Department of Medicine and Department of Pathology and Cell Biology, College of Physicians and Surgeons, Columbia University, New York, NY, USA.
Autophagy. 2013 Jan;9(1):110-1. doi: 10.4161/auto.22403. Epub 2012 Oct 8.
Mutations in the LMNA gene, which encodes lamin A and C (lamin A/C), cause a diverse spectrum of tissue-selective diseases termed laminopathies. The most prevalent form affects striated muscles as dilated cardiomyopathy with variable skeletal muscle involvement, which includes autosomal Emery-Dreifuss muscular dystrophy. Mechanisms underlying the disease pathogenesis are beginning to be understood and they point toward defects in cell signaling. We therefore assessed putative signaling defects in a mouse model carrying a point mutation in Lmna (Lmna (H222P/H222P) ) that faithfully recapitulates human Emery-Dreifuss muscular dystrophy. We found that AKT-mechanistic target of rapamycin (MTOR) signaling was hyperactivated in hearts of Lmna (H222P/H222P) mice and that reducing MTOR activity by pharmacological intervention ameliorated cardiomyopathy. Given the central role of MTOR in regulating autophagy, we assessed fasting-induced autophagic responses and found that they were impaired in hearts of these mice. Moreover, the improved heart function associated with pharmacological blockade of MTOR was correlated with enhanced autophagy. These findings demonstrated that signaling defects that impair autophagy underlie pathogenesis of dilated cardiomyopathy arising from LMNA mutation.
LMNA 基因编码核纤层蛋白 A 和 C(lamin A/C),该基因突变可导致多种组织选择性疾病,称为核纤层病。最常见的形式是影响横纹肌的扩张型心肌病,伴有不同程度的骨骼肌受累,包括常染色体显性遗传的 Emery-Dreifuss 肌营养不良症。疾病发病机制的机制开始被理解,它们指向细胞信号传导的缺陷。因此,我们在携带 Lmna 点突变(Lmna(H222P/H222P))的小鼠模型中评估了潜在的信号传导缺陷,该突变忠实地再现了人类 Emery-Dreifuss 肌营养不良症。我们发现 AKT-雷帕霉素(mTOR)信号通路在 Lmna(H222P/H222P)小鼠的心脏中过度激活,并且通过药理学干预降低 mTOR 活性可改善心肌病。鉴于 mTOR 在调节自噬中的核心作用,我们评估了饥饿诱导的自噬反应,发现这些小鼠的心脏存在自噬受损。此外,与 mTOR 药理学阻断相关的改善心脏功能与增强的自噬相关。这些发现表明,导致 LMNA 突变引起扩张型心肌病的信号传导缺陷可破坏自噬。
