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Reversible acetylation regulates vascular endothelial growth factor receptor-2 activity 被引量:1
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作者 Annalisa Zecchin Lucia Pattarini +6 位作者 Maria Ines Gutierrez Miguel Mano Antonello Mai Sergio Valente Mike P. Myers Sergio Pantano mauro giacca 《Journal of Molecular Cell Biology》 SCIE CAS CSCD 2014年第2期116-127,共12页
酷氨酸 kinase 受体(VEGFR2 ) 脉管的 endothelial 生长因素受体 2 是 angiogenesis 的一个关键管理者。VEGFR2 在在 kinaseinsert 领域形成稠密的簇的四离氨酸残余两个都是在 endothelial 房间的 acetylated,在一个单身者,离氨酸在... 酷氨酸 kinase 受体(VEGFR2 ) 脉管的 endothelial 生长因素受体 2 是 angiogenesis 的一个关键管理者。VEGFR2 在在 kinaseinsert 领域形成稠密的簇的四离氨酸残余两个都是在 endothelial 房间的 acetylated,在一个单身者,离氨酸在受体激活环定位的 Herewe 表演。这些修正在动态 controlof 下面是 acetyltransferase p300 和二 deacetylases HDAC5 和 HDAC6。我们实质上表明那 VEGFR2 acetylation regulatesreceptor phosphorylation。特别地, VEGFR2 acetylation 显著地改变受体 phosphorylationafter ligand 绑定的动力学,允许受体 phosphorylation 并且在在激活循环的离氨酸的那 acetylation 贡献的有模拟显示的 VEGF.Molecular 动力学的延长刺激之上的细胞内部的发信号 transitionto 一个开的活跃状态,在哪个酷氨酸 phosphorylation 被 kinase 目标残余的更好的暴露赞成。Thesefindings 显示由 acetylation 的那 translational 以后修正是直接影响 VEGFR2function 的批评机制。 展开更多
关键词 血管内皮生长因子受体 活性状态 乙酰化 酪氨酸激酶受体 酪氨酸磷酸化 分子动力学模拟 化调 可逆
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Modified fibrin hydrogel for sustained delivery of RNAi lipopolyplexes in skeletal muscle
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作者 Ellen Ngarande Emma Doubell +4 位作者 Ousman Tamgue Manuel Mano Paul Human mauro giacca Neil Hamer Davies 《Regenerative Biomaterials》 SCIE EI 2023年第1期261-270,共10页
RNA interference is a promising therapeutical approach presently hindered by delivery concerns such as rapid RNA degradation and targeting of individual tissues.Injectable hydrogels are one potentially simple and dire... RNA interference is a promising therapeutical approach presently hindered by delivery concerns such as rapid RNA degradation and targeting of individual tissues.Injectable hydrogels are one potentially simple and direct route towards overcoming these barriers.Here we report on the utility of a combination of a mildly modified form of the clinically utilised fibrin hydrogel with Invivofectamine^(■)3.0,a lipid nonviral transfection vector,for local and sustained release.PEGylation of fibrin allowed for controlled release of small interfering RNA(siRNA)-lipopolyplexes for at least 10 days and greatly increased the stability of fibrin in vitro and in vivo.A 3D cell culture model and a release study showed transfection efficacy of siRNA-lipopolyplexes was retained for a minimum of 7 days.Injection in conjunction with PEGylated-fibrinogen significantly increased retention of siRNA-lipopolyplexes in mouse skeletal muscle and enhanced knockdown of myostatin mRNA that correlated with muscle growth.Thus,the increased efficacy observed here for the combination of a lipid nanoparticle,the only type of nonviral vector approved for the clinic,with fibrin,might allow for more rapid translation of injectable hydrogel-based RNA interference. 展开更多
关键词 RNA interference controlled release fibrin lipopolyplex
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