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哺乳动物视网膜中的细胞重塑:实验性视网膜脱离研究结果

Cellular remodeling in mammalian retina: results from studies of experimental retinal detachment.

作者信息

Fisher Steven K, Lewis Geoffrey P, Linberg Kenneth A, Verardo Mark R

机构信息

Neuroscience Research Institute, University of California, Santa Barbara, Santa Barbara, CA 93106, USA.

出版信息

Prog Retin Eye Res. 2005 May;24(3):395-431. doi: 10.1016/j.preteyeres.2004.10.004. Epub 2005 Jan 13.

Abstract

Retinal detachment, the separation of the neural retina from the retinal pigmented epithelium, starts a cascade of events that results in cellular changes throughout the retina. While the degeneration of the light sensitive photoreceptor outer segments is clearly an important event, there are many other cellular changes that have the potential to significantly effect the return of vision after successful reattachment. Using animal models of detachment and reattachment we have identified many cellular changes that result in significant remodeling of the retinal tissue. These changes range from the retraction of axons by rod photoreceptors to the growth of neurites into the subretinal space and vitreous by horizontal and ganglion cells. Some neurite outgrowths, as in the case of rod bipolar cells, appear to be directed towards their normal presynaptic target. Horizontal cells may produce some directed neurites as well as extensive outgrowths that have no apparent target. A subset of reactive ganglion cells all fall into the latter category. Muller cells, the radial glia of the retina, undergo numerous changes ranging from proliferation to a wholesale structural reorganization as they grow into the subretinal space (after detachment) or vitreous after reattachment. In a few cases have we been able to identify molecular changes that correlate with the structural remodeling. Similar changes to those observed in the animal models have now been observed in human tissue samples, leading us to conclude that this research may help us understand the imperfect return of vision occurring after successful reattachment surgery. The mammalian retina clearly has a vast repertoire of cellular responses to injury, understanding these may help us improve upon current therapies or devise new therapies for blinding conditions.

摘要

视网膜脱离,即神经视网膜与视网膜色素上皮的分离,引发了一系列事件,导致整个视网膜发生细胞变化。虽然光敏感光感受器外段的退化显然是一个重要事件,但还有许多其他细胞变化可能会显著影响成功复位后视力的恢复。利用视网膜脱离和复位的动物模型,我们已经确定了许多导致视网膜组织显著重塑的细胞变化。这些变化范围从视杆光感受器的轴突回缩到水平细胞和神经节细胞的神经突向视网膜下间隙和玻璃体生长。一些神经突生长,如视杆双极细胞的情况,似乎是朝着它们正常的突触前靶点生长。水平细胞可能会产生一些有方向的神经突以及没有明显靶点的广泛生长。一部分反应性神经节细胞都属于后一种情况。米勒细胞,即视网膜的放射状胶质细胞,在脱离后生长到视网膜下间隙或复位后生长到玻璃体中时,会经历从增殖到全面结构重组的许多变化。在少数情况下,我们能够确定与结构重塑相关的分子变化。现在在人类组织样本中也观察到了与动物模型中类似的变化,这使我们得出结论,这项研究可能有助于我们理解成功复位手术后视力恢复不理想的原因。哺乳动物视网膜对损伤显然有大量的细胞反应,了解这些反应可能有助于我们改进当前的治疗方法或为致盲疾病设计新的治疗方法。

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