The roX genes encode redundant male‐specific lethal transcripts required for targeting of the MSL complex
The roX1 and roX2 genes of Drosophila produce male‐specific non‐coding RNAs that co‐localize with the Male‐Specific Lethal (MSL) protein complex. This complex mediates up‐regulation of the male X chromo some by increasing histone H4 acetylation, thus contributing to the equalization of X‐linked gene...
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Veröffentlicht in: | The EMBO journal 2002-03, Vol.21 (5), p.1084-1091 |
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Format: | Artikel |
Sprache: | eng |
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Zusammenfassung: | The
roX1
and
roX2
genes of
Drosophila
produce male‐specific non‐coding RNAs that co‐localize with the Male‐Specific Lethal (MSL) protein complex. This complex mediates up‐regulation of the male X chromo some by increasing histone H4 acetylation, thus contributing to the equalization of X‐linked gene expression between the sexes. Both
roX
genes overlap two of ∼35 chromatin entry sites, DNA sequences proposed to act
in cis
to direct the MSL complex to the X chromosome. Although dosage compensation is essential in males, an intact
roX1
gene is not required by either sex. We have generated flies lacking
roX2
and find that this gene is also non‐essential. However, simultaneous removal of both
roX
RNAs causes a striking male‐specific reduction in viability accompanied by relocation of the MSL proteins and acetylated histone H4 from the X chromosome to autosomal sites and heterochromatin. Males can be rescued by
roX
cDNAs from autosomal transgenes, demonstrating the genetic separation of the chromatin entry and RNA‐encoding functions. Therefore, the
roX1
and
roX2
genes produce redundant,
male‐specific lethal
transcripts required for targeting the MSL complex. |
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ISSN: | 0261-4189 1460-2075 |
DOI: | 10.1093/emboj/21.5.1084 |