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1 型肌强直性营养不良 DMSXL 小鼠模型的纵向体内肌肉功能分析。

Longitudinal in vivo muscle function analysis of the DMSXL mouse model of myotonic dystrophy type 1.

机构信息

Institut de Myologie, UPMC Univ. Paris 6 UM76, Inserm U974, CNRS UMR7215, F-75651 Paris Cedex 13, France.

出版信息

Neuromuscul Disord. 2013 Dec;23(12):1016-25. doi: 10.1016/j.nmd.2013.07.014. Epub 2013 Aug 12.

Abstract

Myotonic dystrophy is the most common adult muscle dystrophy. In view of emerging therapies, which use animal models as a proof of principle, the development of reliable outcome measures for in vivo longitudinal study of mouse skeletal muscle function is becoming crucial. To satisfy this need, we have developed a device to measure ankle dorsi- and plantarflexion torque in rodents. We present an in vivo 8-month longitudinal study of the contractile properties of the skeletal muscles of the DMSXL mouse model of myotonic dystrophy type 1. Between 4 and 12 months of age, we observed a reduction in muscle strength in the ankle dorsi- and plantarflexors of DMSXL compared to control mice although the strength per muscle cross-section was normal. Mild steady myotonia but no abnormal muscle fatigue was also observed in the DMSXL mice. Magnetic resonance imaging and histological analysis performed at the end of the study showed respectively reduced muscle cross-section area and smaller muscle fibre diameter in DMSXL mice. In conclusion, our study demonstrates the feasibility of carrying out longitudinal in vivo studies of muscle function over several months in a mouse model of myotonic dystrophy confirming the feasibility of this method to test preclinical therapeutics.

摘要

强直性肌营养不良症是最常见的成人肌肉营养不良症。鉴于新兴疗法使用动物模型作为原理的证明,开发用于在体纵向研究小鼠骨骼肌功能的可靠结果测量方法变得至关重要。为了满足这一需求,我们开发了一种用于测量啮齿动物踝关节背屈和跖屈扭矩的设备。我们提出了一项针对 1 型强直性肌营养不良症 DMSXL 小鼠模型的骨骼肌收缩特性的 8 个月的体内纵向研究。在 4 至 12 个月大时,我们观察到 DMSXL 小鼠的踝关节背屈和跖屈肌力量较对照组小鼠降低,尽管每块肌肉横截面积的力量正常。DMSXL 小鼠也观察到轻度稳定的肌强直,但没有异常的肌肉疲劳。研究结束时进行的磁共振成像和组织学分析分别显示 DMSXL 小鼠的肌肉横截面积减小和肌肉纤维直径减小。总之,我们的研究证明了在强直性肌营养不良症小鼠模型中进行数月的体内肌肉功能纵向研究的可行性,证实了这种方法用于测试临床前治疗的可行性。

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