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Src 通过 WNT/FGFRL 信号作用来模式化扁形动物的前后轴。

Src acts with WNT/FGFRL signaling to pattern the planarian anteroposterior axis.

机构信息

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. 2022 Apr 1;149(7). doi: 10.1242/dev.200125. Epub 2022 Mar 30.

Abstract

Tissue identity determination is crucial for regeneration, and the planarian anteroposterior (AP) axis uses positional control genes expressed from body wall muscle to determine body regionalization. Canonical Wnt signaling establishes anterior versus posterior pole identities through notum and wnt1 signaling, and two Wnt/FGFRL signaling pathways control head and trunk domains, but their downstream signaling mechanisms are not fully understood. Here, we identify a planarian Src homolog that restricts head and trunk identities to anterior positions. src-1(RNAi) animals formed enlarged brains and ectopic eyes and also duplicated trunk tissue, similar to a combination of Wnt/FGFRL RNAi phenotypes. src-1 was required for establishing territories of positional control gene expression in Schmidtea mediterranea, indicating that it acts at an upstream step in patterning the AP axis. Double RNAi experiments and eye regeneration assays suggest src-1 can act in parallel to at least some Wnt and FGFRL factors. Co-inhibition of src-1 with other posterior-promoting factors led to dramatic patterning changes and a reprogramming of Wnt/FGFRLs into controlling new positional outputs. These results identify src-1 as a factor that promotes robustness of the AP positional system that instructs appropriate regeneration.

摘要

组织身份确定对于再生至关重要,而扁形动物的前后(AP)轴利用来自体壁肌肉表达的位置控制基因来确定身体区域化。经典 Wnt 信号通过背板和 wnt1 信号建立前后极的身份,并且两个 Wnt/FGFRL 信号通路控制头部和躯干区域,但它们的下游信号机制尚未完全了解。在这里,我们鉴定了一种扁形动物 Src 同源物,该同源物将头部和躯干的身份限制在前部位置。src-1(RNAi) 动物形成了扩大的大脑和异位眼睛,并且还复制了躯干组织,类似于 Wnt/FGFRL RNAi 表型的组合。src-1 对于在 Schmidtea mediterranea 中建立位置控制基因表达的领地是必需的,表明它在 AP 轴模式形成的上游步骤中起作用。双 RNAi 实验和眼睛再生测定表明,src-1 可以与至少一些 Wnt 和 FGFRL 因子平行作用。与其他促进后极的因子共同抑制 src-1 会导致显著的模式变化,并将 Wnt/FGFRL 重新编程为控制新的位置输出。这些结果表明 src-1 是一种促进适当再生的 AP 位置系统稳健性的因素。

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