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卤夫酮对mdx小鼠肌肉纤维化的预防及肌肉性能的改善

Prevention of muscle fibrosis and improvement in muscle performance in the mdx mouse by halofuginone.

作者信息

Turgeman Tidhar, Hagai Yosey, Huebner Kyla, Jassal Davinder S, Anderson Judy E, Genin Olga, Nagler Arnon, Halevy Orna, Pines Mark

机构信息

Institute of Animal Sciences, The Volcani Center, P.O. Box 6, Bet Dagan 50250, Israel.

出版信息

Neuromuscul Disord. 2008 Nov;18(11):857-68. doi: 10.1016/j.nmd.2008.06.386. Epub 2008 Jul 30.

Abstract

Fibrosis is a known feature of dystrophic muscles, particularly the diaphragm, in the mdx mouse. In this study we evaluated the effect of halofuginone, a collagen synthesis inhibitor, on collagen synthesis in various muscles of young wild-type (C57/BL/6J) and mdx mice. Halofuginone prevented the age-dependent increase in collagen synthesis in the diaphragms of mdx with no effect on wild-type mice (n = 5 for each time point). This was associated with a decrease in the degenerated areas and number of central nuclei. Halofuginone also inhibited collagen synthesis in cardiac muscle. Moreover, enhanced motor coordination, balance and improved cardiac muscle function were observed implying reduced muscle injury. Halofuginone inhibited Smad3 phosphorylation downstream of TGFbeta in the diaphragm and cardiac muscles, in C2 cell line and in primary mouse myoblast cultures representing various muscular dystrophies. We suggest that via its effect on Smad3 phosphorylation, halofuginone inhibits muscle fibrosis and improves cardiac and skeletal muscle functions in mdx mice.

摘要

纤维化是mdx小鼠营养不良性肌肉,尤其是膈肌的一个已知特征。在本研究中,我们评估了胶原合成抑制剂常山酮对年轻野生型(C57/BL/6J)和mdx小鼠各肌肉中胶原合成的影响。常山酮可防止mdx小鼠膈肌中胶原合成随年龄增长而增加,对野生型小鼠无影响(每个时间点n = 5)。这与退化区域和中央核数量的减少有关。常山酮还抑制心肌中的胶原合成。此外,观察到运动协调性增强、平衡改善以及心肌功能改善,这意味着肌肉损伤减少。常山酮在膈肌和心肌中、C2细胞系以及代表各种肌肉营养不良的原代小鼠成肌细胞培养物中抑制TGFβ下游的Smad3磷酸化。我们认为,通过其对Smad3磷酸化的影响,常山酮可抑制mdx小鼠的肌肉纤维化,并改善心脏和骨骼肌功能。

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