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Publication : Meiotic cohesin SMC1β provides prophase I centromeric cohesion and is required for multiple synapsis-associated functions.

First Author  Biswas U Year  2013
Journal  PLoS Genet Volume  9
Issue  12 Pages  e1003985
PubMed ID  24385917 Mgi Jnum  J:207501
Mgi Id  MGI:5558997 Doi  10.1371/journal.pgen.1003985
Citation  Biswas U, et al. (2013) Meiotic cohesin SMC1beta provides prophase I centromeric cohesion and is required for multiple synapsis-associated functions. PLoS Genet 9(12):e1003985
abstractText  Cohesin subunit SMC1beta is specific and essential for meiosis. Previous studies showed functions of SMC1beta in determining the axis-loop structure of synaptonemal complexes (SCs), in providing sister chromatid cohesion (SCC) in metaphase I and thereafter, in protecting telomere structure, and in synapsis. However, several central questions remained unanswered and concern roles of SMC1beta in SCC and synapsis and processes related to these two processes. Here we show that SMC1beta substantially supports prophase I SCC at centromeres but not along chromosome arms. Arm cohesion and some of centromeric cohesion in prophase I are provided by non-phosphorylated SMC1alpha. Besides supporting synapsis of autosomes, SMC1beta is also required for synapsis and silencing of sex chromosomes. In absence of SMC1beta, the silencing factor gammaH2AX remains associated with asynapsed autosomes and fails to localize to sex chromosomes. Microarray expression studies revealed up-regulated sex chromosome genes and many down-regulated autosomal genes. SMC1beta is further required for non-homologous chromosome associations observed in absence of SPO11 and thus of programmed double-strand breaks. These breaks are properly generated in Smc1beta(-)/(-) spermatocytes, but their repair is delayed on asynapsed chromosomes. SMC1alpha alone cannot support non-homologous associations. Together with previous knowledge, three main functions of SMC1beta have emerged, which have multiple consequences for spermatocyte biology: generation of the loop-axis architecture of SCs, homologous and non-homologous synapsis, and SCC starting in early prophase I.
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