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抑制性Smads蛋白和骨形态发生蛋白(BMP)在涡虫眼再生过程中调节前感光细胞数量。

Inhibitory Smads and bone morphogenetic protein (BMP) modulate anterior photoreceptor cell number during planarian eye regeneration.

作者信息

González-Sastre Alejandro, Molina Ma Dolores, Saló Emili

机构信息

Departament de Genètica, Facultat de Biologia, Universitat de Barcelona, Barcelona, Catalunya, Spain.

出版信息

Int J Dev Biol. 2012;56(1-3):155-63. doi: 10.1387/ijdb.123494ag.

Abstract

Planarians represent an excellent model to study the processes of body axis and organ re-specification during regeneration. Previous studies have revealed a conserved role for the bone morphogenetic protein (BMP) pathway and its intracellular mediators Smad1/5/8 and Smad4 in planarian dorsoventral (DV) axis re-establishment. In an attempt to gain further insight into the role of this signalling pathway in planarians, we have isolated and functionally characte-rized the inhibitory Smads (I-Smads) in Schmidtea mediterranea. Two I-Smad homologues have been identified: Smed-smad6/7-1 and Smed-smad6/7-2. Expression of smad6/7-1 was detected in the parenchyma, while smad6/7-2 was found to be ex-pressed in the central nervous system and the eyes. Neither single smad6/7-1 and smad6/7-2 nor double smad6/7-1,-2 silencing gave rise to any apparent disruption of the DV axis. However, both regenerating and intact smad6/7-2 (RNAi) planarians showed defects in eye morphogenesis and displayed small, rounded eyes that lacked the anterior subpopulation of photoreceptor cells. The number of pigment cells was also reduced in these animals at later stages of regeneration. In contrast, after low doses of Smed-bmp(RNAi), planarians regenerated larger eyes in which the anterior subpopulation of photoreceptor cells was expanded. Our results suggest that Smed-smad6/7-2 and Smed-bmp control the re-specification and maintenance of anterior photoreceptor cell number in S. mediterranea.

摘要

涡虫是研究再生过程中身体轴和器官重新特化的优秀模型。先前的研究已经揭示了骨形态发生蛋白(BMP)信号通路及其细胞内介质Smad1/5/8和Smad4在涡虫背腹(DV)轴重建中的保守作用。为了进一步深入了解该信号通路在涡虫中的作用,我们分离并对地中海涡虫中的抑制性Smads(I-Smads)进行了功能表征。已鉴定出两个I-Smad同源物:Smed-smad6/7-1和Smed-smad6/7-2。在实质组织中检测到smad6/7-1的表达,而smad6/7-2在中枢神经系统和眼睛中表达。单独沉默smad6/7-1和smad6/7-2以及同时沉默smad6/7-1和smad6/7-2均未导致DV轴出现明显破坏。然而,再生的和完整的smad6/7-2(RNA干扰)涡虫在眼睛形态发生方面均表现出缺陷,眼睛小且呈圆形,缺乏前部感光细胞亚群。在再生后期,这些动物中的色素细胞数量也减少了。相比之下,低剂量的Smed-bmp(RNA干扰)后,涡虫再生出更大的眼睛,其中前部感光细胞亚群扩大。我们的结果表明,Smed-smad6/7-2和Smed-bmp控制地中海涡虫前部感光细胞数量的重新特化和维持。

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