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Brain endogenous liver X receptor ligands selectively promote midbrain neurogenesis

  作者 THEOFILOPOULOS SPYRIDON; WANG YUQIN; KITAMBI SATISH SRINIVAS; SACCHETTI PAOLA; SOUSA KYLE M; BODIN KARL; KIRK JAYNE; SALTO CARMEN; GUSTAFSSON MAGNUS; TOLEDO ENRIQUE M; KARU KERSTI; GUSTAFSSON JANAKE; STEFFENSEN KNUT R; ERNFORS PATRIK; SJOVALL JAN; GRIFFITHS WILLIAM J; ARENAS ERNEST  
  选自 期刊  NATURE CHEMICAL BIOLOGY;  卷期  2013年9-2;  页码  126-133  
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[摘要]Liver X receptors (Lxr alpha and Lxr beta) are ligand-dependent nuclear receptors critical for ventral midbrain neurogenesis in vivo. However, no endogenous midbrain Lxr ligand has so far been identified. Here we used LC/MS and functional assays to identify cholic acid as a new Lxr ligand. Moreover, 24(S),25-epoxycholesterol (24,25-EC) was found to be the most potent and abundant Lxr ligand in the developing mouse midbrain. Both Lxr ligands promoted neural development in an Lxr-dependent manner in zebrafish in vivo. Notably, each ligand selectively regulated the development of distinct midbrain neuronal populations. Whereas cholic acid increased survival and neurogenesis of Brn3a-positive red nucleus neurons, 24,25-EC promoted dopaminergic neurogenesis. These results identify an entirely new class of highly selective and cell type-specific regulators of neurogenesis and neuronal survival. Moreover, 24,25-EC promoted dopaminergic differentiation of embryonic stem cells, suggesting that Lxr ligands may thus contribute to the development of cell replacement and regenerative therapies for Parkinson's disease.

 
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