Smidt Heart Institute, Cedars-Sinai Medical Center, Los Angeles, California, USA.
Aging Cell. 2024 Oct;23(10):e14259. doi: 10.1111/acel.14259. Epub 2024 Jul 3.
Hutchinson-Gilford progeria syndrome (HGPS) is a rare premature aging disorder resulting from de novo mutations in the lamin A gene. Children with HGPS typically pass away in their teenage years due to cardiovascular diseases such as atherosclerosis, myocardial infarction, heart failure, and stroke. In this study, we characterized the G608G HGPS mouse model and explored cardiac and skeletal muscle function, along with senescence-associated phenotypes in fibroblasts. Homozygous G608G HGPS mice exhibited cardiac dysfunction, including decreased cardiac output and stroke volume, and impaired left ventricle relaxation. Additionally, skeletal muscle exhibited decreased isometric tetanic torque, muscle atrophy, and increased fibrosis. HGPS fibroblasts showed nuclear abnormalities, decreased proliferation, and increased expression of senescence markers. These findings provide insights into the pathophysiology of the G608G HGPS mouse model and inform potential therapeutic strategies for HGPS.
亨廷顿氏舞蹈症-早衰综合征(HGPS)是一种罕见的早发性衰老紊乱,由 lamin A 基因突变引起。患有 HGPS 的儿童通常会因心血管疾病(如动脉粥样硬化、心肌梗死、心力衰竭和中风)在青少年时期去世。在这项研究中,我们对 G608G HGPS 小鼠模型进行了表征,并探讨了心脏和骨骼肌功能以及成纤维细胞的衰老相关表型。G608G HGPS 纯合子小鼠表现出心脏功能障碍,包括心输出量和每搏量减少,以及左心室舒张功能受损。此外,骨骼肌表现出等长强直收缩扭矩降低、肌肉萎缩和纤维化增加。HGPS 成纤维细胞表现出核异常、增殖减少和衰老标志物表达增加。这些发现为 G608G HGPS 小鼠模型的病理生理学提供了深入了解,并为 HGPS 的潜在治疗策略提供了信息。
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