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转录因子肌细胞增强因子2家族在发育过程中的差异表达:心脏因子BBF-1是心脏发生的早期标志物。

Differential expression of the myocyte enhancer factor 2 family of transcription factors in development: the cardiac factor BBF-1 is an early marker for cardiogenesis.

作者信息

Goswami S, Qasba P, Ghatpande S, Carleton S, Deshpande A K, Baig M, Siddiqui M A

机构信息

Department of Anatomy and Cell Biology, State University of New York Health Science Center at Brooklyn 11203.

出版信息

Mol Cell Biol. 1994 Aug;14(8):5130-8. doi: 10.1128/mcb.14.8.5130-5138.1994.

Abstract

In the present study, we have used single chicken blastoderms of defined early developmental stages, beginning with the prestreak stage, stage 1 (V. Hamburger and H. L. Hamilton, J. Morphol. 88:49-92, 1951), to analyze the onset of cardiac myogenesis by monitoring the appearance of selected cardiac muscle tissue-specific gene transcripts and the functional expression of the myocyte enhancer factor 2 (MEF-2) proteins. Using gene-specific oligonucleotide primers in reverse transcriptase PCR assay, we have demonstrated that the cardiac myosin light-chain 2 (MLC2) and alpha-actin gene transcripts appear as early as stage 5, i.e., immediately after the cardiogenic fate assignment at stage 4. Consistent with this observation is the developmental expression pattern of DNA-binding activity of BBF-1, a cardiac muscle-specific member of the MEF-2 protein family, which also begins at stage 5 prior to MEF-2. Differential expression of DNA-binding complexes is also observed with another AT-rich DNA sequence (CArG box) as probe, but the binding pattern with the ubiquitous TATA-binding proteins remains unchanged during the same developmental period. Thus, the cardiogenic commitment and differentiation of the precardiac mesoderm, as exemplified by the appearance of cardiac MEF-2, MLC2, and alpha-actin gene products, occur earlier than previously thought and appear to be closely linked. The onset of skeletal myogenic program follows that of the cardiogenic program with the appearance of skeletal MLC2 at stage 8. We also observed that mRNA for the MEF-2 family of proteins appears as early as stage 2 and that for CMD-1, the chicken counterpart of MyoD, appears at stage 5. The temporal separation of activation of cardiac and skeletal MLC2 genes, which appears immediately after the respective fate assignments, and those of cardiac MEF-2 and CMD-1, which occur before, are consistent with the established appearance of the myogenic programs and with the acquisition pattern of the two tissue-specific morphological characteristics in the early embryo. The preferential appearance of BBF-1 activity in precardiac moesderm, relative to that of MEF-2, indicates that these two protein factors are distinct members of the MEF-2 family and provides a compelling argument in support of the potential role of BBF-1 as a regulator of the cardiogenic cell lineage determination, while cardiac MEF-2 might be involved in maintenance of the cardiac differentiative state.

摘要

在本研究中,我们使用了处于特定早期发育阶段的单个鸡胚盘,从原条期(第1阶段,V. 汉堡和H. L. 汉密尔顿,《形态学杂志》88:49 - 92,1951年)开始,通过监测特定心肌组织特异性基因转录本的出现以及肌细胞增强因子2(MEF - 2)蛋白的功能表达,来分析心肌发生的起始。在逆转录酶PCR分析中使用基因特异性寡核苷酸引物,我们证明心肌肌球蛋白轻链2(MLC2)和α - 肌动蛋白基因转录本最早在第5阶段出现,即在第4阶段确定心脏发生命运之后立即出现。与这一观察结果一致的是,MEF - 2蛋白家族的心肌特异性成员BBF - 1的DNA结合活性的发育表达模式也在第5阶段开始,早于MEF - 2。用另一个富含AT的DNA序列(CArG框)作为探针也观察到了DNA结合复合物的差异表达,但在相同发育时期,与普遍存在的TATA结合蛋白的结合模式保持不变。因此,心脏中胚层的心脏发生定向和分化,以心脏MEF - 2、MLC2和α - 肌动蛋白基因产物的出现为例,比以前认为的发生得更早,并且似乎紧密相连。骨骼肌发生程序的起始在心脏发生程序之后,在第8阶段出现骨骼肌MLC2。我们还观察到MEF - 2蛋白家族的mRNA最早在第2阶段出现,而鸡MyoD对应物CMD - 1的mRNA在第5阶段出现。心脏和骨骼肌MLC2基因的激活在各自命运确定后立即出现,而心脏MEF - 2和CMD - 1的激活在之前发生,这种时间上的分离与已确定的肌发生程序的出现以及早期胚胎中两种组织特异性形态特征的获得模式一致。相对于MEF - 2,BBF - 1活性在心脏前中胚层中优先出现,这表明这两种蛋白质因子是MEF - 2家族的不同成员,并有力地支持了BBF - 1作为心脏发生细胞谱系决定调节因子的潜在作用,而心脏MEF - 2可能参与维持心脏分化状态。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e750/359032/b58675af980e/molcellb00008-0124-a.jpg

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