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BMP 抑制 WNT 以整合成年涡虫体轴的正交模式。

BMP suppresses WNT to integrate patterning of orthogonal body axes in adult planarians.

机构信息

Department of Molecular Biosciences, Northwestern University; Evanston Illinois, United States of America.

Robert Lurie Comprehensive Cancer Center, Northwestern University; Evanston, Illinois, United States of America.

出版信息

PLoS Genet. 2023 Sep 20;19(9):e1010608. doi: 10.1371/journal.pgen.1010608. eCollection 2023 Sep.

Abstract

Adult regeneration restores patterning of orthogonal body axes after damage in a post-embryonic context. Planarians regenerate using distinct body-wide signals primarily regulating each axis dimension: anteroposterior Wnts, dorsoventral BMP, and mediolateral Wnt5 and Slit determinants. How regeneration can coordinate perpendicular tissue axes without symmetry-breaking embryonic events is not fully understood. Here, we report that the planarian dorsoventral regulator bmp4 suppresses the posterior determinant wnt1 to provide patterning input to the anteroposterior axis. Double-FISH identified distinct anteroposterior domains within dorsal midline muscle that express either bmp4 or wnt1. Homeostatic inhibition bmp4 and smad1 expanded the wnt1 expression anteriorly, while elevation of BMP signaling through nog1;nog2 RNAi reduced the wnt1 expression domain and elevated bmp4 expression. Homeostatic BMP signal perturbation broadly affected anteroposterior identity as measured by expression of posterior Wnt pathway factors, and caused mislocalization of AP-regionalized pharynx progenitors, without strongly affecting expression domains of anterior regulators. Additionally, wnt1 inhibition elevated bmp4 expression in the tip of the tail. Therefore, dorsal BMP signals and posterior wnt1 mutually antagonize for patterning the tail. Furthermore, homeostatic bmp4 RNAi caused medial expansion of the lateral determinant wnt5 and reduced expression of the medial regulator slit. By contrast, nog1;nog2 RNAi restricted wnt5 expression. Double RNAi of bmp4 and wnt5 resulted in lateral ectopic eye phenotypes, suggesting bmp4 acts upstream of wnt5 to pattern the mediolateral axis. These results indicate bmp4 controls dorsoventral information and also, through suppression of Wnt signals, influences anteroposterior and mediolateral identity. Based on related functions across vertebrates and Cnidarians, Wnt and BMP cross-regulation could form an ancient mechanism for coordinating orthogonal axis patterning.

摘要

成年再生在胚胎后环境中损伤后恢复正交体轴的模式。水螅通过使用主要调节每个轴维度的独特全身信号进行再生:前后 Wnts、背腹 BMP 和左右 Wnt5 和 Slit 决定因素。再生如何在没有破坏对称性的胚胎事件的情况下协调垂直组织轴尚不完全清楚。在这里,我们报告水螅的背腹调节剂 bmp4 抑制后向决定因素 wnt1,为前后轴提供模式输入。双重-FISH 鉴定了在背中线肌肉内表达 bmp4 或 wnt1 的独特前后域。bmp4 和 smad1 的稳态抑制使 wnt1 表达向前扩展,而通过 nog1; nog2 RNAi 升高 BMP 信号降低了 wnt1 表达域并升高了 bmp4 表达。稳态 BMP 信号扰动广泛影响前后身份,如后向 Wnt 途径因子的表达,并导致 AP 区域化咽祖细胞的位置错误,而对前向调节剂的表达域没有强烈影响。此外,wnt1 抑制在尾巴的尖端升高了 bmp4 的表达。因此,背侧 BMP 信号和后向 wnt1 相互拮抗以模式化尾巴。此外,稳态 bmp4 RNAi 导致侧向决定因素 wnt5 的内侧扩展,并降低了内侧调节剂 slit 的表达。相比之下,nog1; nog2 RNAi 限制了 wnt5 的表达。bmp4 和 wnt5 的双重 RNAi 导致了外侧异位眼表型,表明 bmp4 在上游作用于 wnt5 以模式化中侧轴。这些结果表明 bmp4 控制背腹信息,并且通过抑制 Wnt 信号,还影响前后和中侧身份。基于脊椎动物和刺胞动物的相关功能,Wnt 和 BMP 的交叉调节可能形成协调正交轴模式的古老机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e0b8/10545109/2ed6de757927/pgen.1010608.g001.jpg

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