Global analysis of protein folding using massively parallel design, synthesis, and testing

Rocklin Gabriel J.; Chidyausiku Tamuka M.; Goreshnik Inna; Ford Alex; Houliston Scott; Lemak Alexander; Carter Lauren; Ravichandran Rashmi; Mulligan Vikram K.; Chevalier Aaron; Arrowsmith Cheryl H.; Baker David

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Global analysis of protein folding using massively parallel design, synthesis, and testing

机译：使用大规模并行设计，合成和测试对蛋白质折叠进行全局分析

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Proteins fold into unique native structures stabilized by thousands of weak interactions that collectively overcome the entropic cost of folding. Although these forces are "encoded" in the thousands of known protein structures, "decoding" them is challenging because of the complexity of natural proteins that have evolved for function, not stability. We combined computational protein design, next-generation gene synthesis, and a high-throughput protease susceptibility assay to measure folding and stability for more than 15,000 de novo designed miniproteins, 1000 natural proteins, 10,000 point mutants, and 30,000 negative control sequences. This analysis identified more than 2500 stable designed proteins in four basic folds-a number sufficient to enable us to systematically examine how sequence determines folding and stability in uncharted protein space. Iteration between design and experiment increased the design success rate from 6% to 47%, produced stable proteins unlike those found in nature for topologies where design was initially unsuccessful, and revealed subtle contributions to stability as designs became increasingly optimized. Our approach achieves the long-standing goal of a tight feedback cycle between computation and experiment and has the potential to transform computational protein design into a data-driven science.

机译：蛋白质折叠成独特的天然结构，这种结构通过成千上万的弱相互作用而稳定下来，这些相互作用共同克服了熵的折叠成本。尽管这些作用力已“编码”成千上万种已知的蛋白质结构，但由于已针对功能而非稳定性而进化的天然蛋白质非常复杂，因此对其进行“解码”具有挑战性。我们将计算蛋白设计，下一代基因合成和高通量蛋白酶敏感性分析相结合，以测量超过15,000个从头设计的微型蛋白，1000种天然蛋白，10,000个点突变体和30,000个阴性对照序列的折叠和稳定性。这项分析确定了2500种稳定设计的蛋白质，它们具有四个基本折叠，这一数量足以使我们能够系统地检查序列如何确定未知蛋白质空间中的折叠和稳定性。设计和实验之间的迭代将设计成功率从6％提高到47％，产生了稳定的蛋白质，这不同于自然界中最初设计失败的拓扑所发现的蛋白质，并且随着设计的不断优化，揭示了对稳定性的微妙贡献。我们的方法实现了长期的目标，即在计算和实验之间建立紧密的反馈循环，并且有潜力将蛋白质的计算设计转变为数据驱动的科学。

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《Science》 |2017年第6347期|168-175|共8页
作者
Rocklin Gabriel J.; Chidyausiku Tamuka M.; Goreshnik Inna; Ford Alex; Houliston Scott; Lemak Alexander; Carter Lauren; Ravichandran Rashmi; Mulligan Vikram K.; Chevalier Aaron; Arrowsmith Cheryl H.; Baker David;
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作者单位

Univ Washington, Dept Biochem, Seattle, WA 98195 USA|Univ Washington, Inst Prot Design, Seattle, WA 98195 USA;

Univ Washington, Dept Biochem, Seattle, WA 98195 USA|Univ Washington, Inst Prot Design, Seattle, WA 98195 USA|Univ Washington, Grad Program Biol Phys Struct & Design, Seattle, WA 98195 USA;

Univ Washington, Dept Biochem, Seattle, WA 98195 USA|Univ Washington, Inst Prot Design, Seattle, WA 98195 USA;

Univ Washington, Dept Biochem, Seattle, WA 98195 USA|Univ Washington, Inst Prot Design, Seattle, WA 98195 USA|Univ Washington, Grad Program Biol Phys Struct & Design, Seattle, WA 98195 USA;

