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Dynamic complexes of A-type lamins and emerin influence adipogenic capacity of the cell via nucleocytoplasmic distribution of β-catenin

机译:A型lamin和emerin的动态复合物影响成脂作用 通过核质的细胞分布能力 β-连环蛋白

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摘要

It is well documented that adipogenic differentiation of the cell is associated with downregulation of Wnt/β-catenin signalling. Using preadipocytes and dermal fibroblasts, we have found that activation of the adipogenic program was associated with marked changes in the expression of nuclear β-catenin-interacting partners, emerin and lamins A/C, to influence expression and activation of peroxisome proliferators-activated receptors γ (PPARγ). In addition, silencing of protein expression with siRNA revealed that β-catenin and emerin influenced each other's levels of expression and the onset of adipogenesis, suggesting that changes in the expression of nuclear lamina proteins were intimately linked to the stability of β-catenin. By contrast, dermal fibroblasts, which are emerin null, demonstrated increased nuclear accumulation of stable β-catenin and constant lamin expression. This was also associated with an unusual adipogenic capacity of the cells, with adipogenesis occurring in the presence of activated β-catenin but declining upon silencing of the protein expression with siRNA. We propose that the process of adipogenesis is affected by a dynamic link between complexes of emerin and lamins A/C at the nuclear envelope and nucleocytoplasmic distribution of β-catenin, to influence cellular plasticity and differentiation.
机译:众所周知,细胞的成脂分化与Wnt /β-catenin信号的下调有关。使用前脂肪细胞和真皮成纤维细胞,我们发现脂肪形成程序的激活与核β-catenin相互作用伙伴,emerin和lamins A / C表达的显着变化有关,从而影响过氧化物酶体增殖物激活受体的表达和激活。 γ(PPARγ)。此外,使用siRNA沉默蛋白质表达后发现,β-catenin和emerin相互影响表达水平和脂肪形成的开始,这表明核纤层蛋白表达的变化与β-catenin的稳定性密切相关。与此相反,真皮成纤维细胞为Emerin无效,表现出稳定的β-catenin的核蓄积增加和恒定的Lamin表达。这也与细胞异常的成脂能力有关,成脂作用在活化的β-连环蛋白存在下发生,但在siRNA沉默蛋白表达后下降。我们建议成脂过程受核蛋白和核蛋白的β-catenin分布在核膜的emerin和lamins A / C的复杂之间的动态联系,以影响细胞的可塑性和分化。

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