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PPA1 Facilitates Thermogenesis in Brown and Beige Fat by Regulating the Mitochondrial Localization of FUS
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作者 Yue Sun Heng-le Ding +5 位作者 Jin-fu Zhang Yuan-yuan Su Nan Yang Ye Yin Hai-yan Lin Xiao-rong Zhu 《Current Medical Science》 2025年第6期1447-1459,共13页
Objective Brown and beige adipocytes dissipate energy through thermogenesis,and the impaired thermogenic function of these adipocytes is a key driver of obesity and related metabolic disorders.However,the molecular me... Objective Brown and beige adipocytes dissipate energy through thermogenesis,and the impaired thermogenic function of these adipocytes is a key driver of obesity and related metabolic disorders.However,the molecular mechanisms governing adipocyte thermogenesis are not fully understood.This study investigated the role of inorganic pyrophosphatase 1(PPA1)in regulating adipocyte thermogenesis and assessed its potential as a therapeutic target for obesity and metabolic disorders.Methods To investigate the function of PPA1 in adipose tissue thermogenesis,we generated adipose-specific heterozygous PPA1 knockout mice via the Cre-loxP system and established cold exposure models.PPA1 deletion effects were assessed by hematoxylin and eosin(H&E)staining,immunofluorescence,quantitative polymerase chain reaction(qPCR),and immunoblotting.Mitochondrial changes during browning were further characterized via transmission electron microscopy(TEM),mitochondrial DNA(mtDNA)quantification,qPCR,and Western blotting.The molecular mechanisms involved were subsequently dissected via mass spectrometry,coimmunoprecipitation(Co-IP),and immunofluorescence colocalization.Results Adi-PPA1^(fl/+)mice presented impaired adipose tissue thermogenesis upon cold exposure.Mechanistically,PPA1 deficiency impaired adipose browning in an enzyme activity-independent manner.PPA1 knockdown promoted the aberrant translocation and accumulation of fused in sarcoma(FUS)to mitochondria,which triggered mitochondrial dysfunction and suppressed browning.Crucially,silencing FUS effectively rescued the mitochondrial defects caused by PPA1 depletion.Conclusion PPA1 functions as a nonenzymatic positive regulator of adipocyte thermogenesis by interacting with FUS to prevent its mitochondrial mislocalization,thereby maintaining mitochondrial function and promoting adipose browning.These findings highlight PPA1 as a potential therapeutic avenue for obesity and metabolic disorders. 展开更多
关键词 ppa1 Adipose browning THERMOGENESIS Mitochondria FUS Obesity
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青杄中sPPa1的cDNA序列克隆及其生物信息学分析
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作者 曹一博 刘亚静 张凌云 《植物科学学报》 CAS CSCD 北大核心 2012年第4期394-401,共8页
以青杄(Picea wilsonii)均一化cDNA文库为模板,通过RACE方法克隆得到青杄PPa1基因cDNA全长,对该cDNA序列、核苷酸序列的相似性、理化性质、疏水性、二级结构、三级结构及是否跨膜进行了分析预测;进行了多序列比对并构建了系统树,同时对P... 以青杄(Picea wilsonii)均一化cDNA文库为模板,通过RACE方法克隆得到青杄PPa1基因cDNA全长,对该cDNA序列、核苷酸序列的相似性、理化性质、疏水性、二级结构、三级结构及是否跨膜进行了分析预测;进行了多序列比对并构建了系统树,同时对PPa1在青杄各组织中的表达量进行了检测。结果表明:青杄PPa1基因共由216个氨基酸组成,分子量为24.55 kD,理论PI为5.83,属可溶性蛋白;二级结构主要由α-螺旋、不规则卷曲和β-折叠构成;PPa1在青杄花粉中表达量最高。研究为进一步研究青杄PPa1的功能奠定了基础。 展开更多
关键词 青杄 ppa1 克隆 RACE 生物信息学
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小鼠PPA1重组腺病毒的构建及在胰岛β细胞中的表达 被引量:1
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作者 郑月 张许 韩晓 《南京医科大学学报(自然科学版)》 CAS CSCD 北大核心 2014年第8期1019-1024,共6页
目的:构建小鼠PPA1重组腺病毒,观察重组腺病毒在小鼠胰岛和β-TC6细胞中的表达,以及对脂肪酸引起的胰岛β细胞凋亡的影响。方法:将目的基因PPA1插入到腺病毒穿梭质粒pAdtrack-CMV中,质粒经PCR鉴定正确后用PmeⅠ酶切线性化,转到含有腺病... 目的:构建小鼠PPA1重组腺病毒,观察重组腺病毒在小鼠胰岛和β-TC6细胞中的表达,以及对脂肪酸引起的胰岛β细胞凋亡的影响。方法:将目的基因PPA1插入到腺病毒穿梭质粒pAdtrack-CMV中,质粒经PCR鉴定正确后用PmeⅠ酶切线性化,转到含有腺病毒骨架pAdeasy-1的BJ5183细菌中进行同源重组,重组成功的质粒经PacⅠ酶切线性化后转染QBI-293A细胞,经包装得到Ad-PPA1腺病毒。根据绿色荧光蛋白(GFP)检测病毒滴度和感染效率。用病毒感染小鼠胰岛和β-TC6细胞,以Western blot法检测PPA1蛋白表达水平。Hoechst染色法检测PPA1对细胞凋亡的影响。结果:重组腺病毒载体pAdeasyPPA1经酶切鉴定确认构建成功,将pAdeasy-PPA1转染QBI-293A细胞,观察细胞病变效应提示病毒成功包装。重组腺病毒能够有效感染小鼠胰岛和β-TC6细胞并成功过表达PPA1蛋白。Hoechst染色结果表明过表达PPA1可保护脂肪酸引起的胰岛β细胞凋亡。结论:成功构建携带小鼠PPA1基因的重组腺病毒,并证实过表达PPA1具有抗凋亡的作用,为进一步研究PPA1在胰岛β细胞中的功能奠定了基础。 展开更多
关键词 ppa1 腺病毒载体 胰岛Β细胞
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