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成年斑马鱼光感受器变性慢性和急性模型中基因与蛋白质表达的比较分析。

A comparative analysis of gene and protein expression in chronic and acute models of photoreceptor degeneration in adult zebrafish.

作者信息

Kramer Ashley C, Carthage Justin, Berry Yasmeen, Gurdziel Katherine, Cook Tiffany A, Thummel Ryan

机构信息

Department of Ophthalmology, Visual and Anatomical Sciences, Wayne State University School of Medicine, Detroit, MI, United States.

Genomic Sciences Core, Wayne State University, Detroit, MI, United States.

出版信息

Front Cell Dev Biol. 2023 Sep 7;11:1233269. doi: 10.3389/fcell.2023.1233269. eCollection 2023.

Abstract

Adult zebrafish are capable of photoreceptor (PR) regeneration following acute phototoxic lesion (AL). We developed a chronic low light (CLL) exposure model that more accurately reflects chronic PR degeneration observed in many human retinal diseases. Here, we characterize the morphological and transcriptomic changes associated with acute and chronic models of PR degeneration at 8 time-points over a 28-day window using immunohistochemistry and 3'mRNA-seq. We first observed a differential sensitivity of rod and cone PRs to CLL. Next, we found no evidence for Müller glia (MG) gliosis or regenerative cell-cycle re-entry in the CLL model, which is in contrast to the robust gliosis and proliferative response from resident MG in the AL model. Differential responses of microglia between the models was also observed. Transcriptomic comparisons between the models revealed gene-specific networks of PR regeneration and degeneration, including genes that are activated under conditions of chronic PR stress. Finally, we showed that CLL is at least partially reversible, allowing for rod and cone outer segment outgrowth and replacement of rod cell nuclei via an apparent upregulation of the existing rod neurogenesis mechanism. Collectively, these data provide a direct comparison of the morphological and transcriptomic PR degeneration and regeneration models in zebrafish.

摘要

成年斑马鱼在急性光毒性损伤(AL)后能够进行光感受器(PR)再生。我们开发了一种慢性低光照(CLL)暴露模型,该模型能更准确地反映在许多人类视网膜疾病中观察到的慢性PR变性。在此,我们使用免疫组织化学和3'mRNA测序,在28天的时间窗口内的8个时间点,对与PR变性的急性和慢性模型相关的形态学和转录组变化进行了表征。我们首先观察到视杆和视锥PR对CLL的敏感性存在差异。接下来,我们发现在CLL模型中没有证据表明米勒胶质细胞(MG)发生胶质增生或再生细胞周期重新进入,这与AL模型中驻留MG的强烈胶质增生和增殖反应形成对比。在模型之间也观察到了小胶质细胞的不同反应。模型之间的转录组比较揭示了PR再生和变性的基因特异性网络,包括在慢性PR应激条件下被激活的基因。最后,我们表明CLL至少部分是可逆的,通过现有视杆神经发生机制的明显上调,允许视杆和视锥外段生长并替换视杆细胞核。总的来说,这些数据对斑马鱼中PR变性和再生的形态学和转录组模型进行了直接比较。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f585/10512720/379729d5ef97/fcell-11-1233269-g001.jpg

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