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与肽结合的GGA-GAE和γ1-耳的结构测定:膜运输中低亲和力复合物的结晶

Structure determination of GGA-GAE and gamma1-ear in complex with peptides: crystallization of low-affinity complexes in membrane traffic.

作者信息

Yamada Yusuke, Inoue Michio, Shiba Tomoo, Kawasaki Masato, Kato Ryuichi, Nakayama Kazuhisa, Wakatsuki Soichi

机构信息

Structural Biology Research Center, Photon Factory, High Energy Accelerator Research Organization, Japan.

出版信息

Acta Crystallogr D Biol Crystallogr. 2005 Jun;61(Pt 6):731-6. doi: 10.1107/S0907444905009595. Epub 2005 May 26.

DOI:10.1107/S0907444905009595
PMID:15930630
Abstract

Crystallization of protein-protein complexes is an important step in the studies of biological functions of proteins. However, weak and transient, even though specific, interactions often present difficulties in crystallization of protein complexes due to the heterogeneity of the sample mixture. For example, the gamma1-ear domain of the AP-1 complex and the GAE domain of GGA1, responsible for the interaction with accessory proteins involved in vesicular transport, are known to interact with target proteins with affinities of the order of 1-100 microM. Such low affinities have hampered crystallization trials of the complexes. To overcome this problem, the gamma1-ear and GAE domains were first co-crystallized with excess amounts of the peptides. Co-crystals of both domains were obtained and the complex structures were determined at 2.5-2.9 A resolution. Based on the crystal packing of gamma1-ear and the cognate peptide, gamma1-ear fused with a peptide tag at the N-terminus was prepared. The peptide-tagged gamma1-ear readily crystallized and the crystal diffracted far better, 1.9-2.2 A resolution, compared with the co-crystallized complex, giving significantly more details without affecting the overall complex structure.

摘要

蛋白质-蛋白质复合物的结晶是研究蛋白质生物学功能的重要步骤。然而,由于样品混合物的异质性,即使是特异性的相互作用,其弱且短暂的性质常常给蛋白质复合物的结晶带来困难。例如,AP-1复合物的γ1-耳结构域和GGA1的GAE结构域负责与参与囊泡运输的辅助蛋白相互作用,已知它们与靶蛋白的亲和力约为1-100微摩尔。如此低的亲和力阻碍了复合物的结晶试验。为克服这一问题,首先将γ1-耳结构域和GAE结构域与过量的肽共结晶。获得了两个结构域 的共晶体,并在2.5-2.9埃分辨率下确定了复合物结构。基于γ1-耳结构域和同源肽的晶体堆积,制备了在N端与肽标签融合的γ1-耳结构域。与共结晶复合物相比,带有肽标签的γ1-耳结构域很容易结晶,并且晶体衍射效果要好得多,分辨率为1.9-2.2埃,在不影响整体复合物结构的情况下给出了更多细节。

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