首页> 美国卫生研究院文献>Development (Cambridge England) >Retinoic acid guides eye morphogenetic movements via paracrine signaling but is unnecessary for retinal dorsoventral patterning
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Retinoic acid guides eye morphogenetic movements via paracrine signaling but is unnecessary for retinal dorsoventral patterning

机译:维甲酸可通过旁分泌信号传导引导眼部形态发生运动但对于视网膜背腹模式而言则是不必要的

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摘要

Retinoic acid (RA) is required for patterning of the posterior nervous system, but its role in the retina remains unclear. RA is synthesized in discrete regions of the embryonic eye by three retinaldehyde dehydrogenases (RALDHs) displaying distinct expression patterns. Overlapping functions of these enzymes have hampered genetic efforts to elucidate RA function in the eye. Here, we report Raldh1, Raldh2 and Raldh3 single, double and triple null mice exhibiting progressively less or no RA synthesis in the eye. Our genetic studies indicate that RA signaling is not required for the establishment or maintenance of dorsoventral patterning in the retina, as we observe normal expression of Tbx5 and ephrin B2 (Efnb2) dorsally, plus Vax2 and Ephb2 ventrally. Instead, RA is required for the morphogenetic movements needed to shape the developing retina and surrounding mesenchyme. At early stages, Raldh2 expressed in mesenchyme and Raldh3 expressed in the retinal pigmented epithelium generate RA that delivers an essential signal to the neural retina required for morphogenetic movements that lead to ventral invagination of the optic cup. At later stages, Raldh1 expressed in dorsal neural retina and Raldh3 expressed in ventral neural retina (plus weaker expression of each in lens/corneal ectoderm) generates RA that travels to surrounding mesenchyme, where it is needed to limit the anterior invasion of perioptic mesenchyme during the formation of corneal mesenchyme and eyelids. At all stages, RA target tissues are distinct from locations of RA synthesis, indicating that RALDHs function cell-nonautonomously to generate paracrine RA signals that guide morphogenetic movements in neighboring cells.
机译:维甲酸(RA)是后神经系统模式所必需的,但其在视网膜中的作用仍不清楚。 RA通过三种显示不同表达模式的视黄醛脱氢酶(RALDH)在胚胎眼的离散区域合成。这些酶的重叠功能阻碍了阐明眼睛中RA功能的遗传工作。在这里,我们报告Raldh1,Raldh2和Raldh3单,双和三无效小鼠在眼睛中表现出越来越少或没有RA合成。我们的基因研究表明,视网膜的背腹模式的建立或维持不需要RA信号传导,因为我们观察到背侧Tbx5和ephrin B2(Efnb2)以及腹侧Vax2和Ephb2的正常表达。取而代之的是,需要RA来塑造发育中的视网膜和周围的间充质所需的形态发生运动。在早期阶段,间充质中表达的Raldh2和视网膜色素上皮中表达的Raldh3产生RA,RA向形态发生运动所需的神经视网膜传递重要信号,从而导致视杯的腹腔内陷。在后期,在背侧神经视网膜中表达的Raldh1和在腹侧神经视网膜中表达的Raldh3(加上在晶状体/角膜外胚层中每个表达较弱)会产生RA,该RA行进到周围的间充质,在此需要限制周围性间质的前向侵入形成角膜间质和眼睑。在所有阶段,RA靶组织均不同于RA合成的位置,这表明RALDHs非自主地发挥细胞功能以产生旁分泌RA信号,该信号指导邻近细胞的形态发生运动。

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