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Uroplakins play conserved roles in egg fertilization and acquired additional urothelial functions during mammalian divergence

机译:泌尿素原蛋白在卵子受精中发挥保守作用在哺乳动物分化过程中获得额外的尿道上皮功能

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摘要

Uroplakin (UP) tetraspanins and their associated proteins are major mammalian urothelial differentiation products that form unique two-dimensional crystals of 16-nm particles (“urothelial plaques”) covering the apical urothelial surface. Although uroplakins are highly expressed only in mammalian urothelium and are often referred to as being urothelium specific, they are also expressed in several mouse nonurothelial cell types in stomach, kidney, prostate, epididymis, testis/sperms, and ovary/oocytes. In oocytes, uroplakins colocalize with CD9 on cell-surface and multivesicular body-derived exosomes, and the cytoplasmic tail of UPIIIa undergoes a conserved fertilization-dependent, Fyn-mediated tyrosine phosphorylation that also occurs in Xenopus laevis eggs. Uroplakin knockout and antibody blocking reduce mouse eggs’ fertilization rate in in vitro fertilization assays, and UPII/IIIa double-knockout mice have a smaller litter size. Phylogenetic analyses showed that uroplakin sequences underwent significant mammal-specific changes. These results suggest that, by mediating signal transduction and modulating membrane stability that do not require two-dimensional-crystal formation, uroplakins can perform conserved and more ancestral fertilization functions in mouse and frog eggs. Uroplakins acquired the ability to form two-dimensional-crystalline plaques during mammalian divergence, enabling them to perform additional functions, including umbrella cell enlargement and the formation of permeability and mechanical barriers, to protect/modify the apical surface of the modern-day mammalian urothelium.
机译:尿白蛋白(UP)四跨膜蛋白及其相关蛋白是主要的哺乳动物尿路上皮分化产物,形成覆盖顶端尿道上皮表面的16 nm颗粒的独特二维晶体(“尿道上皮斑块”)。尽管uroplakins仅在哺乳动物尿路上皮中高度表达,并且通常被称为尿路上皮特异性的,但它们还在胃,肾,前列腺,附睾,睾丸/精子和卵巢/卵母细胞的几种小鼠非尿路上皮细胞类型中表达。在卵母细胞中,uroplakins与CD9在细胞表面和多囊体来源的外泌体上共定位,并且UPIIIa的细胞质尾巴受到保守的受精依赖性Fyn介导的酪氨酸磷酸化,这也发生在非洲爪蟾卵中。在体外受精试验中,Uroplakin基因敲除和抗体阻断降低了小鼠卵的受精率,而UPII / IIIa双敲除小鼠的窝产仔数较小。系统发育分析表明,uroplakin序列发生了明显的哺乳动物特异性变化。这些结果表明,通过介导不需要二维晶体形成的信号转导和调节膜的稳定性,uroplakins可以在小鼠和蛙卵中发挥保守的祖先受精功能。 Uroplakins具有在哺乳动物分化过程中形成二维晶体斑块的能力,从而使其能够执行其他功能,包括保护伞细胞扩大以及形成通透性和机械屏障,以保护/修饰现代哺乳动物尿道上皮的顶端表面。

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