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Parenchymal and stromal tissue regeneration of tooth organ by pivotal signals reinstated in decellularized matrix.

Nat Mater. 2019-06; 
HeLing,ZhouJian,ChenMo,LinChyuan-Sheng,KimSahng G,ZhouYue,XiangLusai,XieMing,BaiHanying,YaoHai,ShiChangcheng,CoelhoPaulo G,BromageTimothy G,HuBin,TovarNick,WitekLukasz,WuJiaqian,ChenKenian,GuWei,ZhengJinxuan,SheuTzong-Jen,ZhongJuan,WenJin,NiuYuting,ChengBin,GongQimei,OwensDavid M,StanislauskasMilda,PeiJasmine,ChotkowskiGregory,WangSainan,YangGuodong,ZegarelliDavid J,ShiXin,FinkelMyron,ZhangWen,LiJunyuan,ChengJiayi,TarnowDennis P,ZhouXuedong,WangZuolin,JiangXinquan,RomanovAlexander,RoweDavid W,WangSonglin,YeLing,LingJunqi,MaoJe
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Custom Vector Construction Alx3’s reading frame was cloned into the pWPI vector with GenScript, control pWPI (plasmid no. 12254 (Addgene)) or pWPI-Alx3 (6.25μg), pMD2.G (plasmid no. 12259 (Addgene)) (0.625μg) and psPAX2 (plasmid no. 12260 (Addgene)) (3.125μg), as per our previous methods. Get A Quote

摘要

Cells are transplanted to regenerate an organs' parenchyma, but how transplanted parenchymal cells induce stromal regeneration is elusive. Despite the common use of a decellularized matrix, little is known as to the pivotal signals that must be restored for tissue or organ regeneration. We report that Alx3, a developmentally important gene, orchestrated adult parenchymal and stromal regeneration by directly transactivating Wnt3a and vascular endothelial growth factor. In contrast to the modest parenchyma formed by native adult progenitors, Alx3-restored cells in decellularized scaffolds not only produced vascularized stroma that involved vascular endothelial growth factor signalling, but also parenc... More

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