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Transcriptomic analysis elucidates the enhanced skeletal muscle mass, reduced fat accumulation, and metabolically benign liver in human follistatin-344 transgenic pigs 被引量:3
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作者 LONG Ke-ren LI Xiao-kai +13 位作者 ZHANG Ruo-wei GU Yi-ren du Min-jie XING Xiang-yang du jia-xiang MAI Miao-miao WANG Jing JIN Long TANG Qian-zi HU Si-lu MA Ji-deng WANG Xun PAN Deng-ke LI Ming-zhou 《Journal of Integrative Agriculture》 SCIE CAS CSCD 2022年第9期2675-2690,共16页
Follistatin(FST) is an important regulator of skeletal muscle growth and adipose deposition through its ability to bind to several members of the transforming growth factor-β(TGF-β) superfamily, and thus may be a go... Follistatin(FST) is an important regulator of skeletal muscle growth and adipose deposition through its ability to bind to several members of the transforming growth factor-β(TGF-β) superfamily, and thus may be a good candidate for future animal breeding programs. However, the molecular mechanisms underlying the phenotypic changes have yet to be clarified in pig. We generated transgenic(TG) pigs that express human FST specifically in skeletal muscle tissues and characterized the phenotypic changes compared with the same tissues in wild-type pigs. The TG pigs showed increased skeletal muscle growth, decreased adipose deposition, and improved metabolism status(P<0.05). Transcriptome analysis detected important roles of the PIK3–AKT signaling pathway, calcium-mediated signaling pathway, and amino acid metabolism pathway in FST-induced skeletal muscle hypertrophy, and depot-specific oxidative metabolism changes in psoas major muscle. Furthermore, the lipid metabolism-related process was changed in adipose tissue in the TG pigs. Gene set enrichment analysis revealed that genes related to lipid synthesis, lipid catabolism, and lipid storage were down-regulated(P<0.01) in the TG pigs for subcutaneous fat, whereas genes related to lipid catabolism were significantly up-regulated(P<0.05) in the TG pigs for retroperitoneal fat compared with their expression levels in wild-type pigs. In liver, genes related to the TGF-β signaling pathway were over-represented in the TG pigs, which is consistent with the inhibitory role of FST in regulating TGF-β signaling. Together, these results provide new insights into the molecular mechanisms underlying the phenotypic changes in pig. 展开更多
关键词 FOLLISTATIN transgenic pig TRANSCRIPTOME skeletal muscle LIVER ADIPOSE
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牦牛成纤维细胞敲低HO-1基因后对相关基因表达的影响 被引量:2
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作者 杜嘉祥 张全伟 +3 位作者 王琪 张勇 马友记 赵兴绪 《中国兽医学报》 CAS CSCD 北大核心 2019年第8期1616-1621,共6页
血红素加氧酶1(heme oxygenase1,HO-1),是血红素分解代谢过程中的限速酶,起到重要的抗氧化损伤作用,HO-1活性的改变直接影响抗氧化损伤能力的变化。为研究HO-1基因在牦牛高海拔低氧适应的氧化损伤功能,通过构建HO-1基因的siRNA序列,转... 血红素加氧酶1(heme oxygenase1,HO-1),是血红素分解代谢过程中的限速酶,起到重要的抗氧化损伤作用,HO-1活性的改变直接影响抗氧化损伤能力的变化。为研究HO-1基因在牦牛高海拔低氧适应的氧化损伤功能,通过构建HO-1基因的siRNA序列,转染牦牛胎儿成纤维细胞,试验前期发现HO-1基因过表达后与CYGB(胞红蛋白)、eNOS(内皮型一氧化氮合酶)基因相关。通过qRT-PCR和蛋白免疫印记(Western blot)检测转染HO-1 siRNA序列的牦牛成纤维细胞在正常条件和低氧条件(5%氧气)下0,24,48,72 h相关基因和蛋白表达变化。结果显示:siRNA转染牦牛成纤维细胞后,试验组HO-1的表达量显著低于空白组和阴性组(P<0.01),试验组CYGB表达量也低于空白组和阴性组(P<0.01),且HO-1、CYGB蛋白表达量在72 h最低,试验组eNOS mRNA表达量显著低于空白组和阴性组,eNOS蛋白未见表达。结果揭示:牦牛成纤维细胞敲低HO-1基因后,HO-1基因和蛋白表达量明显下调,且对携氧蛋白CYGB及eNOS信号通路的表达具有相同的影响。该结果为牦牛HO-1的功能及其在牦牛缺氧保护机制的研究提供理论依据。 展开更多
关键词 血红素氧化酶-1 牦牛成纤维细胞 SIRNA
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