<scp>PDS</scp>
            5 proteins regulate the length of axial elements and telomere integrity during male mouse meiosis

Viera, Alberto; Berenguer, Inés; Ruiz‐Torres, Miguel; Gómez, Rocío; Guajardo, Andrea; Barbero, José Luís; Losada, Ana; Suja, José Á.

doi:10.15252/embr.201949273

Cited by 24 publications

(20 citation statements)

References 75 publications

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“…Therefore, alterations in Pds5 to modulate axis length are an efficient way of regulating recombination frequency. Pds5 is conserved because decreased axis length and recombination frequency have also been observed in fission yeast and mammals when Pds5 is depleted during meiosis ( 23 , 27 , 28 , 55 ).…”

Section: Discussionmentioning

confidence: 99%

“…The depletion of cohesin results in shorter axes during mammalian meiosis ( 20 , 24 , 25 ). Pds5 meiotic depletion mutants show shorter chromosome axis in budding and fission yeast meiosis and also in mammal spermatogenesis ( 22 , 27 , 28 ). Our current study demonstrates that Pds5 and Rec8 dosage-dependently regulate meiotic chromosome axes in budding yeast.…”

Section: Discussionmentioning

confidence: 99%

“…Pds5, an important cohesin regulator, localizes on chromosome axes during meiotic prophase I ( 22 , 27 – 29 ). Meiosis-specific depletion of Pds5 during meiosis results in markedly short chromosome axes in budding yeast, fission yeast, and male mouse ( 22 , 27 , 28 ). Currently, the prevailing view is that Pds5 regulates the chromosome axis by modulating cohesin ( 27 , 30 ).…”

Section: Introductionmentioning

confidence: 99%

“…However, whether and how Pds5 works with cohesin to modulate the chromosome axis is poorly understood. Moreover, meiotic depletion of Pds5 results in decreased homolog pairing and recombination frequencies ( 22 , 23 , 27 , 28 ). We are also interested to investigate how Pds5 regulates these processes.…”

Section: Introductionmentioning

confidence: 99%

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Interplay between Pds5 and Rec8 in regulating chromosome axis length and crossover frequency

et al. 2021

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Meiotic chromosomes have a loop/axis architecture, with axis length determining crossover frequency. Meiosis-specific Pds5 depletion mutants have shorter chromosome axes and lower homologous chromosome pairing and recombination frequency. However, it is poorly understood how Pds5 coordinately regulates these processes. In this study, we show that only ~20% of wild-type level of Pds5 is required for homolog pairing and that higher levels of Pds5 dosage-dependently regulate axis length and crossover frequency. Moderate changes in Pds5 protein levels do not explicitly impair the basic recombination process. Further investigations show that Pds5 does not regulate chromosome axes by altering Rec8 abundance. Conversely, Rec8 regulates chromosome axis length by modulating Pds5. These findings highlight the important role of Pds5 in regulating meiosis and its relationship with Rec8 to regulate chromosome axis length and crossover frequency with implications for evolutionary adaptation.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Interplay between Pds5 and Rec8 in regulating chromosome axis length and crossover frequency

et al. 2021

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“…PDS5A and PDS5B have their unique and redundant functions in the cell cycle, and depletion of both proteins will cause severe defects or cell death [ 75 , 93 , 96 , 182 ]. The redundant function of PDS5A and PDS5B provides a possibility to develop a therapeutic approach by using a synthetic lethal strategy.…”

Section: Cancermentioning

confidence: 99%

PDS5A and PDS5B in Cohesin Function and Human Disease

Zhang

Coutinho

Pati

2021

IJMS

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Precocious dissociation of sisters 5 (PDS5) is an associate protein of cohesin that is conserved from yeast to humans. It acts as a regulator of the cohesin complex and plays important roles in various cellular processes, such as sister chromatid cohesion, DNA damage repair, gene transcription, and DNA replication. Vertebrates have two paralogs of PDS5, PDS5A and PDS5B, which have redundant and unique roles in regulating cohesin functions. Herein, we discuss the molecular characteristics and functions of PDS5, as well as the effects of its mutations in the development of diseases and their relevance for novel therapeutic strategies.

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Learning to tango with four (or more): the molecular basis of adaptation to polyploid meiosis

Bomblies

2022

Plant Reprod

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Polyploidy, which arises from genome duplication, has occurred throughout the history of eukaryotes, though it is especially common in plants. The resulting increased size, heterozygosity, and complexity of the genome can be an evolutionary opportunity, facilitating diversification, adaptation and the evolution of functional novelty. On the other hand, when they first arise, polyploids face a number of challenges, one of the biggest being the meiotic pairing, recombination and segregation of the suddenly more than two copies of each chromosome, which can limit their fertility. Both for developing polyploidy as a crop improvement tool (which holds great promise due to the high and lasting multi-stress resilience of polyploids), as well as for our basic understanding of meiosis and plant evolution, we need to know both the specific nature of the challenges polyploids face, as well as how they can be overcome in evolution. In recent years there has been a dramatic uptick in our understanding of the molecular basis of polyploid adaptations to meiotic challenges, and that is the focus of this review.

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PDS 5 proteins regulate the length of axial elements and telomere integrity during male mouse meiosis

Cited by 24 publications

References 75 publications

Interplay between Pds5 and Rec8 in regulating chromosome axis length and crossover frequency

Interplay between Pds5 and Rec8 in regulating chromosome axis length and crossover frequency

PDS5A and PDS5B in Cohesin Function and Human Disease

Learning to tango with four (or more): the molecular basis of adaptation to polyploid meiosis

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