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在视网膜发育过程中,新生的水平细胞在神经上皮中双向迁移。

Newborn horizontal cells migrate bi-directionally across the neuroepithelium during retinal development.

作者信息

Edqvist Per-Henrik D, Hallböök Finn

机构信息

Department of Neuroscience, Unit of Developmental Neuroscience, Biomedical Center, Uppsala Univeristy, S-751 23, Uppsala, Sweden.

出版信息

Development. 2004 Mar;131(6):1343-51. doi: 10.1242/dev.01018. Epub 2004 Feb 18.

Abstract

Cell migration plays an important role during the development of the retina. In this work we have studied the migration of newborn horizontal cells in avian embryonic retina. Using the pattern of the early expressed transcription factors Lim1 and Prox1 we have shown that horizontal cells migrate bi-directionally from their site of birth, close to the ventricular side, to the adjacent (vitreal) side of the neuroepithelium, where they align just next to the prospective ganglion cell layer before migrating back again to their final laminar position in the external part of the inner nuclear layer. The migration occurs between Hamburger and Hamilton stages 24 and 33, which is equivalent to embryonic day 4.5 and 8. Between stages 26 and 30 the horizontal cells reside close to the ganglion cell layer and intra ocular injections of a cytochalasin D, an actin polymerisation blocker that inhibit migration, at stage 29 interfered with the migration of the horizontal cells to their final destination. Furthermore, using biolistic gene transfer with a green fluorescence protein expression vector of retinal slices we were able to record ventricle-directed migration by time-lapse microscopy. Combining biolistics with immunohistochemistry we showed that transfected cells, which have also been translocated in a ventricular direction were positive for the horizontal cell markers Lim1 and Prox1. The alternative path of migration that is described in this work differs from the generally accepted one for horizontal cells and this knowledge will influence the view of how the molecular determination of horizontal cells is specified.

摘要

细胞迁移在视网膜发育过程中起着重要作用。在这项研究中,我们研究了鸡胚视网膜中新生水平细胞的迁移。利用早期表达的转录因子Lim1和Prox1的模式,我们发现水平细胞从其靠近脑室侧的出生地双向迁移到神经上皮的相邻(玻璃体)侧,在那里它们在再次迁移回内核层外部的最终层位之前,排列在预期的神经节细胞层旁边。迁移发生在Hamburger和Hamilton分期的24至33期之间,相当于胚胎第4.5天和第8天。在26至30期之间,水平细胞靠近神经节细胞层,在第29期眼内注射细胞松弛素D(一种抑制迁移的肌动蛋白聚合阻滞剂)会干扰水平细胞向其最终目的地的迁移。此外,使用带有绿色荧光蛋白表达载体的生物弹道基因转移技术对视网膜切片进行研究,我们能够通过延时显微镜记录向脑室方向的迁移。将生物弹道技术与免疫组织化学相结合,我们发现也向脑室方向迁移的转染细胞对水平细胞标记物Lim1和Prox1呈阳性。这项研究中描述的替代迁移路径与水平细胞普遍接受的迁移路径不同,这一知识将影响对水平细胞分子决定机制的看法。

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