Princess Margaret Canc Ctr, Toronto, ON M5G 1L7, Canada|Univ Toronto, Struct Genom Consortium, Toronto, ON M5G 1L7, Canada;

Princess Margaret Canc Ctr, Toronto, ON M5G 1L7, Canada;

Univ Washington, Dept Biochem, Seattle, WA 98195 USA|Univ Washington, Inst Prot Design, Seattle, WA 98195 USA;

Univ Washington, Dept Biochem, Seattle, WA 98195 USA|Univ Washington, Inst Prot Design, Seattle, WA 98195 USA;

Univ Washington, Dept Biochem, Seattle, WA 98195 USA|Univ Washington, Inst Prot Design, Seattle, WA 98195 USA;

Univ Washington, Dept Biochem, Seattle, WA 98195 USA|Univ Washington, Inst Prot Design, Seattle, WA 98195 USA;

Princess Margaret Canc Ctr, Toronto, ON M5G 1L7, Canada|Univ Toronto, Struct Genom Consortium, Toronto, ON M5G 1L7, Canada|Univ Toronto, Dept Med Biophys, Toronto, ON M5G 1L7, Canada;

Univ Washington, Dept Biochem, Seattle, WA 98195 USA|Univ Washington, Inst Prot Design, Seattle, WA 98195 USA|Univ Washington, Howard Hughes Med Inst, Seattle, WA 98195 USA;

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收录信息美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
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1. STRUCTURAL ANALYSIS OF PEPTIDES ENCOMPASSING ALL ALPHA-HELICES OF THREE ALPHA/BETA PARALLEL PROTEINS - CHE-Y, FLAVODOXIN AND P21-RAS - IMPLICATIONS FOR ALPHA-HELIX STABILITY AND THE FOLDING OF ALPHA/BETA PARALLEL PROTEINS [J] . Munoz V., Jimenez MA., Rico M., Journal of Molecular Biology . 1995,第4期

机译：包含三种α/ BETA平行蛋白-CHE-Y，黄酮毒素和P21-RAS的所有α-肽的肽的结构分析-对α-HELIX稳定性的影响以及对α/ BETA平行蛋白的折叠
2. Folding mechanism of the alpha-subunit of tryptophan synthase, an alpha/beta barrel protein: global analysis highlights the interconversion of multiple native, intermediate, and unfolded forms through parallel channels. [J] . Bilsel O, Zitzewitz JA, Bowers KE, Biochemistry . 1999,第3期

机译：色氨酸合酶，α/β桶蛋白的α-亚基的折叠机制：全局分析强调了多种天然，中间和未折叠形式通过平行通道的相互转化。
3. Sequential vs. parallel protein-folding mechanisms: experimental tests for complex folding reactions [Review] [J] . Wallace LA., Matthews CR. Biophysical Chemistry: An International Journal Devoted to the Physical Chemistry of Biological Phenomena . 2002,第0期

机译：顺序与平行蛋白质折叠机制：复杂折叠反应的实验测试[综述]
4. All atom protein folding with massively parallel computers [C] . ABHINAV VERMA, JUNG S. OH, KYU H. LEE, WSEAS International Conference on Cellular and Molecular Biology - Biophysics and Bioengineering . 2007

机译：所有原子蛋白质折叠与大规模平行的计算机
5. Biomolecular assembly in silico: Using massively parallel simulations to probe protein and RNA folding dynamics. [D] . Sorin, Eric J. 2007

机译：计算机中的生物分子组装：使用大规模并行模拟来探测蛋白质和RNA折叠动力学。
6. Global analysis of protein folding using massively parallel design synthesis and testing [O] . Gabriel J. Rocklin, Tamuka M. Chidyausiku, Inna Goreshnik, -1

