As a prevalent primary myocardial disease, dilated cardiomyopathy (DCM) represents the most common cause of heart failure in the young and the most frequent indication for cardiac transplantation. Aggregating evidence highlights the genetic basis of DCM. However, due to substantial genetic heterogeneity, the genetic defects of DCM in most cases remain elusive. In the current investigation, the entire coding exons and splicing junctions of the KLF5 gene, which encodes a key transcription factor required for cardiac structural and functional remodeling, were sequenced in 234 probands affected with DCM, and a heterozygous KLF5 mutation, NM_001730.5: c.1100T > A; p.(Leu367*), was identified in a proband. Genetic analysis of the proband's family members revealed that the identified KLF5 mutation co-segregated with DCM in the family with complete penetrance. The nonsense mutation was neither detected in 506 control individuals nor reported in such population-genetics databases as ExAC, dbSNP and gnomAD. Biological assays with a dual-luciferase reporter assay system demonstrated that the mutant KLF5 protein had no transcriptional activity when compared with its wildtype counterpart. Furthermore, the mutation abrogated the synergistic transactivation between KLF5 and NFKB1, another pivotal transcription factor that has been causally linked to DCM. The whole-exome sequencing analysis of the proband's family members revealed no other causative genes. The findings indicate KLF5 as a new gene contributing to DCM in humans, implying potential implications for the precision medicine of DCM.
基金:
National Natural Science Foundation of ChinaNational Natural Science Foundation of China (NSFC) [81470372, 81600228]; Medicine Guided Program of Shanghai, China [19411971900]; Clinical Medicine Program of Shanghai, China [19401970200]; Program of Health and Family Planning Commission of Shanghai, China [20154Y0026]; Natural Science Foundation of Minhang District, Shanghai, China [2018MHZ072, 2019MHZ014]; Acute Heart Failure Specialty Program of Health and Family Planning Commission of Changning District, Shanghai, China [20162002]; Key Project of the Fifth People's Hospital of Shanghai, Fudan University, China [2018WYZD05]
通讯机构:[1]Fudan Univ, Peoples Hosp Shanghai 5, Dept Cardiol, 801 Heqing Rd, Shanghai 200240, Peoples R China[2]Fudan Univ, Peoples Hosp Shanghai 5, Ctr Complex Cardiac Arrhythmias Minhang Dist, Shanghai, Peoples R China[5]Fudan Univ, Peoples Hosp Shanghai 5, Cardiovasc Res Lab, 801 Heqing Rd, Shanghai 200240, Peoples R China[6]Fudan Univ, Peoples Hosp Shanghai 5, Cent Lab, Shanghai, Peoples R China[*1]Department of Cardiology, The Fifth People's Hospital of Shanghai, Fudan University, 801 Heqing Road, Shanghai, 200240, China.[*2]Cardiovascular Research Laboratory, The Fifth People's Hospital of Shanghai, Fudan University, 801 Heqing Road, Shanghai, 200240, China.
推荐引用方式(GB/T 7714):
Di Ruo-Min,Yang Chen-Xi,Zhao Cui-Mei,et al.Identification and functional characterization of KLF5 as a novel disease gene responsible for familial dilated cardiomyopathy[J].EUROPEAN JOURNAL OF MEDICAL GENETICS.2020,63(4):doi:10.1016/j.ejmg.2019.103827.
APA:
Di, Ruo-Min,Yang, Chen-Xi,Zhao, Cui-Mei,Yuan, Fang,Qiao, Qi...&Yang, Yi-Qing.(2020).Identification and functional characterization of KLF5 as a novel disease gene responsible for familial dilated cardiomyopathy.EUROPEAN JOURNAL OF MEDICAL GENETICS,63,(4)
MLA:
Di, Ruo-Min,et al."Identification and functional characterization of KLF5 as a novel disease gene responsible for familial dilated cardiomyopathy".EUROPEAN JOURNAL OF MEDICAL GENETICS 63..4(2020)
