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Weisberg, E. et al.

A mouse homologue of FAST-1 transduces TGF beta superfamily signals and is expressed during early embryogenesis.

The transcription factor FAST-1 has recently been shown to play a key role in the specification of mesoderm by TGF beta superfamily signals in the early Xenopus embryo. We have cloned Fast1, a mouse homologue of Xenopus FAST-1, and characterized its expression during embryogenesis and function in activin/ TGF beta signal transduction. In vitro, Fast1 associates with Smads in response to an activin/ TGF beta signal to form a complex that recognizes the Xenopus activin responsive element (ARE) targeted by Xenopus FAST-1. In intact cells, introduction of Fast1 confers activin/ TGF beta regulation of an ARE-luciferase reporter. In embryos, Fast1 is expressed predominantly throughout the epiblast before gastrulation and declines as development progresses. We propose that mouse Fast1, like Xenopus FAST-1, mediates TGF beta superfamily signals specifying developmental fate during early embryogenesis.[1]

References

A mouse homologue of FAST-1 transduces TGF beta superfamily signals and is expressed during early embryogenesis. Weisberg, E., Winnier, G.E., Chen, X., Farnsworth, C.L., Hogan, B.L., Whitman, M. Mech. Dev. (1998) [Pubmed]

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