机译：使用大规模并行设计合成和测试对蛋白质折叠进行全局分析
7. Decision-making is the process of analyzing information about a problem situation and comparing it to a specific conclusion in order to solve a specific problematic (Yıkılmaz, 2001; Miller and Byrnes, 2001). Decision-making styles are a mechanism that is influenced by the internal and external conditions that determine the direction of the decisions of the individual, the content of the decision-making process, and the outcome of the decision-making process (Payne, Bettman and Johson, 1993; Bavol’ár and Orosová, 2015). ACT is a contemporary member of the Cognitive Behavioral Therapy family. ACT (Acceptance and commitment therapy) has both similar and different directions with Behavioral Therapies and Cognitive Therapies (Herbet and Forman, 2011; Hayes, 2004). KKT responds to classical behavioral treatments using both existential and cognitive approaches in the analysis of behavior. KKT is a science wing that tries to solve human problems with a wider perspective aimed at solving problematic human behaviors (Plumb, Stewart, Dahl and Lundgren, 2009). It is seen that there is very little research about the new approach of ACT approach when the aiming country of our country is screened and it is thought that our country will contribute to the field of psychological counseling with the work done. In the scope of the research, experimental and control groups and preliminary test, post-test and follow-up measurements of 2x3 experimental design were used. The study's study group consists of a total of 24 (12 experimental and 12 control groups) university students studying in different departments and levels, continuing their education in the academic year of 2015-2016 in Ağrı province and İbrahim Chechen University in 2015-2016 academic year. The average age of participants in the experiment and control group is 20. There were 12 participants in the experimental group, 7 female and 5 male, and 12 participants, 7 female and 5 male in the control group. Personal Information Form and Decision Making Style Scale prepared by the researcher were used in the research. In order to decide on the tests to be used in the course of analyzing the data, the scores of the participant's Decision Styles Scale pre-test, which are placed primarily in the experimental and control groups, it was analyzed whether the basic expectations of parametric tests were answered. As a result of the analysis made, the scores, skewness and kurtosis coefficients obtained from the Decision Making Styles Scale were given to the experimental and control groups. It was determined that the distribution was normal in the result of Shapiro-Wilk test, in which the skewness and kurtosis coefficients of each sub-scale were ranked between -1 and +1. Participants in the experimental and control groups; homogeneity test results for decision-style pre-test measurements indicate that the data are homogeneous. According to the results of the Mauchly Globalness Test, it has been determined that working supports the hypothesis. It was determined that there was no significant difference between the pre-test scores obtained from dependent decision-making style of experiment and control groups, but the test group showed lower mean scores at the significant level within the scores of post-test and follow-up tests. Therefore, it can be said that the ACT-oriented psychoeducation program applied to the experimental group reduces the dependent decision-making style scores from the decision style sub-dimensions and the psychoeducation program has a lasting effect. It was determined that there was no significant difference between pre-test, post-test and follow-up scores obtained from the Spontaneous-Instant Decision Style of experiment and control groups. Thus, it can be said that this situation does not cause a significant difference in the Spontaneous-Decision-Making Style scores from the decision style sub-dimensions of the ACT-oriented psychoeducation program applied to the experimental group. The ACT -oriented psychoeducation program had a decline in the intuitive decision-making styles of the individuals, but this decrease did not create significant differences. Thus, it can be said that this situation does not make a meaningful difference in the intuitive decision style scores from the decision style sub-dimensions of the KKT oriented psychoeducation program applied to the experimental group. The pre-test scores obtained from the rational decision-making style of the experimental and control groups showed that there was a difference between the post-test and the follow-up scores, but this difference was not significant. As a result of the analysis, it was determined that the test group had higher levels of rational decision style than the pre - test scores in the post test and follow - up scores, whereas the post test and follow - up test scores in the control group rational decision style showed a decrease compared to the pre - test scores. the pre - test scores. Decision-making Styles Scale Avoidant Decision Making As a result of the analysis of the mean scores of the subscale scores of pre-test, post-test and follow-up measures, the group effect was found to be insignificant. It was determined that the experimental and control groups differed significantly from the pre-test scores obtained from the avoidant decision-making style but did not show any significant change within the scores of the post-test and follow-up tests. [O] . mustafa ercengiz, ali haydar şar 2018

