通过对祖细胞进行镶嵌图案化,高度并行地生产出设计器官。

Cell systems Pub Date : 2024-07-17 Epub Date: 2024-07-08 DOI:10.1016/j.cels.2024.06.004
Catherine M Porter, Grace C Qian, Samuel H Grindel, Alex J Hughes
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引用次数: 0

摘要

从人类干细胞中提取的类器官是一种用于疾病建模、再生医学和基础研究的前景广阔的方法。然而,类器官的可变性和对形态结果的有限控制仍是一项挑战。一个悬而未决的问题是,对培养条件的工程控制能在多大程度上引导类器官形成特定的成分。在这里,我们扩展了一种DNA "魔术贴 "细胞模式化方法,在微孔阵列中精确控制人类诱导多能干细胞衍生祖细胞的数量和比例,从而形成肾小球祖细胞(NP)类器官和镶嵌NP/输尿管芽(UB)顶端细胞类器官。我们展示了与几何限制脱钩的对器官大小和形态的长期控制。然后,我们展示了取决于初始祖细胞组成的器官组织比例的新趋势。这些趋势包括在镶嵌式 NP/UB 有机体与纯 NP 有机体中肾小球和基质细胞的比例较高,以及镶嵌式有机体中的 "金锁 "初始细胞比例能优化近端小管结构的形成。
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Highly parallel production of designer organoids by mosaic patterning of progenitors.

Organoids derived from human stem cells are a promising approach for disease modeling, regenerative medicine, and fundamental research. However, organoid variability and limited control over morphological outcomes remain as challenges. One open question is the extent to which engineering control over culture conditions can guide organoids to specific compositions. Here, we extend a DNA "velcro" cell patterning approach, precisely controlling the number and ratio of human induced pluripotent stem cell-derived progenitors contributing to nephron progenitor (NP) organoids and mosaic NP/ureteric bud (UB) tip cell organoids within arrays of microwells. We demonstrate long-term control over organoid size and morphology, decoupled from geometric constraints. We then show emergent trends in organoid tissue proportions that depend on initial progenitor cell composition. These include higher nephron and stromal cell representation in mosaic NP/UB organoids vs. NP-only organoids and a "goldilocks" initial cell ratio in mosaic organoids that optimizes the formation of proximal tubule structures.

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