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初步研究:鉴定酒精性慢性胰腺炎特有的循环miRNA特征及其对酒精介导的胰腺组织损伤的影响。

Pilot study identifying circulating miRNA signature specific to alcoholic chronic pancreatitis and its implication on alcohol-mediated pancreatic tissue injury.

作者信息

Chhatriya Bishnupriya, Sarkar Piyali, Nath Debashis, Ray Sukanta, Das Kshaunish, Mohapatra Saroj K, Goswami Srikanta

机构信息

National Institute of Biomedical Genomics Kalyani India.

Department of Cytogenetics Tata Medical Centre Kolkata India.

出版信息

JGH Open. 2020 Jul 15;4(6):1079-1087. doi: 10.1002/jgh3.12389. eCollection 2020 Dec.

Abstract

BACKGROUND AND AIM

Alcohol exerts its effects on organs in multiple ways. Alcoholic chronic pancreatitis (ACP) is a disease in which alcohol triggers the pathological changes in pancreas, leading to chronic inflammation and fibrosis. The molecular mechanism behind these changes is not clear. Identification of key circulating miRNA changes in ACP patients and determination of the fraction that is secreted from diseased pancreas not only could serve as potential biomarker for assessing disease severity, but also could help identifying the molecular alterations prevailing in the organ precipitating the disease, to some extent.

METHODS

We performed microRNA microarray using the Affymetrix miRNA 4.0 platform to identify differentially expressed miRNAs in serum of ACP patients as compared to alcoholic control individuals and then found out how many of them could be pancreas-specific and exosomally secreted. We further analyzed a pancreatitis-specific gene expression data set to find out the differentially expressed genes in diseased pancreas and explored the possible role of those selected miRNAs in regulation of gene expression in ACP.

RESULTS

We identified 14 miRNAs differentially expressed in both serum and pancreas and also identified their experimentally validated targets. Transcription factors modulating the miRNA expression in an alcohol-dependent manner were also identified and characterized to derive the miRNA-gene-TF interaction network responsible for progression of the disease.

CONCLUSIONS

Differentially expressed miRNA signature demonstrated significant changes in both pro- and anti-inflammatory pathways probably balancing the chronic inflammation in the pancreas. Our findings also suggested possible involvement of pancreatic stellate cells in disease progression.

摘要

背景与目的

酒精通过多种方式对器官产生影响。酒精性慢性胰腺炎(ACP)是一种酒精引发胰腺病理变化,导致慢性炎症和纤维化的疾病。这些变化背后的分子机制尚不清楚。鉴定ACP患者关键循环miRNA的变化以及确定病变胰腺分泌的部分,不仅可作为评估疾病严重程度的潜在生物标志物,还能在一定程度上帮助识别引发该疾病的器官中普遍存在的分子改变。

方法

我们使用Affymetrix miRNA 4.0平台进行miRNA微阵列分析,以鉴定ACP患者血清中与酒精对照个体相比差异表达的miRNA,然后确定其中有多少可能是胰腺特异性且通过外泌体分泌的。我们进一步分析了一个胰腺炎特异性基因表达数据集,以找出病变胰腺中差异表达的基因,并探讨这些选定miRNA在调控ACP基因表达中的可能作用。

结果

我们鉴定出14种在血清和胰腺中均差异表达的miRNA,并确定了它们经过实验验证的靶点。还鉴定并表征了以酒精依赖方式调节miRNA表达的转录因子,以推导负责疾病进展的miRNA-基因-TF相互作用网络。

结论

差异表达的miRNA特征表明,促炎和抗炎途径均发生了显著变化,这可能在平衡胰腺中的慢性炎症。我们的研究结果还表明胰腺星状细胞可能参与疾病进展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9706/7731805/e0a07d84f86c/JGH3-4-1079-g001.jpg

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