由两性α螺旋组成的多面螺旋网;螺旋肽轮的下一个维度。

IF 2.6 4区 综合性期刊 Q2 MULTIDISCIPLINARY SCIENCES Science Progress Pub Date : 2024-10-01 DOI:10.1177/00368504241266357
Terrance J Sereda, Jordan Beck, Paul Semchuk, Asmaa S Abu Maziad, Jason A Wertheim, Kyle M Koss
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引用次数: 0

摘要

螺旋蛋白的两亲性对其在广泛的生理例子中的结合特征至关重要,包括热休克蛋白和透明质酸(HA)受体结合。利用氨基酸的两亲性平衡及其在螺旋面的呈现,可以设计新的合成肽来改善生物功能。我们提出了一种使用多方面分析设计合成α螺旋肽的新方法,这允许新的生物工程设计的两性α螺旋。两亲螺旋肽具有明显的疏水性和亲水性;两个系列的类似物,即肽AX9和AX7,被设计分别包含疏水性和亲水性面。一个系列的多肽表现出明显的疏水性,第二个系列表现出明显的亲水性,这被反相色谱法证实(C8)。利用多方面的方法来分析两亲螺旋的潜在面,我们证明了这些螺旋包含七个不同的“侧面”螺旋面(基于AXP系列类似物的疏水面),这提供了额外的空间维度信息,超出了从螺旋轮的“自上而下”视图产生的疏水力矩的平均效应。此外,我们以这种方式交叉比较了我们最近发表的ha结合肽,以证明最重要的结合与(1)平衡的两致病性和(2)关键ha结合结构域B1(X7)B2的空间分布有关。例如,我们最有效的肽结合剂17x-3在7个面中有5个面具有B1(X7)B2结构域,而阳性对照mPEP35只有3个面,这反映了较低的亲和力。有了这样的工具,人们能够在一个额外的维度上绘制螺旋肽,以表征和重新设计基本的两性特性以及其他关键特性,例如糖和聚糖结合,这是几乎每个生物系统中细胞相互作用的基本特征。
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The multifaceted helical net of amphipathic alpha-helices; the next dimension of the helical peptide wheel.

The amphipathic nature of helical proteins is crucial to their binding features across a broad spectrum of physiological examples, including heat-shock proteins and hyaluronic acid (HA) receptor binding. By taking advantage of the amphipathic balance of amino acids and their presentation in helical faces, novel synthetic peptides can be designed to improve biofunctionality. We present a new approach for designing synthetic alpha helical peptides using a multifaceted analysis, which allows for new bioengineering designs of amphipathic alpha helices. Amphipathic helical peptides were presented with distinct hydrophobic and hydrophilic faces; two series of analogs, namely, peptides AX9 and AX7, were designed to contain a hydrophobic and hydrophilic face, respectively. The presence of one series of peptides exhibited a distinct hydrophobic face and the second series exhibited a distinct hydrophilic face, which was corroborated with reversed-phase chromatography (C8). Using a multifaceted approach to analyze the potential faces of an amphipathic helix, we demonstrated that these helices contain seven distinct "side-viewed" helical faces (based on the hydrophobic face of the AXP series of analogs), which provides additional spatial dimensional information beyond the averaging effect of the hydrophobic moment generated from the "top-down" view of a helical wheel. Furthermore, we cross-compared our recently published HA-binding peptide in this manner to demonstrate that the most significant binding was related to (1) balanced amphipathicity and (2) a distribution of the key HA-binding domain B1(X7)B2 presented spatially. For example, our most effective peptide binder 17x-3 has five of seven faces with B1(X7)B2 domains, while the positive control mPEP35 has three, which reflects a lower affinity. With such a tool, one is able to map helical peptides on an additional dimension to characterize and redesign fundamental amphipathic properties among other critical characteristics, such as sugar and glycan binding, which is a fundamental characteristic feature of cellular interactions in almost every biological system.

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来源期刊
Science Progress
Science Progress Multidisciplinary-Multidisciplinary
CiteScore
3.80
自引率
0.00%
发文量
119
期刊介绍: Science Progress has for over 100 years been a highly regarded review publication in science, technology and medicine. Its objective is to excite the readers'' interest in areas with which they may not be fully familiar but which could facilitate their interest, or even activity, in a cognate field.
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