首页> 美国卫生研究院文献>Molecular and Cellular Biology >C/EBPβ When Expressed from the C/ebpα Gene Locus Can Functionally Replace C/EBPα in Liver but Not in Adipose Tissue
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C/EBPβ When Expressed from the C/ebpα Gene Locus Can Functionally Replace C/EBPα in Liver but Not in Adipose Tissue

机译:从C /ebpα基因位点表达时C /EBPβ可以功能性替代肝脏中的C /EBPα但不能替代脂肪组织中的C /EBPα

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摘要

Knockout of C/EBPα causes a severe loss of liver function and, subsequently, neonatal lethality in mice. By using a gene replacement approach, we generated a new C/EBPα-null mouse strain in which C/EBPβ, in addition to its own expression, substituted for C/EBPα expression in tissues. The homozygous mutant mice C/ebpαβ/β are viable and fertile and show none of the overt liver abnormalities found in the previous C/EBPα-null mouse line. Levels of hepatic PEPCK mRNA are not different between C/ebpαβ/β and wild-type mice. However, despite their normal growth rate, C/ebpαβ/β mice have markedly reduced fat storage in their white adipose tissue (WAT). Expression of two adipocyte-specific factors, adipsin and leptin, is significantly reduced in the WAT of C/ebpαβ/β mice. In addition, expression of the non-adipocyte-specific genes for transferrin and cysteine dioxygenase is reduced in WAT but not in liver. Our study demonstrates that when expressed from the C/ebpα gene locus, C/EBPβ can act for C/EBPα to maintain liver functions during development. Moreover, our studies with the C/ebpαβ/β mice provide new insights into the nonredundant functions of C/EBPα and C/EBPβ on gene regulation in WAT.
机译:敲除C /EBPα会导致肝功能严重丧失,并随后导致小鼠的新生儿致死率。通过使用基因替代方法,我们生成了一个新的C /EBPα-null小鼠品系,其中C /EBPβ除了自身的表达外还替代了组织中C /EBPα的表达。纯合突变小鼠C /ebpαβ/β具有活力和繁殖力,在以前的C /EBPα-null小鼠品系中均未发现明显的肝脏异常。 C /ebpαβ/β与野生型小鼠的肝PEPCK mRNA水平无差异。然而,尽管C /ebpαβ/β小鼠的生长速度正常,但其白色脂肪组织(WAT)中的脂肪存储量明显减少。在C /ebpαβ/β小鼠的WAT中,两种脂肪细胞特异性因子adipsin和leptin的表达显着降低。另外,在WAT中,运铁蛋白和半胱氨酸双加氧酶的非脂肪细胞特异性基因的表达降低,但在肝中则降低。我们的研究表明,当从C /ebpα基因位点表达时,C /EBPβ可以充当C /EBPα在发育过程中维持肝功能。此外,我们对C /ebpαβ/β小鼠的研究为C /EBPα和C /EBPβ在WAT基因调控中的非冗余功能提供了新的见解。

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