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鉴定鼠源磷酸二酯酶 5A 同工型及其在 HL-1 心脏细胞系中的功能特征。

Identification of murine phosphodiesterase 5A isoforms and their functional characterization in HL-1 cardiac cell line.

机构信息

Department of Experimental Medicine, Sapienza University, Rome, Italy.

Department of Anatomical, Histological, Forensic Medicine and Orthopedic Sciences, Sapienza University, Rome, Italy.

出版信息

J Cell Physiol. 2018 Jan;233(1):325-337. doi: 10.1002/jcp.25880. Epub 2017 May 18.

DOI:10.1002/jcp.25880
PMID:28247930
Abstract

Phosphodiesterase 5A (PDE5A) specifically degrades the ubiquitous second messenger cGMP and experimental and clinical data highlight its important role in cardiac diseases. To address PDE5A role in cardiac physiology, three splice variants of the PDE5A were cloned for the first time from mouse cDNA library (mPde5a1, mPde5a2, and mPde5a3). The predicted amino acidic sequences of the three murine isoforms are different in the N-terminal regulatory domain. mPDE5A isoforms were transfected in HEK293T cells and they showed high affinity for cGMP and similar sensitivity to sildenafil inhibition. RT-PCR analysis showed that mPde5a1, mPde5a2, and mPde5a3 had differential tissue distribution. In the adult heart, mPde5a1 and mPde5a2 were expressed at different levels whereas mPde5a3 was undetectable. Overexpression of mPDE5As induced an increase of HL-1 number cells which progress into cell cycle. mPDE5A1 and mPDE5A3 overexpression increased the number of polyploid and binucleated cells, mPDE5A3 widened HL-1 areas, and modulated hypertrophic markers more efficiently respect to the other mPDE5A isoforms. Moreover, mPDE5A isoforms had differential subcellular localization: mPDE5A1 was mainly localized in the cytoplasm, mPDE5A2 and mPDE5A3 were also nuclear localized. These results demonstrate for the first time the existence of three PDE5A isoforms in mouse and highlight their potential role in the induction of hypertrophy.

摘要

磷酸二酯酶 5A(PDE5A)特异性降解普遍存在的第二信使 cGMP,实验和临床数据突出了其在心脏疾病中的重要作用。为了解决 PDE5A 在心脏生理学中的作用,首次从小鼠 cDNA 文库中克隆了 PDE5A 的三种剪接变体(mPde5a1、mPde5a2 和 mPde5a3)。三种鼠源同工型的预测氨基酸序列在 N 端调节域不同。将 mPDE5A 同工型转染 HEK293T 细胞,它们对 cGMP 表现出高亲和力和对西地那非抑制的相似敏感性。RT-PCR 分析显示 mPde5a1、mPde5a2 和 mPde5a3 在组织分布上存在差异。在成年心脏中,mPde5a1 和 mPde5a2 表达水平不同,而 mPde5a3 无法检测到。mPDE5As 的过表达诱导 HL-1 细胞数量增加并进入细胞周期。mPDE5A1 和 mPDE5A3 的过表达增加了多倍体和双核细胞的数量,mPDE5A3 扩大了 HL-1 区域,并比其他 mPDE5A 同工型更有效地调节肥大标志物。此外,mPDE5A 同工型具有不同的亚细胞定位:mPDE5A1 主要定位于细胞质,mPDE5A2 和 mPDE5A3 也定位于核内。这些结果首次证明了三种 PDE5A 同工型在小鼠中的存在,并强调了它们在诱导肥大中的潜在作用。

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