Mutations in the DSL (Delta, Serrate, Lag2) Notch (N) ligand Delta-like (Dll) 3 cause skeletal abnormalities in spondylocostal dysostosis, which is consistent with a critical role for N signaling during somitogenesis. Understanding how Dll3 functions is complicated by reports that DSL ligands both activate and inhibit N signaling. In contrast to other DSL ligands, we show that Dll3 does not activate N signaling in multiple assays. Consistent with these findings, Dll3 does not bind to cells expressing any of the four N receptors, and N1 does not bind Dll3-expressing cells. However, in a cell-autonomous manner, Dll3 suppressed N signaling, as was found for other DSL ligands. Therefore, Dll3 functions not as an activator as previously reported but rather as a dedicated inhibitor of N signaling. As an N antagonist, Dll3 promoted Xenopus laevis neurogenesis and inhibited glial differentiation of mouse neural progenitors. Finally, together with the modulator lunatic fringe, Dll3 altered N signaling levels that were induced by other DSL ligands.
The divergent DSL ligand Dll3 does not activate Notch signaling but cell autonomously attenuates signaling induced by other DSL ligands
E. Ladi's present address is Department of Molecular and Cellular Biology, University of California, Berkeley, Berkeley, CA 94720.
Abbreviations used in this paper: Dll, Delta-like; GFAP, glial fibrillary acidic protein; LFng, lunatic fringe; mDll, mouse Dll; MLC2, myosin light chain 2; NICD, Notch intracellular domain; NRARP, Notch-regulated ankyrin repeat protein; NSC, neural stem cell; NT-DSL, NH2-terminal and DSL domains; PSM, presomitic mesoderm; rDll, rat Dll; SAV, streptavidin; WCL, whole cell lysate.
Ena Ladi, James T. Nichols, Weihong Ge, Alison Miyamoto, Christine Yao, Liang-Tung Yang, Jim Boulter, Yi E. Sun, Chris Kintner, Gerry Weinmaster; The divergent DSL ligand Dll3 does not activate Notch signaling but cell autonomously attenuates signaling induced by other DSL ligands . J Cell Biol 12 September 2005; 170 (6): 983–992. doi: https://doi.org/10.1083/jcb.200503113
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