Qiong Zhan
Southern Medical University
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Publication
Featured researches published by Qiong Zhan.
Molecular Medicine Reports | 2018
Zuheng Liu; Jinghai Hua; Wanqiang Cai; Qiong Zhan; Wenyan Lai; Qingchun Zeng; Hao Ren; Dingli Xu
N-terminal truncated peroxisome proliferator-activated receptor-γ coactivator-1α (NT-PGC-1α) is an alternative splice variant of PGC-1α. NT-PGC-1α exhibits stronger anti-obesity effects in adipose tissue than PGC-1α; however, NT-PGC-1α has not yet been investigated in neonatal rat cardiomyocytes (NRCMs). The present study aimed to investigate the role of NT-PGC-1α in mitochondrial fatty acid metabolism and its possible regulatory mechanism in NRCMs. NRCMs were exposed to phenylephrine (PE) or angiotensin II (Ang II) to induce cardiac hypertrophy. Following this, NRCMs were infected with adenovirus expressing NT-PGC-1α, and adenosine 5′-triphsophate (ATP) levels, reactive oxygen species (ROS) generation and mitochondrial membrane potential were subsequently detected. In addition, western blotting, lipid droplet staining and oxygen consumption assays were performed to examine the function of NT-PGC-1α in fatty acid metabolism. NT-PGC-1α was demonstrated to be primarily expressed in the cytoplasm, which differed from full-length PGC-1α, which was predominantly expressed in the nucleus. NT-PGC-1α overexpression alleviated mitochondrial function impairment, including ATP generation, ROS production and mitochondrial membrane potential integrity. Furthermore, NT-PGC-1α overexpression alleviated the PE-induced suppression of fatty acid metabolism-associated protein expression, increased extracellular oxygen consumption and decreased lipid droplet accumulation in NRCMs. Taken together, the present study demonstrated that NT-PGC-1α alleviated PE-induced mitochondrial impairment and decreased lipid droplet accumulation in NRCMs, indicating that NT-PGC-1α may have ameliorated mitochondrial energy defects in NRCMs, and may be considered as a potential target for the treatment of heart failure.
Journal of the American College of Cardiology | 2018
Wenjun Xiong; Jiaying Li; Zhengliang Peng; Zhuang Ma; Xiangkun Xie; Hanlin Li; Zhen Se; Wenyan Lai; Qiong Zhan; Qingchun Zeng; Hao Ren; Dingli Xu
Angiotensin Ⅱ (Ang Ⅱ)-induced cardiac injury can result in elevated oxidative stress and decreased mitochondrial quality. Meanwhile, PTEN induced putative kinase 1 (PINK1) participate in mitochondrial quality control. However, the mechanism of PINK1 in Ang Ⅱ-induced cardiac injury remain
Medical Science Monitor | 2018
Jinghai Hua; Zhanghua Liu; Zuheng Liu; Dongqi An; Wenyan Lai; Qiong Zhan; Qingchun Zeng; Hao Ren; Dingli Xu
Journal of the American College of Cardiology | 2018
Qingchun Zeng; Zuheng Liu; Jiaying Li; Haiyue Liu; Ying Tang; Wenyan Lai; Yan Tu; Zhonghua Teng; Qiong Zhan; Yujia Bai; Hao Ren; Dingli Xu
Journal of the American College of Cardiology | 2018
Jiaying Li; Qingchun Zeng; Xi Yang; Zuheng Liu; Wenjun Xiong; Tianyu Xu; Qiong Zhan; Yujia Bai; Wenyan Lai; Hao Ren; Dingli Xu
Journal of Hypertension | 2018
Yuli Huang; Zhihui Deng; Zhen Se; Yujia Bai; Chuanjie Yan; Qiong Zhan; Qingchun Zeng; Ping Ouyang; Meng Dai; Dingli Xu
Journal of the American College of Cardiology | 2017
Qingchun Zeng; Tianyu Xu; Jiaying Li; Xi Yang; Qiong Zhan; Yufeng Zhai; Lihua Ao; Xianzhong Meng; Dingli Xu
Journal of the American College of Cardiology | 2017
Jiaying Li; Qingchun Zeng; Xi Yang; Tianyu Xu; Dongqi An; Qiong Zhan; Xingfu Huang; Yan Tu; Wenyan Lai; Dingli Xu
Journal of the American College of Cardiology | 2017
Xi Yang; Qingchun Zeng; Jiaying Li; Tianyu Xu; Dingji Zhu; Dongqi An; Haobin Zhou; Zuheng Liu; Wanqiang Cai; Qiong Zhan; Wenyan Lai; Dingli Xu
Journal of the American College of Cardiology | 2017
Dongqi An; Qiong Zhan; Yujia Bai; Xingfu Huang; Wenyan Lai; Qingchun Zeng; Hao Ren; Dingli Xu
