Your search keyword '"SYNAPTONEMAL COMPLEX"' showing total 1,112 results

1. Centrosome dysfunction associated with somatic expression of the synaptonemal complex protein TEX12

Author

Sandhu, Sumit, Sou, Ieng F, Hunter, Jill E, Salmon, Lucy, Wilson, Caroline L, Perkins, Neil D, Hunter, Neil, Davies, Owen R, and McClurg, Urszula L

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Biological Sciences, Genetics, Cancer, Animals, Cell Cycle Proteins, Cell Line, Tumor, Centrosome, Gene Expression, Humans, Mice, Synaptonemal Complex, Biological sciences, Biomedical and clinical sciences

Abstract

The synaptonemal complex (SC) is a supramolecular protein scaffold that mediates chromosome synapsis and facilitates crossing over during meiosis. In mammals, SC proteins are generally assumed to have no other function. Here, we show that SC protein TEX12 also localises to centrosomes during meiosis independently of chromosome synapsis. In somatic cells, ectopically expressed TEX12 similarly localises to centrosomes, where it is associated with centrosome amplification, a pathology correlated with cancer development. Indeed, TEX12 is identified as a cancer-testis antigen and proliferation of some cancer cells is TEX12-dependent. Moreover, somatic expression of TEX12 is aberrantly activated via retinoic acid signalling, which is commonly disregulated in cancer. Structure-function analysis reveals that phosphorylation of TEX12 on tyrosine 48 is important for centrosome amplification but not for recruitment of TEX12 to centrosomes. We conclude that TEX12 normally localises to meiotic centrosomes, but its misexpression in somatic cells can contribute to pathological amplification and dysfunction of centrosomes in cancers.

Published

2021

2. BRUCE preserves genomic stability in the male germline of mice

Author

Che, Lixiao, Alavattam, Kris G, Stambrook, Peter J, Namekawa, Satoshi H, and Du, Chunying

Subjects

Genetics, Human Genome, Contraception/Reproduction, Aetiology, Underpinning research, 1.1 Normal biological development and functioning, 2.1 Biological and endogenous factors, Animals, Ataxia Telangiectasia Mutated Proteins, BRCA1 Protein, Cell Cycle Proteins, Chromosome Breakage, Chromosomes, Mammalian, DNA Breaks, Double-Stranded, DNA Repair, DNA-Binding Proteins, Genomic Instability, Germ Cells, Inhibitor of Apoptosis Proteins, Male, Meiosis, Mice, Inbred C57BL, Mice, Knockout, Signal Transduction, Spermatocytes, Spermatogenesis, Synaptonemal Complex, Tamoxifen, Testis, Biological Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology

Abstract

BRUCE is a DNA damage response protein that promotes the activation of ATM and ATR for homologous recombination (HR) repair in somatic cells, making BRUCE a key protector of genomic stability. Preservation of genomic stability in the germline is essential for the maintenance of species. Here, we show that BRUCE is required for the preservation of genomic stability in the male germline of mice, specifically in spermatogonia and spermatocytes. Conditional knockout of Bruce in the male germline leads to profound defects in spermatogenesis, including impaired maintenance of spermatogonia and increased chromosomal anomalies during meiosis. Bruce-deficient pachytene spermatocytes frequently displayed persistent DNA breaks. Homologous synapsis was impaired, and nonhomologous associations and rearrangements were apparent in up to 10% of Bruce-deficient spermatocytes. Genomic instability was apparent in the form of chromosomal fragmentation, translocations, and synapsed quadrivalents and hexavalents. In addition, unsynapsed regions of rearranged autosomes were devoid of ATM and ATR signaling, suggesting an impairment in the ATM- and ATR-dependent DNA damage response of meiotic HR. Taken together, our study unveils crucial functions for BRUCE in the maintenance of spermatogonia and in the regulation of meiotic HR-functions that preserve the genomic stability of the male germline.

Published

2020

3. Preparation of Meiotic Chromosome Spreads from Zebrafish Spermatocytes.

Author

Blokhina, Yana P, Olaya, Ivan, and Burgess, Sean M

Subjects

Testis, Spermatocytes, Chromosomes, Chromatin, Animals, Zebrafish, Fluorescent Antibody Technique, In Situ Hybridization, Fluorescence, Chromosome Segregation, Chromosome Pairing, Meiosis, Male, Genetics, Issue 157, meiosis, zebrafish, testis, chromosome spreads, synaptonemal complex, telomeres, PNA probes, hybridization, immunofluorescence microscopy, super-resolution microscopy, antibody staining, fluorescence in situ hybridization, FISH, Biochemistry and Cell Biology, Psychology, Cognitive Sciences

Abstract

Meiosis is the key cellular process required to create haploid gametes for sexual reproduction. Model organisms have been instrumental in understanding the chromosome events that take place during meiotic prophase, including the pairing, synapsis, and recombination events that ensure proper chromosome segregation. While the mouse has been an important model for understanding the molecular mechanisms underlying these processes, not all meiotic events in this system are analogous to human meiosis. We recently demonstrated the exciting potential of the zebrafish as a model of human spermatogenesis. Here we describe, in detail, our methods to visualize meiotic chromosomes and associated proteins in chromosome spread preparations. These preparations have the advantage of allowing high resolution analysis of chromosome structures. First, we describe the procedure for dissecting testes from adult zebrafish, followed by cell dissociation, lysis, and spreading of the chromosomes. Next, we describe the procedure for detecting the localization of meiotic chromosome proteins, by immunofluorescence detection, and nucleic acid sequences, by fluorescence in situ hybridization (FISH). These techniques comprise a useful set of tools for the cytological analysis of meiotic chromatin architecture in the zebrafish system. Researchers in the zebrafish community should be able to quickly master these techniques and incorporate them into their standard analyses of reproductive function.

Published

2020

4. Phosphoregulation of HORMA domain protein HIM-3 promotes asymmetric synaptonemal complex disassembly in meiotic prophase in Caenorhabditis elegans

Author

Sato-Carlton, Aya, Nakamura-Tabuchi, Chihiro, Li, Xuan, Boog, Hendrik, Lehmer, Madison K, Rosenberg, Scott C, Barroso, Consuelo, Martinez-Perez, Enrique, Corbett, Kevin D, and Carlton, Peter Mark

Subjects

Biochemistry and Cell Biology, Biological Sciences, Genetics, Underpinning research, 1.1 Normal biological development and functioning, Generic health relevance, Animals, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Cell Cycle Proteins, Chromosomal Proteins, Non-Histone, Chromosome Pairing, Chromosome Segregation, Chromosomes, Meiosis, Phosphorylation, Prophase, Protein Domains, Synaptonemal Complex, Developmental Biology

Abstract

In the two cell divisions of meiosis, diploid genomes are reduced into complementary haploid sets through the discrete, two-step removal of chromosome cohesion, a task carried out in most eukaryotes by protecting cohesion at the centromere until the second division. In eukaryotes without defined centromeres, however, alternative strategies have been innovated. The best-understood of these is found in the nematode Caenorhabditis elegans: after the single off-center crossover divides the chromosome into two segments, or arms, several chromosome-associated proteins or post-translational modifications become specifically partitioned to either the shorter or longer arm, where they promote the correct timing of cohesion loss through as-yet unknown mechanisms. Here, we investigate the meiotic axis HORMA-domain protein HIM-3 and show that it becomes phosphorylated at its C-terminus, within the conserved "closure motif" region bound by the related HORMA-domain proteins HTP-1 and HTP-2. Binding of HTP-2 is abrogated by phosphorylation of the closure motif in in vitro assays, strongly suggesting that in vivo phosphorylation of HIM-3 likely modulates the hierarchical structure of the chromosome axis. Phosphorylation of HIM-3 only occurs on synapsed chromosomes, and similarly to other previously-described phosphorylated proteins of the synaptonemal complex, becomes restricted to the short arm after designation of crossover sites. Regulation of HIM-3 phosphorylation status is required for timely disassembly of synaptonemal complex central elements from the long arm, and is also required for proper timing of HTP-1 and HTP-2 dissociation from the short arm. Phosphorylation of HIM-3 thus plays a role in establishing the identity of short and long arms, thereby contributing to the robustness of the two-step chromosome segregation.

Published

2020

5. Molecular organization of mammalian meiotic chromosome axis revealed by expansion STORM microscopy

Author

Xu, Huizhong, Tong, Zhisong, Ye, Qing, Sun, Tengqian, Hong, Zhenmin, Zhang, Lunfeng, Bortnick, Alexandra, Cho, Sunglim, Beuzer, Paolo, Axelrod, Joshua, Hu, Qiongzheng, Wang, Melissa, Evans, Sylvia M, Murre, Cornelis, Lu, Li-Fan, Sun, Sha, Corbett, Kevin D, and Cang, Hu

Subjects

Genetics, Underpinning research, 1.1 Normal biological development and functioning, Generic health relevance, Animals, Cell Cycle Proteins, Chromosomes, Mammalian, DNA-Binding Proteins, Male, Mammals, Meiosis, Mice, Microscopy, Spermatocytes, Staining and Labeling, Synaptonemal Complex, synaptonemal complex, meiosis, chromosome axis, expansion microscopy, STORM

Abstract

During prophase I of meiosis, chromosomes become organized as loop arrays around the proteinaceous chromosome axis. As homologous chromosomes physically pair and recombine, the chromosome axis is integrated into the tripartite synaptonemal complex (SC) as this structure's lateral elements (LEs). While the components of the mammalian chromosome axis/LE-including meiosis-specific cohesin complexes, the axial element proteins SYCP3 and SYCP2, and the HORMA domain proteins HORMAD1 and HORMAD2-are known, the molecular organization of these components within the axis is poorly understood. Here, using expansion microscopy coupled with 2-color stochastic optical reconstruction microscopy (STORM) imaging (ExSTORM), we address these issues in mouse spermatocytes at a resolution of 10 to 20 nm. Our data show that SYCP3 and the SYCP2 C terminus, which are known to form filaments in vitro, form a compact core around which cohesin complexes, HORMADs, and the N terminus of SYCP2 are arrayed. Overall, our study provides a detailed structural view of the meiotic chromosome axis, a key organizational and regulatory component of meiotic chromosomes.

Published

2019

6. Dynamic reorganization of the genome shapes the recombination landscape in meiotic prophase

Author

Patel, Lucas, Kang, Rhea, Rosenberg, Scott C, Qiu, Yunjiang, Raviram, Ramya, Chee, Sora, Hu, Rong, Ren, Bing, Cole, Francesca, and Corbett, Kevin D

Subjects

Biochemistry and Cell Biology, Genetics, Biological Sciences, Biotechnology, Human Genome, 1.1 Normal biological development and functioning, Underpinning research, Animals, Chromatin, Chromosome Pairing, Chromosomes, DNA Breaks, Genome, Homologous Recombination, Male, Meiotic Prophase I, Mice, Mice, Inbred C57BL, Spermatocytes, Spermatogenesis, Synaptonemal Complex, Chemical Sciences, Medical and Health Sciences, Biophysics, Developmental Biology, Biological sciences, Biomedical and clinical sciences, Chemical sciences

Abstract

In meiotic prophase, chromosomes are organized into compacted loop arrays to promote homolog pairing and recombination. Here, we probe the architecture of the mouse spermatocyte genome in early and late meiotic prophase using chromosome conformation capture (Hi-C). Our data support the established loop array model of meiotic chromosomes, and infer loops averaging 0.8-1.0 megabase pairs (Mb) in early prophase and extending to 1.5-2.0 Mb in late prophase as chromosomes compact and homologs undergo synapsis. Topologically associating domains (TADs) are lost in meiotic prophase, suggesting that assembly of the meiotic chromosome axis alters the activity of chromosome-associated cohesin complexes. While TADs are lost, physically separated A and B compartments are maintained in meiotic prophase. Moreover, meiotic DNA breaks and interhomolog crossovers preferentially form in the gene-dense A compartment, revealing a role for chromatin organization in meiotic recombination. Finally, direct detection of interhomolog contacts genome-wide reveals the structural basis for homolog alignment and juxtaposition by the synaptonemal complex.

