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线粒体靶向荧光染料对肌肉分化的控制。

Control of muscle differentiation by a mitochondria-targeted fluorophore.

机构信息

Department of Chemistry, New York University, New York, New York 10003, USA.

出版信息

J Am Chem Soc. 2010 Jan 20;132(2):576-9. doi: 10.1021/ja906862g.

Abstract

During muscle differentiation, mitochondria undergo dramatic changes in their morphology and distribution to prepare for the higher rate of energy consumption. By applying a mitochondria-targeted rosamine library in C2C12 myogenesis, we discovered one compound that controls muscle differentiation. When treated to undifferentiated myoblasts, our selected compound, B25, inhibited myotube formation, and when treated to fully differentiated myotubes, it induced fission of multinucleated myotubes into mononucleated fragments. Compared to myoseverin, which is known for inducing myotube fission by destabilizing microtubules, B25 affects neither microtubule stability nor cell cycle. Further investigation identified that B25 induces myotube fission through the activation of NF-kappaB, which is one of the important signaling pathways linked to skeletal muscle differentiation. So far, the use of small-molecule fluorophores is limited in the discovery of labeling agents or sensors. In addition to their potential as a sensor, here we show the application of fluorescent small molecules in the discovery of a bioactive probe that induces a specific cellular response.

摘要

在肌肉分化过程中,线粒体的形态和分布会发生显著变化,为更高的能量消耗做好准备。通过在 C2C12 肌发生中应用一种线粒体靶向若丹明文库,我们发现了一种控制肌肉分化的化合物。当用未分化的成肌细胞处理时,我们选择的化合物 B25 抑制肌管形成,而当用完全分化的肌管处理时,它诱导多核肌管分裂成单核片段。与已知通过破坏微管诱导肌管分裂的肌抑素相比,B25 既不影响微管稳定性也不影响细胞周期。进一步的研究表明,B25 通过激活 NF-κB 诱导肌管分裂,NF-κB 是与骨骼肌分化相关的重要信号通路之一。到目前为止,小分子荧光染料在标记剂或传感器的发现中的应用有限。除了作为传感器的潜力之外,我们在这里还展示了荧光小分子在发现诱导特定细胞反应的生物活性探针中的应用。

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