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佛波醇12-肉豆蔻酸酯13-乙酸酯对胚胎鸡骨骼肌成肌细胞分化程序的影响。

Effects of phorbol 12-myristate 13-acetate on the differentiation program of embryonic chick skeletal myoblasts.

作者信息

Dlugosz A A, Tapscott S J, Holtzer H

出版信息

Cancer Res. 1983 Jun;43(6):2780-9.

PMID:6342759
Abstract

The effects of phorbol 12-myristate 13-acetate (PMA) on three aspects of myogenesis have been analyzed: (a) fusion of mononucleated myogenic cells to form myotubes; (b) synthesis and accumulation of two muscle-specific proteins; and (c) DNA synthesis. Using autoradiography combined with immunofluorescent localization of muscle-specific light meromyosin and the muscle-specific intermediate filament protein desmin, we have found that embryonic chick myogenic cells cultured in the presence of PMA (50 nM) initiate the synthesis of both desmin and muscle-specific light meromyosin and, by these criteria, partially differentiate. These cells differ from normal definitive postmitotic myoblasts, however, since they (a) do not fuse; (b) do not assemble normal myofibrils; and (c) incorporate [3H]thymidine. PMA does not appear to induce DNA synthesis in postmitotic myoblasts, but it apparently permits cells to initiate expression of muscle-specific proteins while preventing complete withdrawal from the cell cycle. Inhibition of fusion by PMA has been reported, but continued incorporation of [3H]thymidine in nuclei of cells expressing muscle-specific proteins is a previously undescribed effect of PMA. This effect is not achieved by 4-alpha-phorbol-12, 13-didecanoate, a nonpromoting phorbol ester, and may be relevant to the action of PMA as a tumor promoter.

摘要

已分析佛波醇12 -肉豆蔻酸酯13 -乙酸酯(PMA)对肌生成三个方面的影响:(a)单核肌原性细胞融合形成肌管;(b)两种肌肉特异性蛋白质的合成与积累;以及(c)DNA合成。通过放射自显影结合肌肉特异性轻酶解肌球蛋白和肌肉特异性中间丝蛋白结蛋白的免疫荧光定位,我们发现,在PMA(50 nM)存在下培养的胚胎鸡肌原性细胞开始合成结蛋白和肌肉特异性轻酶解肌球蛋白,根据这些标准,这些细胞部分分化。然而,这些细胞与正常的终末有丝分裂后成肌细胞不同,因为它们(a)不融合;(b)不组装正常的肌原纤维;并且(c)掺入[3H]胸腺嘧啶核苷。PMA似乎不会在终末有丝分裂后成肌细胞中诱导DNA合成,但它显然允许细胞开始表达肌肉特异性蛋白质,同时阻止细胞完全退出细胞周期。已有报道PMA会抑制融合,但在表达肌肉特异性蛋白质的细胞的细胞核中持续掺入[3H]胸腺嘧啶核苷是PMA之前未被描述的一种作用。4-α-佛波醇-12,13-二十二酸酯(一种无促癌作用的佛波醇酯)不会产生这种作用,并且这一作用可能与PMA作为肿瘤促进剂的作用相关。

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