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小鼠新皮层与丘脑在器官型共培养中的促生长相互作用。

Growth-promoting interactions between the murine neocortex and thalamus in organotypic co-cultures.

作者信息

Rennie S, Lotto R B, Price D J

机构信息

Department of Physiology, University Medical School, Edinburgh, U.K.

出版信息

Neuroscience. 1994 Aug;61(3):547-64. doi: 10.1016/0306-4522(94)90433-2.

Abstract

The aim of this study was to assess whether developing cerebral cortex produces diffusible factors that can affect the growth of thalamic cells and, if so, what the role of these factors might be during the formation of thalamocortical connections. We studied interactions between cultured organotypic explants from mice maintained in defined serum-free medium. First, we cultured explants of embryonic dorsolateral thalamus in isolation from any other tissue; after culture, these explants were viewed intact and then sectioned. We estimated the numbers of healthy and pyknotic cells before and after culture, and the rates of mitosis in the explants during culture (using bromodeoxyuridine). Based on these data, we concluded that the majority of cells in the thalamic explants survived, although significant numbers of pyknotic cells did accumulate. Thalamic explants extended either very few or no neurites when cultured alone. We then cultured explants of embryonic thalamus near to explants from other tissues. A gap was always maintained between the explants, and we measured the length and density of neurite outgrowth from each thalamic explant. Slices of embryonic cortex promoted a small but significant increase in the amount of growth from thalamic explants. Postnatal cortex stimulated much more profuse neurite outgrowth; postnatal cerebellum had less of an effect, and postnatal medulla or liver had none. We showed that there was significantly more outgrowth from thalamic explants cultured in medium that had been preconditioned with cortical slices than from thalamic explants cultured in control medium, confirming that diffusible factors were produced by the cortex. The survival and mitotic rates of thalamic cells were unaffected by co-culture with the cortex. We conclude that the developing cortex releases diffusible factors that stimulate the growth of thalamic neurites and that other regions of the brain may also release the same substance(s). The lack of a specific source of thalamic growth promoting factor(s) argues against a role for these factors in guiding thalamic axons to specific targets; indeed, we were unable to demonstrate any chemotropic guidance of thalamic axons towards cortical explants in collagen gels. Since postnatal cortex has a more potent stimulatory effect than prenatal cortex, it seems possible that, in vivo, the cortical-derived factors act mainly on thalamocortical axons that have located their targets and are in the process of arborizing and refining their connections.

摘要

本研究的目的是评估发育中的大脑皮层是否会产生可扩散因子,这些因子能否影响丘脑细胞的生长,以及如果存在这种情况,这些因子在丘脑皮质连接形成过程中可能发挥什么作用。我们研究了在特定无血清培养基中培养的小鼠器官型外植体之间的相互作用。首先,我们单独培养胚胎背外侧丘脑的外植体,使其不与任何其他组织接触;培养后,观察这些外植体的整体情况,然后进行切片。我们估计了培养前后健康细胞和固缩细胞的数量,以及培养过程中外植体中的有丝分裂率(使用溴脱氧尿苷)。基于这些数据,我们得出结论,丘脑外植体中的大多数细胞存活了下来,尽管确实积累了大量固缩细胞。单独培养时,丘脑外植体伸出的神经突很少或没有。然后,我们将胚胎丘脑的外植体与其他组织的外植体靠近培养。外植体之间始终保持一定间隙,我们测量了每个丘脑外植体神经突生长的长度和密度。胚胎皮层切片促进了丘脑外植体生长量的小幅但显著增加。出生后皮层刺激神经突生长更为旺盛;出生后小脑的作用较小,而出生后延髓或肝脏则没有作用。我们发现,与在对照培养基中培养的丘脑外植体相比,在预先用皮层切片处理过的培养基中培养的丘脑外植体长出的神经突明显更多,这证实了皮层会产生可扩散因子。丘脑细胞的存活率和有丝分裂率不受与皮层共培养的影响。我们得出结论,发育中的皮层释放可扩散因子,刺激丘脑神经突的生长,并且大脑的其他区域可能也会释放相同的物质。缺乏促进丘脑生长因子的特定来源表明这些因子在引导丘脑轴突到达特定靶点方面不起作用;实际上,我们无法在胶原凝胶中证明丘脑轴突对皮层外植体有任何趋化性引导。由于出生后皮层比产前皮层具有更强的刺激作用,因此在体内,皮层衍生的因子似乎主要作用于已经找到靶点并正在进行分支和优化连接的丘脑皮质轴突。

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