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用抗Pl-粘连蛋白单克隆抗体处理的骨骼发育受阻的海胆胚胎中外胚层的调节性特化

Regulative specification of ectoderm in skeleton disrupted sea urchin embryos treated with monoclonal antibody to Pl-nectin.

作者信息

Zito F, Nakano E, Sciarrino S, Matranga V

机构信息

Istituto di Biologia dello Sviluppo del Consiglio Nazionale delle Ricerche, Palermo, Italy.

出版信息

Dev Growth Differ. 2000 Oct;42(5):499-506. doi: 10.1046/j.1440-169x.2000.00531.x.

Abstract

Pl-nectin is a glycoprotein first discovered in the extracellular matrix (ECM) of Paracentrotus lividus sea urchin embryo, apically located on ectoderm and endoderm cells. The molecule has been described as functioning as an adhesive substrate for embryonic cells and its contact to ectoderm cells is essential for correct skeletogenesis. The present study was undertaken to elucidate the biochemical characteristics of Pl-nectin and to extend knowledge on its in vivo biological function. Here it is shown that the binding of mesenchyme blastula cells to Pl-nectin-coated substrates was calcium dependent, and reached its optimum at 10 mM Ca2+. Perturbation studies using monoclonal antibody (McAb) to Pl-nectin, which prevent ectoderm cell-Pl-nectin contact, show that dorsoventral axis formation and ectoderm differentiation were retarded. At later stages, embryos recovered and, even if growth and patterning of the skeleton was greatly affected, the establishment of dorsoventral asymmetry was reached. Similarly, the expression of specific ectoderm and endoderm territorial markers was achieved, although occurring with some delay. Endoderm differentiation and patterning was not obviously affected. These results suggest that both endoderm and ectoderm cells have regulative capacities and differentiation of territories is restored after a lag period. On the contrary, failure of inductive differentiation of the skeleton cannot be rescued, even though the ectoderm has recovered.

摘要

Pl-粘连蛋白是一种糖蛋白,最初在紫海胆胚胎的细胞外基质(ECM)中被发现,顶端位于外胚层和内胚层细胞上。该分子被描述为胚胎细胞的粘附底物,其与外胚层细胞的接触对于正确的骨骼发生至关重要。本研究旨在阐明Pl-粘连蛋白的生化特性,并扩展对其体内生物学功能的认识。研究表明,间充质囊胚细胞与包被有Pl-粘连蛋白的底物的结合是钙依赖性的,在10 mM Ca2+时达到最佳状态。使用针对Pl-粘连蛋白的单克隆抗体(McAb)进行的干扰研究表明,该抗体可阻止外胚层细胞与Pl-粘连蛋白的接触,结果显示背腹轴形成和外胚层分化受到抑制。在后期阶段,胚胎恢复,即使骨骼的生长和模式受到极大影响,但背腹不对称性仍得以建立。同样,特定外胚层和内胚层区域标记物的表达也得以实现,尽管出现了一些延迟。内胚层分化和模式没有受到明显影响。这些结果表明,内胚层和外胚层细胞都具有调节能力,并且区域分化在延迟期后得以恢复。相反,即使外胚层已经恢复,骨骼诱导分化的失败也无法挽救。

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