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来自集胞藻PCC6803分裂dnaE基因的内含肽的晶体结构揭示了不含倒数第二个组氨酸的催化模型以及锌离子抑制蛋白质剪接的机制。

Crystal structures of an intein from the split dnaE gene of Synechocystis sp. PCC6803 reveal the catalytic model without the penultimate histidine and the mechanism of zinc ion inhibition of protein splicing.

作者信息

Sun Ping, Ye Sheng, Ferrandon Sebastien, Evans Thomas C, Xu Ming-Qun, Rao Zihe

机构信息

Laboratory of Structural Biology, Tsinghua University, Beijing 100084, People's Republic of China.

出版信息

J Mol Biol. 2005 Nov 11;353(5):1093-105. doi: 10.1016/j.jmb.2005.09.039. Epub 2005 Sep 30.

DOI:10.1016/j.jmb.2005.09.039
PMID:16219320
Abstract

The first naturally occurring split intein was found in the dnaE gene of Synechocystis sp. PCC6803 and belongs to a subclass of inteins without a penultimate histidine residue. We describe two high-resolution crystal structures, one derived from an excised Ssp DnaE intein and the second from a splicing-deficient precursor protein. The X-ray structures indicate that His147 in the conserved block F activates the side-chain N(delta) atom of the intein C-terminal Asn159, leading to a nucleophilic attack on the peptide bond carbonyl carbon atom at the C-terminal splice site. In this process, Arg73 appears to stabilize the transition state by interacting with the carbonyl oxygen atom of the scissile bond. Arg73 also seems to substitute for the conserved penultimate histidine residue in the formation of an oxyanion hole, as previously identified in other inteins. The finding that the precursor structure contains a zinc ion chelating the highly conserved Cys160 and Asp140 reveals the structural basis of Zn2+-mediated inhibition of protein splicing. Furthermore, it is of interest to observe that the carbonyl carbon atom of Asn159 and N(eta) of Arg73 are 2.6 angstroms apart in the free intein structure and 10.6 angstroms apart in the precursor structure. The orientation change of the aromatic ring of Tyr-1 following the initial acyl shift may be a key switching event contributing to the alignment of Arg73 and the C-terminal scissile bond, and may explain the sequential reaction property of the Ssp DnaE intein.

摘要

首个天然存在的分裂内含肽是在集胞藻属PCC6803的dnaE基因中发现的,属于不含倒数第二个组氨酸残基的内含肽亚类。我们描述了两种高分辨率晶体结构,一种源自切除后的Ssp DnaE内含肽,另一种源自剪接缺陷型前体蛋白。X射线结构表明,保守结构域F中的His147激活了内含肽C末端Asn159的侧链N(δ)原子,导致对C末端剪接位点处肽键羰基碳原子的亲核攻击。在此过程中,Arg73似乎通过与可裂解键的羰基氧原子相互作用来稳定过渡态。Arg73在形成氧负离子洞时似乎也替代了其他内含肽中保守的倒数第二个组氨酸残基。前体结构包含一个螯合高度保守的Cys160和Asp140的锌离子,这一发现揭示了Zn2+介导的蛋白质剪接抑制的结构基础。此外,有趣的是观察到在游离内含肽结构中Asn159的羰基碳原子与Arg73的N(η)相距2.6埃,而在前体结构中相距10.6埃。初始酰基转移后Tyr-1芳香环的取向变化可能是促成Arg73与C末端可裂解键对齐的关键转换事件,并且可能解释了Ssp DnaE内含肽的顺序反应特性。

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