Published

2019

7. A conserved filamentous assembly underlies the structure of the meiotic chromosome axis.

Author

West, Alan Mv, Rosenberg, Scott C, Ur, Sarah N, Lehmer, Madison K, Ye, Qiaozhen, Hagemann, Götz, Caballero, Iracema, Usón, Isabel, MacQueen, Amy J, Herzog, Franz, and Corbett, Kevin D

Subjects

Chromosomes, Synaptonemal Complex, Animals, Mice, Saccharomyces cerevisiae, Zygosaccharomyces, Arabidopsis, Cell Cycle Proteins, Saccharomyces cerevisiae Proteins, Nuclear Proteins, Chromosomal Proteins, Non-Histone, Two-Hybrid System Techniques, Protein Interaction Mapping, Meiosis, Recombination, Genetic, Kinetics, Haploidy, Mutation, Synchrotrons, Scattering, Radiation, Mass Spectrometry, DNA Breaks, Double-Stranded, Protein Domains, A. thaliana, HORMAD protein, S. cerevisiae, Zygosaccharomyces rouxii, chromosomes, coiled-coil, gene expression, meiotic chromosome axis, meiotic recombination, molecular biophysics, mouse, structural biology, Biochemistry and Cell Biology

Abstract

The meiotic chromosome axis plays key roles in meiotic chromosome organization and recombination, yet the underlying protein components of this structure are highly diverged. Here, we show that 'axis core proteins' from budding yeast (Red1), mammals (SYCP2/SYCP3), and plants (ASY3/ASY4) are evolutionarily related and play equivalent roles in chromosome axis assembly. We first identify 'closure motifs' in each complex that recruit meiotic HORMADs, the master regulators of meiotic recombination. We next find that axis core proteins form homotetrameric (Red1) or heterotetrameric (SYCP2:SYCP3 and ASY3:ASY4) coiled-coil assemblies that further oligomerize into micron-length filaments. Thus, the meiotic chromosome axis core in fungi, mammals, and plants shares a common molecular architecture, and likely also plays conserved roles in meiotic chromosome axis assembly and recombination control.

Published

2019

8. The tumor suppressor BRCA1-BARD1 complex localizes to the synaptonemal complex and regulates recombination under meiotic dysfunction in Caenorhabditis elegans.

Author

Li, Qianyan, Saito, Takamune T, Martinez-Garcia, Marina, Deshong, Alison J, Nadarajan, Saravanapriah, Lawrence, Katherine S, Checchi, Paula M, Colaiacovo, Monica P, and Engebrecht, JoAnne

Subjects

Germ Cells, Synaptonemal Complex, Embryo, Nonmammalian, Animals, Caenorhabditis elegans, Ubiquitin-Protein Ligases, Caenorhabditis elegans Proteins, Tumor Suppressor Proteins, BRCA1 Protein, Recombinant Fusion Proteins, Meiosis, DNA Replication, Recombination, Genetic, Protein Transport, Alleles, Genes, Reporter, Rad51 Recombinase, Embryo, Nonmammalian, Recombination, Genetic, Genes, Reporter, Developmental Biology, Genetics

Abstract

Breast cancer susceptibility gene 1 (BRCA1) and binding partner BRCA1-associated RING domain protein 1 (BARD1) form an essential E3 ubiquitin ligase important for DNA damage repair and homologous recombination. The Caenorhabditis elegans orthologs, BRC-1 and BRD-1, also function in DNA damage repair, homologous recombination, as well as in meiosis. Using functional GFP fusions we show that in mitotically-dividing germ cells BRC-1 and BRD-1 are nucleoplasmic with enrichment at foci that partially overlap with the recombinase RAD-51. Co-localization with RAD-51 is enhanced under replication stress. As cells enter meiosis, BRC-1-BRD-1 remains nucleoplasmic and in foci, and beginning in mid-pachytene the complex co-localizes with the synaptonemal complex. Following establishment of the single asymmetrically positioned crossover on each chromosome pair, BRC-1-BRD-1 concentrates to the short arm of the bivalent. Localization dependencies reveal that BRC-1 and BRD-1 are interdependent and the complex fails to properly localize in both meiotic recombination and chromosome synapsis mutants. Consistent with a role for BRC-1-BRD-1 in meiotic recombination in the context of the synaptonemal complex, inactivation of BRC-1 or BRD-1 enhances the embryonic lethality of mutants defective in chromosome synapsis. Our data suggest that under meiotic dysfunction, BRC-1-BRD-1 stabilizes the RAD-51 filament and alters the recombination landscape; these two functions can be genetically separated from BRC-1-BRD-1's role in the DNA damage response. Together, we propose that BRC-1-BRD-1 serves a checkpoint function at the synaptonemal complex where it monitors and modulates meiotic recombination.

Published

2018

9. Shugoshin Is Essential for Meiotic Prophase Checkpoints in C. elegans

Author

Bohr, Tisha, Nelson, Christian R, Giacopazzi, Stefani, Lamelza, Piero, and Bhalla, Needhi

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Biotechnology, Genetics, Underpinning research, 1.1 Normal biological development and functioning, Generic health relevance, Animals, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Cell Cycle Checkpoints, Cell Cycle Proteins, Chromosomal Proteins, Non-Histone, Chromosome Segregation, Meiosis, Prophase, Synaptonemal Complex, DNA damage response, HORMADs, checkpoint, chromosome axis, cohesin, homologous chromosome, meiosis, recombination, synapsis, Medical and Health Sciences, Psychology and Cognitive Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences, Psychology

Abstract

The conserved factor Shugoshin is dispensable in C. elegans for the two-step loss of sister chromatid cohesion that directs the proper segregation of meiotic chromosomes. We show that the C. elegans ortholog of Shugoshin, SGO-1, is required for checkpoint activity in meiotic prophase. This role in checkpoint function is similar to that of conserved proteins that structure meiotic chromosome axes. Indeed, null sgo-1 mutants exhibit additional phenotypes similar to that of a partial loss-of-function allele of the axis component, HTP-3: premature synaptonemal complex disassembly, the activation of alternate DNA repair pathways, and an inability to recruit a conserved effector of the DNA damage pathway, HUS-1. SGO-1 localizes to pre-meiotic nuclei when HTP-3 is present but not yet loaded onto chromosome axes and genetically interacts with a central component of the cohesin complex, SMC-3, suggesting that it contributes to meiotic chromosome metabolism early in meiosis by regulating cohesin. We propose that SGO-1 acts during pre-meiotic replication to ensure fully functional meiotic chromosome architecture, rendering these chromosomes competent for checkpoint activity and normal progression of meiotic recombination. Given that most research on Shugoshin has focused on its regulation of sister chromatid cohesion during chromosome segregation, this novel role may be conserved but previously uncharacterized in other organisms. Further, our findings expand the repertoire of Shugoshin's functions beyond coordinating regulatory activities at the centromere.

Published

2018

10. A compartmentalized signaling network mediates crossover control in meiosis.

Author

Zhang, Liangyu, Köhler, Simone, Rillo-Bohn, Regina, and Dernburg, Abby F

Subjects

Synaptonemal Complex, Animals, Caenorhabditis elegans, Signal Transduction, Cell Compartmentation, Chromosome Segregation, Meiosis, Crossing Over, Genetic, C. elegans, RING finger ligase, Turing pattern, cell biology, chromosomes, crossover control, gene expression, homologous recombination, meiosis, synaptonemal Complex, Crossing Over, Genetic, Genetics, 1.1 Normal biological development and functioning, Generic Health Relevance, Biochemistry and Cell Biology

Abstract

During meiosis, each pair of homologous chromosomes typically undergoes at least one crossover (crossover assurance), but these exchanges are strictly limited in number and widely spaced along chromosomes (crossover interference). The molecular basis for this chromosome-wide regulation remains mysterious. A family of meiotic RING finger proteins has been implicated in crossover regulation across eukaryotes. Caenorhabditis elegans expresses four such proteins, of which one (ZHP-3) is known to be required for crossovers. Here we investigate the functions of ZHP-1, ZHP-2, and ZHP-4. We find that all four ZHP proteins, like their homologs in other species, localize to the synaptonemal complex, an unusual, liquid crystalline compartment that assembles between paired homologs. Together they promote accumulation of pro-crossover factors, including ZHP-3 and ZHP-4, at a single recombination intermediate, thereby patterning exchanges along paired chromosomes. These proteins also act at the top of a hierarchical, symmetry-breaking process that enables crossovers to direct accurate chromosome segregation.

Published

2018

11. The synaptonemal complex has liquid crystalline properties and spatially regulates meiotic recombination factors.

Author

Rog, Ofer, Köhler, Simone, and Dernburg, Abby F

Subjects

Chromosomes, Synaptonemal Complex, Animals, Caenorhabditis elegans, Recombinases, Meiosis, Crossing Over, Genetic, Liquid Crystals, C. elegans, D. melanogaster, S. cerevisiae, cell biology, chromosomes, crossover interference, genes, liquid crystals, meiosis, phase transitions, subcellular compartmentalization, synaptonemal complex, Crossing Over, Genetic, Genetics, Generic Health Relevance, Biochemistry and Cell Biology

Abstract

The synaptonemal complex (SC) is a polymer that spans ~100 nm between paired homologous chromosomes during meiosis. Its striated, periodic appearance in electron micrographs led to the idea that transverse filaments within this structure 'crosslink' the axes of homologous chromosomes, stabilizing their pairing. SC proteins can also form polycomplexes, three-dimensional lattices that recapitulate the periodic structure of SCs but do not associate with chromosomes. Here we provide evidence that SCs and polycomplexes contain mobile subunits and that their assembly is promoted by weak hydrophobic interactions, indicative of a liquid crystalline phase. We further show that in the absence of recombination intermediates, polycomplexes recapitulate the dynamic localization of pro-crossover factors during meiotic progression, revealing how the SC might act as a conduit to regulate chromosome-wide crossover distribution. Properties unique to liquid crystals likely enable long-range signal transduction along meiotic chromosomes and underlie the rapid evolution of SC proteins.

Published

2017

12. Synaptonemal Complex Components Are Required for Meiotic Checkpoint Function in Caenorhabditis elegans

Author

Bohr, Tisha, Ashley, Guinevere, Eggleston, Evan, Firestone, Kyra, and Bhalla, Needhi

Subjects

Biochemistry and Cell Biology, Biological Sciences, Genetics, 1.1 Normal biological development and functioning, Underpinning research, Animals, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Cell Cycle Proteins, Chromosomal Proteins, Non-Histone, Chromosome Pairing, Meiosis, Mutation, Synaptonemal Complex, meiosis, synapsis, chromosome, checkpoint, synaptonemal complex, Developmental Biology, Biochemistry and cell biology

Abstract

Synapsis involves the assembly of a proteinaceous structure, the synaptonemal complex (SC), between paired homologous chromosomes, and is essential for proper meiotic chromosome segregation. In Caenorhabditis elegans, the synapsis checkpoint selectively removes nuclei with unsynapsed chromosomes by inducing apoptosis. This checkpoint depends on pairing centers (PCs), cis-acting sites that promote pairing and synapsis. We have hypothesized that the stability of homolog pairing at PCs is monitored by this checkpoint. Here, we report that SC components SYP-3, HTP-3, HIM-3, and HTP-1 are required for a functional synapsis checkpoint. Mutation of these components does not abolish PC function, demonstrating they are bona fide checkpoint components. Further, we identify mutant backgrounds in which the instability of homolog pairing at PCs does not correlate with the synapsis checkpoint response. Altogether, these data suggest that, in addition to homolog pairing, SC assembly may be monitored by the synapsis checkpoint.

Published

2016

13. Ultra-High Resolution 3D Imaging of Whole Cells.

Author

Huang, Fang, Sirinakis, George, Allgeyer, Edward S, Schroeder, Lena K, Duim, Whitney C, Kromann, Emil B, Phan, Thomy, Rivera-Molina, Felix E, Myers, Jordan R, Irnov, Irnov, Lessard, Mark, Zhang, Yongdeng, Handel, Mary Ann, Jacobs-Wagner, Christine, Lusk, C Patrick, Rothman, James E, Toomre, Derek, Booth, Martin J, and Bewersdorf, Joerg

Subjects

Spermatocytes, Synaptonemal Complex, COP-Coated Vesicles, Golgi Apparatus, Animals, Mice, Bacteriophages, Microscopy, Fluorescence, Cytological Techniques, Male, Single Molecule Imaging, Bioengineering, Underpinning research, 1.1 Normal biological development and functioning, 1.5 Resources and infrastructure (underpinning), Generic health relevance, Biological Sciences, Medical and Health Sciences, Developmental Biology

Abstract

Fluorescence nanoscopy, or super-resolution microscopy, has become an important tool in cell biological research. However, because of its usually inferior resolution in the depth direction (50-80 nm) and rapidly deteriorating resolution in thick samples, its practical biological application has been effectively limited to two dimensions and thin samples. Here, we present the development of whole-cell 4Pi single-molecule switching nanoscopy (W-4PiSMSN), an optical nanoscope that allows imaging of three-dimensional (3D) structures at 10- to 20-nm resolution throughout entire mammalian cells. We demonstrate the wide applicability of W-4PiSMSN across diverse research fields by imaging complex molecular architectures ranging from bacteriophages to nuclear pores, cilia, and synaptonemal complexes in large 3D cellular volumes.

