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作为蛋白质支架的正交合成拉链

Orthogonal Synthetic Zippers as Protein Scaffolds.

作者信息

Anderson George P, Shriver-Lake Lisa C, Liu Jinny L, Goldman Ellen R

机构信息

Center for BioMolecular Science and Engineering, U.S. Naval Research Laboratory, 4555 Overlook Avenue SW, Washington, District of Columbia 20375, United States.

出版信息

ACS Omega. 2018 May 31;3(5):4810-4815. doi: 10.1021/acsomega.8b00156. Epub 2018 May 2.

Abstract

Protein scaffolds have proven useful for co-localization of enzymes, providing control over stoichiometry and leading to higher local enzyme concentrations, which have led to improved product formation. To broaden their usefulness, it is necessary to have a wide choice of building blocks to mix and match for scaffold generation. Ideally, the scaffold building blocks should function at any location within the scaffold and have high affinity interactions with their binding partners. We examined the utility of orthogonal synthetic coiled coils (zippers) as scaffold components. The orthogonal zippers are coiled coil domains that form heterodimers only with their specific partner and not with other zipper domains. Focusing on two orthogonal zipper pairs, we demonstrated that they are able to function on either end or in the middle of a multiblock assembly. Surface plasmon resonance was employed to assess the binding kinetics of zipper pairs placed at the start, middle, or end of a construct. Size-exclusion chromatography was used to demonstrate the ability of a scaffold with two zipper domains to bind their partners simultaneously. We then expanded the study to examine the binding kinetics and cross-reactivities of three additional zipper pairs. By validating the affinities and specificities of synthetic zipper pairs, we demonstrated the potential for zipper domains to provide an expanded library of scaffolding parts for tethering enzymes in complex pathways for synthetic biology applications.

摘要

蛋白质支架已被证明可用于酶的共定位,能够控制化学计量并导致更高的局部酶浓度,从而提高产物形成。为了扩大其用途,需要有多种构建模块可供混合和匹配以生成支架。理想情况下,支架构建模块应能在支架内的任何位置发挥作用,并与其结合伙伴具有高亲和力相互作用。我们研究了正交合成卷曲螺旋(拉链)作为支架组件的效用。正交拉链是仅与其特定伙伴而非其他拉链结构域形成异二聚体的卷曲螺旋结构域。聚焦于两对正交拉链,我们证明它们能够在多模块组装体的两端或中间发挥作用。采用表面等离子体共振来评估置于构建体起始、中间或末端的拉链对的结合动力学。尺寸排阻色谱用于证明具有两个拉链结构域的支架同时结合其伙伴的能力。然后我们扩展研究以考察另外三对拉链的结合动力学和交叉反应性。通过验证合成拉链对的亲和力和特异性,我们证明了拉链结构域为合成生物学应用中复杂途径中的酶系拴系提供扩展支架部件库的潜力。

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