Lankenau Institute for Medical Research, 100 Lancaster Avenue, Wynnewood, PA 19096, USA.
Dev Biol. 2009 Dec 1;336(1):30-41. doi: 10.1016/j.ydbio.2009.09.022. Epub 2009 Sep 22.
A subpopulation of cells expresses MyoD mRNA and the cell surface G8 antigen in the epiblast prior to the onset of gastrulation. When an antibody to the G8 antigen was applied to the epiblast, labeled cells were later found in the ocular primordia and muscle and non-muscle forming tissues of the eyes. In the lens, retina and periocular mesenchyme, G8-positive cells synthesized MyoD mRNA and the bone morphogenetic protein inhibitor Noggin. MyoD expressing cells were ablated in the epiblast by labeling them with the G8 MAb and lysing them with complement. Their ablation in the epiblast resulted in eye defects, including anopthalmia, micropthalmia, altered pigmentation and malformations of the lens and/or retina. The right eye was more severely affected than the left eye. The asymmetry of the eye defects in ablated embryos correlated with differences in the number of residual Noggin producing, MyoD-positive cells in ocular tissues. Exogenously supplied Noggin compensated for the ablated epiblast cells. This study demonstrates that MyoD expressing cells serve as a Noggin delivery system to regulate the morphogenesis of the lens and optic cup.
在原肠胚形成之前,细胞的一个亚群在上胚层中表达 MyoD mRNA 和细胞表面 G8 抗原。当将针对 G8 抗原的抗体施加到上胚层时,后来在眼原基和肌肉及非肌肉形成组织中发现标记的细胞。在上皮细胞中,G8 阳性细胞合成 MyoD mRNA 和骨形态发生蛋白抑制剂 Noggin。通过用 G8 MAb 标记上胚层中的 MyoD 表达细胞并用补体裂解它们,可以在上胚层中消融 MyoD 表达细胞。在上胚层中的消融导致眼睛缺陷,包括无眼、小眼、色素改变以及晶状体和/或视网膜畸形。右眼比左眼受影响更严重。消融胚胎中眼睛缺陷的不对称性与眼组织中产生剩余 Noggin 的、MyoD 阳性细胞的数量差异相关。外源性提供的 Noggin 补偿了被消融的上胚层细胞。这项研究表明,表达 MyoD 的细胞作为 Noggin 输送系统,以调节晶状体和视杯的形态发生。