A functional antagonism between the pgc germline repressor and torso in the development of somatic cells
Segregation of the germline is a fundamental event during early development. In Drosophila , germ cells are specified at the posterior pole of the embryo by the germplasm. As zygotic expression is activated, germ cells remain transcriptionally silent owing to the polar granule component (Pgc), a sma...
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Veröffentlicht in: | EMBO reports 2009-09, Vol.10 (9), p.1059-1065 |
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Hauptverfasser: | , , , |
Format: | Artikel |
Sprache: | eng |
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Zusammenfassung: | Segregation of the germline is a fundamental event during early development. In
Drosophila
, germ cells are specified at the posterior pole of the embryo by the germplasm. As zygotic expression is activated, germ cells remain transcriptionally silent owing to the polar granule component (Pgc), a small peptide present in germ cells. Somatic cells at both the embryonic ends are specified by the torso (Tor) receptor tyrosine kinase, and in
tor
mutants the somatic cells closer to the germ cells fail to cellularize correctly. Here, we show that extra wild‐type gene copies of
pgc
cause a similar cellularization phenotype, and that both excessive
pgc
and a lack of
tor
are associated with an impairment of transcription in somatic cells. Moreover, a lack of
pgc
partly ameliorates the cellularization defect of
tor
mutants, thus revealing a functional antagonism between
pgc
and
tor
in the specification of germline and somatic properties. As transcriptional quiescence is a general feature of germ cells, similar mechanisms might operate in many organisms to ‘protect’ somatic cells that adjoin germ cells from inappropriately succumbing to such quiescence. |
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ISSN: | 1469-221X 1469-3178 |
DOI: | 10.1038/embor.2009.128 |