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Using a novel clumpiness measure to unite data with metadata: Finding common sequence patterns in immune receptor germline V genes

机译:使用一种新颖的度量方法将数据与元数据结合起来:在免疫受体种系V基因中发现常见的序列模式

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摘要

When finding relationships in biological systems, we often describe hierarchies based on one facet of the data. However, when using this hierarchy to elucidate relationships between metadata, the distribution of metadata labels within the hierarchy may exhibit different levels of aggregation-uniform, random, or clumped. As of now, there exists no measure for finding the level of aggregation, or "clumpiness", between labels distributed among the leaves of a hierarchical container. We propose a clumpiness measure to aid in the quantification of relationships between metadata. We validated our measure with random trees and found that the measure is resistant to changes in the tree size, label size, and the number of types of labels, compared to the closest alternative measures. We used our clumpiness measure to quantify the relationships between light and heavy chains in human and mouse B cell and T cell receptor V genes based on their motifs. We found that the B cell heavy chains were the most aggregated while the T cell chains were the least aggregated and that the IGL chain was clumped the most with the T cell chains out of all of the B cell chains. (C) 2016 Elsevier B.V. All rights reserved.
机译:在生物系统中查找关系时,我们经常根据数据的一个方面来描述层次结构。但是,当使用此层次结构阐明元数据之间的关系时,层次结构内元数据标签的分布可能会表现出不同级别的聚合均匀,随机或成簇。到目前为止,还没有找到用于发现在分层容器的叶子之间分布的标签之间的聚集或“块状”程度的措施。我们提出一种笨拙的措施来帮助量化元数据之间的关系。我们使用随机树对我们的度量进行了验证,发现与最接近的替代度量相比,该度量可抵抗树大小,标签大小和标签类型数量的变化。我们使用团聚度来量化人类和小鼠B细胞和T细胞受体V基因中的轻链和重链之间的关系,基于它们的基序。我们发现B细胞重链聚集最多,而T细胞链聚集最少,并且在所有B细胞链中,IGL链的T细胞链聚集最多。 (C)2016 Elsevier B.V.保留所有权利。

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