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多器官类器官源自人类诱导多能干细胞,显示出视网膜、角膜和视网膜色素上皮谱系。

Multiocular organoids from human induced pluripotent stem cells displayed retinal, corneal, and retinal pigment epithelium lineages.

机构信息

Ophthalmology Research Group, Vall d'Hebron Institut de Recerca (VHIR), Vall d'Hebron Barcelona Hospital Campus, Passeig Vall d'Hebron 119-129, 08035, Barcelona, Spain.

Regenerative Medicine Program IDIBELL, L'Hospitalet de Llobregat, Barcelona, Spain.

出版信息

Stem Cell Res Ther. 2021 Nov 22;12(1):581. doi: 10.1186/s13287-021-02651-9.

Abstract

BACKGROUND

Recently, great efforts have been made to design protocols for obtaining ocular cells from human stem cells to model diseases or for regenerative purposes. Current protocols generally focus on isolating retinal cells, retinal pigment epithelium (RPE), or corneal cells and fail to recapitulate the complexity of the tissue during eye development. Here, the generation of more advanced in vitro multiocular organoids from human induced pluripotent stem cells (hiPSCs) is demonstrated.

METHODS

A 2-step method was established to first obtain self-organized multizone ocular progenitor cells (mzOPCs) from 2D hiPSC cultures within three weeks. Then, after the cells were manually isolated and grown in suspension, 3D multiocular organoids were generated to model important cellular features of developing eyes.

RESULTS

In the 2D culture, self-formed mzOPCs spanned the neuroectoderm, surface ectoderm, neural crest, and RPE, mimicking early stages of eye development. After lifting, mzOPCs developed into different 3D multiocular organoids composed of multiple cell lineages including RPE, retina, and cornea, and interactions between the different cell types and regions of the eye system were observed. Within these organoids, the retinal regions exhibited correct layering and contained all major retinal cell subtypes as well as retinal morphological cues, whereas the corneal regions closely resembled the transparent ocular-surface epithelium and contained of corneal, limbal, and conjunctival epithelial cells. The arrangement of RPE cells also formed organoids composed of polarized pigmented epithelial cells at the surface that were completely filled with collagen matrix.

CONCLUSIONS

This approach clearly demonstrated the advantages of the combined 2D-3D construction tissue model as it provided a more ocular native-like cellular environment than that of previous models. In this complex preparations, multiocular organoids may be used to model the crosstalk between different cell types in eye development and disease.

摘要

背景

最近,人们做出了巨大努力来设计从人类干细胞中获取眼部细胞的方案,以用于疾病建模或再生目的。目前的方案通常侧重于分离视网膜细胞、视网膜色素上皮 (RPE) 或角膜细胞,而无法重现眼发育过程中的组织复杂性。在这里,展示了从人类诱导多能干细胞 (hiPSC) 生成更先进的体外多器官眼类器官的方法。

方法

建立了一种两步法,首先在三周内从 2D hiPSC 培养物中获得自我组织的多区眼部祖细胞 (mzOPC)。然后,在手动分离和悬浮培养细胞后,生成 3D 多器官类器官,以模拟发育中眼睛的重要细胞特征。

结果

在 2D 培养中,自形成的 mzOPC 跨越神经外胚层、表面外胚层、神经嵴和 RPE,模拟眼睛发育的早期阶段。提起后,mzOPC 发育成不同的 3D 多器官类器官,由包括 RPE、视网膜和角膜在内的多种细胞谱系组成,并观察到不同细胞类型和眼部系统区域之间的相互作用。在这些类器官中,视网膜区域表现出正确的分层,并包含所有主要的视网膜细胞亚型以及视网膜形态学线索,而角膜区域则与透明的眼部表面上皮非常相似,并且包含角膜、角膜缘和结膜上皮细胞。RPE 细胞的排列也形成了由表面的极化色素上皮细胞组成的类器官,这些细胞完全被胶原蛋白基质填充。

结论

该方法清楚地证明了 2D-3D 构建组织模型的优势,因为它提供了比以前的模型更具眼部原生样的细胞环境。在这种复杂的制剂中,多器官类器官可用于模拟眼部发育和疾病中不同细胞类型之间的串扰。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a4c0/8607587/5f9350cfd069/13287_2021_2651_Fig1_HTML.jpg

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