内质网应激相关lncrna影响腹主动脉瘤炎症和VSMC功能的鉴定

IF 7.7 2区医学 Q1 MEDICINE, RESEARCH & EXPERIMENTAL

Clinical science Pub Date : 2025-03-25 DOI:10.1042/CS20242476

Rafael Almendra-Pegueros, Cristina Rodriguez, Mercedes Camacho, David Sánchez-Infantes, J Luis Sánchez-Quesada, Susana Cáncer, Elvira Pérez-Marlasca, Gema Medina-Gómez, José Martinez-González, Ana B García-Redondo, María Galán

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引用次数: 0

摘要

内质网（ER）应激在腹主动脉瘤（AAA）中起关键作用，腹主动脉瘤是一种以炎症、破坏性重塑和血管平滑肌细胞（VSMC）功能障碍为特征的危及生命的疾病。目前的治疗依赖于手术修复，但没有有效的药物策略来限制动脉瘤的进展。lncrna是健康和疾病的重要因素，然而，它们对AAA发展的具体贡献及其与内质网应激的关系仍未被探索。在这里，我们进行了一项全基因组转录组学分析，表征了AAA中lncRNAs的表达谱。我们在AAA患者和健康供者的腹主动脉中进行了RNA测序。我们鉴定了6576个差异表达（DE） mrna和1283个DE- lncrna。有趣的是，生物信息学分析揭示了一组368个de - lncrna与内质网应激相关。在大量AAA患者队列中验证了诱导最多的lncrna （IL-21-AS1、ITPKB-IT、PCED1B-AS1、TCL-6、LINC00494、LINC00582、LINC00626、LINC00861和LINC00892）的差异表达，并通过ROC曲线和logistic回归分析建立了这些lncrna区分AAA患者和健康受试者的能力。在人主动脉VSMC和Jurkat t细胞中，tunicamycin诱导的内质网应激触发了IL21-AS1、LINC00626、LINC00494、LINC00892、PCED1B-AS1、ITPKB-IT和TCL-6的表达，而TUDCA抵消了这些影响。最后，对mRNA-lncRNA共表达的综合分析揭示了所选择的lncrna与参与免疫反应和肌肉收缩的de - mrna之间的相关性。因此，这些可能参与内质网应激反应（AAA的病理过程）的de - lncrna可以被认为是治疗AAA的潜在治疗靶点。

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Identification of endoplasmic reticulum stress-associated lncRNAs influencing inflammation and VSMC function in abdominal aortic aneurysm.

Endoplasmic reticulum (ER) stress plays a critical role in the abdominal aortic aneurysm (AAA), a life-threatening disease characterized by inflammation, destructive remodeling, and vascular smooth muscle cells (VSMCs) dysfunction. The current therapy relies on surgical repair, but no effective pharmacological strategies are available to limit aneurysm progression. Long non-coding RNAs (lncRNAs) are essential factors in health and disease; however, their specific contribution to AAA development and its relationship with ER stress remain unexplored. Here, we have performed a whole-genome transcriptomic analysis characterizing the expression profile of lncRNAs in AAA. RNA sequencing was carried out in abdominal aorta from patients with AAA and healthy donors. We identified 6576 differentially expressed (DE)-mRNAs and 1283 DE-lncRNAs. Interestingly, bioinformatic analysis revealed a set of 368 DE-lncRNAs related to ER stress. The differential expression of the most induced lncRNAs (IL-21-AS1, ITPKB-IT, PCED1B-AS1, TCL-6, LINC00494, LINC00582, LINC00626, LINC00861, and LINC00892) was validated in a large cohort of patients with AAA. The ability of these selected lncRNAs to discriminate patients with AAA from healthy subjects was established by receiveroperating characteristic curves and logistic regression analysis. In human aortic VSMC and Jurkat T-cells, tunicamycin-induced ER stress triggered the expression of IL21-AS1, LINC00626, LINC00494, LINC00892, PCED1B-AS1, ITPKB-IT, and TCL-6, while tauroursodeoxycholic acid counteracted these effects. Finally, an integrated analysis of mRNA-lncRNA co-expression revealed the correlation between the selected lncRNAs and the DE-mRNAs involved in immune response and muscle contraction. Therefore, these DE-lncRNAs potentially implicated in the ER stress response, a pathological process in AAA, could be considered as potential therapeutic target to handle AAA.

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来源期刊

Clinical science 医学-医学：研究与实验

CiteScore

11.40

自引率

0.00%

发文量

189

审稿时长

4-8 weeks

期刊介绍： Translating molecular bioscience and experimental research into medical insights, Clinical Science offers multi-disciplinary coverage and clinical perspectives to advance human health. Its international Editorial Board is charged with selecting peer-reviewed original papers of the highest scientific merit covering the broad spectrum of biomedical specialities including, although not exclusively: Cardiovascular system Cerebrovascular system Gastrointestinal tract and liver Genomic medicine Infection and immunity Inflammation Oncology Metabolism Endocrinology and nutrition Nephrology Circulation Respiratory system Vascular biology Molecular pathology.