Published

2016

14. The Chromosome Axis Controls Meiotic Events through a Hierarchical Assembly of HORMA Domain Proteins

Author

Kim, Yumi, Rosenberg, Scott C, Kugel, Christine L, Kostow, Nora, Rog, Ofer, Davydov, Vitaliy, Su, Tiffany Y, Dernburg, Abby F, and Corbett, Kevin D

Subjects

Underpinning research, 1.1 Normal biological development and functioning, Generic health relevance, Animals, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Cell Cycle Proteins, Chromosome Pairing, Chromosome Segregation, Chromosomes, Meiosis, Mutation, Synaptonemal Complex, Biological Sciences, Medical and Health Sciences, Developmental Biology

Abstract

Proteins of the HORMA domain family play central, but poorly understood, roles in chromosome organization and dynamics during meiosis. In Caenorhabditis elegans, four such proteins (HIM-3, HTP-1, HTP-2, and HTP-3) have distinct but overlapping functions. Through combined biochemical, structural, and in vivo analysis, we find that these proteins form hierarchical complexes through binding of their HORMA domains to cognate peptides within their partners' C-terminal tails, analogous to the "safety belt" binding mechanism of Mad2. These interactions are critical for recruitment of HIM-3, HTP-1, and HTP-2 to chromosome axes. HTP-3, in addition to recruiting the other HORMA domain proteins to the axis, plays an independent role in sister chromatid cohesion and double-strand break formation. Finally, we find that mammalian HORMAD1 binds a motif found both at its own C terminus and at that of HORMAD2, indicating that this mode of intermolecular association is a conserved feature of meiotic chromosome structure in eukaryotes.

Published

2014

15. Antagonistic roles of ubiquitin ligase HEI10 and SUMO ligase RNF212 regulate meiotic recombination

Author

Qiao, Huanyu, Prasada Rao, HBD, Yang, Ye, Fong, Jared H, Cloutier, Jeffrey M, Deacon, Dekker C, Nagel, Kathryn E, Swartz, Rebecca K, Strong, Edward, Holloway, J Kim, Cohen, Paula E, Schimenti, John, Ward, Jeremy, and Hunter, Neil

Subjects

Agricultural, Veterinary and Food Sciences, Biological Sciences, Bioinformatics and Computational Biology, Genetics, Agricultural Biotechnology, Biotechnology, Animals, Cell Cycle Proteins, Crossing Over, Genetic, Electrophoresis, Polyacrylamide Gel, In Situ Nick-End Labeling, Indoles, Ligases, Male, Meiosis, Mice, Mice, Inbred C57BL, SUMO-1 Protein, Spermatocytes, Statistics, Nonparametric, Synaptonemal Complex, Ubiquitin, Ubiquitin-Protein Ligases, Medical and Health Sciences, Developmental Biology, Agricultural biotechnology, Bioinformatics and computational biology

Abstract

Crossover recombination facilitates the accurate segregation of homologous chromosomes during meiosis. In mammals, poorly characterized regulatory processes ensure that every pair of chromosomes obtains at least one crossover, even though most recombination sites yield non-crossovers. Designation of crossovers involves selective localization of the SUMO ligase RNF212 to a minority of recombination sites, where it stabilizes pertinent factors such as MutSγ (ref. 4). Here we show that the ubiquitin ligase HEI10 (also called CCNB1IP1) is essential for this crossover/non-crossover differentiation process. In HEI10-deficient mice, RNF212 localizes to most recombination sites, and dissociation of both RNF212 and MutSγ from chromosomes is blocked. Consequently, recombination is impeded, and crossing over fails. In wild-type mice, HEI10 accumulates at designated crossover sites, suggesting that it also has a late role in implementing crossing over. As with RNF212, dosage sensitivity for HEI10 indicates that it is a limiting factor for crossing over. We suggest that SUMO and ubiquitin have antagonistic roles during meiotic recombination that are balanced to effect differential stabilization of recombination factors at crossover and non-crossover sites.

Published

2014

16. Meiotic chromosome structures constrain and respond to designation of crossover sites.

Author

Libuda, Diana E, Uzawa, Satoru, Meyer, Barbara J, and Villeneuve, Anne M

Subjects

Chromosomes, Synaptonemal Complex, Animals, Caenorhabditis elegans, DNA-Binding Proteins, Caenorhabditis elegans Proteins, Nuclear Proteins, Chromosome Segregation, Chromosome Pairing, Meiosis, Crossing Over, Genetic, DNA Breaks, Double-Stranded, Homologous Recombination, General Science & Technology

Abstract

Crossover recombination events between homologous chromosomes are required to form chiasmata, temporary connections between homologues that ensure their proper segregation at meiosis I. Despite this requirement for crossovers and an excess of the double-strand DNA breaks that are the initiating events for meiotic recombination, most organisms make very few crossovers per chromosome pair. Moreover, crossovers tend to inhibit the formation of other crossovers nearby on the same chromosome pair, a poorly understood phenomenon known as crossover interference. Here we show that the synaptonemal complex, a meiosis-specific structure that assembles between aligned homologous chromosomes, both constrains and is altered by crossover recombination events. Using a cytological marker of crossover sites in Caenorhabditis elegans, we show that partial depletion of the synaptonemal complex central region proteins attenuates crossover interference, increasing crossovers and reducing the effective distance over which interference operates, indicating that synaptonemal complex proteins limit crossovers. Moreover, we show that crossovers are associated with a local 0.4-0.5-micrometre increase in chromosome axis length. We propose that meiotic crossover regulation operates as a self-limiting system in which meiotic chromosome structures establish an environment that promotes crossover formation, which in turn alters chromosome structure to inhibit other crossovers at additional sites.

Published

2013

17. Interplay between synaptonemal complex, homologous recombination, and centromeres during mammalian meiosis.

Author

Qiao, Huanyu, Chen, Jefferson K, Reynolds, April, Höög, Christer, Paddy, Michael, and Hunter, Neil

Subjects

Spermatocytes, Chromosomes, Centromere, Synaptonemal Complex, Animals, Mice, Inbred C57BL, Mice, Endodeoxyribonucleases, Cation Transport Proteins, Nuclear Proteins, Chromosome Pairing, Meiosis, Male, Homologous Recombination, DNA-Binding Proteins, Inbred C57BL, Genetics, Developmental Biology

Abstract

The intimate synapsis of homologous chromosome pairs (homologs) by synaptonemal complexes (SCs) is an essential feature of meiosis. In many organisms, synapsis and homologous recombination are interdependent: recombination promotes SC formation and SCs are required for crossing-over. Moreover, several studies indicate that initiation of SC assembly occurs at sites where crossovers will subsequently form. However, recent analyses in budding yeast and fruit fly imply a special role for centromeres in the initiation of SC formation. In addition, in budding yeast, persistent SC-dependent centromere-association facilitates the disjunction of chromosomes that have failed to become connected by crossovers. Here, we examine the interplay between SCs, recombination, and centromeres in a mammal. In mouse spermatocytes, centromeres do not serve as SC initiation sites and are invariably the last regions to synapse. However, centromeres are refractory to de-synapsis during diplonema and remain associated by short SC fragments. Since SC-dependent centromere association is lost before diakinesis, a direct role in homolog segregation seems unlikely. However, post-SC disassembly, we find evidence of inter-centromeric connections that could play a more direct role in promoting homolog biorientation and disjunction. A second class of persistent SC fragments is shown to be crossover-dependent. Super-resolution structured-illumination microscopy (SIM) reveals that these structures initially connect separate homolog axes and progressively diminish as chiasmata form. Thus, DNA crossing-over (which occurs during pachynema) and axis remodeling appear to be temporally distinct aspects of chiasma formation. SIM analysis of the synapsis and crossover-defective mutant Sycp1⁻/⁻ implies that SCs prevent unregulated fusion of homolog axes. We propose that SC fragments retained during diplonema stabilize nascent bivalents and help orchestrate local chromosome reorganization that promotes centromere and chiasma function.

Published

2012

18. Hormad1 mutation disrupts synaptonemal complex formation, recombination, and chromosome segregation in mammalian meiosis.

Author

Shin, Yong-Hyun, Choi, Youngsok, Erdin, Serpil Uckac, Yatsenko, Svetlana A, Kloc, Malgorzata, Yang, Fang, Wang, P Jeremy, Meistrich, Marvin L, and Rajkovic, Aleksandar

Subjects

Ovary, Oocytes, Spermatozoa, Sex Chromosomes, Synaptonemal Complex, Fetus, Animals, Mice, Aneuploidy, Protein-Serine-Threonine Kinases, Cell Cycle Proteins, DNA-Binding Proteins, Tumor Suppressor Proteins, Nuclear Proteins, RNA, Messenger, Chromosome Segregation, Meiosis, Spermatogenesis, Organ Specificity, Recombination, Genetic, Protein Transport, Phosphorylation, Embryonic Development, Mutation, Female, Male, Ataxia Telangiectasia Mutated Proteins, RNA, Messenger, Recombination, Genetic, Genetics, Developmental Biology

Abstract

Meiosis is unique to germ cells and essential for reproduction. During the first meiotic division, homologous chromosomes pair, recombine, and form chiasmata. The homologues connect via axial elements and numerous transverse filaments to form the synaptonemal complex. The synaptonemal complex is a critical component for chromosome pairing, segregation, and recombination. We previously identified a novel germ cell-specific HORMA domain encoding gene, Hormad1, a member of the synaptonemal complex and a mammalian counterpart to the yeast meiotic HORMA domain protein Hop1. Hormad1 is essential for mammalian gametogenesis as knockout male and female mice are infertile. Hormad1 deficient (Hormad1(-/) (-)) testes exhibit meiotic arrest in the early pachytene stage, and synaptonemal complexes cannot be visualized by electron microscopy. Hormad1 deficiency does not affect localization of other synaptonemal complex proteins, SYCP2 and SYCP3, but disrupts homologous chromosome pairing. Double stranded break formation and early recombination events are disrupted in Hormad1(-/) (-) testes and ovaries as shown by the drastic decrease in the γH2AX, DMC1, RAD51, and RPA foci. HORMAD1 co-localizes with γH2AX to the sex body during pachytene. BRCA1, ATR, and γH2AX co-localize to the sex body and participate in meiotic sex chromosome inactivation and transcriptional silencing. Hormad1 deficiency abolishes γH2AX, ATR, and BRCA1 localization to the sex chromosomes and causes transcriptional de-repression on the X chromosome. Unlike testes, Hormad1(-/) (-) ovaries have seemingly normal ovarian folliculogenesis after puberty. However, embryos generated from Hormad1(-/) (-) oocytes are hyper- and hypodiploid at the 2 cell and 8 cell stage, and they arrest at the blastocyst stage. HORMAD1 is therefore a critical component of the synaptonemal complex that affects synapsis, recombination, and meiotic sex chromosome inactivation and transcriptional silencing.

Published

2010

19. Identification of chromosome sequence motifs that mediate meiotic pairing and synapsis in C. elegans

Author

Phillips, Carolyn M, Meng, Xiangdong, Zhang, Lei, Chretien, Jacqueline H, Urnov, Fyodor D, and Dernburg, Abby F

Subjects

1.1 Normal biological development and functioning, Underpinning research, Animals, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Cell Cycle Proteins, Chromosomal Proteins, Non-Histone, Chromosome Pairing, Crossing Over, Genetic, Disorders of Sex Development, Female, Genotype, Immunohistochemistry, In Situ Hybridization, Fluorescence, Male, Meiosis, Microscopy, Fluorescence, RNA Interference, SELEX Aptamer Technique, Synaptonemal Complex, X Chromosome, Biological Sciences, Medical and Health Sciences, Developmental Biology

Abstract

Caenorhabditis elegans chromosomes contain specialized regions called pairing centres, which mediate homologous pairing and synapsis during meiosis. Four related proteins, ZIM-1, 2, 3 and HIM-8, associate with these sites and are required for their essential functions. Here we show that short sequence elements enriched in the corresponding chromosome regions selectively recruit these proteins in vivo. In vitro analysis using SELEX indicates that the binding specificity of each protein arises from a combination of two zinc fingers and an adjacent domain. Insertion of a cluster of recruiting motifs into a chromosome lacking its endogenous pairing centre is sufficient to restore homologous pairing, synapsis, crossover recombination and segregation. These findings help to illuminate how chromosome sites mediate essential aspects of meiotic chromosome dynamics.

