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Kindlin-1 controls Wnt and TGF-? availability to regulate cutaneous stem cell proliferation.


ABSTRACT: Kindlin-1 is an integrin tail binding protein that controls integrin activation. Mutations in the FERMT-1 gene, which encodes for Kindlin-1, lead to Kindler syndrome in man, which is characterized by skin blistering, premature skin aging and skin cancer of unknown etiology. Here we show that loss of Kindlin-1 in mouse keratinocytes recapitulates Kindler syndrome and also produces enlarged and hyperactive stem cell compartments, which lead to hyperthickened epidermis, ectopic hair follicle development and increased skin tumor susceptibility. Mechanistically, Kindlin-1 controls keratinocyte adhesion through ?1-class integrins and proliferation and differentiation of cutaneous epithelial stem cells by promoting ?(v)?(6) integrin-mediated transforming growth factor-? (TGF-?) activation and inhibiting Wnt-?-catenin signaling through integrin-independent regulation of Wnt ligand expression. Our findings assign Kindlin-1 the previously unknown and essential task of controlling cutaneous epithelial stem cell homeostasis by balancing TGF-?-mediated growth-inhibitory signals and Wnt-?-catenin-mediated growth-promoting signals.

SUBMITTER: Rognoni E 

PROVIDER: S-EPMC3982140 | biostudies-literature | 2014 Apr

REPOSITORIES: biostudies-literature

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Kindlin-1 is an integrin tail binding protein that controls integrin activation. Mutations in the FERMT-1 gene, which encodes for Kindlin-1, lead to Kindler syndrome in man, which is characterized by skin blistering, premature skin aging and skin cancer of unknown etiology. Here we show that loss of Kindlin-1 in mouse keratinocytes recapitulates Kindler syndrome and also produces enlarged and hyperactive stem cell compartments, which lead to hyperthickened epidermis, ectopic hair follicle develo  ...[more]

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