Marian A J, Wu Y, Lim D S, McCluggage M, Youker K, Yu Q T, Brugada R, DeMayo F, Quinones M, Roberts R
Section of Cardiology, Department of Medicine, Baylor College of Medicine, Houston, Texas 77030, USA.
J Clin Invest. 1999 Dec;104(12):1683-92. doi: 10.1172/JCI7956.
Certain mutations in genes for sarcomeric proteins cause hypertrophic cardiomyopathy (HCM). We have developed a transgenic rabbit model for HCM caused by a common point mutation in the beta-myosin heavy chain (MyHC) gene, R400Q. Wild-type and mutant human beta-MyHC cDNAs were cloned 3' to a 7-kb murine beta-MyHC promoter. We injected purified transgenes into fertilized zygotes to generate two lines each of the wild-type and mutant transgenic rabbits. Expression of transgene mRNA and protein were confirmed by Northern blotting and 2-dimensional gel electrophoresis followed by immunoblotting, respectively. Animals carrying the mutant transgene showed substantial myocyte disarray and a 3-fold increase in interstitial collagen expression in their myocardia. Mean septal thicknesses were comparable between rabbits carrying the wild type transgene and their nontransgenic littermates (NLMs) but were significantly increased in the mutant transgenic animals. Posterior wall thickness and left ventricular mass were also increased, but dimensions and systolic function were normal. Premature death was more common in mutant than in wild-type transgenic rabbits or in NLMs. Thus, cardiac expression of beta-MyHC-Q(403) in transgenic rabbits induced hypertrophy, myocyte and myofibrillar disarray, interstitial fibrosis, and premature death, phenotypes observed in humans patients with HCM due to beta-MyHC-Q(403).
肌节蛋白基因的某些突变会导致肥厚型心肌病(HCM)。我们构建了一种转基因兔模型,用于研究由β-肌球蛋白重链(MyHC)基因常见点突变R400Q引起的HCM。将野生型和突变型人β-MyHC cDNA克隆到7 kb小鼠β-MyHC启动子的3'端。我们将纯化的转基因注射到受精卵中,分别产生了野生型和突变型转基因兔各两个品系。分别通过Northern印迹法和二维凝胶电泳后免疫印迹法证实了转基因mRNA和蛋白质的表达。携带突变转基因的动物心肌细胞出现明显紊乱,心肌间质胶原表达增加了3倍。携带野生型转基因的兔子与其非转基因同窝仔兔(NLMs)之间的平均室间隔厚度相当,但突变转基因动物的平均室间隔厚度显著增加。后壁厚度和左心室质量也增加,但尺寸和收缩功能正常。突变型转基因兔比野生型转基因兔或NLMs更容易过早死亡。因此,转基因兔中β-MyHC-Q(403)的心脏表达诱导了肥大、心肌细胞和肌原纤维紊乱、间质纤维化和过早死亡,这些表型也出现在因β-MyHC-Q(403)导致的HCM人类患者中。