Published

2009

20. ZHP-3 acts at crossovers to couple meiotic recombination with synaptonemal complex disassembly and bivalent formation in C. elegans.

Author

Bhalla, Needhi, Wynne, David, Jantsch, Verena, and Dernburg, Abby

Subjects

Animals, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Chromosomal Proteins, Non-Histone, Chromosome Segregation, Chromosomes, Crossing Over, Genetic, Meiosis, Synaptonemal Complex

Abstract

Crossover recombination and the formation of chiasmata normally ensure the proper segregation of homologous chromosomes during the first meiotic division. zhp-3, the Caenorhabditis elegans ortholog of the budding yeast ZIP3 gene, is required for crossover recombination. We show that ZHP-3 protein localization is highly dynamic. At a key transition point in meiotic prophase, the protein shifts from along the length of the synaptonemal complex (SC) to an asymmetric localization on the SC and eventually becomes restricted to foci that mark crossover recombination events. A zhp-3::gfp transgene partially complements a null mutation and reveals a separation of function; although the fusion protein can promote nearly wild-type levels of recombination, aneuploidy among the progeny is high, indicating defects in meiotic chromosome segregation. The structure of bivalents is perturbed in this mutant, suggesting that the chromosome segregation defect results from an inability to properly remodel chromosomes in response to crossovers. smo-1 mutants exhibit phenotypes similar to zhp-3::gfp mutants at higher temperatures, and smo-1; zhp-3::gfp double mutants exhibit more severe meiotic defects than either single mutant, consistent with a role for SUMO in the process of SC disassembly and bivalent differentiation. We propose that coordination of crossover recombination with SC disassembly and bivalent formation reflects a conserved role of Zip3/ZHP-3 in coupling recombination with SC morphogenesis.

Published

2008

21. Premeiotic pairing of homologous chromosomes during

Author

Thomas, Rubin, Nicolas, Macaisne, Ana Maria, Vallés, Clara, Guilleman, Isabelle, Gaugué, Laurine, Dal Toe, and Jean-René, Huynh

Subjects

Male, Chromosome Pairing, Meiosis, Synaptonemal Complex, Chromosome Segregation, Centromere, Animals, Female, Drosophila, Chromosomes

Abstract

In the early stages of meiosis, maternal and paternal chromosomes pair with their homologous partner and recombine to ensure exchange of genetic information and proper segregation. These events can vary drastically between species and between males and females of the same species. In

Published

2023

22. Heterologous synapsis in C. elegans is regulated by meiotic double-strand breaks and crossovers

Author

Hanwenheng Liu, Ofer Rog, and Spencer G. Gordon

Subjects

Synaptonemal Complex, Synapsis, Chromosome, Heterologous, Biology, Article, Cell biology, Chromosome Pairing, Meiosis, Synaptonemal complex, Prophase, Synapses, Genetics, Homologous chromosome, Animals, Crossing Over, Genetic, Caenorhabditis elegans, Developmental biology, Genetics (clinical)

Abstract

Alignment of the parental chromosomes during meiotic prophase is key to the formation of genetic exchanges, or crossovers, and consequently to the successful production of gametes. In almost all studied organisms, alignment involves synapsis: the assembly of a conserved inter-chromosomal interface called the synaptonemal complex (SC). While the SC usually synapses homologous sequences, it can assemble between heterologous sequences. However, little is known about the regulation of heterologous synapsis. Here, we study the dynamics of heterologous synapsis in the nematode C. elegans. We characterize two experimental scenarios: SC assembly onto a folded-back chromosome that cannot pair with its homologous partner; and synapsis of pseudo-homologs, a fusion chromosome partnering with an unfused chromosome half its size. We observed elevated levels of heterologous synapsis when the number of meiotic double-strand breaks or crossovers were reduced, indicating that the promiscuity of synapsis is regulated by break formation or repair. In addition, our data suggests the existence of both chromosome-specific and nucleus-wide regulation on heterologous synapsis.

Published

2021

23. Super-Resolution Microscopy of the Synaptonemal Complex within the Caenorhabditis elegans Germline

Author

Ivana, Čavka, Rory M, Power, Dietrich, Walsh, Timo, Zimmermann, and Simone, Köhler

Subjects

Meiosis, Microscopy, Germ Cells, Synaptonemal Complex, Animals, Caenorhabditis elegans

Abstract

During meiosis, homologous chromosomes must recognize and adhere to one another to allow for their correct segregation. One of the key events that secures the interaction of homologous chromosomes is the assembly of the synaptonemal complex (SC) in meiotic prophase I. Even though there is little sequence homology between protein components within the SC among different species, the general structure of the SC has been highly conserved during evolution. In electron micrographs, the SC appears as a tripartite, ladder-like structure composed of lateral elements or axes, transverse filaments, and a central element. However, precisely identifying the localization of individual components within the complex by electron microscopy to determine the molecular structure of the SC remains challenging. By contrast, fluorescence microscopy allows for the identification of individual protein components within the complex. However, since the SC is only ~100 nm wide, its substructure cannot be resolved by diffraction-limited conventional fluorescence microscopy. Thus, determining the molecular architecture of the SC requires super-resolution light microscopy techniques such as structured illumination microscopy (SIM), stimulated-emission depletion (STED) microscopy, or single-molecule localization microscopy (SMLM). To maintain the structure and interactions of individual components within the SC, it is important to observe the complex in an environment that is close to its native environment in the germ cells. Therefore, we demonstrate an immunohistochemistry and imaging protocol that enables the study of the substructure of the SC in intact, extruded Caenorhabditis elegans germline tissue with SMLM and STED microscopy. Directly fixing the tissue to the coverslip reduces the movement of the samples during imaging and minimizes aberrations in the sample to achieve the high resolution necessary to visualize the substructure of the SC in its biological context.

Published

2022

24. ESA1 regulates meiotic chromosome axis and crossover frequency via acetylating histone H4

Author

Taicong Tan, Binyuan Zhai, Tingting Chu, Xiao Yang, Liangran Zhang, Yingjin Tan, Meihui Song, Shuxian Zhang, Shunxin Wang, Jiaming Zhang, Xuan Yang, and Ying Wang

Subjects

Saccharomyces cerevisiae Proteins, AcademicSubjects/SCI00010, Cell Cycle Proteins, Saccharomyces cerevisiae, Genome Integrity, Repair and Replication, Biology, Interference (genetic), Histones, Histone H4, Chromosome segregation, Meiosis, Chromosome Segregation, Genetics, Animals, DNA Breaks, Double-Stranded, Crossing Over, Genetic, Caenorhabditis elegans, Homologous Recombination, Histone Acetyltransferases, Synaptonemal Complex, Synapsis, Acetylation, Spores, Fungal, Chromatin, Cell biology, Chromosome Pairing, Histone, biology.protein, Homologous recombination

Abstract

Meiotic recombination is integrated into and regulated by meiotic chromosomes, which is organized as loop/axis architecture. However, the regulation of chromosome organization is poorly understood. Here, we show Esa1, the NuA4 complex catalytic subunit, is constitutively expressed and localizes on chromatin loops during meiosis. Esa1 plays multiple roles including homolog synapsis, sporulation efficiency, spore viability, and chromosome segregation in meiosis. Detailed analyses show the meiosis-specific depletion of Esa1 results in decreased chromosome axis length independent of another axis length regulator Pds5, which further leads to a decreased number of Mer2 foci, and consequently a decreased number of DNA double-strand breaks, recombination intermediates, and crossover frequency. However, Esa1 depletion does not impair the occurrence of the obligatory crossover required for faithful chromosome segregation, or the strength of crossover interference. Further investigations demonstrate Esa1 regulates chromosome axis length via acetylating the N-terminal tail of histone H4 but not altering transcription program. Therefore, we firstly show a non-chromosome axis component, Esa1, acetylates histone H4 on chromatin loops to regulate chromosome axis length and consequently recombination frequency but does not affect the basic meiotic recombination process. Additionally, Esa1 depletion downregulates middle induced meiotic genes, which probably causing defects in sporulation and chromosome segregation.

Published

2021

25. Targeting Polo-like kinase in space and time during C. elegans meiosis

Author

James N. Brandt and Yumi Kim

Subjects

chromosome dynamics, Review, Polo-like kinase, Protein Serine-Threonine Kinases, Biology, Chromosomes, Prophase, Meiosis, Animals, Meiotic Prophase I, Phosphorylation, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Molecular Biology, meiotic prophase, Binding Sites, c. elegans, Synapsis, Chromosome, Cell Biology, Cell biology, Chromosome Pairing, Synaptonemal complex, Gene Expression Regulation, Pairing, Homologous recombination, Protein Binding, Signal Transduction, Developmental Biology

Abstract

A central player in meiotic chromosome dynamics is the conserved Polo-like kinase (PLK) family. PLKs are dynamically localized to distinct structures during meiotic prophase and phosphorylate a diverse group of substrates to control homolog pairing, synapsis, and meiotic recombination. In a recent study, we uncovered the mechanisms that control the targeting of a meiosis-specific PLK-2 in C. elegans. In early meiotic prophase, PLK-2 localizes to special chromosome regions known as pairing centers and drives homolog pairing and synapsis. PLK-2 then relocates to the synaptonemal complex (SC) after crossover designation and mediates chromosome remodeling required for homolog separation. What controls this intricate targeting of PLK-2 in space and time? We discuss recent findings and remaining questions for the future.

Published

2021

26. Multi-color dSTORM microscopy in Hormad1-/spermatocytes reveals alterations in meiotic recombination intermediates and synaptonemal complex structure

Author

Lieke Koornneef, Johan A. Slotman, Esther Sleddens-Linkels, Wiggert A. van Cappellen, Marco Barchi, Attila Tóth, Joost Gribnau, Adriaan B. Houtsmuller, Willy M. Baarends, Developmental Biology, Erasmus MC other, Cell biology, and Pathology

Subjects

Male, Mice, Knockout, Cancer Research, Microscopy, Settore BIO/16, Synaptonemal Complex, Knockout, Cell Cycle Proteins, DNA, Recombinases, Meiosis, Mice, SDG 3 - Good Health and Well-being, Spermatocytes, Genetics, Animals, Rad51 Recombinase, Molecular Biology, Genetics (clinical), Ecology, Evolution, Behavior and Systematics

Abstract

Recombinases RAD51 and its meiosis-specific paralog DMC1 accumulate on single-stranded DNA (ssDNA) of programmed DNA double strand breaks (DSBs) in meiosis. Here we used three-color dSTORM microscopy, and a mouse model with severe defects in meiotic DSB formation and synapsis (Hormad1-/-) to obtain more insight in the recombinase accumulation patterns in relation to repair progression. First, we used the known reduction in meiotic DSB frequency in Hormad1-/- spermatocytes to be able to conclude that the RAD51/DMC1 nanofoci that preferentially localize at distances of ~300 nm form within a single DSB site, whereas a second preferred distance of ~900 nm, observed only in wild type, represents inter-DSB distance. Next, we asked whether the proposed role of HORMAD1 in repair inhibition affects the RAD51/DMC1 accumulation patterns. We observed that the two most frequent recombinase configurations (1 DMC1 and 1 RAD51 nanofocus (D1R1), and D2R1) display coupled frequency dynamics over time in wild type, but were constant in the Hormad1-/- model, indicating that the lifetime of these intermediates was altered. Recombinase nanofoci were also smaller in Hormad1-/- spermatocytes, consistent with changes in ssDNA length or protein accumulation. Furthermore, we established that upon synapsis, recombinase nanofoci localized closer to the synaptonemal complex (SYCP3), in both wild type and Hormad1-/- spermatocytes. Finally, the data also revealed a hitherto unknown function of HORMAD1 in inhibiting coil formation in the synaptonemal complex. SPO11 plays a similar but weaker role in coiling and SYCP1 had the opposite effect. Using this large super-resolution dataset, we propose models with the D1R1 configuration representing one DSB end containing recombinases, and the other end bound by other ssDNA binding proteins, or both ends loaded by the two recombinases, but in below-resolution proximity. This may then often evolve into D2R1, then D1R2, and finally back to D1R1, when DNA synthesis has commenced.

