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plakophilin-3 对于晚期胚胎期两栖动物的发育是必需的,其在外胚层和神经组织中发挥作用。

Plakophilin-3 is required for late embryonic amphibian development, exhibiting roles in ectodermal and neural tissues.

机构信息

Department of Biochemistry and Molecular Biology, University of Texas M.D. Anderson Cancer Center, Houston, Texas, United States of America.

出版信息

PLoS One. 2012;7(4):e34342. doi: 10.1371/journal.pone.0034342. Epub 2012 Apr 5.

Abstract

The p120-catenin family has undergone a significant expansion during the evolution of vertebrates, resulting in varied functions that have yet to be discerned or fully characterized. Likewise, members of the plakophilins, a related catenin subfamily, are found throughout the cell with little known about their functions outside the desmosomal plaque. While the plakophilin-3 (Pkp3) knockout mouse resulted in skin defects, we find larger, including lethal effects following its depletion in Xenopus. Pkp3, unlike some other characterized catenins in amphibians, does not have significant maternal deposits of mRNA. However, during embryogenesis, two Pkp3 protein products whose temporal expression is partially complimentary become expressed. Only the smaller of these products is found in adult Xenopus tissues, with an expression pattern exhibiting distinctions as well as overlaps with those observed in mammalian studies. We determined that Xenopus Pkp3 depletion causes a skin fragility phenotype in keeping with the mouse knockout, but more novel, Xenopus tailbud embryos are hyposensitive to touch even in embryos lacking outward discernable phenotypes, and we additionally resolved disruptions in certain peripheral neural structures, altered establishment and migration of neural crest, and defects in ectodermal multiciliated cells. The use of two distinct morpholinos, as well as rescue approaches, indicated the specificity of these effects. Our results point to the requirement of Pkp3 in amphibian embryogenesis, with functional roles in a number of tissue types.

摘要

p120 连环蛋白家族在脊椎动物的进化过程中经历了显著的扩张,导致其功能多样化,但其功能尚未被发现或完全阐明。同样, plakophilin 家族的成员在整个细胞中都有发现,但其在桥粒斑之外的功能知之甚少。虽然 plakophilin-3 (Pkp3) 敲除小鼠导致皮肤缺陷,但我们发现其在非洲爪蟾中的消耗会导致更大的缺陷,包括致命影响。与一些在两栖动物中具有特征的连环蛋白不同,Pkp3 没有大量的母体 mRNA 沉积。然而,在胚胎发生过程中,两种 Pkp3 蛋白产物的表达时间部分互补。只有较小的产物在成年非洲爪蟾组织中被发现,其表达模式与在哺乳动物研究中观察到的表达模式既有区别又有重叠。我们确定,非洲爪蟾 Pkp3 的消耗导致皮肤脆弱表型与小鼠敲除一致,但更具新颖性的是,非洲爪蟾尾芽胚胎对触摸的敏感性降低,即使在缺乏明显表型的胚胎中也是如此,并且我们还解决了某些外周神经结构的破坏、神经嵴的建立和迁移改变以及外胚层多纤毛细胞的缺陷。两种不同的 morpholino 的使用以及挽救方法表明了这些效应的特异性。我们的结果表明 Pkp3 在两栖动物胚胎发生中的必要性,以及其在许多组织类型中的功能作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3b83/3320641/ccda3718b7eb/pone.0034342.g001.jpg

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