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高迁移率族蛋白 B 在斑马鱼和爪蟾早期发育过程中调节中胚层形成和背腹模式形成。

High mobility group B proteins regulate mesoderm formation and dorsoventral patterning during zebrafish and Xenopus early development.

机构信息

School of Life Sciences, Shandong University, 27 Shanda Nan Road, Jinan 250100, China.

出版信息

Mech Dev. 2012 Sep-Dec;129(9-12):263-74. doi: 10.1016/j.mod.2012.07.001. Epub 2012 Jul 20.

Abstract

The high mobility group (HMG) proteins constitute a superfamily of nuclear proteins that regulate the expression of a wide range of genes through architectural remodeling of the chromatin structure, and the formation of multiple protein complexes on promoter/enhancer regions, but their function in germ layer specification during early development is not clear. Here we show that hmgb genes regulate mesoderm formation and dorsoventral patterning both in zebrafish and Xenopus early embryos. Overexpression of hmgb3 blocks the expression of the pan-mesoderm gene no tail/Xbra and other ventrolateral mesoderm genes, and results in embryos with shortened anteroposterior axis, while overexpression of hmgb3EnR, which contains the engrailed repressor domain, most potently repressed no tail expression and mesoderm formation. However, hmgb3VP16, which contains the transcriptional activation domain of VP16, had an opposite effect, indicating that hmgb3 may function as a repressor during mesoderm induction and patterning. In addition, we show that hmgb3 inhibits target gene expression downstream of mesoderm-inducing factors. Furthermore, using reporter gene assays in Xenopus whole embryos, we show that hmgb3 differentially regulates the activation of various mesendoderm reporter genes. In particular, it up-regulates the goosecoid, but inhibits the Xbra reporter gene activation. Therefore, our results suggest that hmgb genes may function to fine-tune the specification and/or dorsoventral patterning of mesoderm during zebrafish and Xenopus development.

摘要

高迁移率族(HMG)蛋白构成了一个核蛋白超家族,通过重塑染色质结构和在启动子/增强子区域形成多种蛋白质复合物,调节广泛基因的表达,但它们在早期发育中对胚层特化的功能尚不清楚。在这里,我们表明 hmgb 基因在斑马鱼和非洲爪蟾早期胚胎中调节中胚层的形成和背腹模式。hmgb3 的过表达阻断了 pan-mesoderm 基因 no tail/Xbra 和其他腹侧中胚层基因的表达,并导致胚胎前后轴缩短,而含有 engrailed 抑制结构域的 hmgb3EnR 的过表达最有效地抑制 no tail 表达和中胚层形成。然而,含有 VP16 转录激活结构域的 hmgb3VP16 则有相反的效果,这表明 hmgb3 在中胚层诱导和模式形成过程中可能作为一种抑制因子发挥作用。此外,我们表明 hmgb3 抑制中胚层诱导因子下游靶基因的表达。此外,我们在非洲爪蟾整体胚胎报告基因实验中表明,hmgb3 对各种中胚层报告基因的激活有不同的调节作用。特别是,它上调 goosecoid 的表达,但抑制 Xbra 报告基因的激活。因此,我们的结果表明,hmgb 基因可能在斑马鱼和非洲爪蟾发育过程中精细调节中胚层的特化和/或背腹模式。

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