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Molecular cloning of SLC35D3 and analysis of its role during porcine intramuscular preadipocyte differentiation

机译:SLC35D3的分子克隆及其在猪肌内前脂肪细胞分化中的作用分析

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Solute carrier family 35 (SLC35) is one of a large number of membrane transporter protein families. Member D3 of this family is thought to be involved in adipose deposition and metabolic control. We obtained 2238?bp cDNA of porcine SLC35D3, it contains a 1272?bp ORF, encoding a 423 amino acid polypeptide, and a 966?bp 3′ UTR. BLAST results revealed that the amino acid sequence of porcine SLC35D3 had the closest phylogenetic relationship with members of the genus Ovis aries. Further bioinformatics analysis showed that the SLC35D3 protein contains 8 transmembrane domains, and that there is no signal peptide structure. The secondary structure of the protein mainly contains 37.12% α-helixes, 7.8% in β-folds, and 33.57% random coils. mRNA expression analysis showed that SLC35D3 is expressed in lung, liver, heart, spleen, kidney, longissimus dorsi muscle (LDM), leaf fat (LF), and subcutaneous adipose tissue (SAT). To examine the effects of SLC35D3 expression on fat synthesis and catabolism, SLC35D3-siRNA was transfected into cultured intramuscular adipocytes. SLC35D3 silenced cells showed increased expression of genes related to fat synthesis, and increased deposition of intramuscular fat (IMF), abundance of lipid droplets, and the level of free fatty acid (FFA) in the culture medium. In contrast, the siRNA decreased the expression genes involved in fat catabolism. Our results demonstrate that silenced SLC35D3 results in increased adipogenic processes in pig intramuscular adipocytes. These data represent the first exploration of SLC35D3 expression in swine, and provide valuable insights into the functions of SLC35D3 in adipocyte differentiation.
机译:溶质载体家族35(SLC35)是大量膜转运蛋白家族之一。认为这个家庭的成员D3参与脂肪沉积和代谢控制。我们获得了猪SLC35D3的2238 bp cDNA,它含有1272μlbporf,编码423氨基酸多肽,和966μl3'UTR。 BLAST结果表明,猪SLC35D3的氨基酸序列与卵巢属植物的成员具有最近的系统发育关系。进一步的生物信息学分析表明,SLC35D3蛋白含有8个跨膜结构域,并且没有信号肽结构。蛋白质的二级结构主要含有37.12%的α-螺旋,7.8%,β折叠,33.57%随机线圈。 mRNA表达分析表明,SLC35D3在肺,肝,心脏,脾,肾,长鼻菌,肌肉(LDM),叶脂(LF)和皮下脂肪组织(SAT)中表达。为了检查SLC35D3表达对脂肪合成和分解代谢的影响,将SLC35D3-siRNA转染到培养的肌内脂肪细胞中。 SLC35D3沉默的细胞显示出与脂肪合成相关的基因的表达增加,并增加肌内脂肪(IMF)的沉积,脂肪液滴的丰度,以及培养基中的游离脂肪酸(FFA)的水平。相反,siRNA降低了脂肪分解代谢的表达基因。我们的结果表明,沉默的SLC35D3导致猪肌内脂肪细胞中的脂肪生成过程增加。这些数据代表SWINE中SLC35D3表达的首次探索,并为SLC35D3在脂肪细胞分化中提供有价值的见解。

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