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首页> 外文期刊>Journal of Cell Science >Muscle regeneration by reconstitution with bone marrow or fetal liver cells from green fluorescent protein-gene transgenic mice
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Muscle regeneration by reconstitution with bone marrow or fetal liver cells from green fluorescent protein-gene transgenic mice

机译:通过绿色荧光蛋白基因转基因小鼠的骨髓或胎儿肝细胞重建肌肉再生

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The myogenic potential of bone marrow and fetal liver cells was examined using donor cells from green fluorescent protein (GFP)-gene transgenic mice transferred into chimeric mice. Lethally irradiated X-chromosome-linked muscular dystrophy (mdx) mice receiving bone marrow cells from the transgenic mice exhibited significant numbers of fluorescence(+) and dystrophin(+) muscle fibres. In order to compare the generating capacity of fetal liver cells with bone marrow cells in neonatal chimeras, these two cell types from the transgenic mice were injected into busulfan-treated normal or mdx neonatal mice, and muscular generation in the chimeras was examined. Cardiotoxin-induced (or -uninduced, for mdx recipients) muscle regeneration in chimeras also produced fluorescence(+) muscle fibres. The muscle reconstitution efficiency of the bone marrow cells was almost equal to that of fetal liver cells. However, the myogenic cell frequency was higher in fetal livers than in bone marrow. Among the neonatal chimeras of normal recipients, several fibres expressed the fluorescence in the cardiotoxin-untreated muscle. Moreover, fluorescence(+) mononuclear cells were observed beneath the basal lamina of the cardiotoxin-untreated muscle of chimeras, a position where satellite cells are localizing. It was also found that mononuclear fluorescence(+) and desmin(+) cells were observed in the explantation cultures of untreated muscles of neonatal chimeras. The fluorescence(+) muscle fibres were generated in the second recipient mice receiving muscle single cells from the cardiotoxin-untreated neonatal chimeras. The results suggest that both bone marrow and fetal liver cells may have the potential to differentiate into muscle satellite cells and participate in muscle regeneration after muscle damage as well as in physiological muscle generation. [References: 48]
机译:使用来自绿色荧光蛋白(GFP)-基因转基因小鼠的供体细胞转移到嵌合小鼠中,检查了骨髓和胎儿肝细胞的成肌潜力。接受来自转基因小鼠骨髓细胞的经X射线照射的X染色体连锁的肌肉营养不良(mdx)小鼠表现出大量的荧光(+)和肌营养不良蛋白(+)肌纤维。为了比较新生儿嵌合体中胎儿肝细胞和骨髓细胞的生成能力,将来自转基因小鼠的这两种细胞类型注射入白消安治疗的正常或mdx新生小鼠中,并检查嵌合体中的肌肉生成。嵌合体中由心脏毒素诱导的(或对于mdx受体而言,是非诱导的)肌肉再生也产生了荧光(+)肌肉纤维。骨髓细胞的肌肉重建效率几乎等于胎儿肝细胞的肌肉重建效率。但是,胎儿肝脏中的成肌细胞频率高于骨髓。在正常受体的新生儿嵌合体中,几根纤维在未经心脏毒素处理的肌肉中表达荧光。此外,在未经过心毒素处理的嵌合体肌肉的基底层下方观察到了荧光(+)单核细胞,该位置是卫星细胞所在的位置。还发现在未处理的新生儿嵌合体肌肉的外植培养物中观察到单核荧光(+)和结蛋白(+)细胞。荧光(+)肌纤维是在第二只接受小鼠的细胞中产生的,第二只接受来自未经心脏毒素处理的新生儿嵌合体的肌肉单细胞。结果表明,骨髓和胎儿肝细胞都可能具有分化为肌肉卫星细胞并参与肌肉损伤后肌肉再生以及生理性肌肉生成的潜力。 [参考:48]

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