Published

2022

27. Synaptonemal complex proteins modulate the level of genome integrity in cancers

Author

Noriko Hosoya and Kiyoshi Miyagawa

Subjects

0301 basic medicine, Genome instability, Cancer Research, Genome integrity, Somatic cell, nuclear microenvironment, synaptonemal complex protein, Cell Cycle Proteins, homologous recombination, Review Article, Biology, DNA damage response, Genomic Instability, Epigenesis, Genetic, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Meiosis, Neoplasms, Animals, Humans, DNA Breaks, Double-Stranded, Review Articles, Synaptonemal Complex, Nuclear Proteins, Recombinational DNA Repair, General Medicine, Cell biology, DNA-Binding Proteins, Synaptonemal complex, 030104 developmental biology, Oncology, chemistry, 030220 oncology & carcinogenesis, Models, Animal, cancer therapy, Ectopic expression, Homologous recombination, DNA

Abstract

The synaptonemal complex (SC) is a proteinaceous structure that is transiently formed during meiosis to promote homologous recombination between maternal and paternal chromosomes. As this structure is required only for meiotic recombination, the proteins constituting the complex are almost undetectable in normal somatic cells, but they can be expressed under the conditions in which the transcriptional machinery is deregulated. Accumulating evidence indicates that they are epigenetically expressed in cancers of various origin. Not surprisingly, in contrast to their meiotic roles, the somatic roles of the SC proteins remain to be investigated. However, it has recently been reported that SYCP3 and SYCE2 control DNA double‐strand break repair negatively and positively, respectively, suggesting that the ectopic expression of the SC proteins in somatic cells could be associated with the maintenance of genomic instability. Thus, it is highly likely that the investigation of the somatic roles of the SC proteins would improve our understanding of the mechanisms underlying tumor development., The synaptonemal complex (SC) is a proteinaceous structure that is transiently formed during meiosis to promote homologous recombination. Although the proteins constituting the complex are highly expressed in meiotic cells and almost undetectable in normal somatic cells, accumulating evidence indicates that they are epigenetically expressed in cancers of various origin. Recent studies report that the SC proteins regulate the endogenous cellular machinery that maintains genome integrity in somatic cells. In this review, we focus on the clinical significance of the SC proteins and the possible mechanism underlying their ectopic expression in human cancers.

Published

2021

28. Meiotic synapsis of homeologous chromosomes and mismatch repair protein detection in the parthenogenetic rock lizard Darevskia unisexualis

Author

Varos G. Petrosyan, Victor Spangenberg, Marine Arakelyan, Marcelo de Bello Cioffi, Elena Martynova, A.N. Bogomazova, Thomas Liehr, Fedor A. Osipov, Eduard A. Galoyan, I. A. Martirosyan, Ahmed Al-Rikabi, and Oxana Kolomiets

Subjects

0301 basic medicine, Parthenogenesis, Robertsonian translocation, Biology, medicine.disease_cause, DNA Mismatch Repair, 03 medical and health sciences, Meiotic Prophase I, 0302 clinical medicine, Meiosis, Genetics, medicine, Animals, Cells, Cultured, Gene Rearrangement, 030219 obstetrics & reproductive medicine, Synaptonemal Complex, Synapsis, Chromosome, Lizards, Karyotype, Cell Biology, Synaptonemal complex, 030104 developmental biology, Evolutionary biology, Ploidy, MutL Protein Homolog 1, Developmental Biology

Abstract

Parthenogenetic species of Caucasian rock lizards of the genus Darevksia are important evidence for reticulate evolution and speciation by hybridization in vertebrates. Female-only lineages formed through interspecific hybridization have been discovered in many groups. Nevertheless, critical mechanisms of oogenesis and specifics of meiosis that provide long-term stability of parthenogenetic species are still unknown. Here we report cytogenetic characteristics of somatic karyotypes and meiotic prophase I nuclei in the diploid parthenogenetic species Darevskia unisexualis from the new population "Keti" in Armenia which contains an odd number of chromosomes 2n = 37, instead of the usual 2n = 38. We revealed 36 acrocentric chromosomes and a single metacentric autosomal chromosome, resulting from Robertsonian translocation. Comparative genomic hybridization revealed that chromosome fusion occurred between two chromosomes inherited from the maternal species, similar to another parthenogenetic species D. rostombekowi. To trace the chromosome behaviour in meiosis, we performed an immunocytochemical study of primary oocytes' spread nuclei and studied chromosome synapsis during meiotic prophase I in D. unisexualis based on analysis of synaptonemal complexes (SCs). We found meiotic SC-trivalent composed of one metacentric and two acrocentric chromosomes. We confirmed that the SC was assembled between homeologous chromosomes inherited from two parental species. Immunostaining of the pachytene and diplotene nuclei revealed a mismatch repair protein MLH1 loaded to all autosomal SC bivalents. Possible mechanisms of meiotic recombination between homeologous chromosomes are discussed.

Published

2021

29. EWSR1 affects PRDM9-dependent histone 3 methylation and provides a link between recombination hotspots and the chromosome axis protein REC8

Author

Petko M. Petkov, Hui Tian, and Timothy Billings

Subjects

Male, DNA Repair, Chromosomal Proteins, Non-Histone, Regulator, Cell Cycle Proteins, Biology, Methylation, Histones, 03 medical and health sciences, 0302 clinical medicine, Meiosis, Animals, DNA Breaks, Double-Stranded, Crossing Over, Genetic, Molecular Biology, PRDM9, 030304 developmental biology, Mice, Knockout, Recombination, Genetic, 0303 health sciences, Cohesin, Synaptonemal Complex, Cell Cycle, Chromosome, DNA, Histone-Lysine N-Methyltransferase, Articles, Cell Biology, Chromosomes, Mammalian, Spermatozoa, Cell biology, Histone, biology.protein, Protein Multimerization, RNA-Binding Protein EWS, 030217 neurology & neurosurgery, Recombination, Protein Binding

Abstract

Meiotic recombination in most mammals requires recombination hotspot activation through the action of the histone 3 Lys-4 and Lys-36 methyltransferase PRDM9 to ensure successful double-strand-break initiation and repair. Here we show that EWSR1, a protein whose role in meiosis was not previously clarified in detail, binds to both PRDM9 and pREC8, a phosphorylated meiosis-specific cohesin, in male meiotic cells. We created a Ewsr1 conditional knockout mouse model to deplete EWSR1 before the onset of meiosis and found that absence of EWSR1 causes meiotic arrest with decreased histone trimethylation at meiotic hotspots, impaired DNA double-strand-break repair, and reduced crossover number. Our results demonstrate that EWSR1 is essential for promoting PRDM9-dependent histone methylation and normal meiotic progress, possibly by facilitating the linking between PRDM9-bound hotspots and the nascent chromosome axis through its component cohesin pREC8.

Published

2021

30. Robust designation of meiotic crossover sites by CDK-2 through phosphorylation of the MutSγ complex

Author

Jocelyn Haversat, Alexander Woglar, Kayla Klatt, Chantal C. Akerib, Victoria Roberts, Shin-Yu Chen, Swathi Arur, Anne M. Villeneuve, and Yumi Kim

Subjects

DNA-Binding Proteins, Meiosis, Multidisciplinary, Synaptonemal Complex, Chromosome Segregation, Cyclin-Dependent Kinase 2, Animals, Crossing Over, Genetic, Phosphorylation, Caenorhabditis elegans, Caenorhabditis elegans Proteins

Abstract

Crossover formation is essential for proper segregation of homologous chromosomes during meiosis. Here, we show that Caenorhabditis elegans cyclin-dependent kinase 2 (CDK-2) partners with cyclin-like protein COSA-1 to promote crossover formation by promoting conversion of meiotic double-strand breaks into crossover–specific recombination intermediates. Further, we identify MutSγ component MSH-5 as a CDK-2 phosphorylation target. MSH-5 has a disordered C-terminal tail that contains 13 potential CDK phosphosites and is required to concentrate crossover–promoting proteins at recombination sites. Phosphorylation of the MSH-5 tail appears dispensable in a wild-type background, but when MutSγ activity is partially compromised, crossover formation and retention of COSA-1 at recombination sites are exquisitely sensitive to phosphosite loss. Our data support a model in which robustness of crossover designation reflects a positive feedback mechanism involving CDK-2–mediated phosphorylation and scaffold-like properties of the MSH5 C-terminal tail, features that combine to promote full recruitment and activity of crossover–promoting complexes.

Published

2022

31. PLK1 depletion alters homologous recombination and synaptonemal complex disassembly events during mammalian spermatogenesis

Author

Stephen R, Wellard, Marnie W, Skinner, Xueqi, Zhao, Chris, Shults, and Philip W, Jordan

Subjects

Male, Mammals, Synaptonemal Complex, Cell Cycle Proteins, DNA, Cell Biology, Protein Serine-Threonine Kinases, Chromosome Pairing, Meiosis, Mice, Proto-Oncogene Proteins, Animals, Homologous Recombination, Spermatogenesis, Molecular Biology

Abstract

Homologous recombination (HR) is an essential meiotic process that contributes to the genetic variation of offspring and ensures accurate chromosome segregation. Recombination is facilitated by the formation and repair of programmed DNA double-strand breaks. These DNA breaks are repaired via recombination between maternal and paternal homologous chromosomes and a subset result in the formation of crossovers. HR and crossover formation is facilitated by synapsis of homologous chromosomes by a proteinaceous scaffold structure known as the synaptonemal complex (SC). Recent studies in yeast and worms have indicated that polo-like kinases (PLKs) regulate several events during meiosis, including DNA recombination and SC dynamics. Mammals express four active PLKs (PLK1-4), and our previous work assessing localization and kinase function in mouse spermatocytes suggested that PLK1 coordinates nuclear events during meiotic prophase. Therefore, we conditionally mutated

Published

2022

32. Syce1 and Syce3 regulate testosterone and dihydrotestosterone synthesis via steroidogenic pathways in mouse Sertoli and Leydig cells

Author

Qi Wang, Qiu Yan, Jinghong Nan, Jie Wang, Yong Zhang, and Xingxu Zhao

Subjects

Male, Sertoli Cells, Synaptonemal Complex, Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Leydig Cells, Dihydrotestosterone, Cell Biology, Biochemistry, Mice, Endocrinology, Testis, Molecular Medicine, Animals, Testosterone, Molecular Biology, Testosterone Congeners

Abstract

Testosterone (T) and dihydrotestosterone (DHT) are the main hormones regulating reproduction and development of male animals. Although their synthesis and secretion are regulated by the endocrine system [hypothalamic-pituitary-gonadal (adrenal) axis], it is also possible to synthesize T and DHT from the induction of two proteins: Syce1 and Syce3. As central elements of the synaptonemal complex (SC), Syce1 and Syce3 play a key role in the association of homologous chromosomes during meiosis. However, Syce1 and Syce3 also promote the synthesis of T and DHT, although potential mechanisms have yet to be revealed. In this study, Leydig and Sertoli cells, which are responsible for the production and regulation of steroid hormones in testis, were transfected with recombinant Syce1/Syce3 and silence sequence. Our results revealed the highest expression of Syce1 and Syce3 in spermatogenic cells of the testis. Moreover, overexpression or knockdown of Syce1 and Syce3 in Sertoli and Leydig cells resulted in activation or suppression of steroidogenic genes Star and Hsd3b, which are involved in a steroidogenic pathway that upregulates T synthesis. Upregulated expression of Syce1 resulted in a significant increase in Srd5a1, which can promote DHT secretion. Interestingly, Syce1 and Syce3 overexpression synergistically promoted each other's abundance. Our results define a previously unknown mechanism of Syce1 and Syce3 dependent activation of steroidogenic signaling in Sertoli and Leydig cells.

