作用。然而,当tau被神经元cdc2样蛋白激酶聚集或磷酸化时,它失去了该功能。这表明tau的类似抗伴侣蛋白的功能依赖于其天然构象。

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