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埃弗林-A2、埃弗林-A5及其他功能性导向信号的细胞定位是跨物种视网膜拓扑发育的基础。

Cellular localization of ephrin-A2, ephrin-A5, and other functional guidance cues underlies retinotopic development across species.

作者信息

Davenport R W, Thies E, Zhou R, Nelson P G

机构信息

Laboratory of Developmental Neurobiology, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, Maryland 20892, USA.

出版信息

J Neurosci. 1998 Feb 1;18(3):975-86. doi: 10.1523/JNEUROSCI.18-03-00975.1998.

Abstract

Avian retinotectal and rodent retinocollicular systems are general model systems used to examine developmental processes that underpin topographically organized neuronal circuits. The two systems rely on guidance components to establish their precise retinotopic maps, but many cellular events differ during their development. For example, compared with the chick, a generally less restricted outgrowth pattern is observed when retinae innervate their targets in rodents. Cellular or molecular distributions of guidance components may account for such differences in retinotopic development across species. Candidate repellent molecules, such as ephrin-A2 and ephrin-A5, have been cloned in both chick and rodents; however, it has not yet been shown in rodents that living cells express sufficient amounts of any repellent components to deter outgrowth. We used a coculture assay that gives cellular resolution of retinotarget interactions and demonstrate that living, caudal superior colliculus cells selectively prevent extension of axons from temporal regions of the retinae. Time-lapse video microscopy revealed the cellular localization of permissive and repulsive guidance components in rodents, which differed from that in chick. To analyze the potential molecular basis for these differences, we investigated the function and localization of ephrin-A2 and -A5. Cells transfected with ephrin-A2 and -A5 selectively repelled retinal axons. Ephrin-A2 and -A5 RNA expression patterns differed across cell populations and between species, suggesting molecular mechanisms and key cellular interactions that may underlie fundamental differences in the development of retinotectal and retinocollicular maps.

摘要

鸟类的视网膜 - 顶盖系统和啮齿动物的视网膜 - 丘脑系统是用于研究构成拓扑组织化神经回路基础的发育过程的通用模型系统。这两个系统依靠导向成分来建立其精确的视网膜拓扑图谱,但在它们的发育过程中许多细胞事件是不同的。例如,与鸡相比,当视网膜在啮齿动物中支配其靶标时,观察到一种通常限制较少的生长模式。导向成分的细胞或分子分布可能解释了跨物种视网膜拓扑发育中的这种差异。候选排斥分子,如ephrin - A2和ephrin - A5,已在鸡和啮齿动物中克隆出来;然而,在啮齿动物中尚未证明活细胞表达足够量的任何排斥成分来阻止生长。我们使用了一种共培养试验,该试验能够在细胞水平上解析视网膜 - 靶标相互作用,并证明活的尾侧上丘细胞选择性地阻止视网膜颞侧区域的轴突延伸。延时视频显微镜揭示了啮齿动物中允许性和排斥性导向成分的细胞定位,这与鸡中的不同。为了分析这些差异的潜在分子基础,我们研究了ephrin - A2和 - A5的功能和定位。用ephrin - A2和 - A5转染的细胞选择性地排斥视网膜轴突。Ephrin - A2和 - A5的RNA表达模式在不同细胞群体之间以及物种之间存在差异,这表明分子机制和关键细胞相互作用可能是视网膜 - 顶盖图谱和视网膜 - 丘脑图谱发育中根本差异的基础。

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