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猫心肌转录组在健康和肥厚型心肌病中的研究——人类疾病的转化动物模型。

Feline myocardial transcriptome in health and in hypertrophic cardiomyopathy-A translational animal model for human disease.

机构信息

University of Guelph, Ontario Veterinary College, Department of Pathobiology, Guelph, Ontario, Canada.

University of Guelph, Ontario Veterinary College, Department of Clinical Studies, Guelph, Ontario, Canada.

出版信息

PLoS One. 2023 Mar 16;18(3):e0283244. doi: 10.1371/journal.pone.0283244. eCollection 2023.

Abstract

Hypertrophic cardiomyopathy (HCM) is the most common heart disease in cats, characterized by primary left ventricular hypertrophy. Feline HCM closely resembles human HCM and is suggested as translational animal model for the human disease. A genetic cause is established in humans and suspected for cats, but little is known about the gene expression and pathways involved in the pathogenesis of HCM. To investigate the myocardial transcriptome changes in HCM, RNA sequencing was conducted on left ventricle (LV) and left atrium (LA) samples of healthy cats and cats with HCM (each n = 5; 20 samples). Ingenuity Pathway Analysis was used to determine functional pathways, regulators, and networks. Distinct gene expression profiles were identified in the LV and LA of the feline healthy and HCM myocardium. Analysis of differentially expressed mRNAs (>2 fold; FDR < 0.01) found chamber-specific (LV vs. LA) expression in both healthy and HCM groups, with higher transcriptional activity in the LA. Genes that contribute to the distinct structure and function of each chamber in health and HCM were identified in the regional comparison. The gene expression profiles of HCM compared to healthy hearts revealed disease related genes, including THBS4 and KLHL33 (LV), FAM177B and THRSP (LA), the latter 3 have not been reported for the myocardium so far, as the top differently expressed genes in the HCM heart. Differently expressed genes and functional pathways found in the HCM heart are associated with cardiac remodeling and fibrosis, inflammation, microvascular changes, calcium signaling and cardiac metabolism, with some regional differences. RhoGDI-RhoGTPase signaling, integrin and ILK signaling pathways, the LXR/RXR pathway in the LA, and the PPARα/RXRα, HIF1α and CXCR4 pathways in the LV might be of particular importance in the HCM disease process. This study identified region-specific myocardial gene transcription patterns as well as novel genes and pathways associated with HCM.

摘要

肥厚型心肌病(HCM)是猫最常见的心脏病,其特征是原发性左心室肥厚。猫 HCM 与人类 HCM 非常相似,被认为是人类疾病的转化动物模型。在人类中已确定了遗传原因,并怀疑猫也存在遗传原因,但对 HCM 发病机制中涉及的基因表达和途径知之甚少。为了研究 HCM 中的心肌转录组变化,对健康猫和 HCM 猫的左心室(LV)和左心房(LA)样本(每组 n = 5;共 20 个样本)进行了 RNA 测序。使用 Ingenuity Pathway Analysis 确定功能途径、调节剂和网络。在 HCM 猫的 LV 和 LA 中鉴定到明显不同的基因表达谱。在健康和 HCM 组中均发现了 LV 与 LA 之间的腔室特异性(LV 与 LA)表达,且 LA 的转录活性更高。在区域比较中鉴定到了健康和 HCM 中每个腔室的独特结构和功能的基因。与健康心脏相比,HCM 心脏的基因表达谱揭示了与疾病相关的基因,包括 LV 中的 THBS4 和 KLHL33,以及 LA 中的 FAM177B 和 THRSP,后 3 个基因在心肌中尚未报道,它们是 HCM 心脏中差异表达最高的基因。在 HCM 心脏中发现的差异表达基因和功能途径与心脏重构和纤维化、炎症、微血管变化、钙信号和心脏代谢有关,在某些区域存在差异。LA 中的 RhoGDI-RhoGTPase 信号通路、整合素和 ILK 信号通路、LXR/RXR 通路,以及 LV 中的 PPARα/RXRα、HIF1α 和 CXCR4 通路可能在 HCM 疾病过程中具有特别重要的意义。本研究确定了与 HCM 相关的区域特异性心肌基因转录模式以及新的基因和途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/511a/10019628/71db6eb04fe1/pone.0283244.g001.jpg

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