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外限制膜的药理学破坏导致移植的光感受器前体细胞的视网膜整合增加。

Pharmacological disruption of the outer limiting membrane leads to increased retinal integration of transplanted photoreceptor precursors.

作者信息

West E L, Pearson R A, Tschernutter M, Sowden J C, MacLaren R E, Ali R R

机构信息

Division of Molecular Therapy, University College London, Institute of Ophthalmology, 11-43 Bath Street, London EC1V 9EL, UK.

出版信息

Exp Eye Res. 2008 Apr;86(4):601-11. doi: 10.1016/j.exer.2008.01.004. Epub 2008 Jan 12.

Abstract

Retinal degeneration is the leading cause of untreatable blindness in the developed world. Cell transplantation strategies provide a novel therapeutic approach to repair the retina and restore sight. Previously, we have shown that photoreceptor precursor cells can integrate and form functional photoreceptors after transplantation into the subretinal space of the adult mouse. In a clinical setting, however, it is likely that far greater numbers of integrated photoreceptors would be required to restore visual function. We therefore sought to assess whether the outer limiting membrane (OLM), a natural barrier between the subretinal space and the outer nuclear layer (ONL), could be reversibly disrupted and if disruption of this barrier could lead to enhanced numbers of transplanted photoreceptors integrating into the ONL. Transient chemical disruption of the OLM was induced in adult mice using the glial toxin, dl-alpha-aminoadipic acid (AAA). Dissociated early post-natal neural retinal cells were transplanted via subretinal injection at various time-points after AAA administration. At 3 weeks post-injection, the number of integrated, differentiated photoreceptor cells was assessed and compared with those found in the PBS-treated contralateral eye. We demonstrate for the first time that the OLM can be reversibly disrupted in adult mice, using a specific dose of AAA administered by intravitreal injection. In this model, OLM disruption is maximal at 72 h, and recovers by 2 weeks. When combined with cell transplantation, disruption of the OLM leads to a significant increase in the number of photoreceptors integrated within the ONL compared with PBS-treated controls. This effect was only seen in animals in which AAA had been administered 72 h prior to transplantation, i.e. when precursor cells were delivered into the subretinal space at a time coincident with maximal OLM disruption. These findings suggest that the OLM presents a physical barrier to photoreceptor integration following transplantation into the subretinal space in the adult mouse. Reversible disruption of the OLM may provide a strategy for increasing cell integration in future therapeutic applications.

摘要

视网膜变性是发达国家不可治愈性失明的主要原因。细胞移植策略为修复视网膜和恢复视力提供了一种新的治疗方法。此前,我们已经表明,光感受器前体细胞移植到成年小鼠的视网膜下间隙后可以整合并形成功能性光感受器。然而,在临床环境中,可能需要大量整合的光感受器才能恢复视觉功能。因此,我们试图评估视网膜下间隙与外核层(ONL)之间的天然屏障——外限制膜(OLM)是否可以被可逆性破坏,以及破坏该屏障是否会导致更多移植的光感受器整合到ONL中。使用神经胶质毒素dl-α-氨基己二酸(AAA)在成年小鼠中诱导OLM的短暂化学破坏。在给予AAA后的不同时间点,通过视网膜下注射移植出生后早期分离的神经视网膜细胞。注射后3周,评估整合的、分化的光感受器细胞数量,并与经磷酸盐缓冲盐水(PBS)处理的对侧眼中的细胞数量进行比较。我们首次证明,通过玻璃体内注射特定剂量的AAA,可以在成年小鼠中可逆性破坏OLM。在这个模型中,OLM破坏在72小时时最大,并在2周内恢复。与PBS处理的对照组相比,当与细胞移植相结合时,OLM的破坏导致整合到ONL中的光感受器数量显著增加。这种效应仅在移植前72小时给予AAA的动物中观察到,即在前体细胞在OLM破坏最大时被递送到视网膜下间隙时。这些发现表明,OLM对成年小鼠视网膜下间隙移植后的光感受器整合构成了物理屏障。OLM的可逆性破坏可能为未来治疗应用中增加细胞整合提供一种策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/542d/2394572/2f2eeda37fce/gr1.jpg

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