Transformation by FosB requires a trans-activation domain missing in FosB2 that can be substituted by heterologous activation domains.

doi:10.1101/gad.6.4.667

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GENES & DEVELOPMENT 6:667-675, 1992
ISSN 0890-9369

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Transformation by FosB requires a trans-activation domain missing in FosB2 that can be substituted by heterologous activation domains.

R Wisdom, J Yen, D Rashid, and I M Verma

Molecular Biology and Virology Laboratory, Salk Institute, San Diego, California 92186-5800.

Abstract

Two functionally distinct proteins derived from the FosB geneby alternative splicing have recently been described. FosB proteintransforms fibroblasts efficiently, whereas FosB2 protein, acarboxy-terminally truncated form of FosB, does not, despitethe fact that both proteins can participate in high-affinity,sequence-specific DNA binding as part of a heterodimeric complexwith c-Jun protein. We show here that the functional differencebetween these proteins is the result of the presence of a potentproline-rich transcriptional activation domain in the carboxy-terminalamino acids unique to FosB. This conclusion is supported bythree lines of evidence: (1) Mutations in the carboxy-terminalregion of FosB that impair transcriptional activation also reducetransforming potential, despite the fact that DNA binding aspart of a complex with c-Jun is not affected; (2) the carboxy-terminalregion unique to FosB functions as an activation domain whenfused to the DNA-binding domain of GAL4; and (3) transformingpotential can be conferred on FosB2 by fusing any of severaldifferent well-characterized trans-activation domains. Theseresults identify an additional functional requirement for transformationby Fos proteins and have implications for the mechanism(s) ofmitogenic signaling by the AP-1 transcription complex.

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