Comparison of Three Antagonists of Hedgehog Pathway to Promote Skeletal Muscle Regeneration after High Dose Irradiation.

IF 2.5 3区 医学 Q2 BIOLOGY Radiation research Pub Date : 2024-05-01 DOI:10.1667/RADE-23-00140.1
Emmanuelle Rota Graziosi, Sabine François, Farah Nasser, Michel Gauthier, Myriam Oger, Anne-Laure Favier, Michel Drouet, Nicolas Jullien, Diane Riccobono
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Abstract

The current geopolitical context has brought the radiological nuclear risk to the forefront of concerns. High-dose localized radiation exposure leads to the development of a musculocutaneous radiation syndrome affecting the skin and subcutaneous muscles. Despite the implementation of a gold standard treatment based on an invasive surgical procedure coupled with autologous cell therapy, a muscular defect frequently persists. Targeting the modulation of the Hedgehog (Hh) signaling pathway appears to be a promising therapeutic approach. Activation of this pathway enhances cell survival and promotes proliferation after irradiation, while inhibition by Cyclopamine facilitates differentiation. In this study, we compared the effects of three antagonists of Hh, Cyclopamine (CA), Vismodegib (VDG) and Sonidegib (SDG) on differentiation. A stable cell line of murine myoblasts, C2C12, was exposed to X-ray radiation (5 Gy) and treated with CA, VDG or SDG. Analysis of proliferation, survival (apoptosis), morphology, myogenesis genes expression and proteins production were performed. According to the results, VDG does not have a significant impact on C2C12 cells. SDG increases the expression/production of differentiation markers to a similar extent as CA, while morphologically, SDG proves to be more effective than CA. To conclude, SDG can be used in the same way as CA but already has a marketing authorization with an indication against basal cell cancers, facilitating their use in vivo. This proof of concept demonstrates that SDG represents a promising alternative to CA to promotes differentiation of murine myoblasts. Future studies on isolated and cultured satellite cells and in vivo will test this proof of concept.

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比较三种促进高剂量照射后骨骼肌再生的刺猬蛋白通路拮抗剂
当前的地缘政治背景使核放射风险成为人们关注的焦点。高剂量局部辐射照射会导致肌肉皮肤辐射综合征,影响皮肤和皮下肌肉。尽管实施了以侵入性外科手术和自体细胞疗法为基础的金标准治疗,但肌肉缺损经常持续存在。靶向调节刺猬(Hh)信号通路似乎是一种很有前景的治疗方法。激活该通路可提高细胞存活率并促进照射后的增殖,而环胺抑制则可促进分化。在这项研究中,我们比较了三种 Hh 拮抗剂:环丙胺(CA)、Vismodegib(VDG)和 Sonidegib(SDG)对分化的影响。将稳定的小鼠成肌细胞系 C2C12 暴露于 X 射线辐射(5 Gy),并用 CA、VDG 或 SDG 处理。对细胞的增殖、存活(凋亡)、形态、成肌基因表达和蛋白质生成进行了分析。结果显示,VDG 对 C2C12 细胞无明显影响。SDG 增加分化标记物的表达/产生的程度与 CA 相似,而在形态上,SDG 被证明比 CA 更有效。总之,SDG 的使用方法与 CA 相同,但已经获得了针对基底细胞癌的上市许可,这为在体内使用 SDG 提供了便利。这一概念验证表明,SDG 是替代 CA 促进小鼠成肌细胞分化的一种很有前途的方法。未来对分离和培养的卫星细胞以及体内卫星细胞的研究将检验这一概念证明。
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来源期刊
Radiation research
Radiation research 医学-核医学
CiteScore
5.10
自引率
8.80%
发文量
179
审稿时长
1 months
期刊介绍: Radiation Research publishes original articles dealing with radiation effects and related subjects in the areas of physics, chemistry, biology and medicine, including epidemiology and translational research. The term radiation is used in its broadest sense and includes specifically ionizing radiation and ultraviolet, visible and infrared light as well as microwaves, ultrasound and heat. Effects may be physical, chemical or biological. Related subjects include (but are not limited to) dosimetry methods and instrumentation, isotope techniques and studies with chemical agents contributing to the understanding of radiation effects.
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