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红螺菌核心捕光α和β多肽的溶液结构:对色素-蛋白质和蛋白质-蛋白质相互作用的启示

Solution structures of the core light-harvesting alpha and beta polypeptides from Rhodospirillum rubrum: implications for the pigment-protein and protein-protein interactions.

作者信息

Wang Zheng-Yu, Gokan Kazutaka, Kobayashi Masayuki, Nozawa Tsunenori

机构信息

Department of Biomolecular Engineering, Graduate School of Engineering, Tohoku University, Aramaki-aza, Aoba, Aoba-ku, Sendai 980-8579, Japan.

出版信息

J Mol Biol. 2005 Mar 25;347(2):465-77. doi: 10.1016/j.jmb.2005.01.017. Epub 2005 Jan 25.

DOI:10.1016/j.jmb.2005.01.017
PMID:15740753
Abstract

We have determined the solution structures of the core light-harvesting (LH1) alpha and beta-polypeptides from wild-type purple photosynthetic bacterium Rhodospirillum rubrum using multidimensional NMR spectroscopy. The two polypeptides form stable alpha helices in organic solution. The structure of alpha-polypeptide consists of a long helix of 32 amino acid residues over the central transmembrane domain and a short helical segment at the N terminus that is followed by a three-residue loop. Pigment-coordinating histidine residue (His29) in the alpha-polypeptide is located near the middle of the central helix. The structure of beta-polypeptide shows a single helix of 32 amino acid residues in the membrane-spanning region with the pigment-coordinating histidine residue (His38) at a position close to the C-terminal end of the helix. Strong hydrogen bonds have been identified for the backbone amide protons over the central helical regions, indicating a rigid property of the two polypeptides. The overall structures of the R.rubrum LH1 alpha and beta-polypeptides are different from those previously reported for the LH1 beta-polypeptide of Rhodobacter sphaeroides, but are very similar to the structures of the corresponding LH2 alpha and beta-polypeptides determined by X-ray crystallography. A model constructed for the structural subunit (B820) of LH1 complex using the solution structures reveals several important features on the interactions between the LH1 alpha and beta-polypeptides. The significance of the N-terminal regions of the two polypeptides for stabilizing both B820 and LH1 complexes, as clarified by many experiments, may be attributed to the interactions between the short N-terminal helix (Trp2-Gln6) of alpha-polypeptide and a GxxxG motif in the beta-polypeptide.

摘要

我们利用多维核磁共振光谱法测定了野生型紫色光合细菌红螺菌核心光捕获(LH1)α和β多肽的溶液结构。这两种多肽在有机溶液中形成稳定的α螺旋。α多肽的结构由中央跨膜结构域上32个氨基酸残基的长螺旋和N端的短螺旋段组成,随后是一个三残基环。α多肽中与色素配位的组氨酸残基(His29)位于中央螺旋的中部附近。β多肽的结构在跨膜区域显示出一个32个氨基酸残基的单螺旋,与色素配位的组氨酸残基(His38)位于靠近螺旋C端的位置。已确定中央螺旋区域的主链酰胺质子存在强氢键,表明这两种多肽具有刚性。红螺菌LH1α和β多肽的整体结构与先前报道的球形红杆菌LH1β多肽的结构不同,但与通过X射线晶体学测定的相应LH2α和β多肽的结构非常相似。利用溶液结构构建的LH1复合物结构亚基(B820)模型揭示了LH1α和β多肽之间相互作用的几个重要特征。许多实验表明,这两种多肽的N端区域对稳定B820和LH1复合物具有重要意义,这可能归因于α多肽的短N端螺旋(Trp2-Gln6)与β多肽中的GxxxG基序之间的相互作用。

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