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结肠类器官的体外极化以创建肠道干细胞区室。

In Vitro Polarization of Colonoids to Create an Intestinal Stem Cell Compartment.

作者信息

Attayek Peter J, Ahmad Asad A, Wang Yuli, Williamson Ian, Sims Christopher E, Magness Scott T, Allbritton Nancy L

机构信息

Department of Biomedical Engineering, University of North Carolina, Chapel Hill, NC 27599 and North Carolina State University, Raleigh, NC, 27695, United States of America.

Department of Chemistry, University of North Carolina, Chapel Hill, NC, 27599, United States of America.

出版信息

PLoS One. 2016 Apr 21;11(4):e0153795. doi: 10.1371/journal.pone.0153795. eCollection 2016.

Abstract

The polarity of proliferative and differentiated cellular compartments of colonic crypts is believed to be specified by gradients of key mitogens and morphogens. Indirect evidence demonstrates a tight correlation between Wnt- pathway activity and the basal-luminal patterning; however, to date there has been no direct experimental manipulation demonstrating that a chemical gradient of signaling factors can produce similar patterning under controlled conditions. In the current work, colonic organoids (colonoids) derived from cultured, multicellular organoid fragments or single stem cells were exposed in culture to steep linear gradients of two Wnt-signaling ligands, Wnt-3a and R-spondin1. The use of a genetically engineered Sox9-Sox9EGFP:CAGDsRED reporter gene mouse model and EdU-based labeling enabled crypt patterning to be quantified in the developing colonoids. Colonoids derived from multicellular fragments cultured for 5 days under a Wnt-3a or a combined Wnt-3a and R-spondin1 gradient were highly polarized with proliferative cells localizing to the region of the higher morphogen concentration. In a Wnt-3a gradient, Sox9EGFP polarization was 7.3 times greater than that of colonoids cultured in the absence of a gradient; and the extent of EdU polarization was 2.2 times greater than that in the absence of a gradient. Under a Wnt-3a/R-spondin1 gradient, Sox9EGFP polarization was 8.2 times greater than that of colonoids cultured in the absence of a gradient while the extent of EdU polarization was 10 times greater than that in the absence of a gradient. Colonoids derived from single stem cells cultured in Wnt-3a/R-spondin1 gradients were most highly polarized demonstrated by a Sox9EGFP polarization 20 times that of colonoids grown in the absence of a gradient. This data provides direct evidence that a linear gradient of Wnt signaling factors applied to colonic stem cells is sufficient to direct patterning of the colonoid unit in culture.

摘要

结肠隐窝增殖和分化细胞区室的极性被认为是由关键促有丝分裂原和形态发生素的梯度所决定的。间接证据表明Wnt信号通路活性与基底-管腔模式之间存在紧密关联;然而,迄今为止,尚无直接的实验操作表明信号因子的化学梯度在可控条件下能产生类似的模式。在当前研究中,将源自培养的多细胞类器官片段或单个干细胞的结肠类器官(结肠小体)在培养中暴露于两种Wnt信号配体Wnt-3a和R-spondin1的陡峭线性梯度中。使用基因工程的Sox9-Sox9EGFP:CAGDsRED报告基因小鼠模型和基于EdU的标记能够在发育中的结肠小体中对隐窝模式进行量化。在Wnt-3a或Wnt-3a与R-spondin1组合梯度下培养5天的多细胞片段衍生的结肠小体高度极化,增殖细胞定位于较高形态发生素浓度区域。在Wnt-3a梯度下,Sox9EGFP的极化比无梯度培养的结肠小体高7.3倍;EdU极化程度比无梯度培养时高2.2倍。在Wnt-3a/R-spondin1梯度下,Sox9EGFP极化比无梯度培养的结肠小体高8.2倍,而EdU极化程度比无梯度培养时高10倍。在Wnt-3a/R-spondin1梯度中培养的单个干细胞衍生的结肠小体极化程度最高,Sox9EGFP极化是无梯度培养的结肠小体的20倍。该数据提供了直接证据,表明应用于结肠干细胞的Wnt信号因子线性梯度足以在培养中指导结肠小体单元的模式形成。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3939/4839657/df6941420f71/pone.0153795.g001.jpg

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