Coiled coils are well suited to drive subunit oligomerization and are widely used in applications ranging from basic research to medicine. The optimization of these applications requires a detailed understanding of the molecular determinants that control of coiled-coil formation. Although many of these determinants have been identified and characterized in great detail, a puzzling observation is that their presence does not necessarily correlate with the oligomerization state of a given coiled-coil structure. Thus, other determinants must play a key role. To address this issue, we recently investigated the unrelated coiled-coil domains from GCN4, ATF1 and cortexillin-1 as model systems. We found that well-known trimer-specific oligomerization-state determinants, such as the distribution of isoleucine residues at heptad-repeat core positions or the trimerization motif Arg-h-x-x-h-Glu (where h = hydrophobic amino acid; x = any amino acid), switch the peptide’s topology from a dimer to a trimer only when inserted into the trigger sequence, a site indispensable for coiled-coil formation. Because high-resolution structural information could not be obtained for the full-length, three-stranded cortexillin-1 coiled coil, we here report the detailed biophysical and structural characterization of a shorter variant spanning the trigger sequence using circular dichroism, anatytical ultracentrifugation and x-ray crystallography. We show that the peptide forms a stable α-helical trimer in solution. We further determined the crystal structure of an optimised variant at a resolution of 1.65 Å, revealing that the peptide folds into a parallel, three-stranded coiled coil. The two complemented R-IxxIE trimerization motifs and the additional hydrophobic core isoleucine residue adopt the conformations seen in other extensively characterized parallel, three-stranded coiled coils. These findings not only confirm the structural basis for the switch in oligomerization state from a dimer to a trimer observed for the full-length cortexillin-1 coiled-coil domain, but also provide further evidence for a general link between oligomerization-state specificity and trigger-sequence function.
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机译:盘绕线圈非常适合驱动亚基的低聚反应,广泛用于从基础研究到医学的各种应用中。这些应用的优化要求对控制卷曲螺旋形成的分子决定因素有详细的了解。尽管已经详细确定了许多这些决定因素并对其进行了详细描述,但令人费解的观察是,它们的存在并不一定与给定卷曲螺旋结构的低聚状态相关。因此,其他决定因素必须发挥关键作用。为了解决这个问题,我们最近研究了来自GCN4,ATF1和cortexillin-1的不相关螺旋线圈结构域作为模型系统。我们发现了众所周知的三聚体特异性寡聚化状态决定簇,例如七聚体重复核心位置处异亮氨酸残基的分布或三聚化基序Arg-hxxh-Glu(其中h =疏水氨基酸; x =任何氨基酸)仅在插入触发序列时才将肽的拓扑结构从二聚体切换为三聚体,而这是卷曲螺旋形成必不可少的位点。由于无法获得全长三链cortexillin-1卷曲螺旋的高分辨率结构信息,因此我们在此报告了使用圆二色性,超分辨超速离心和x触发范围较短的变异体的详细生物物理和结构表征射线晶体学。我们显示该肽在溶液中形成稳定的α-螺旋三聚体。我们进一步确定了一个优化变体的晶体结构,分辨率为1.65Å,揭示了该肽折叠成平行的三链卷曲螺旋。两个互补的R-IxxIE三聚体基序和其他疏水性核心异亮氨酸残基采用在其他广泛表征的平行三链卷曲线圈中看到的构象。这些发现不仅证实了在全长cortexillin-1卷曲螺旋结构域中观察到的低聚状态从二聚体向三聚体的转变的结构基础,而且还为低聚态特异性与触发之间的一般联系提供了进一步的证据。 -序列功能。
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