analysis of thisbe and pyramus functional domains reveals evidence for cleavage of drosophila fgfs提斯柏和皮拉摩斯功能域的分析,将揭示果蝇fgf乳沟的证据.pdfVIP
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analysis of thisbe and pyramus functional domains reveals evidence for cleavage of drosophila fgfs提斯柏和皮拉摩斯功能域的分析,将揭示果蝇fgf乳沟的证据
Tulin and Stathopoulos BMC Developmental Biology 2010, 10:83
/1471-213X/10/83
RESEARCH ARTICLE Open Access
Analysis of Thisbe and Pyramus functional
domains reveals evidence for cleavage of
Drosophila FGFs
*
Sarah Tulin, Angelike Stathopoulos
Abstract
Background: As important regulators of developmental and adult processes in metazoans, Fibroblast Growth
Factor (FGF) proteins are potent signaling molecules whose activities must be tightly regulated. FGFs are known to
play diverse roles in many processes, including mesoderm induction, branching morphogenesis, organ formation,
wound healing and malignant transformation; yet much more remains to be learned about the mechanisms of
regulation used to control FGF activity.
Results: In this work, we conducted an analysis of the functional domains of two Drosophila proteins, Thisbe (Ths)
and Pyramus (Pyr), which share homology with the FGF8 subfamily of ligands in vertebrates. Ths and Pyr proteins
are secreted from Drosophila Schneider cells (S2) as smaller N-terminal fragments presumably as a result of
intracellular proteolytic cleavage. Cleaved forms of Ths and Pyr can be detected in embryonic extracts as well. The
FGF-domain is contained within the secreted ligand portion, and this domain alone is capable of functioning in
the embryo when ectopically expressed. Through targeted ectopic expression experiments in which we assay the
ability of full-length, truncated, and chimeric proteins to support cell differentiation, we find evidence that (1) the
C-terminal domain of Pyr is retained inside the cell and does not seem to be required for receptor activation and
(2) the C-terminal domain of Ths is secreted and, while also not required for receptor activation, this domain does
plays a role in limiting the activity of Ths when
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