Your search keyword '"Marcus, B."' showing total 11 results

1. A TOPBP1 allele causing male infertility uncouples XY silencing dynamics from sex body formation

Author

Carolline Ascenção, Jennie R Sims, Alexis Dziubek, William Comstock, Elizabeth A Fogarty, Jumana Badar, Raimundo Freire, Andrew Grimson, Robert S Weiss, Paula E Cohen, and Marcus B Smolka

Subjects

TOPBP1, ATR, meiosis, MSCI, Medicine, Science, Biology (General), QH301-705.5

Abstract

Meiotic sex chromosome inactivation (MSCI) is a critical feature of meiotic prophase I progression in males. While the ATR kinase and its activator TOPBP1 are key drivers of MSCI within the specialized sex body (SB) domain of the nucleus, how they promote silencing remains unclear given their multifaceted meiotic functions that also include DNA repair, chromosome synapsis, and SB formation. Here we report a novel mutant mouse harboring mutations in the TOPBP1-BRCT5 domain. Topbp1B5/B5 males are infertile, with impaired MSCI despite displaying grossly normal events of early prophase I, including synapsis and SB formation. Specific ATR-dependent events are disrupted, including phosphorylation and localization of the RNA:DNA helicase Senataxin. Topbp1B5/B5 spermatocytes initiate, but cannot maintain ongoing, MSCI. These findings reveal a non-canonical role for the ATR-TOPBP1 signaling axis in MSCI dynamics at advanced stages in pachynema and establish the first mouse mutant that separates ATR signaling and MSCI from SB formation.

Published

2024

2. Mec1-independent activation of the Rad53 checkpoint kinase revealed by quantitative analysis of protein localization dynamics

Author

Brandon Ho, Ethan J Sanford, Raphael Loll-Krippleber, Nikko P Torres, Marcus B Smolka, and Grant W Brown

Subjects

DNA repair, protein localization, cell cycle checkpoint, protein kinase, retrograde signaling, Medicine, Science, Biology (General), QH301-705.5

Abstract

The replication checkpoint is essential for accurate DNA replication and repair, and maintenance of genomic integrity when a cell is challenged with genotoxic stress. Several studies have defined the complement of proteins that change subcellular location in the budding yeast Saccharomyces cerevisiae following chemically induced DNA replication stress using methyl methanesulfonate (MMS) or hydroxyurea (HU). How these protein movements are regulated remains largely unexplored. We find that the essential checkpoint kinases Mec1 and Rad53 are responsible for regulating the subcellular localization of 159 proteins during MMS-induced replication stress. Unexpectedly, Rad53 regulation of the localization of 52 proteins is independent of its known kinase activator Mec1, and in some scenarios independent of Tel1 or the mediator proteins Rad9 and Mrc1. We demonstrate that Rad53 is phosphorylated and active following MMS exposure in cells lacking Mec1 and Tel1. This noncanonical mode of Rad53 activation depends partly on the retrograde signaling transcription factor Rtg3, which also facilitates proper DNA replication dynamics. We conclude that there are biologically important modes of Rad53 protein kinase activation that respond to replication stress and operate in parallel to Mec1 and Tel1.

Published

2023

3. Multiple 9-1-1 complexes promote homolog synapsis, DSB repair, and ATR signaling during mammalian meiosis

Author

Catalina Pereira, Gerardo A Arroyo-Martinez, Matthew Z Guo, Michael S Downey, Emma R Kelly, Kathryn J Grive, Shantha K Mahadevaiah, Jennie R Sims, Vitor M Faca, Charlton Tsai, Carl J Schiltz, Niek Wit, Heinz Jacobs, Nathan L Clark, Raimundo Freire, James Turner, Amy M Lyndaker, Miguel A Brieno-Enriquez, Paula E Cohen, Marcus B Smolka, and Robert S Weiss

Subjects

meiosis, DNA damage response, DNA break repair, meiotic silencing, 9-1-1 complex, ATR, Medicine, Science, Biology (General), QH301-705.5

Abstract

DNA damage response mechanisms have meiotic roles that ensure successful gamete formation. While completion of meiotic double-strand break (DSB) repair requires the canonical RAD9A-RAD1-HUS1 (9A-1-1) complex, mammalian meiocytes also express RAD9A and HUS1 paralogs, RAD9B and HUS1B, predicted to form alternative 9-1-1 complexes. The RAD1 subunit is shared by all predicted 9-1-1 complexes and localizes to meiotic chromosomes even in the absence of HUS1 and RAD9A. Here, we report that testis-specific disruption of RAD1 in mice resulted in impaired DSB repair, germ cell depletion, and infertility. Unlike Hus1 or Rad9a disruption, Rad1 loss in meiocytes also caused severe defects in homolog synapsis, impaired phosphorylation of ATR targets such as H2AX, CHK1, and HORMAD2, and compromised meiotic sex chromosome inactivation. Together, these results establish critical roles for both canonical and alternative 9-1-1 complexes in meiotic ATR activation and successful prophase I completion.

