Cancer Research UK Molecular Oncology Laboratories, Weatherall Institute of Molecular Medicine, University of Oxford, John Radcliffe Hospital, Oxford, United Kingdom.
Blood. 2010 Sep 30;116(13):2385-94. doi: 10.1182/blood-2009-08-239228. Epub 2010 Jun 17.
Notch signaling is an evolutionary conserved pathway that is mediated by cell-cell contact. It is involved in a variety of developmental processes and has an essential role in vascular development and angiogenesis. Delta-like 4 (Dll4) is a Notch ligand that is up-regulated during angiogenesis. It is expressed in endothelial cells and regulates the differentiation between tip cells and stalk cells of neovasculature. Here, we present evidence that Dll4 is incorporated into endothelial exosomes. It can also be incorporated into the exosomes of tumor cells that overexpress Dll4. These exosomes can transfer the Dll4 protein to other endothelial cells and incorporate it into their cell membrane, which results in an inhibition of Notch signaling and a loss of Notch receptor. Transfer of Dll4 was also shown in vivo from tumor cells to host endothelium. Addition of Dll4 exosomes confers a tip cell phenotype on the endothelial cell, which results in a high Dll4/Notch-receptor ratio, low Notch signaling, and filopodia formation. This was further evidenced by increased branching in a tube-formation assay and in vivo. This reversal in phenotype appears to enhance vessel formation and is a new form of signaling for Notch ligands that expands their signaling potential beyond cell-cell contact.
Notch 信号通路是一种进化上保守的途径,由细胞-细胞接触介导。它参与多种发育过程,在血管发育和血管生成中起着至关重要的作用。Delta-like 4(Dll4)是 Notch 配体,在血管生成过程中上调。它在内皮细胞中表达,并调节新血管的尖端细胞和柄细胞之间的分化。在这里,我们提供了证据表明 Dll4 被纳入内皮细胞外体。它也可以被过度表达 Dll4 的肿瘤细胞纳入外体。这些外体可以将 Dll4 蛋白转移到其他内皮细胞,并将其纳入其细胞膜,从而抑制 Notch 信号和 Notch 受体的丢失。还显示了 Dll4 从肿瘤细胞到宿主内皮的体内转移。添加 Dll4 外体赋予内皮细胞尖端细胞表型,导致 Dll4/Notch 受体比值高、Notch 信号低和丝状伪足形成。这在管形成测定和体内进一步得到证实。这种表型的逆转似乎增强了血管形成,是 Notch 配体的一种新的信号形式,将其信号潜力扩展到超出细胞-细胞接触的范围。
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