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Wnt/Notum空间反馈抑制控制新生细胞分化以调节涡虫大脑的可逆生长。

Wnt/Notum spatial feedback inhibition controls neoblast differentiation to regulate reversible growth of the planarian brain.

作者信息

Hill Eric M, Petersen Christian P

机构信息

Department of Molecular Biosciences, Northwestern University, Evanston, IL 60208, USA.

Department of Molecular Biosciences, Northwestern University, Evanston, IL 60208, USA Robert Lurie Comprehensive Cancer Center, Northwestern University, Evanston, IL 60208, USA

出版信息

Development. 2015 Dec 15;142(24):4217-29. doi: 10.1242/dev.123612. Epub 2015 Nov 2.

Abstract

Mechanisms determining final organ size are poorly understood. Animals undergoing regeneration or ongoing adult growth are likely to require sustained and robust mechanisms to achieve and maintain appropriate sizes. Planarians, well known for their ability to undergo whole-body regeneration using pluripotent adult stem cells of the neoblast population, can reversibly scale body size over an order of magnitude by controlling cell number. Using quantitative analysis, we showed that after injury planarians perfectly restored brain:body proportion by increasing brain cell number through epimorphosis or decreasing brain cell number through tissue remodeling (morphallaxis), as appropriate. We identified a pathway controlling a brain size set-point that involves feedback inhibition between wnt11-6/wntA/wnt4a and notum, encoding conserved antagonistic signaling factors expressed at opposite brain poles. wnt11-6/wntA/wnt4a undergoes feedback inhibition through canonical Wnt signaling but is likely to regulate brain size in a non-canonical pathway independently of beta-catenin-1 and APC. Wnt/Notum signaling tunes numbers of differentiated brain cells in regenerative growth and tissue remodeling by influencing the abundance of brain progenitors descended from pluripotent stem cells, as opposed to regulating cell death. These results suggest that the attainment of final organ size might be accomplished by achieving a balance of positional signaling inputs that regulate the rates of tissue production.

摘要

决定最终器官大小的机制目前还知之甚少。经历再生或持续成年生长的动物可能需要持续且强大的机制来实现并维持合适的大小。涡虫以其利用新成体中多能成体干细胞进行全身再生的能力而闻名,它们可以通过控制细胞数量可逆地将身体大小调整一个数量级。通过定量分析,我们发现受伤后的涡虫通过适当的方式,即通过再生增加脑细胞数量或通过组织重塑(形态重建)减少脑细胞数量,完美地恢复了脑体比例。我们确定了一条控制脑大小设定点的途径,该途径涉及wnt11 - 6/wntA/wnt4a与notum之间的反馈抑制,notum编码在脑的相对两极表达的保守拮抗信号因子。wnt11 - 6/wntA/wnt4a通过经典Wnt信号传导进行反馈抑制,但可能通过独立于β - 连环蛋白 - 1和APC的非经典途径调节脑大小。Wnt/Notum信号传导通过影响源自多能干细胞的脑祖细胞的丰度,而不是调节细胞死亡,来调节再生生长和组织重塑中分化脑细胞的数量。这些结果表明,最终器官大小的实现可能是通过调节组织产生速率的位置信号输入的平衡来完成的。

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