Phenotype similarities in automatically grouped T2D patients by variation-based clustering of IL-1β gene expression.

Q2 Medicine Electronic Journal of the International Federation of Clinical Chemistry and Laboratory Medicine Pub Date : 2023-10-16 eCollection Date: 2023-10-01
Lucio José Pantazis, Gustavo Daniel Frechtel, Gloria Edith Cerrone, Rafael García, Andrea Elena Iglesias Molli
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Abstract

Background: Analyzing longitudinal gene expression data is extremely challenging due to limited prior information, high dimensionality, and heterogeneity. Similar difficulties arise in research of multifactorial diseases such as Type 2 Diabetes. Clustering methods can be applied to automatically group similar observations. Common clinical values within the resulting groups suggest potential associations. However, applying traditional clustering methods to gene expression over time fails to capture variations in the response. Therefore, shape-based clustering could be applied to identify patient groups by gene expression variation in a large time metabolic compensatory intervention.

Objectives: To search for clinical grouping patterns between subjects that showed similar structure in the variation of IL-1β gene expression over time.

Methods: A new approach for shape-based clustering by IL-1β expression behavior was applied to a real longitudinal database of Type 2 Diabetes patients. In order to capture correctly variations in the response, we applied traditional clustering methods to slopes between measurements.

Results: In this setting, the application of K-Medoids using the Manhattan distance yielded the best results for the corresponding database. Among the resulting groups, one of the clusters presented significant differences in many key clinical values regarding the metabolic syndrome in comparison to the rest of the data.

Conclusions: The proposed method can be used to group patients according to variation patterns in gene expression (or other applications) and thus, provide clinical insights even when there is no previous knowledge on the subject clinical profile and few timepoints for each individual.

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通过IL-1β基因表达的变异聚类自动分组的T2D患者的表型相似性。
背景:由于先验信息有限、维度高和异质性,分析纵向基因表达数据极具挑战性。在2型糖尿病等多因素疾病的研究中也出现了类似的困难。聚类方法可以用于自动对相似的观察结果进行分组。结果组中的共同临床价值表明了潜在的关联。然而,随着时间的推移,将传统的聚类方法应用于基因表达并不能捕捉到反应的变化。因此,基于形状的聚类可以应用于在大时间代谢补偿干预中通过基因表达变化来识别患者群体。目的:寻找IL-1β基因表达随时间变化具有相似结构的受试者之间的临床分组模式。方法:将一种新的基于IL-1β表达行为的形状聚类方法应用于2型糖尿病患者的真实纵向数据库。为了正确地捕捉响应的变化,我们将传统的聚类方法应用于测量之间的斜率。结果:在这种情况下,使用曼哈顿距离的K-Medoids的应用在相应的数据库中产生了最好的结果。在由此产生的组中,与其他数据相比,其中一个聚类在代谢综合征的许多关键临床价值方面存在显著差异。结论:所提出的方法可用于根据基因表达的变化模式(或其他应用)对患者进行分组,因此,即使在之前没有关于受试者临床概况的知识,每个人的时间点很少的情况下,也能提供临床见解。
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