RNA Splicing Events in Circulation Distinguish Individuals with and without New-Onset Type 1 Diabetes.

Bobbie-Jo M Webb-Robertson,Wenting Wu,Javier E Flores,Lisa M Bramer,Farooq Syed,Sarah A Tersey,Sarah C May,Emily K Sims,Carmella Evans-Molina,Raghavendra G Mirmira
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Abstract

CONTEXT Alterations in RNA splicing may influence protein isoform diversity that contributes to or reflects the pathophysiology of certain diseases. Whereas specific RNA splicing events in pancreatic islets have been investigated in models of inflammation in vitro, how RNA splicing in the circulation correlates with or is reflective of T1D disease pathophysiology in humans remains unexplored. OBJECTIVE To use machine learning to investigate if alternative RNA splicing events differ between individuals with and without new-onset type 1 diabetes (T1D) and to determine if these splicing events provide insight into T1D pathophysiology. METHODS RNA deep sequencing was performed on whole blood samples from two independent cohorts: a training cohort consisting of 12 individuals with new-onset T1D and 12 age- and sex-matched nondiabetic controls and a validation cohort of the same size and demographics. Machine learning analysis was used to identify specific isoforms that could distinguish individuals with T1D from controls. RESULTS Distinct patterns of RNA splicing differentiated participants with T1D from unaffected controls. Notably, certain splicing events, particularly involving retained introns, showed significant association with T1D. Machine learning analysis using these splicing events as features from the training cohort demonstrated high accuracy in distinguishing between T1D subjects and controls in the validation cohort. Gene Ontology pathway enrichment analysis of the retained intron category showed evidence for a systemic viral response in T1D subjects. CONCLUSIONS Alternative RNA splicing events in whole blood are significantly enriched in individuals with new-onset T1D and can effectively distinguish these individuals from unaffected controls. Our findings also suggest that RNA splicing profiles offer the potential to provide insights into disease pathogenesis.
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血液循环中的 RNA 剪接事件可区分新发 1 型糖尿病患者与非新发 1 型糖尿病患者。
摘要:RNA剪接的变化可能会影响蛋白质同工酶的多样性,从而导致或反映某些疾病的病理生理学。目的利用机器学习研究新发1型糖尿病(T1D)患者与非新发1型糖尿病(T1D)患者之间的RNA剪接事件是否存在差异,并确定这些剪接事件是否有助于深入了解T1D的病理生理学。方法对两个独立队列的全血样本进行了RSNA深度测序:一个训练队列由12名新发T1D患者和12名年龄和性别匹配的非糖尿病对照组组成,另一个验证队列具有相同的规模和人口统计学特征。结果不同的 RNA 剪接模式将 T1D 患者与未受影响的对照组区分开来。值得注意的是,某些剪接事件,尤其是涉及保留内含子的剪接事件,与 T1D 有显著关联。使用这些剪接事件作为训练队列特征的机器学习分析表明,在区分验证队列中的 T1D 受试者和对照组时具有很高的准确性。对保留的内含子类别进行的基因本体通路富集分析表明,有证据表明 T1D 受试者存在全身性病毒反应。我们的研究结果还表明,RNA剪接图谱具有深入了解疾病发病机制的潜力。
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