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Model of Early Stage Intermediate in Respect to Its Final Structure

机译:最终中间体的早期中间体模型

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摘要

The model, describing a method of determining the structure of an early intermediate in the process of protein folding to analyze nonredundant PDB protein bases, allows determining the relationship between the sequence of tetrapeptides and their structural forms expressed by structural codes. The contingency table expressing such a relationship can be used to predict the structure of polypeptides by proposing a structural form with a precision limited to the structural code. However, by analyzing structural forms in native forms of proteins based on the fuzzy oil drop model, one can also determine the status of polypeptide chain fragments with respect to the assumptions of this model. Whether the probability distributions for both compliant and noncompliant forms were similar or whether the tetrapeptide sequences showed some differences at a level of a set of structural codes was investigated. The analysis presented here indicated that some sequences in both forms revealed differences in probability distributions expressed as a negative statistically significant correlation coefficient. This meant that the identified sections (tetrapeptides) took different forms against the fuzzy oil drop model. It may suggest that the information of the final status with respect to hydrophobic core formation is already carried by the structure of the early-stage intermediate.
机译:该模型描述了一种确定蛋白质折叠过程中早期中间体结构的方法,以分析非冗余的PDB蛋白质碱基,该模型可以确定四肽序列及其由结构代码表示的结构形式之间的关系。表达这种关系的列联表可以通过提出具有限于结构密码的精度的结构形式来用于预测多肽的结构。然而,通过基于模糊油滴模型分析蛋白质天然形式的结构形式,相对于该模型的假设,还可以确定多肽链片段的状态。研究了顺应性和不顺应性形式的概率分布是否相似,或者四肽序列在一组结构密码的水平上是否显示出一些差异。此处进行的分析表明,两种形式的某些序列都揭示了概率分布的差异,表示为负的统计显着相关系数。这意味着针对模糊油滴模型,识别出的部分(四肽)采取不同的形式。可能暗示有关疏水核形成的最终状态的信息已经被早期中间体的结构所携带。

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