Mating-type switching by homology-directed recombinational repair: a matter of choice
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Mating-type switching by homology-directed recombinational repair : a matter of choice. / Thon, Genevieve; Maki, Takahisa; Haber, James E; Iwasaki, Hiroshi.
In: Current Genetics, Vol. 65, No. 2, 2019, p. 351-362.Research output: Contribution to journal › Journal article › Research › peer-review
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TY - JOUR
T1 - Mating-type switching by homology-directed recombinational repair
T2 - a matter of choice
AU - Thon, Genevieve
AU - Maki, Takahisa
AU - Haber, James E
AU - Iwasaki, Hiroshi
PY - 2019
Y1 - 2019
N2 - In eukaryotes, all DNA transactions happen in the context of chromatin that often takes part in regulatory mechanisms. In particular, chromatin structure can regulate exchanges of DNA occurring through homologous recombination. Few systems have provided as detailed a view on this phenomenon as mating-type switching in yeast. Mating-type switching entails the choice of a template for the gene conversions of the expressed mating-type locus. In the fission yeast Schizosaccharomyces pombe, correct template choice requires two competing small recombination enhancers, SRE2 and SRE3, that function in the context of heterochromatin. These two enhancers act with the Swi2/Swi5 recombination accessory complex to initiate strand exchange in a cell-type-specific manner, from SRE2 in M cells and SRE3 in P cells. New research indicates that the Set1C complex, responsible for H3K4 methylation, and the Brl2 ubiquitin ligase, that catalyzes H2BK119 ubiquitylation, participate in the cell-type-specific selection of SRE2 or SRE3. Here, we review these findings, compare donor preference in S. pombe to the distantly related budding yeast Saccharomyces cerevisiae, and contrast the positive effects of heterochromatin on the donor selection process with other situations, where heterochromatin represses recombination.
AB - In eukaryotes, all DNA transactions happen in the context of chromatin that often takes part in regulatory mechanisms. In particular, chromatin structure can regulate exchanges of DNA occurring through homologous recombination. Few systems have provided as detailed a view on this phenomenon as mating-type switching in yeast. Mating-type switching entails the choice of a template for the gene conversions of the expressed mating-type locus. In the fission yeast Schizosaccharomyces pombe, correct template choice requires two competing small recombination enhancers, SRE2 and SRE3, that function in the context of heterochromatin. These two enhancers act with the Swi2/Swi5 recombination accessory complex to initiate strand exchange in a cell-type-specific manner, from SRE2 in M cells and SRE3 in P cells. New research indicates that the Set1C complex, responsible for H3K4 methylation, and the Brl2 ubiquitin ligase, that catalyzes H2BK119 ubiquitylation, participate in the cell-type-specific selection of SRE2 or SRE3. Here, we review these findings, compare donor preference in S. pombe to the distantly related budding yeast Saccharomyces cerevisiae, and contrast the positive effects of heterochromatin on the donor selection process with other situations, where heterochromatin represses recombination.
KW - Chromatin structure
KW - Gene conversion
KW - Histone modifications
KW - Homology-directed repair
KW - Mating-type switching
KW - Recombination
U2 - 10.1007/s00294-018-0900-2
DO - 10.1007/s00294-018-0900-2
M3 - Journal article
C2 - 30382337
AN - SCOPUS:85055980062
VL - 65
SP - 351
EP - 362
JO - Current Genetics
JF - Current Genetics
SN - 0172-8083
IS - 2
ER -
ID: 209799919