DESCRIPTION: This revised application describes studies to elucidate
the functional role and molecular mechanism of action of tif, a new
member of the axl family of receptors. Tif, which was cloned by RTPCR
from a K562 library, is an extremely interesting receptor in
that it bears extracellular fibronectin domains as well as Ig
domains, suggesting a role in cell-matrix attachment and signalling.
In addition, its pattern of RNA expression, gonad>brain>other
tissues, suggests a potential role in primitive cell maintenance
and self-renewal. In this application, the Applicant proposes to:
1) Study the transforming potential of tif by enforced over-
expression; 2) Investigate the role of tif in hematopoietic
determination and differentiation by analyzing the phenotype of
both K562 and Ba/F3 cells constitutively expressing activated tif,
and by differentiating ES cells with a targeted gene disruption of
the tif locus; 3)Identify the immediate downstream components of
the tif signaling pathway via immonocoprecipitation and via the yeast
two-hybrid system; 4)Search for a functional interaction between tif
and the Epo receptor by enforced expression of an EpoR/tif
chimera, analyzing signal transduction and cellular phenotype in
transfected Ba/F3 and K562 cells; and 5)Identify and clone the tif
ligand via expression or affinity column chromatography. These
studies are designed to provide the first important steps towards
understanding the role of Tif in hematopoietic differentiation.
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