Published

2022

4. Phosphoproteomics of ATR signaling in mouse testes

Author

Jennie R Sims, Vitor M Faça, Catalina Pereira, Carolline Ascenção, William Comstock, Jumana Badar, Gerardo A Arroyo-Martinez, Raimundo Freire, Paula E Cohen, Robert S Weiss, and Marcus B Smolka

Subjects

ATR, meiosis, sex body, 9-1-1, prophase I, Medicine, Science, Biology (General), QH301-705.5

Abstract

The phosphatidylinositol 3′ kinase (PI3K)‐related kinase ATR is crucial for mammalian meiosis. ATR promotes meiotic progression by coordinating key events in DNA repair, meiotic sex chromosome inactivation (MSCI), and checkpoint-dependent quality control during meiotic prophase I. Despite its central roles in meiosis, the ATR-dependent meiotic signaling network remains largely unknown. Here, we used phosphoproteomics to define ATR signaling events in testes from mice following chemical and genetic ablation of ATR signaling. Quantitative analysis of phosphoproteomes obtained after germ cell-specific genetic ablation of the ATR activating 9-1-1 complex or treatment with ATR inhibitor identified over 14,000 phosphorylation sites from testes samples, of which 401 phosphorylation sites were found to be dependent on both the 9-1-1 complex and ATR. Our analyses identified ATR-dependent phosphorylation events in crucial DNA damage signaling and DNA repair proteins including TOPBP1, SMC3, MDC1, RAD50, and SLX4. Importantly, we identified ATR and RAD1-dependent phosphorylation events in proteins involved in mRNA regulatory processes, including SETX and RANBP3, whose localization to the sex body was lost upon ATR inhibition. In addition to identifying the expected ATR-targeted S/T-Q motif, we identified enrichment of an S/T-P-X-K motif in the set of ATR-dependent events, suggesting that ATR promotes signaling via proline-directed kinase(s) during meiosis. Indeed, we found that ATR signaling is important for the proper localization of CDK2 in spermatocytes. Overall, our analysis establishes a map of ATR signaling in mouse testes and highlights potential meiotic-specific actions of ATR during prophase I progression.

Published

2022

5. A TOPBP1 allele causing male infertility uncouples XY silencing dynamics from sex body formation.

Author

Ascenção, Carolline, Sims, Jennie R., Dziubek, Alexis, Comstock, William, Fogarty, Elizabeth A., Badar, Jumana, Freire, Raimundo, Grimson, Andrew, Weiss, Robert S., Cohen, Paula E., and Smolka, Marcus B.

Published

2024

6. Protein polyglutamylation catalyzed by the bacterial calmodulin-dependent pseudokinase SidJ

Author

Alan Sulpizio, Marena E Minelli, Min Wan, Paul D Burrowes, Xiaochun Wu, Ethan J Sanford, Jung-Ho Shin, Byron C Williams, Michael L Goldberg, Marcus B Smolka, and Yuxin Mao

Subjects

Legionella pneumophila, glutamylation, ubiquitin, SdeA, phosphoribosyl ubiquitination, SidJ, Medicine, Science, Biology (General), QH301-705.5

Abstract

Pseudokinases are considered to be the inactive counterparts of conventional protein kinases and comprise approximately 10% of the human and mouse kinomes. Here, we report the crystal structure of the Legionella pneumophila effector protein, SidJ, in complex with the eukaryotic Ca2+-binding regulator, calmodulin (CaM). The structure reveals that SidJ contains a protein kinase-like fold domain, which retains a majority of the characteristic kinase catalytic motifs. However, SidJ fails to demonstrate kinase activity. Instead, mass spectrometry and in vitro biochemical analyses demonstrate that SidJ modifies another Legionella effector SdeA, an unconventional phosphoribosyl ubiquitin ligase, by adding glutamate molecules to a specific residue of SdeA in a CaM-dependent manner. Furthermore, we show that SidJ-mediated polyglutamylation suppresses the ADP-ribosylation activity. Our work further implies that some pseudokinases may possess ATP-dependent activities other than conventional phosphorylation.

Published

2019

7. Mec1-independent activation of the Rad53 checkpoint kinase revealed by quantitative analysis of protein localization dynamics.

