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利用类器官中WNT和SHH的正交梯度对人类脑区谱系进行特异性分化。

Specification of human regional brain lineages using orthogonal gradients of WNT and SHH in organoids.

作者信息

Scuderi Soraya, Kang Tae-Yun, Jourdon Alexandre, Yang Liang, Wu Feinan, Nelson Alex, Anderson George M, Mariani Jessica, Sarangi Vivekananda, Abyzov Alexej, Levchenko Andre, Vaccarino Flora M

出版信息

bioRxiv. 2024 May 19:2024.05.18.594828. doi: 10.1101/2024.05.18.594828.

DOI:10.1101/2024.05.18.594828
PMID:38798404
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11118582/
Abstract

The repertory of neurons generated by progenitor cells depends on their location along antero-posterior and dorso-ventral axes of the neural tube. To understand if recreating those axes was sufficient to specify human brain neuronal diversity, we designed a mesofluidic device termed Duo-MAPS to expose induced pluripotent stem cells (iPSC) to concomitant orthogonal gradients of a posteriorizing and a ventralizing morphogen, activating WNT and SHH signaling, respectively. Comparison of single cell transcriptomes with fetal human brain revealed that Duo-MAPS-patterned organoids generated the major neuronal lineages of the forebrain, midbrain, and hindbrain. Morphogens crosstalk translated into early patterns of gene expression programs predicting the generation of specific brain lineages. Human iPSC lines from six different genetic backgrounds showed substantial differences in response to morphogens, suggesting that interindividual genomic and epigenomic variations could impact brain lineages formation. Morphogen gradients promise to be a key approach to model the brain in its entirety.

摘要

由祖细胞产生的神经元库取决于它们在神经管前后轴和背腹轴上的位置。为了了解重建这些轴是否足以确定人类大脑神经元的多样性,我们设计了一种称为Duo-MAPS的微流控装置,以使诱导多能干细胞(iPSC)暴露于分别激活WNT和SHH信号的后化和腹化形态发生素的伴随正交梯度中。将单细胞转录组与胎儿人类大脑进行比较发现,经Duo-MAPS模式化的类器官产生了前脑、中脑和后脑的主要神经元谱系。形态发生素的串扰转化为预测特定脑谱系产生的基因表达程序的早期模式。来自六种不同遗传背景的人类iPSC系对形态发生素的反应存在显著差异,这表明个体间的基因组和表观基因组变异可能会影响脑谱系的形成。形态发生素梯度有望成为一种全面模拟大脑的关键方法。