Division of Pulmonary Medicine, Department of Pediatrics, School of Medicine, Duke University, Durham, NC 27710, USA.
J Smooth Muscle Res. 2021;57(0):8-18. doi: 10.1540/jsmr.57.8.
Pompe disease is a lysosomal storage disease caused by mutations within the GAA gene, which encodes acid α-glucosidase (GAA)-an enzyme necessary for lysosomal glycogen degradation. A lack of GAA results in an accumulation of glycogen in cardiac and skeletal muscle, as well as in motor neurons. The only FDA approved treatment for Pompe disease-an enzyme replacement therapy (ERT)-increases survival of patients, but has unmasked previously unrecognized clinical manifestations of Pompe disease. These clinical signs and symptoms include tracheo-bronchomalacia, vascular aneurysms, and gastro-intestinal discomfort. Together, these previously unrecognized pathologies indicate that GAA-deficiency impacts smooth muscle in addition to skeletal and cardiac muscle. Thus, we sought to characterize smooth muscle pathology in the airway, vascular, gastrointestinal, and genitourinary in the Gaa mouse model. Increased levels of glycogen were present in smooth muscle cells of the aorta, trachea, esophagus, stomach, and bladder of Gaa mice, compared to wild type mice. In addition, there was an increased abundance of both lysosome membrane protein (LAMP1) and autophagosome membrane protein (LC3) indicating vacuolar accumulation in several tissues. Taken together, we show that GAA deficiency results in subsequent pathology in smooth muscle cells, which may lead to life-threatening complications if not properly treated.
庞贝病是一种溶酶体贮积病,由 GAA 基因内的突变引起,该基因编码酸性α-葡萄糖苷酶(GAA),这是溶酶体糖原降解所必需的酶。缺乏 GAA 会导致糖原在心、骨骼肌和运动神经元中积累。唯一获得 FDA 批准的庞贝病治疗方法——酶替代疗法(ERT)——提高了患者的生存率,但也揭示了以前未被认识的庞贝病临床表现。这些临床体征和症状包括气管支气管软化、血管动脉瘤和胃肠道不适。这些以前未被认识的病理学表明,GAA 缺乏除了影响骨骼肌和心脏肌肉外,还会影响平滑肌。因此,我们试图在 Gaa 小鼠模型中描述气道、血管、胃肠道和泌尿生殖道的平滑肌病理学。与野生型小鼠相比,Gaa 小鼠的主动脉、气管、食管、胃和膀胱的平滑肌细胞中糖原水平升高。此外,溶酶体膜蛋白(LAMP1)和自噬体膜蛋白(LC3)的丰度均增加,表明在几种组织中存在空泡积累。总之,我们表明 GAA 缺乏会导致平滑肌细胞随后发生病理变化,如果得不到适当治疗,可能会导致危及生命的并发症。
