Mek1 Down Regulates Rad51 Activity during Yeast Meiosis by Phosphorylation of Hed1

Callender, Tracy L.; Laureau, Raphaëlle; Wan, Lihong; Chen, Xiangyu; Sandhu, Rima; Laljee, Saif; Zhou, Sai; Suhandynata, Ray T.; Prugar, Evelyn; Gaines, William A.; Kwon, Young Ho; Börner, G. Valentin; Nicolas, Alain; Neiman, Aaron M.; Hollingsworth, Nancy M.

doi:10.1371/journal.pgen.1006226

Cited by 87 publications

(167 citation statements)

References 83 publications

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“…This hypothesis is supported by the observation that Dmc1 foci formation is compromised in vivo when Rad51 is absent (7,18), the finding that Rad51 is downregulated by Hed1 and Mek1 during meiosis (14,16,17), and the finding that Rad51 strand invasion activity is not required during meiosis (13). We wanted to test the possibility that Dmc1 might also exert some influence over Rad51 by comparing the disassembly rates of Rad51 only, Dmc1 only, and mixed filaments containing both recombinases.…”

Section: Models For Mixed Recombinase Filaments -Rad51mentioning

confidence: 96%

“…Despite these many commonalities, Dmc1 is the recombinase responsible for performing strand invasion during meiosis (13). In contrast, Rad51 is actively downregulated by Hed1-and Mek1-mediated inhibition of its interactions with Rad54, which is a cofactor that is required for Rad51 strand invasion activity (11,(14)(15)(16)(17). However, Rad51 is required for normal progression through meiosis and promotes Dmc1 foci formation, consistent with a role for Rad51 as a Dmc1 accessory factor (6,7,13,18).…”

Section: Introductionmentioning

confidence: 99%

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Spontaneous self-segregation of Rad51 and Dmc1 DNA recombinases within mixed recombinase filaments

Crickard

Kaniecki

Kwon

et al. 2018

Journal of Biological Chemistry

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During meiosis, the two DNA recombinases Rad51 and Dmc1, form specialized presynaptic filaments that are adapted for performing recombination between homologous chromosomes. There is currently a limited understanding of how these two recombinases are organized within the meiotic presynaptic filament. Here, we used single molecule imaging to examine the properties of presynaptic complexes comprised of both Rad51 and Dmc1. We demonstrate that Rad51 and Dmc1 have an intrinsic ability to selfsegregate, even in the absence of any other recombination accessory proteins. Moreover, we found that the presence of Dmc1 stabilizes the adjacent Rad51 filaments, suggesting that crosstalk between these two recombinases may affect their biochemical properties. Based upon these findings, we describe a model for the organization of Rad51 and Dmc1 within the meiotic presynaptic complex, which is also consistent with in vivo observations, genetic findings and biochemical expectations. This model argues against the existence of extensively intermixed filaments, and we propose that Rad51 and Dmc1 have intrinsic capacities to form spatially distinct filaments, suggesting that additional recombination cofactors are not required to segregate the Rad51 and Dmc1 filaments.

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Section: Models For Mixed Recombinase Filaments -Rad51mentioning

confidence: 96%

Section: Introductionmentioning

confidence: 99%

Spontaneous self-segregation of Rad51 and Dmc1 DNA recombinases within mixed recombinase filaments

Crickard

Kaniecki

Kwon

et al. 2018

Journal of Biological Chemistry

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“…Genetic and biochemical studies have shown that Hed1 interacts with Rad51 and inhibits strand exchange activity by preventing Rad54 from associating with the presynaptic complex (Tsubouchi & Roeder, 2006;Busygina et al, 2008Busygina et al, , 2012Callender et al, 2016).…”

Section: Hed1 Interacts Tightly With the Rad51 Presynaptic Complexmentioning

confidence: 99%

“…In support of this model, we find that Rad54 and Hed1 binding interactions are mutually exclusive, and once established, these binding interactions are effectively irreversible over the time scales that might be relevant to meiotic progression ( Fig 7B). Reactivation of Rad51 coincides with inactivation of Mek1, and as a result, Rad54 phosphorylation and Hed1 phosphorylation are lost, and Hed1 is degraded (Callender et al, 2016;Argunhan et al, 2017;Prugar et al, 2017). Interestingly, Rad51 plays a late role in meiotic prophase by repairing residual DSBs after disassembly of the synaptonemal complex (Argunhan et al, 2017;Prugar et al, 2017).…”

Section: Transition From Mitotic To Meiotic Presynaptic Filamentsmentioning

confidence: 99%

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Regulation of Hed1 and Rad54 binding during maturation of the meiosis‐specific presynaptic complex

et al. 2018

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Most eukaryotes have two Rad51/RecA family recombinases, Rad51, which promotes recombination during mitotic double-strand break (DSB) repair, and the meiosis-specific recombinase Dmc1. During meiosis, the strand exchange activity of Rad51 is downregulated through interactions with the meiosis-specific protein Hed1, which helps ensure that strand exchange is driven by Dmc1 instead of Rad51. Hed1 acts by preventing Rad51 from interacting with Rad54, a cofactor required for promoting strand exchange during homologous recombination. However, we have a poor quantitative understanding of the regulatory interplay between these proteins. Here, we use real-time single-molecule imaging to probe how the Hed1- and Rad54-mediated regulatory network contributes to the identity of mitotic and meiotic presynaptic complexes. Based on our findings, we define a model in which kinetic competition between Hed1 and Rad54 helps define the functional identity of the presynaptic complex as cells undergo the transition from mitotic to meiotic repair.

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Meiotic Recombination Pathways

Reitz¹

2020

Encyclopedia of Life Sciences

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During meiosis, one round of DNA replication is followed by two rounds of division to create the gametes that are obligatory for biparental reproduction. To achieve the reductional segregation that is required during the first meiotic division, most eukaryotes utilise a program that involves the deliberate formation of DNA double‐stranded breaks in their genomes, followed by regulated homologous recombination and reciprocal exchange of genetic material between homologous chromosomes. This reciprocal exchange of genetic information physically links the homologous chromosomes to one another and provides the tension that is necessary for their segregation. Meiotic recombination is highly regulated to ensure that at least one reciprocal crossover event occurs between each pair of homologous chromosomes. Key Concepts Meiotic recombination physically links the homologous chromosomes to one another, creating the tension that is required for their segregation. Meiosis I is a reductional segregation that halves the ploidy of the cell. This process requires bi‐orientation of the homologous chromosomes but mono‐orientation of the sister chromatids, a feat that is achieved through structural modification of the sister chromatid centromeres by monopolin. Directed homologous recombination physically links the homologous chromosomes to one another, through preferential use of the homologous chromosome as the repair template, rather than the sister chromatid, followed by resolution of the recombination intermediate into a crossover. DNA double‐stranded break fate is decided early in the meiotic recombination pathway, with crossovers exclusively arising through a double‐Holliday junction intermediate and non‐crossovers primarily being formed through the synthesis‐dependent strand annealing pathway. Formation of the synaptonemal complex, a proteinaceous structure that assembles between homologous chromosomes during meiosis, is interdependent with meiotic recombination.

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Mek1 Down Regulates Rad51 Activity during Yeast Meiosis by Phosphorylation of Hed1

Cited by 87 publications

References 83 publications

Spontaneous self-segregation of Rad51 and Dmc1 DNA recombinases within mixed recombinase filaments

Spontaneous self-segregation of Rad51 and Dmc1 DNA recombinases within mixed recombinase filaments

Regulation of Hed1 and Rad54 binding during maturation of the meiosis‐specific presynaptic complex

Meiotic Recombination Pathways

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