Author

Ho, Brandon, Sanford, Ethan J., Loll-Krippleber, Raphael, Torres, Nikko P., Smolka, Marcus B., and Brown, Grant W.

Published

2023

8. Phosphoproteomics of ATR signaling in mouse testes

Author

Catalina Pereira, Vitor M Faça, Jennie R Sims, Carolline Ascenção, William Comstock, Jumana Badar, Gerardo A Arroyo-Martinez, Raimundo Freire, Paula E Cohen, Robert S Weiss, and Marcus B Smolka

Subjects

Male, sex body, DNA Repair, Proteome, QH301-705.5, Morpholines, Science, Ataxia Telangiectasia Mutated Proteins, General Biochemistry, Genetics and Molecular Biology, stomatognathic system, Spermatocytes, Testis, prophase I, Animals, meiosis, RNA, Messenger, Phosphorylation, Biology (General), General Immunology and Microbiology, General Neuroscience, General Medicine, Mice, Inbred C57BL, Pyrimidines, ATR, Medicine, biological phenomena, cell phenomena, and immunity, 9-1-1, DNA Damage, Signal Transduction

Abstract

The phosphatidylinositol 3′ kinase (PI3K)‐related kinase ATR is crucial for mammalian meiosis. ATR promotes meiotic progression by coordinating key events in DNA repair, meiotic sex chromosome inactivation (MSCI), and checkpoint-dependent quality control during meiotic prophase I. Despite its central roles in meiosis, the ATR-dependent meiotic signaling network remains largely unknown. Here, we used phosphoproteomics to define ATR signaling events in testes from mice following chemical and genetic ablation of ATR signaling. Quantitative analysis of phosphoproteomes obtained after germ cell-specific genetic ablation of the ATR activating 9-1-1 complex or treatment with ATR inhibitor identified over 14,000 phosphorylation sites from testes samples, of which 401 phosphorylation sites were found to be dependent on both the 9-1-1 complex and ATR. Our analyses identified ATR-dependent phosphorylation events in crucial DNA damage signaling and DNA repair proteins including TOPBP1, SMC3, MDC1, RAD50, and SLX4. Importantly, we identified ATR and RAD1-dependent phosphorylation events in proteins involved in mRNA regulatory processes, including SETX and RANBP3, whose localization to the sex body was lost upon ATR inhibition. In addition to identifying the expected ATR-targeted S/T-Q motif, we identified enrichment of an S/T-P-X-K motif in the set of ATR-dependent events, suggesting that ATR promotes signaling via proline-directed kinase(s) during meiosis. Indeed, we found that ATR signaling is important for the proper localization of CDK2 in spermatocytes. Overall, our analysis establishes a map of ATR signaling in mouse testes and highlights potential meiotic-specific actions of ATR during prophase I progression.

Published

2022

9. Phosphoproteomics of ATR signaling in mouse testes

Author

Sims, Jennie R, primary, Faça, Vitor M, primary, Pereira, Catalina, primary, Ascenção, Carolline, additional, Comstock, William, additional, Badar, Jumana, additional, Arroyo-Martinez, Gerardo A, additional, Freire, Raimundo, additional, Cohen, Paula E, additional, Weiss, Robert S, additional, and Smolka, Marcus B, additional

Published

2022

10. Multiple 9-1-1 complexes promote homolog synapsis, DSB repair, and ATR signaling during mammalian meiosis

Author

Pereira, Catalina, primary, Arroyo-Martinez, Gerardo A, additional, Guo, Matthew Z, additional, Downey, Michael S, additional, Kelly, Emma R, additional, Grive, Kathryn J, additional, Mahadevaiah, Shantha K, additional, Sims, Jennie R, additional, Faca, Vitor M, additional, Tsai, Charlton, additional, Schiltz, Carl J, additional, Wit, Niek, additional, Jacobs, Heinz, additional, Clark, Nathan L, additional, Freire, Raimundo, additional, Turner, James, additional, Lyndaker, Amy M, additional, Brieno-Enriquez, Miguel A, additional, Cohen, Paula E, additional, Smolka, Marcus B, additional, and Weiss, Robert S, additional

Published

2022

11. Protein polyglutamylation catalyzed by the bacterial calmodulin-dependent pseudokinase SidJ

Author

Sulpizio, Alan, primary, Minelli, Marena E, additional, Wan, Min, additional, Burrowes, Paul D, additional, Wu, Xiaochun, additional, Sanford, Ethan J, additional, Shin, Jung-Ho, additional, Williams, Byron C, additional, Goldberg, Michael L, additional, Smolka, Marcus B, additional, and Mao, Yuxin, additional

Published

2019