Estrach Soline, Legg James, Watt Fiona M
Wellcome Trust Centre for Stem Cell Research, Tennis Court Road, Cambridge, CB2 1QR, UK.
J Cell Sci. 2007 Aug 15;120(Pt 16):2944-52. doi: 10.1242/jcs.016253. Epub 2007 Jul 31.
In human interfollicular epidermis, stem cell clusters express high levels of the Notch ligand Delta1. Delta1 stimulates neighbouring cells to differentiate and also promotes stem cell clustering. Although Notch signalling is known to stimulate epidermal differentiation, little is known about the mechanism by which Delta1 promotes epidermal cell cohesiveness. This is an important issue, because the location of stem cells determines the local microenvironmental signals they receive. We now show that mutation of the Delta1 PDZ-binding domain abolishes Delta1-mediated keratinocyte cohesiveness, stimulates Notch transcriptional activity and promotes epidermal differentiation. A yeast two-hybrid screen revealed that Delta1 binds to the adaptor protein syntenin - an interaction dependent on the Delta1 PDZ-binding domain. Syntenin, like Delta1, is upregulated in the stem cell clusters of human interfollicular epidermis. Knockdown of syntenin in cells overexpressing full-length Delta1 had the same effects on Notch signalling, epidermal differentiation and adhesion as overexpressing Delta1 with a mutated PDZ-binding domain. Syntenin has previously been reported to regulate membrane traffic, and mutation of the Delta1 PDZ-binding domain or knockdown of syntenin led to rapid internalisation of Delta1. We propose that syntenin binding to Delta1 plays a dual role in promoting intercellular adhesion and regulating Notch signalling.
在人类毛囊间表皮中,干细胞簇表达高水平的Notch配体Delta1。Delta1刺激邻近细胞分化,还促进干细胞聚集。虽然已知Notch信号传导可刺激表皮分化,但对于Delta1促进表皮细胞黏附的机制却知之甚少。这是一个重要问题,因为干细胞的位置决定了它们所接收的局部微环境信号。我们现在表明,Delta1的PDZ结合结构域突变消除了Delta1介导的角质形成细胞黏附,刺激了Notch转录活性并促进了表皮分化。酵母双杂交筛选显示Delta1与衔接蛋白syntenin结合——这种相互作用依赖于Delta1的PDZ结合结构域。与Delta1一样,syntenin在人类毛囊间表皮的干细胞簇中上调。在过表达全长Delta1的细胞中敲低syntenin对Notch信号传导、表皮分化和黏附的影响与过表达具有突变PDZ结合结构域的Delta1相同。此前有报道称syntenin可调节膜运输,Delta1的PDZ结合结构域突变或syntenin敲低会导致Delta1快速内化。我们提出,syntenin与Delta1的结合在促进细胞间黏附和调节Notch信号传导中起双重作用。