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Evidence for a dynamic structure of human neuronal growth inhibitory factor and for major rearrangements of its metal-thiolate clusters.

机译:人类神经元生长抑制因子的动态结构及其金属硫醇盐簇的重大重排的证据。

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摘要

Human neuronal growth inhibitory factor (GIF), a metallothionein-like protein classified as metallothionein-3, impairs the survival and the neurite formation of cultured neurons. Despite its approximately 70% amino acid sequence identity with those of mammalian metallothioneins (MT-1 and MT-2 isoforms), only GIF exhibits growth inhibitory activity. In this study, structural features of the metal-thiolate clusters in recombinant Zn(7)- and Cd(7)-GIF, and in part also in synthetic GIF (68 amino acids), were investigated by using circular dichroism (CD) and (113)Cd NMR. The CD and (113)Cd NMR studies of recombinant Me(7)-GIF confirmed the existence of distinct Me(4)S(11)- and Me(3)S(9)-clusters located in the alpha- and beta-domains of the protein, respectively. Moreover, a mutual structural stabilization of both domains was demonstrated. The (113)Cd NMR studies of recombinant (113)Cd(7)-GIF were conducted at different magnetic fields (66.66 and 133.33 MHz) and temperatures (298 and 323 K). At 298 K the spectra revealed seven (113)Cd signals at 676, 664, 651, 644, 624, 622, and 595 ppm. A striking feature of all resonances is the absence of resolved homonuclear [(113)Cd-(113)Cd] couplings and large apparent line widths (between 140 and 350 Hz), which account for the absence of cross-peaks in [(113)Cd, (113)Cd] COSY. On the basis of a close correspondence in chemical shift positions of the (113)Cd signals at 676, 624, 622, and 595 ppm with those obtained in our previous studies of (113)Cd(4)-GIF(32-68) [Hasler, D. W., Faller, P., and Vasak, M. (1998) Biochemistry 37, 14966], these resonances can be assigned to a Cd(4)S(11)-cluster in the alpha-domain of (113)Cd(7)-GIF. Consequently, the remaining three (113)Cd signals at 664, 651, and 644 ppm originate from a Me(3)S(9) cluster in the beta-domain. However, the latter resonances show a markedly reduced and temperature-independent intensity (approximately 20%) when compared with those of the alpha-domain, indicating that the majority of the signal intensity remained undetected. To account for the observed NMR features of (113)Cd(7)-GIF, we suggest that dynamic processes acting on two different NMR time scales are present: (i) fast exchange processes among conformational cluster substates giving rise to broad, weight-averaged resonances and (ii) additional very slow exchange processes within the beta-domain associated with the formation of configurational cluster substates. The implications of the structure fluctuation for the biological activity of GIF are discussed.
机译:人神经元生长抑制因子(GIF)是一种金属硫蛋白样蛋白,被分类为金属硫蛋白3(metallothionein-3),会损害培养的神经元的存活和神经突的形成。尽管它与哺乳动物金属硫蛋白(MT-1和MT-2同工型)的氨基酸序列具有大约70%的同一性,但只有GIF表现出生长抑制活性。在这项研究中,通过使用圆二色性(CD)和(113)Cd NMR。重组Me(7)-GIF的CD和(113)Cd NMR研究证实了位于alpha-和beta-中的独特Me(4)S(11)-和Me(3)S(9)-簇的存在蛋白质的结构域。而且,证明了两个结构域的相互结构稳定。重组(113)Cd(7)-GIF的(113)Cd NMR研究是在不同的磁场(66.66和133.33 MHz)和温度(298和323 K)下进行的。在298 K处,光谱显示出676、664、651、644、624、622和595 ppm的七个(113)Cd信号。所有共振的一个显着特征是没有解析的同核[(113)Cd-(113)Cd]耦合和较大的表观线宽(140至350 Hz之间),这说明了[[113 (Cd,(113)Cd] COSY。基于(113)Cd信号在676、624、622和595 ppm的化学位移位置与我们先前对(113)Cd(4)-GIF(32-68)的研究得出的信号的紧密对应关系[Hasler,DW,Faller,P.和Vasak,M.(1998)Biochemistry 37,14966],可以将这些共振分配给(113)α域中的Cd(4)S(11)簇。 Cd(7)-GIF。因此,其余的三个(113)Cd信号分别为664、651和644 ppm,来自β域中的Me(3)S(9)簇。但是,与α域相比,后一种共振显示出显着降低的且与温度无关的强度(约20%),表明大部分信号强度仍未被检测到。为了说明观察到的(113)Cd(7)-GIF的NMR特征,我们建议存在作用于两个不同NMR时间尺度的动态过程:(i)构象簇子状态之间的快速交换过程引起宽泛的,重的平均共振和(ii)与结构簇亚态形成相关的β域内其他非常缓慢的交换过程。讨论了结构波动对GIF生物活性的影响。

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