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早期骨形态发生蛋白功能的时间分析确定了不同的抗组织者和中胚层模式形成阶段。

Temporal analysis of the early BMP functions identifies distinct anti-organizer and mesoderm patterning phases.

作者信息

Marom Karen, Levy Vered, Pillemer Graciela, Fainsod Abraham

机构信息

Department of Cellular Biochemistry and Human Genetics, Faculty of Medicine, Hebrew University, POB 12272, Jerusalem 91120, Israel.

出版信息

Dev Biol. 2005 Jun 15;282(2):442-54. doi: 10.1016/j.ydbio.2005.03.024.

Abstract

BMP signaling performs multiple important roles during early embryogenesis. Signaling through the BMP pathway is mediated by different BMP ligands expressed in partially overlapping temporal and spatial patterns. Assignment of different BMP-dependent activities to the individual ligands has relied on the patterns of expression of the various BMP genes. Temporal analysis of BMP signaling prior to and during gastrulation was performed using glucocorticoid-controlled Smad proteins. Overexpression of the BMP-specific Smad1 and Smad5 revealed that suppression of Spemann's organizer formation in Xenopus embryos can only take place by activating the BMP pathway prior to the onset of gastrulation. Blocking BMP signaling with the inhibitory Smad, Smad6, results in dorsalized embryos or secondary axis induction, only when activated up to early gastrula stages. BMP2 efficiently represses organizer-specific transcription from the midblastula transition onwards while BMP4 is unable to prevent the early activation of organizer-specific genes. Manipulation of the BMP pathway during mid/late gastrula affects mesodermal patterning with no external phenotypic effects. These observations suggest that the malformations resulting from inhibition or promotion of organizer formation, ventralized or dorsalized, respectively, are the result of a very early BMP function, through its antagonism of organizer formation. This function is apparently fulfilled by BMP2 and only at its latest phase by BMP4. Subsequently, BMP functions in the patterning of the mesoderm with no apparent phenotypic effects.

摘要

骨形态发生蛋白(BMP)信号在早期胚胎发育过程中发挥着多种重要作用。通过BMP信号通路的信号传导由以部分重叠的时间和空间模式表达的不同BMP配体介导。将不同的BMP依赖性活性分配给各个配体依赖于各种BMP基因的表达模式。在原肠胚形成之前和期间,使用糖皮质激素控制的Smad蛋白对BMP信号进行了时间分析。BMP特异性Smad1和Smad5的过表达表明,非洲爪蟾胚胎中施佩曼组织者形成的抑制只能通过在原肠胚形成开始之前激活BMP信号通路来发生。仅在早期原肠胚阶段之前激活时,用抑制性Smad即Smad6阻断BMP信号会导致胚胎背化或诱导形成次生轴。从囊胚中期过渡开始,BMP2有效地抑制组织者特异性转录,而BMP4无法阻止组织者特异性基因的早期激活。在原肠胚中/后期对BMP信号通路进行操作会影响中胚层模式形成,而没有外部表型效应。这些观察结果表明,分别由组织者形成的抑制或促进导致的畸形,即腹化或背化,是非常早期BMP功能的结果,是通过其对组织者形成的拮抗作用实现的。这种功能显然由BMP2完成,并且仅在其最晚阶段由BMP4完成。随后,BMP在中胚层模式形成中起作用,没有明显的表型效应。

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