机译：决策是分析有关问题情况的信息并将其与特定结论进行比较的过程，以解决特定的问题（Yıkılmaz，2001; Miller和Byrnes，2001）。决策风格是一种机制，受到内部和外部条件的影响，确定个人决定的方向，决策过程的内容以及决策过程的结果（PAYNE，BETTMAN和BEDNE） Johson，1993;Bavol'ár和奥萨洛瓦，2015）。法案是认知行为治疗家庭的当代成员。行为（验收和承诺治疗）具有与行为疗法和认知疗法的类似和不同方向（Herbet和Forman，2011; Hayes，2004）。 KKT在分析行为中使用存在性和认知方法来响应古典行为治疗方法。 KKT是一个科学翼，试图解决人类问题，旨在解决有问题的人类行为（铅垂，斯图尔特，Dahl和Lundgren，2009）。有人认为，当我们国家的瞄准国家进行筛选时，有关行动方法的新方法几乎没有研究，并且认为我们的国家将为完成工作做出贡献的心理咨询领域。在研究的范围内，使用实验和对照组和初步测试，使用后测试和后续测量的2x3实验设计。该研究的研究小组包括共24名（12个实验和12个对照组）大学学生在不同的部门和水平上学习，在2015-2016学术上继续进行2015-2016的学术年度2015-2016学年年。实验和对照组参与者的平均年龄是20.实验组中有12名参与者，7名女性和5名男性，12名参与者，7名女性和5名男性。研究人员准备的个人信息表格和决策制定风格规模在研究中使用。为了决定在分析数据的过程中使用的测试，参与者的决策风格刻度预测的分数主要在实验和对照组中进行，分析了参数的基本期望吗？测试得到了回答。由于对实验和对照组给出了从决策曲调标度获得的分数，偏移和峰度分子系数。确定该分布是正常的在成熟的-WILK试验结果中，其中每亚级的偏差和刚度系数在-1到+1之间排名。实验和对照组的参与者;决策式预测测量的同质性测试结果表明数据是均匀的。根据毛毛环保试验的结果，已确定工作支持假设。据确定，从依赖决策风格的实验和对照组获得的预测分数之间没有显着差异，但测试组在测试后的分数内显示出较低的平均分数和后续的分数 - 测试。因此，可以说，应用于实验组的面向活动的心理教育程序减少了决策风格子维度的依赖决策风格分数，并且心理教育程序具有持久的效果。据确定，从实验和对照组自发决策风格获得的预测试，测试后和后续评分之间没有显着差异。因此，可以说这种情况不会导致从应用于实验组的活动导向的心理教育程序的决策风格分数的自发决策风格分数显着差异。行为的心理教育计划在个人直观的决策风格下降，但这种减少并没有产生显着的差异。因此，可以说，这种情况不会在从应用于实验组的KKT导向的心理教育程序的决策风格分数中产生有意义的决策风格分数。从实验和对照组的理性决策风格获得的预测分数显示后检验后和随访评分之间存在差异，但这种差异并不重要。由于分析，确定测试组的理性决策风格较高，而不是后测试和后续分数的预测分数，而对照组合理决策风格的后测试和后续测试分数显示出与预测试分数相比的减少。预测分数。决策款式扩展避免决策由于分析了预测试，测试后和后续措施的班次评分的平均分数，发现群体效应是微不足道的。确定实验和对照组从避免决策风格获得的预测评分中显着不同，但在测试后和后续测试的分数内没有显示出任何重大变化。
8. Parallel continuation-based global optimization for molecular conformation and protein folding [R] . Coleman, T. F. , Wu, Z. 1994

机译：基于平行连续的分子构象和蛋白质折叠的全局优化

Global analysis of protein folding using massively parallel design, synthesis, and testing

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