Published

2022

33. Phosphorylation of HORMA-domain protein HTP-3 at Serine 285 is dispensable for crossover formation

Author

Debabrata Das, Shalini Trivedi, Jitka Blazícková, Swathi Arur, and Nicola Silva

Subjects

Meiosis, Synaptonemal Complex, Chromosome Segregation, Serine, Genetics, Animals, Cell Cycle Proteins, Phosphorylation, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Molecular Biology, Genetics (clinical)

Abstract

Generation of functional gametes is accomplished through a multilayered and finely orchestrated succession of events during meiotic progression. In the Caenorhabditis elegans germline, the HORMA-domain-containing protein HTP-3 plays pivotal roles for the establishment of chromosome axes and the efficient induction of programmed DNA double-strand breaks, both of which are crucial for crossover formation. Double-strand breaks allow for accurate chromosome segregation during the first meiotic division and therefore are an essential requirement for the production of healthy gametes. Phosphorylation-dependent regulation of HORMAD protein plays important roles in controlling meiotic chromosome behavior. Here, we document a phospho-site in HTP-3 at Serine 285 that is constitutively phosphorylated during meiotic prophase I. pHTP-3S285 localization overlaps with panHTP-3 except in nuclei undergoing physiological apoptosis, in which pHTP-3 is absent. Surprisingly, we observed that phosphorylation of HTP-3 at S285 is independent of the canonical kinases that control meiotic progression in nematodes. During meiosis, the htp-3(S285A) mutant displays accelerated RAD-51 turnover, but no other meiotic abnormalities. Altogether, these data indicate that the Ser285 phosphorylation is independent of canonical meiotic protein kinases and does not regulate HTP-3-dependent meiotic processes. We propose a model wherein phosphorylation of HTP-3 occurs through noncanonical or redundant meiotic kinases and/or is likely redundant with additional phospho-sites for function in vivo.

Published

2022

34. Alternative Synaptonemal Complex Structures: Too Much of a Good Thing?

Author

R. Scott Hawley and Stacie E. Hughes

Subjects

Crossover, Biology, Lateral element, Chromosome segregation, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Meiosis, Chromosome Segregation, Genetics, Homologous chromosome, Animals, Humans, Crossing Over, Genetic, 030304 developmental biology, 0303 health sciences, Synaptonemal Complex, Nuclear Proteins, Cell biology, Chromosome Pairing, Synaptonemal complex, chemistry, 030217 neurology & neurosurgery, DNA, Recombination

Abstract

The synaptonemal complex (SC), a highly conserved structure built between homologous meiotic chromosomes, is required for crossover formation and ensuring proper chromosome segregation. In many organisms, SC components can also form alternative structures, including repeating SC structures that are known as polycomplexes (PCs), and extensively modified SC structures that are maintained late in meiosis. PCs display differences in their ability to localize with lateral element proteins, recombination machinery, and DNA. They can be created by defects in post-translational modification, suggesting that these modifications have roles in preventing alternate SC structures. These SC-like structures provide insight into the rules for building and maintaining the SC by offering an 'in vivo laboratory' for models of SC assembly, structure, and disassembly. Here, we discuss what these structures can tell us about the rules for building the SC and the roles of the SC in meiotic processes.

Published

2020

35. Genetic background impacts the timing of synaptonemal complex breakdown in Drosophila melanogaster

Author

R. Scott Hawley, Emily R. Wesley, and Katherine Kretovich Billmyre

Subjects

Heterozygote, Genotype, Embryonic Development, Biology, Chromosome segregation, Meiosis, Chromosome Segregation, Genetics, Animals, Alleles, Genetic Association Studies, Genetics (clinical), Synaptonemal Complex, Cell Differentiation, Structural component, Genetic background, biology.organism_classification, Null allele, Human genetics, Molecular Imaging, Synaptonemal complex, Drosophila melanogaster, Mutation, Oocytes, Original Article, Developmental biology

Abstract

Experiments performed in different genetic backgrounds occasionally exhibit failure in experimental reproducibility. This is a serious issue in Drosophila where there are no standard control stocks. Here, we illustrate the importance of controlling genetic background by showing that the timing of a major meiotic event, the breakdown of the synaptonemal complex (SC), varies in different genetic backgrounds. We assessed SC breakdown in three different control stocks and found that in one control stock, y w; svspa-pol, the SC broke down earlier than in Oregon-R and w1118 stocks. We further examined SC breakdown in these three control backgrounds with flies heterozygous for a null mutation in c(3)G, which encodes a key structural component of the SC. Flies heterozygous for c(3)G displayed differences in the timing of SC breakdown in different control backgrounds, providing evidence of a sensitizing effect of this mutation. These observations suggest that SC maintenance is associated with the dosage of c(3)G in some backgrounds. Lastly, chromosome segregation was not affected by premature SC breakdown in mid-prophase, consistent with previous findings that chromosome segregation is not dependent on full-length SC in mid-prophase. Thus, genetic background is an important variable to consider with respect to SC behavior during Drosophila meiosis.

Published

2020

36. Trim41 is required to regulate chromosome axis protein dynamics and meiosis in male mice

Author

Seiya Oura, Toshiaki Hino, Takashi Satoh, Taichi Noda, Takayuki Koyano, Ayako Isotani, Makoto Matsuyama, Shizuo Akira, Kei-ichiro Ishiguro, and Masahito Ikawa

Subjects

Male, Mice, Knockout, Cancer Research, Synaptonemal Complex, Ubiquitin-Protein Ligases, Nuclear Proteins, Cell Cycle Proteins, Meiosis, Mice, Spermatocytes, Genetics, Animals, Molecular Biology, Genetics (clinical), Ecology, Evolution, Behavior and Systematics

Abstract

Meiosis is a hallmark event in germ cell development that accompanies sequential events executed by numerous molecules. Therefore, characterization of these factors is one of the best strategies to clarify the mechanism of meiosis. Here, we report tripartite motif-containing 41 (TRIM41), a ubiquitin ligase E3, as an essential factor for proper meiotic progression and fertility in male mice. Trim41 knockout (KO) spermatocytes exhibited synaptonemal complex protein 3 (SYCP3) overloading, especially on the X chromosome. Furthermore, mutant mice lacking the RING domain of TRIM41, required for the ubiquitin ligase E3 activity, phenocopied Trim41 KO mice. We then examined the behavior of mutant TRIM41 (ΔRING-TRIM41) and found that ΔRING-TRIM41 accumulated on the chromosome axes with overloaded SYCP3. This result suggested that TRIM41 exerts its function on the chromosome axes. Our study revealed that Trim41 is essential for preventing SYCP3 overloading, suggesting a TRIM41-mediated mechanism for regulating chromosome axis protein dynamics during male meiotic progression.

Published

2022

37. p53 Controls Meiotic Prophase Progression and Crossover Formation

Author

Marina Marcet-Ortega, Andros Maldonado-Linares, Maria López-Panadés, and Ignasi Roig

Subjects

Male, P53, Organic Chemistry, MLH1, Cell Cycle Proteins, General Medicine, Prophase, DSB repair, Catalysis, Computer Science Applications, Inorganic Chemistry, Mice, Meiosis, p53, meiosis, synaptonemal complex, γH2AX, crossover, Spermatocytes, Crossover, Animals, DNA Breaks, Double-Stranded, Physical and Theoretical Chemistry, Tumor Suppressor Protein p53, Synaptonemal complex, Molecular Biology, Spectroscopy

Abstract

Meiosis initiates with the formation of double strand breaks (DSBs) throughout the genome. To avoid genomic instability, these DSBs need to be correctly repaired by homologous recombination. Surveillance mechanisms involving the DNA damage response (DDR) pathway ATM-CHK2-p53 can detect the persistence of unrepaired DBSs and activate the recombination-dependent arrest at the pachytene stage. However, a complete understanding of p53 functions under normal physiological conditions remains lacking. Here, we report a detailed analysis of the p53 role during meiotic prophase in mice spermatocytes. We show that the absence of p53 regulates prophase progression by slowing down the pachytene stage when the recombination-dependent arrest occurs. Furthermore, our results show that p53 is necessary for proper crossover (CO) formation and localization. Our study contributes to a deeper understanding of p53 roles during the meiotic prophase.

Published

2022

38. Reevaluation of the role of LIP-1 as an ERK/MPK-1 dual specificity phosphatase in the C. elegans germline

Author

Debabrata Das, Jacob Seemann, David Greenstein, Tim Schedl, and Swathi Arur

Subjects

Mitogen-Activated Protein Kinase 1, Multidisciplinary, LIP-1 DUSP, Synaptonemal Complex, MPK-1 ERK, Temperature, Cell Cycle Proteins, Biological Sciences, germline, Substrate Specificity, Enzyme Activation, Germ Cells, Phenotype, Mutation, C. elegans, Oocytes, Animals, Pachytene Stage, Phosphorylation, Protein Tyrosine Phosphatases, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Developmental Biology, Cell Proliferation

Abstract

Significance The RAS–ERK pathway is critical for metazoan development. In development, ERK activity is regulated by a balance of phosphorylation of ERK by MEK (MAPK kinase) and dephosphorylation by DUSPs (dual specificity phosphatases). LIP-1, a DUSP6/7 family member, was previously suggested to regulate MPK-1/ERK activity by dephosphorylating MPK-1 in the Caenorhabditis elegans germline, based on LIP-1's mutant phenotype in the germline and its DUSP role in vulval development. However, our investigations demonstrate that LIP-1 does not function as an MPK-1 DUSP in the germline and likely regulates germline functions through distinct targets. Our results present a cautionary note about misinterpreting similar mutant phenotypes caused by mutations in different genes and assuming that genes function similarly in different tissues., The fidelity of a signaling pathway depends on its tight regulation in space and time. Extracellular signal-regulated kinase (ERK) controls wide-ranging cellular processes to promote organismal development and tissue homeostasis. ERK activation depends on a reversible dual phosphorylation on the TEY motif in its active site by ERK kinase (MEK) and dephosphorylation by DUSPs (dual specificity phosphatases). LIP-1, a DUSP6/7 homolog, was proposed to function as an ERK (MPK-1) DUSP in the Caenorhabditis elegans germline primarily because of its phenotype, which morphologically mimics that of a RAS/let-60 gain-of-function mutant (i.e., small oocyte phenotype). Our investigations, however, reveal that loss of lip-1 does not lead to an increase in MPK-1 activity in vivo. Instead, we show that loss of lip-1 leads to 1) a decrease in MPK-1 phosphorylation, 2) lower MPK-1 substrate phosphorylation, 3) phenocopy of mpk-1 reduction-of-function (rather than gain-of-function) allele, and 4) a failure to rescue mpk-1–dependent germline or fertility defects. Moreover, using diverse genetic mutants, we show that the small oocyte phenotype does not correlate with increased ectopic MPK-1 activity and that ectopic increase in MPK-1 phosphorylation does not necessarily result in a small oocyte phenotype. Together, these data demonstrate that LIP-1 does not function as an MPK-1 DUSP in the C. elegans germline. Our results caution against overinterpretation of the mechanistic underpinnings of orthologous phenotypes, since they may be a result of independent mechanisms, and provide a framework for characterizing the distinct molecular targets through which LIP-1 may mediate its several germline functions.

Published

2022

39. Centrosome dysfunction associated with somatic expression of the synaptonemal complex protein TEX12

Author

Sumit Sandhu, Ieng F. Sou, Jill E. Hunter, Lucy Salmon, Caroline L. Wilson, Neil D. Perkins, Neil Hunter, Owen R. Davies, and Urszula L. McClurg

Subjects

Centrosome, 0303 health sciences, Tumor, QH301-705.5, Synaptonemal Complex, Medicine (miscellaneous), Gene Expression, Cell Cycle Proteins, General Biochemistry, Genetics and Molecular Biology, Article, Cell Line, 03 medical and health sciences, Meiosis, Cell growth, Mice, 0302 clinical medicine, 030220 oncology & carcinogenesis, Cell Line, Tumor, Genetics, Animals, Humans, Biology (General), General Agricultural and Biological Sciences, 030304 developmental biology, Cancer

Abstract

The synaptonemal complex (SC) is a supramolecular protein scaffold that mediates chromosome synapsis and facilitates crossing over during meiosis. In mammals, SC proteins are generally assumed to have no other function. Here, we show that SC protein TEX12 also localises to centrosomes during meiosis independently of chromosome synapsis. In somatic cells, ectopically expressed TEX12 similarly localises to centrosomes, where it is associated with centrosome amplification, a pathology correlated with cancer development. Indeed, TEX12 is identified as a cancer-testis antigen and proliferation of some cancer cells is TEX12-dependent. Moreover, somatic expression of TEX12 is aberrantly activated via retinoic acid signalling, which is commonly disregulated in cancer. Structure-function analysis reveals that phosphorylation of TEX12 on tyrosine 48 is important for centrosome amplification but not for recruitment of TEX12 to centrosomes. We conclude that TEX12 normally localises to meiotic centrosomes, but its misexpression in somatic cells can contribute to pathological amplification and dysfunction of centrosomes in cancers., Sandhu et al. report that the synaptonemal complex (SC) protein, TEX12, localises to centrosomes independently of the SC during meiosis. They also show that it provokes centrosome amplification in somatic cells, a pathology associated with cancer development.

