Transforming growth factor-beta in the early mouse embryo: implications for the regulation of muscle formation and implantation.

H G Slager, W Van Inzen, E Freund, A J Van den Eijnden-Van Raaij, C L Mummery
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引用次数: 89

Abstract

In a search for functions of transforming growth factor-beta during early embryonic development we used two different experimental approaches. In the first we made use of embryonic stem (ES) cells. ES cells in culture differentiate to derivatives of all three germ layers and mimic some aspects of organogenesis when grown as aggregates in suspension to form embryoid bodies. Differentiation proceeds further when the embryoid bodies attach to suitable substrates. Muscle and neuronal cells are among the most readily identified cell types then formed. We examined the effect of all-trans retinoic acid (RA) and members of the transforming growth factor-beta family (TGF-beta 1, TGF-beta 2) under these conditions in an assay where single aggregates formed in hanging microdrops in medium supplemented with serum depleted of lipophilic substances which would include retinoids. Endoderm-like cells formed under all conditions tested. RA at concentrations of 10(-8) M and 10(-7) M induced the formation of neurons but in the absence of RA or at concentrations up to 10(-9) M, neurons were not observed. Instead, beating muscle formed in about one-third of the plated aggregates; this was greatly reduced when RA concentrations increased above 10(-9) M. Immunofluorescent staining for muscle specific myosin showed that two muscle cell types could be distinguished: elongated, non-contractile myoblasts and mononucleate flat cells. The mononucleate flat cells appeared to correspond with rhythmically contracting muscle. The number of non-contractile myoblasts increased 3-fold over controls in the presence of 10(-9) M RA. TGF-beta s increased the number of contractile and non-contractile muscle cells by a factor 3 to 7 over controls, depending on the TGF-beta isoform added and the muscle cell type formed. TGF-beta 2 also invariably increased the rate at which contracting muscle cells were first observed in replated aggregates. The stimulatory effect of TGF-beta s on the formation of mononucleate flat cells was completely abrogated by RA at 10(-9) M while the number of myoblasts under similar conditions was unchanged. These data suggest that a complex interplay between retinoids and TGF-beta isoforms may be involved in regulation of differentiation in early myogenesis. In the second approach, neutralizing polyclonal rabbit antibodies specific for TGF-beta 2 were injected into the cavity of mouse blastocysts 3.5 days post coîtum (pc). After 1 day in culture, embryos were transferred to pseudopregnant females. The number of decidua, embryos and resorptions were counted at day 8.5-9.5 pc.(ABSTRACT TRUNCATED AT 400 WORDS)

早期小鼠胚胎中的转化生长因子- β:对肌肉形成和植入调节的影响。
在寻找转化生长因子- β在早期胚胎发育中的功能时,我们使用了两种不同的实验方法。在第一个实验中,我们使用胚胎干细胞(ES)。胚胎干细胞在培养中分化为所有三种胚层的衍生物,并模仿器官发生的某些方面,当作为聚集体在悬浮中生长形成胚状体时。当胚状体附着在合适的底物上时,分化进一步进行。肌肉细胞和神经细胞是当时形成的最容易识别的细胞类型。在这些条件下,我们检测了全反式维甲酸(RA)和转化生长因子- β家族成员(tgf - β 1, tgf - β 2)的作用,在补充了亲脂性物质(包括类维甲酸)的血清的培养基中,悬挂微滴形成单一聚集体。在所有测试条件下形成内胚层样细胞。10(-8) M和10(-7)M浓度的RA诱导神经元的形成,但在缺乏RA或浓度高达10(-9)M时,未观察到神经元的形成。相反,约三分之一的镀聚集体形成了跳动肌;当RA浓度增加到10(-9)m以上时,这种情况大大减少。肌肉特异性肌球蛋白的免疫荧光染色显示,可以区分出两种肌肉细胞类型:细长的、非收缩的成肌细胞和单核扁平细胞。单核扁平细胞似乎与有节奏收缩的肌肉相对应。在10(-9)M RA的存在下,非收缩性成肌细胞的数量比对照组增加了3倍。根据添加的tgf - β异构体和形成的肌肉细胞类型,tgf - β s使收缩性和非收缩性肌肉细胞的数量比对照组增加了3到7倍。tgf - β 2也不可避免地增加了在复制聚集体中首次观察到收缩肌肉细胞的速率。10(-9) M时,tgf - β - s对单核扁平细胞形成的刺激作用被RA完全消除,而在相同条件下,成肌细胞的数量不变。这些数据表明,类维生素a和tgf - β亚型之间的复杂相互作用可能参与了早期肌肉形成的分化调节。在第二种方法中,将中和的tgf - β 2特异性兔多克隆抗体注射到co tum (pc)后3.5天的小鼠囊胚腔中。培养1天后,将胚胎移植到假孕雌性体内。第8.5 ~ 9.5天计数蜕膜数、胚胎数和再吸收数。(摘要删节为400字)
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