In skin, multipotent stem cells generate the keratinocytes of the epidermis, sebaceous gland, and hair follicles. In this paper, we show that Tcf3 and Lef1 control these differentiation lineages. In contrast to Lef1, which requires Wnt signaling and stabilized -catenin to express the hair-specific keratin genes and control hair differentiation, Tcf3 can act independently of its -catenin interacting domain to suppress features of epidermal terminal differentiation, in which Tcf3 is normally shut off, and promote features of the follicle outer root sheath (ORS) and multipotent stem cells (bulge), the compartments which naturally express Tcf3. These aspects of Tcf3's action are dependent on its DNA binding and Groucho repressor-binding domains. In the absence of its -catenin interacting domain, Lef1's behavior (⌬NLef1) seems to be markedly distinct from that of ⌬NTcf3. ⌬NLef1 does not suppress epidermal differentiation and promote ORS/bulge differentiation, but rather suppresses hair differentiation and gives rise to sebocyte differentiation. Taken together, these findings provide powerful evidence that the status of Tcf3/Lef complexes has a key role in controlling cell fate lineages in multipotent skin stem cells. The canonical Wnt/Wingless signaling pathway directs cell fate in a variety of cell types and has an integral role in organogenesis. At the core of the pathway is the stability of -catenin, a protein that serves a dual role in intercellular junction formation and in transcriptional regulation. Wnt signaling inhibits the amino-terminal phosphorylation and subsequent degradation of -catenin, allowing cytoplasmic pools of -catenin to enter the nucleus and bind to members of the Lef1/Tcf family of HMG domain-containing DNA-binding proteins. -catenin's activation domain and Lef1/Tcf's DNA-binding domain combine to form a bipartite transcriptional activator of target genes (for review, see Willert and Nusse 1998;Korswagen and Clevers 1999;Waltzer and Bienz 1999).Although Lef1/Tcf proteins often function as transactivators, these proteins can also interact with, and behave as, transcriptional repressors. CtBP represses a Wnt/Wingless response and selectively interacts with the carboxy-terminal domain of Tcf proteins, missing in Lef1 (Brannon et al. 1999). In contrast, the Groucho family of repressor proteins associate with the amino-terminal domain of all known Tcf/Lef family members (Cavallo et al. 1998;Roose et al. 1998;Brantjes et al. 2001). Genetically, a Drosophila dTcf-Groucho interaction antagonizes Wnt/Wingless signaling (Cavallo et al. 1998), and expression of Groucho proteins in Xenopus embryos can block axis formation and activation of -catenin target genes, such as siamois and xnr3 ). In zebrafish, embryonic Tcf3 appears to function as a transcriptional repressor, as an amino-terminally truncated Tcf3 (missing its -catenin binding domain) complements the headless phenotype caused by loss-of-function of wild-type Tcf3 (Kim et al. 2000). Therefore, in the absence of a Wnt/Wingless signal, the...