Published

2021

40. A rare frameshift mutation in SYCP1 is associated with human male infertility

Author

Soheila Nabi, Masomeh Askari, Maryam Rezaei-Gazik, Najmeh Salehi, Navid Almadani, Yaser Tahamtani, and Mehdi Totonchi

Subjects

Male, Embryology, Synaptonemal Complex, Obstetrics and Gynecology, Nuclear Proteins, Cell Biology, Oligospermia, DNA-Binding Proteins, Meiosis, Mice, Reproductive Medicine, Genetics, Animals, Humans, Frameshift Mutation, Molecular Biology, Infertility, Male, Developmental Biology

Abstract

Proper assembly of the synaptonemal complex is essential for successful meiosis, and impairments in the process lead to infertility. Meiotic transverse filament proteins encoded by the SYCP1 (synaptonemal complex protein 1) gene are one of the main components of the synaptonemal complex and play an important role in correct synapsis and recombination. Family-based whole-exome sequencing revealed a rare homozygous SYCP1 frameshift mutation (c.2892delA: p.K967Nfs*1) in two men with severe oligozoospermia, followed by validation and segregation through Sanger sequencing. This single nucleotide deletion not only changes lysine 967 (K) into asparagine (N) but also causes a premature stop codon, which leads to deletion of 968–976 residues from the end of the C-tail region of the SYCP1 protein. Although, sycp1 knockout male mice are reported to be sterile with a complete lack of spermatids and spermatozoa, to date no SYCP1 variant has been associated with human oligozoospermia. HADDOCK analysis indicated that this mutation decreases the ability of the truncated SYCP1 protein to bind DNA. Immunodetection of ϒH2AX signals in SYCP1 mutant semen cells, and a 40% DNA fragmentation index might indicate that a small number of DNA double-strand breaks, which require SYCP1 and/or synapsis to be repaired, are not efficiently repaired, resulting in defects in differentiation of germline cells and appearance of the oligozoospermia phenotype. To our knowledge, this is the first report of a homozygous SYCP1 mutation that decreases sperm count. Further studies are required to determine the function of the SYCP1 mutation, which is potentially associated with human oligozoospermia.

Published

2021

41. Unconventional conservation reveals structure-function relationships in the synaptonemal complex

Author

Henry D Cope, Lisa E Kursel, and Ofer Rog

Subjects

Sequence analysis, QH301-705.5, Science, ved/biology.organism_classification_rank.species, Genomics, P. pacificus, Homology (biology), General Biochemistry, Genetics and Molecular Biology, Rhabditida, Structure-Activity Relationship, Meiosis, Species Specificity, evolution, coiled-coil, Animals, meiosis, Biology (General), Caenorhabditis elegans, Peptide sequence, Evolutionary Biology, General Immunology and Microbiology, biology, D. melanogaster, ved/biology, General Neuroscience, synaptonemal complex, Genetics and Genomics, General Medicine, biology.organism_classification, Caenorhabditis, Synaptonemal complex, Pristionchus pacificus, Drosophila melanogaster, Evolutionary biology, indel, C. elegans, Medicine, Other, Function (biology), Research Article, Human

Abstract

Functional requirements constrain protein evolution, commonly manifesting in conserved primary amino acid sequence. Here, we extend this idea to secondary structural features by tracking their conservation in essential meiotic proteins with highly diverged sequences. The synaptonemal complex (SC) aligns parental chromosome pairs and regulates exchanges between them. In electron micrographs of meiocytes from all eukaryotic clades, the SC appears as a ~100 nm-wide ladder-like structure with regular striations. Despite the conserved ultrastructure and functions, the proteins that make up the SC are highly divergent in sequence. Here we found that, within the Caenorhabditis genus, SC proteins are significantly more diverged than other proteins. However, SC proteins have highly conserved protein length and coiled-coil domain structure. The same unconventional conservation signature holds true for SC proteins in Drosophila and mammals, suggesting it could be a universal feature of SC proteins. We used this evolutionary signature to identify a novel SC protein in the nematode Pristionchus pacificus, Ppa-SYP-1, which has no significant homology to any protein outside of Pristionchus. Our work suggests that the length and relative arrangement of coiled-coils play a key role in the structure and function of the SC. Furthermore, our analysis implies that expanding sequence analysis beyond measures of per-site identity or similarity can enhance our understanding of protein evolution and function.Short abstractFunctional requirements constrain protein evolution, commonly manifesting in a conserved amino acid sequence. Here, we extend this idea to secondary structural features by tracking their conservation in essential meiotic proteins with highly diverged sequences. The synaptonemal complex (SC) is a ~100 nm-wide ladder-like meiotic structure present in all eukaryotic clades, where it aligns parental chromosomes and regulates exchanges between them. Despite the conserved ultrastructure and functions of the SC, SC proteins are highly divergent within Caenorhabditis. However, SC proteins have highly conserved length and coiled-coil domain structure. We found the same unconventional conservation signature in Drosophila and mammals, and used it to identify a novel SC protein in Pristionchus pacificus, Ppa-SYP-1. Our work suggests that coiled-coils play wide-ranging roles in the structure and function of the SC, and more broadly, that expanding sequence analysis beyond measures of per-site similarity can enhance our understanding of protein evolution and function.

Published

2021

42. Alterations in synaptonemal complex coding genes and human infertility

Author

Fengguo Zhang, Mengfei Liu, and Jinmin Gao

Subjects

Adult, Male, Synaptonemal Complex, Cell Biology, Applied Microbiology and Biotechnology, Meiosis, Mice, Germ Cells, Chromosome Segregation, Infertility, Animals, Humans, Female, Molecular Biology, Ecology, Evolution, Behavior and Systematics, Developmental Biology

Abstract

About 10% of reproductive-aged couples suffer from infertility. However, the genetic causes of human infertility cases are largely unknown. Meiosis produces haploid gametes for fertilization and errors in meiosis are associated with human infertility in both males and females. Successful meiosis relies on the assembly of the synaptonemal complex (SC) between paired homologous chromosomes during the meiotic prophase. The SC is ultrastructurally and functionally conserved, promoting inter-homologous recombination and crossover formation, thus critical for accurate meiotic chromosome segregation. With whole-genome/exome sequencing and mouse models, a list of mutations in SC coding genes has been linked to human infertility. Here we summarize those findings. We also analyzed SC gene variants present in the general population and presented complex interaction networks associated with SC components. Whether a combination of genetic variations and environmental factors causes human infertility demands further investigations.

Published

2021

43. The organization, regulation, and biological functions of the synaptonemal complex

Author

Jin-Min Gao, Feng-Guo Zhang, and Rui-Rui Zhang

Subjects

crossover, meiotic recombination, Invited Review, Synaptonemal Complex, Urology, synapsis, Meiotic chromosome, Synapsis, General Medicine, Meiotic chromosome segregation, Biology, chromosome axis, Cell biology, Chromosome segregation, reproduction, Synaptonemal complex, Meiosis, Chromosome Segregation, Homologous chromosome, Animals, Homologous recombination

Abstract

The synaptonemal complex (SC) is a meiosis-specific proteinaceous macromolecular structure that assembles between paired homologous chromosomes during meiosis in various eukaryotes. The SC has a highly conserved ultrastructure and plays critical roles in controlling multiple steps in meiotic recombination and crossover formation, ensuring accurate meiotic chromosome segregation. Recent studies in different organisms, facilitated by advances in super-resolution microscopy, have provided insights into the macromolecular structure of the SC, including the internal organization of the meiotic chromosome axis and SC central region, the regulatory pathways that control SC assembly and dynamics, and the biological functions exerted by the SC and its substructures. This review summarizes recent discoveries about how the SC is organized and regulated that help to explain the biological functions associated with this meiosis-specific structure.

Published

2021

44. ATM/ATR kinases link the synaptonemal complex and DNA double-strand break repair pathway choice

Author

Laura I. Láscarez-Lagunas, Saravanapriah Nadarajan, Marina Martinez-Garcia, Julianna N. Quinn, Elena Todisco, Tanuj Thakkar, Elizaveta Berson, Don Eaford, Oliver Crawley, Alex Montoya, Peter Faull, Nuria Ferrandiz, Consuelo Barroso, Sara Labella, Emily Koury, Sarit Smolikove, Monique Zetka, Enrique Martinez-Perez, and Monica P. Colaiácovo

Subjects

Meiosis, DNA Repair, Synaptonemal Complex, Animals, Nuclear Proteins, DNA Breaks, Double-Stranded, DNA, Caenorhabditis elegans, Caenorhabditis elegans Proteins, General Agricultural and Biological Sciences, General Biochemistry, Genetics and Molecular Biology

Abstract

DNA double-strand breaks (DSBs) are deleterious lesions, which must be repaired precisely to maintain genomic stability. During meiosis, programmed DSBs are repaired via homologous recombination (HR) while repair using the nonhomologous end joining (NHEJ) pathway is inhibited, thereby ensuring crossover formation and accurate chromosome segregation.

Published

2022

45. Highly Conservative Pattern of Sex Chromosome Synapsis and Recombination in Neognathae Birds

Author

Lyubov P. Malinovskaya, Nikolai B. Rubtsov, Pavel M. Borodin, Elena P. Shnaider, Anna A. Torgasheva, Anastasia Slobodchikova, and Kira S. Zadesenets

Subjects

crossing over, Zoology, QH426-470, Article, Chromosomal crossover, Birds, Recombination nodule, Hirundo, Genetics, Animals, Passeriformes, avian sex chromosomes, Genetics (clinical), In Situ Hybridization, Fluorescence, Recombination, Genetic, Sex Chromosomes, biology, recombination nodules, synaptonemal complex, Synapsis, MLH1, Wagtail, Black tern, biology.organism_classification, Riparia diluta, Synaptonemal complex, Chromosome Pairing, Oocytes, Female, Pachytene Stage, MutL Protein Homolog 1, Chickens, SYCP3

Abstract

We analyzed the synapsis and recombination between Z and W chromosomes in the oocytes of nine neognath species: domestic chicken Gallus gallus domesticus, grey goose Anser anser, black tern Chlidonias niger, common tern Sterna hirundo, pale martin Riparia diluta, barn swallow Hirundo rustica, European pied flycatcher Ficedula hypoleuca, great tit Parus major and white wagtail Motacilla alba using immunolocalization of SYCP3, the main protein of the lateral elements of the synaptonemal complex, and MLH1, the mismatch repair protein marking mature recombination nodules. In all species examined, homologous synapsis occurs in a short region of variable size at the ends of Z and W chromosomes, where a single recombination nodule is located. The remaining parts of the sex chromosomes undergo synaptic adjustment and synapse non-homologously. In 25% of ZW bivalents of white wagtail, synapsis and recombination also occur at the secondary pairing region, which probably resulted from autosome−sex chromosome translocation. Using FISH with a paint probe specific to the germline-restricted chromosome (GRC) of the pale martin on the oocytes of the pale martin, barn swallow and great tit, we showed that both maternally inherited songbird chromosomes (GRC and W) share common sequences.

Published

2021

46. A motor independent requirement for dynein light chain in Caenorhabditis elegans meiotic synapsis

Author

Sara M Fielder, William G. Kelly, Huiping Ling, Elizabeth J. Gleason, and Tori Kent

Subjects

Genetics, Investigation, Mutation, biology, Dynein, Synapsis, biology.organism_classification, Immunoglobulin light chain, medicine.disease_cause, Cell biology, Synaptonemal complex, Meiosis, Homologous chromosome, medicine, Animals, Caenorhabditis elegans

Abstract

The dynein motor complex is thought to aid in homolog pairing in many organisms by moving chromosomes within the nuclear periphery to promote and test homologous interactions. This precedes synaptonemal complex (SC) formation during homolog synapsis, which stabilizes homolog proximity during recombination. We observed that depletion of the dynein light chain (DLC-1) in Caenorhabditis elegans irreversibly prevents synapsis, causing an increase in off-chromatin formation of SC protein foci with increasing temperature. This requirement for DLC-1 is independent of its function in dynein motors, as SYP protein foci do not form with depletion of other dynein motor components. In contrast to normal SC-related structures, foci formed with DLC-1 depletion are resistant to dissolution with 1,6-hexanediol, similar to aggregates of SC proteins formed in high growth temperatures. Dynein light chains have been shown to act as hub proteins that interact with other proteins through a conserved binding motif. We identified a similar DLC-1 binding motif in the C. elegans SC protein SYP-2, and mutation of the putative motif causes meiosis defects that are exacerbated by elevated temperatures. We propose that DLC-1 acts as a pre-synapsis chaperone-like factor for SYP proteins to help regulate their self-association prior to the signals for SC assembly, a role that is revealed by its increased essentiality at elevated temperatures.

