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PANCR,即PITX2相邻非编码RNA,在人左心房中表达并调节PITX2c的表达。

PANCR, the PITX2 Adjacent Noncoding RNA, Is Expressed in Human Left Atria and Regulates PITX2c Expression.

作者信息

Gore-Panter Shamone R, Hsu Jeffrey, Barnard John, Moravec Christine S, Van Wagoner David R, Chung Mina K, Smith Jonathan D

机构信息

From the Department of Molecular Cardiology, Lerner Research Institute (S.R.G.-P., C.S.M., D.R.V.W., M.K.C.), Department of Cellular & Molecular Medicine, Lerner Research Institute (S.R.G.-P., J.H., J.D.S.), Department of Quantitative Health Sciences (J.B.), and Department of Cardiovascular Medicine (C.S.M., D.R.V.W., M.K.C., J.D.S.), Cleveland Clinic, OH.

出版信息

Circ Arrhythm Electrophysiol. 2016 Jan;9(1):e003197. doi: 10.1161/CIRCEP.115.003197.

Abstract

BACKGROUND

Genome-wide studies reveal that genetic variants at chromosome 4q25 constitute the strongest locus associated with atrial fibrillation, the most frequent arrhythmia. However, the mechanisms underlying this association are unknown. Our goal is to find and characterize left atrial-expressed transcripts in the chromosome 4q25 atrial fibrillation risk locus that may play a role in atrial fibrillation pathogenesis.

METHODS AND RESULTS

RNA sequencing performed on human left/right pairs identified an intergenic long noncoding RNA adjacent to the PITX2 gene, which we have named PANCR (PITX2 adjacent noncoding RNA). In a human tissue screen, PANCR was expressed specifically in the left atria and eye and in no other chambers of the heart. The levels of PANCR and PITX2c RNAs were highly correlated in 233 human left atrial appendage samples. PANCR levels were not associated with either atrial rhythm status or the genotypes of the chromosome 4q25 atrial fibrillation risk variants. Both PANCR and PITX2c RNAs were induced early during differentiation of human embryonic stem cells into cardiomyocytes. Because long noncoding RNAs often control gene expression, we performed siRNA-mediated knockdown of PANCR, and this treatment repressed PITX2c expression and mimicked the effects of PITX2c knockdown on global mRNA and miRNA expression. Cell fractionation studies demonstrate that PANCR is primarily localized in the cytoplasm.

CONCLUSIONS

PANCR and PITX2c are coordinately expressed early during cardiomyocyte differentiation from stem cells. PANCR knockdown decreased PITX2c expression in differentiated cardiomyocytes, altering the transcriptome in a manner similar to PITX2c knockdown.

摘要

背景

全基因组研究表明,4号染色体q25区域的基因变异构成了与心房颤动(最常见的心律失常)相关的最强位点。然而,这种关联背后的机制尚不清楚。我们的目标是在4号染色体q25心房颤动风险位点中寻找并鉴定在左心房表达的转录本,这些转录本可能在心房颤动的发病机制中发挥作用。

方法与结果

对人类左右心房配对样本进行RNA测序,鉴定出一个与PITX2基因相邻的基因间长链非编码RNA,我们将其命名为PANCR(PITX2相邻非编码RNA)。在人体组织筛查中,PANCR仅在左心房和眼睛中表达,在心脏的其他腔室中均未表达。在233份人类左心耳样本中,PANCR和PITX2c RNA的水平高度相关。PANCR水平与心房节律状态或4号染色体q25心房颤动风险变异的基因型均无关。在人类胚胎干细胞分化为心肌细胞的早期,PANCR和PITX2c RNA均被诱导表达。由于长链非编码RNA通常控制基因表达,我们进行了siRNA介导的PANCR敲低实验,该处理抑制了PITX2c的表达,并模拟了PITX2c敲低对整体mRNA和miRNA表达的影响。细胞分级分离研究表明,PANCR主要定位于细胞质中。

结论

PANCR和PITX2c在干细胞向心肌细胞分化早期协同表达。在分化的心肌细胞中,PANCR敲低降低了PITX2c的表达,以类似于PITX2c敲低的方式改变了转录组。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/55a2/4719779/3e621e4b93a6/nihms743440f1.jpg

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