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甲状腺激素诱导动脉平滑肌细胞增殖:发现新的 TRalpha1-Nox1 通路。

Thyroid hormone induces artery smooth muscle cell proliferation: discovery of a new TRalpha1-Nox1 pathway.

机构信息

Department of Physiology, College of Medicine, University of Oklahoma Health Sciences Center (OUHSC), Oklahoma City, OK, USA.

出版信息

J Cell Mol Med. 2010 Jan;14(1-2):368-80. doi: 10.1111/j.1582-4934.2008.00489.x.

DOI:10.1111/j.1582-4934.2008.00489.x
PMID:20414976
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2888973/
Abstract

Thyroid hormone (T3) can stimulate protein synthesis and cell growth. NOX1 is a mitogenic oxidase. The aim of this study was to test a novel hypothesis that T3 induces artery smooth muscle cell proliferation by up-regulating NOX1. Immunofluoresence confocal microscopy was used to visualize the sub-cellular localization of NOX1 and TRalpha1 in rat aorta smooth muscle (RASM) cells. Optical sectioning showed that TRalpha1 and NOX1 co-localized around the nucleus. T3 promoted RASM cell proliferation as determined by the fact that T3 significantly increased the number of cytokinesis cells, proliferating cellular nuclear antigen (PCNA) and smooth muscle alpha-actin (SM alpha-actin). T3 increased NOX1 expression at both the transcription (mRNA) and translation (protein) levels as evaluated by RT-PCR and Western blot, respectively. T3 also significantly increased the intracellular ROS production based on the oxidation of 2',7'-dichlorodihydrofluoresein (H2DCF) to a fluorescent 2',7'-dichlorofluoresein (DCF). RNAi silence of TRalpha1 or NOX1 abolished T3-induced intracellular ROS generation and PCNA and SM alpha-actin expression, indicating that TRalpha1 and NOX1 mediated T3-induced RASM cell proliferation. Notably, RNAi silence of TRalpha1 blocked the T3-induced increase in NOX1 expression, whereas silence of NOX1 did not affect TRalpha1 expression, disclosing a new pathway, i.e. T3-TRalpha1-NOX1-cell proliferation. TRalpha1 and NOX1 co-localized around the nucleus. T3 induced RASM cell proliferation by up-regulating NOX1 in a TRalpha1-dependent manner.

摘要

甲状腺激素 (T3) 可刺激蛋白质合成和细胞生长。NOX1 是一种有丝分裂氧化酶。本研究旨在验证一个新假说,即 T3 通过上调 NOX1 诱导动脉平滑肌细胞增殖。免疫荧光共聚焦显微镜用于观察大鼠主动脉平滑肌 (RASM) 细胞中 NOX1 和 TRalpha1 的亚细胞定位。光学切片显示,TRalpha1 和 NOX1 围绕细胞核共定位。T3 促进 RASM 细胞增殖,因为 T3 显著增加了细胞分裂细胞、增殖细胞核抗原 (PCNA) 和平滑肌α肌动蛋白 (SM α-肌动蛋白) 的数量。T3 分别通过 RT-PCR 和 Western blot 评估分别在转录 (mRNA) 和翻译 (蛋白质) 水平上增加了 NOX1 的表达。T3 还显著增加了基于 2',7'-二氯二氢荧光素 (H2DCF) 氧化为荧光 2',7'-二氯荧光素 (DCF) 的细胞内 ROS 产生。TRalpha1 或 NOX1 的 RNAi 沉默消除了 T3 诱导的细胞内 ROS 产生和 PCNA 和 SM α-肌动蛋白表达,表明 TRalpha1 和 NOX1 介导了 T3 诱导的 RASM 细胞增殖。值得注意的是,TRalpha1 的 RNAi 沉默阻断了 T3 诱导的 NOX1 表达增加,而 NOX1 的沉默不影响 TRalpha1 的表达,揭示了一条新途径,即 T3-TRalpha1-NOX1-细胞增殖。TRalpha1 和 NOX1 围绕细胞核共定位。T3 通过依赖于 TRalpha1 的方式上调 NOX1 诱导 RASM 细胞增殖。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c8bf/3837615/a8f8117b5417/jcmm0014-0368-f1.jpg

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