Published

2021

47. The Zip4 protein directly couples meiotic crossover formation to synaptonemal complex assembly

Author

Valérie Borde, Arnaud De Muyt, Jessica Andreani, Raphael Guerois, and Alexandra Pyatnitskaya

Subjects

Saccharomyces cerevisiae Proteins, Mutant, Cell Cycle Proteins, Saccharomyces cerevisiae, 03 medical and health sciences, 0302 clinical medicine, Meiosis, Genetics, Homologous chromosome, Animals, Crossing Over, Genetic, Central element, 030304 developmental biology, Mammals, 0303 health sciences, Synaptonemal Complex, Chemistry, 030302 biochemistry & molecular biology, Synaptonemal complex assembly, Cell biology, Chromatin, Chromosome Pairing, Synaptonemal complex, Homologous recombination, 030217 neurology & neurosurgery, Developmental Biology

Abstract

SummaryMeiotic recombination is triggered by programmed double-strand breaks (DSBs), a subset of these being repaired as crossovers, promoted by eight evolutionarily conserved proteins, named ZMM. Crossover formation is functionally linked to synaptonemal complex (SC) assembly between homologous chromosomes, but the underlying mechanism is unknown. Here we show that Ecm11, a SC central element protein, localizes on both DSB sites and sites that attach chromatin loops to the chromosome axis, which are the starting points of SC formation, in a way that strictly requires the ZMM protein Zip4. Furthermore, Zip4 directly interacts with Ecm11 and point mutants that specifically abolish this interaction lose Ecm11 binding to chromosomes and exhibit defective SC assembly. This can be partially rescued by artificially tethering interaction-defective Ecm11 to Zip4. Mechanistically, this direct connection ensuring SC assembly from CO sites could be a way for the meiotic cell to shut down further DSB formation once enough recombination sites have been selected for crossovers, thereby preventing excess crossovers. Finally, the mammalian ortholog of Zip4, TEX11, also interacts with the SC central element TEX12, suggesting a general mechanism.

Published

2021

48. Oligopaint DNA FISH reveals telomere-based meiotic pairing dynamics in the silkworm, Bombyx mori

Author

Elissa P. Lei, Ines A Drinnenberg, Jose Gil, Leah F. Rosin, National Institutes of Health [Bethesda] (NIH), Institut Curie [Paris], and Centre de recherche de l'Institut Curie [Paris]

Subjects

Male, Life Cycles, Cancer Research, Chromosomal Proteins, Non-Histone, [SDV]Life Sciences [q-bio], Cell Cycle Proteins, QH426-470, Microtubules, Chromosome segregation, Homologous Chromosomes, Larvae, 0302 clinical medicine, Chromosome Segregation, Medicine and Health Sciences, Cell Cycle and Cell Division, Testes, Genetics (clinical), 0303 health sciences, Chromosome Biology, Synaptonemal Complex, Kinetochore, Autosomes, Telomere, [SDV.MHEP.EM]Life Sciences [q-bio]/Human health and pathology/Endocrinology and metabolism, Chiasma, Cell biology, Ovaries, Meiosis, Synaptonemal complex, Telomeres, Cell Processes, Female, Anatomy, Genital Anatomy, Research Article, Chromosome Structure and Function, Centromere, Biology, Chromosomes, Bivalent (genetics), 03 medical and health sciences, Homologous chromosome, Genetics, Animals, Molecular Biology, Metaphase, Ecology, Evolution, Behavior and Systematics, 030304 developmental biology, fungi, Reproductive System, Biology and Life Sciences, Cell Biology, DNA, Chromosome Pairs, Bombyx, Chromosome Pairing, Pairing, 030217 neurology & neurosurgery, Developmental Biology

Abstract

Accurate chromosome segregation during meiosis is essential for reproductive success. Yet, many fundamental aspects of meiosis remain unclear, including the mechanisms regulating homolog pairing across species. This gap is partially due to our inability to visualize individual chromosomes during meiosis. Here, we employ Oligopaint FISH to investigate homolog pairing and compaction of meiotic chromosomes and resurrect a classical model system, the silkworm Bombyx mori. Our Oligopaint design combines multiplexed barcoding with secondary oligo labeling for high flexibility and low cost. These studies illustrate that Oligopaints are highly specific in whole-mount gonads and on meiotic squashes. We show that meiotic pairing is robust in both males and females and that pairing can occur through numerous partially paired intermediate structures. We also show that pairing in male meiosis occurs asynchronously and seemingly in a transcription-biased manner. Further, we reveal that meiotic bivalent formation in B. mori males is highly similar to bivalent formation in C. elegans, with both of these pathways ultimately resulting in the pairing of chromosome ends with non-paired ends facing the spindle pole. Additionally, microtubule recruitment in both C. elegans and B. mori is likely dependent on kinetochore proteins but independent of the centromere-specifying histone CENP-A. Finally, using super-resolution microscopy in the female germline, we show that homologous chromosomes remain associated at telomere domains in the absence of chiasma and after breakdown and modification to the synaptonemal complex in pachytene. These studies reveal novel insights into mechanisms of meiotic homolog pairing both with or without recombination., Author summary Meiosis is the specialized cell division occurring exclusively in ovaries and testes to produce egg and sperm cells, respectively. The accurate distribution of chromosomes (the genetic material) during this process is essential to prevent infertility/sterility and developmental disorders in offspring. As researchers are specifically unable to study the mechanisms regulating meiosis in depth in humans, identifying broadly conserved aspects of meiotic chromosome segregation is essential for making accurate inferences about human biology. Here, we use a sophisticated chromosome painting approach called Oligopaints to visualize and study chromosomes during meiosis in the silkworm, Bombyx mori. Using this method, we show that chromosome ends (telomeres) play a central role in regulating interactions between maternal and paternal chromosome copies during both sperm and egg development.

Published

2021

49. Whole-chromosome fusions in the karyotype evolution of

Author

Artem P, Lisachov, Katerina V, Tishakova, Svetlana A, Romanenko, Anna S, Molodtseva, Dmitry Yu, Prokopov, Jorge C, Pereira, Malcolm A, Ferguson-Smith, Pavel M, Borodin, and Vladimir A, Trifonov

Subjects

Male, Sex Chromosomes, Synaptonemal Complex, Karyotype, Animals, Lizards, Articles, Biological Evolution

Abstract

Whole-chromosome fusions play a major role in the karyotypic evolution of reptiles. It has been suggested that certain chromosomes tend to fuse with sex chromosomes more frequently than others. However, the comparative genomic synteny data are too scarce to draw strong conclusions. We obtained and sequenced chromosome-specific DNA pools of Sceloporus malachiticus, an iguanian species which has experienced many chromosome fusions. We found that four of seven lineage-specific fusions involved sex chromosomes, and that certain syntenic blocks which constitute the sex chromosomes, such as the homologues of the Anolis carolinensis chromosomes 11 and 16, are repeatedly involved in sex chromosome formation in different squamate species. To test the hypothesis that the karyotypic shift could be associated with changes in recombination patterns, we performed a synaptonemal complex analysis in this species and in Sceloporus variabilis (2n = 34). It revealed that the sex chromosomes in S. malachiticus had two distal pseudoautosomal regions and a medial differentiated region. We found that multiple fusions little affected the recombination rate in S. malachiticus. Our data confirm more frequent involvement of certain chromosomes in sex chromosome formation, but do not reveal a connection between the gonosome–autosome fusions and the evolution of recombination rate. This article is part of the theme issue ‘Challenging the paradigm in sex chromosome evolution: empirical and theoretical insights with a focus on vertebrates (Part II)’.

Published

2021

50. Rad21l1 cohesin subunit is dispensable for spermatogenesis but not oogenesis in zebrafish

Author

Kristi Bispo, Daniel B. Chu, An Nguyen, Yana P. Blokhina, Sean M. Burgess, Bruce W. Draper, Ivan Olaya, Michelle A. Frees, Masuda Sharifi, and Cohen, Paula E

Subjects

p53, Male, Embryology, Cancer Research, Physiology, Chromosomal Proteins, Non-Histone, Eggs, Cell Cycle Proteins, QH426-470, Oogenesis, 0302 clinical medicine, Animal Cells, Reproductive Physiology, Medicine and Health Sciences, Cell Cycle and Cell Division, Zebrafish, Genetics (clinical), 0303 health sciences, biology, Chromosome Biology, Eukaryota, Animal Models, Sex reversal, Cell biology, Chromosomal Proteins, Meiosis, Phenotypes, Synaptonemal complex, Experimental Organism Systems, Osteichthyes, Cell Processes, OVA, Vertebrates, Female, Cellular Types, Anatomy, Genital Anatomy, Research Article, Spo11, Research and Analysis Methods, 03 medical and health sciences, Model Organisms, Homologous chromosome, Genetics, Animals, Gonads, Spermatogenesis, Molecular Biology, Ecology, Evolution, Behavior and Systematics, 030304 developmental biology, Cohesin, Contraception/Reproduction, Embryos, Organisms, Reproductive System, Biology and Life Sciences, Cell Biology, Non-Histone, Genes, p53, biology.organism_classification, Chromosome Pairing, Germ Cells, Fish, Genes, Mutation, Oocytes, Animal Studies, biology.protein, Generic health relevance, Zoology, 030217 neurology & neurosurgery, Developmental Biology

Abstract

During meiosis I, ring-shaped cohesin complexes play important roles in aiding the proper segregation of homologous chromosomes. RAD21L is a meiosis-specific vertebrate cohesin that is required for spermatogenesis in mice but is dispensable for oogenesis in young animals. The role of this cohesin in other vertebrate models has not been explored. Here, we tested if the zebrafish homolog Rad21l1 is required for meiotic chromosome dynamics during spermatogenesis and oogenesis. We found that Rad21l1 localizes to unsynapsed chromosome axes. It is also found between the axes of the mature tripartite synaptonemal complex (SC) in both sexes. We knocked out rad21l1 and found that nearly all rad21l1-/- mutants develop as fertile males, suggesting that the mutation causes a defect in juvenile oogenesis, since insufficient oocyte production triggers female to male sex reversal in zebrafish. Sex reversal was partially suppressed by mutation of the checkpoint gene tp53, suggesting that the rad21l1 mutation activates Tp53-mediated apoptosis or arrest in females. This response, however, is not linked to a defect in repairing Spo11-induced double-strand breaks since deletion of spo11 does not suppress the sex reversal phenotype. Compared to tp53 single mutant controls, rad21l1-/- tp53-/- double mutant females produce poor quality eggs that often die or develop into malformed embryos. Overall, these results indicate that the absence of rad21l1-/- females is due to a checkpoint-mediated response and highlight a role for a meiotic-specific cohesin subunit in oogenesis but not spermatogenesis., Author summary Cohesins are multi-protein, ring-shaped complexes that tether DNA duplexes to one another and are important for nuclear organization of DNA and proper chromosome segregation during cell division. Specialized cohesin subunits play important roles in meiosis, a cell division required to produce gametes. Segregation errors in meiosis can lead to the formation of gametes with the incorrect number of chromosomes (aneuploidy), a major cause of birth defects and pregnancy loss in humans. Here we assess the role of Rad21l1, a cohesin subunit specific to vertebrate animals, by knocking out the gene in zebrafish and examining how oogenesis and spermatogenesis are affected. While males produce normal sperm in the absence of Rad21l1, oocyte production is severely compromised. Oocytes develop partway but then undergo cell death. Deleting tp53, a gene involved in sensing cellular stress, prevents cell death and allows oogenesis to be completed, though most of the resulting eggs are severely poor quality. Thus, our work shows that zebrafish oogenesis requires a special cohesin subunit, without which oocytes die. In contrast, spermatogenesis does not require this subunit.

Published

2021