A protein complex containing Tho2, Hpr1, Mft1 and a novel protein, Thp2, connects transcription elongation with mitotic recombination in Saccharomyces cerevisiae
Transcription‐induced recombination has been reported in all organisms from bacteria to mammals. We have shown previously that the yeast genes HPR1 and THO2 may be keys to the understanding of transcription‐associated recombination, as they both affect transcription elongation and hyper‐recombinatio...
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Veröffentlicht in: | The EMBO journal 2000-11, Vol.19 (21), p.5824-5834 |
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Sprache: | eng |
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Zusammenfassung: | Transcription‐induced recombination has been reported in all organisms from bacteria to mammals. We have shown previously that the yeast genes
HPR1
and
THO2
may be keys to the understanding of transcription‐associated recombination, as they both affect transcription elongation and hyper‐recombination in a concerted manner. Using a yeast strain that has the wild‐type
THO2
gene replaced by one encoding a His
6
‐HA‐tagged version, we have isolated an oligomeric complex containing four proteins: Tho2, Hpr1, Mft1 and a novel protein that we have named Thp2. We have reciprocally identified a complex containing Hpr1, Tho2 and Mft1 using anti‐Mft1 antibodies in immunoprecipitation experiments. The protein complex is mainly nuclear; therefore, Tho2 and Hpr1 are physically associated. Like
hpr1Δ
and
tho2Δ
cells,
mft1Δ
and
thp2Δ
cells show mitotic hyper‐ recombination and impaired transcription elongation, in particular, through the bacterial
lacZ
sequence. Hyper‐recombination conferred by
mft1Δ
and
thp2Δ
is only observed in DNA regions under transcription conditions. We propose that this protein complex acts as a functional unit connecting transcription elongation with the incidence of mitotic recombination. |
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ISSN: | 0261-4189 1460-2075 1460-2075 |
DOI: | 10.1093/emboj/19.21.5824 |