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6,651 results on '"Origin recognition complex"'

1. The Origin Recognition Complex: From Origin Selection to Replication Licensing in Yeast and Humans.

Author

Tye, Bik-Kwoon and Zhai, Yuanliang

Subjects
*DNA replication, *HUMAN DNA, *REPLISOMES, *BINDING sites, *HUMAN beings
Abstract

Simple Summary: The origin recognition complex (ORC) selects sites for replication initiation by recruiting a pair of hexameric minichromosome maintenance (MCM) complexes to replication origins where the pre-replication complex (Pre-RC) is assembled, and the bidirectional replisomes are formed. In yeast, site selection by ORC is largely based on sequence-specific binding and Pre-RCs are established where ORC binds. In humans, site selection by ORC is largely based on chromatin landscapes and Pre-RCs are formed far away from ORC binding sites. This review compares these two very different modes of origin selection that can be traced to a small variation in the structures of subunit 4 of the yeast and human ORC. Understanding human DNA replication through the study of yeast has been an extremely fruitful journey. The minichromosome maintenance (MCM) 2–7 genes that encode the catalytic core of the eukaryotic replisome were initially identified through forward yeast genetics. The origin recognition complexes (ORC) that load the MCM hexamers at replication origins were purified from yeast extracts. We have reached an age where high-resolution cryoEM structures of yeast and human replication complexes can be compared side-by-side. Their similarities and differences are converging as alternative strategies that may deviate in detail but are shared by both species. [ABSTRACT FROM AUTHOR]

Published
2024
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2. A dual role for the chromatin reader ORCA/LRWD1 in targeting the origin recognition complex to chromatin.

Author

Sahu, Sumon, Ekundayo, Babatunde E, Kumar, Ashish, and Bleichert, Franziska

Subjects
*DNA helicases, *HISTONES, *DNA replication, *HETEROCHROMATIN, *AMINO acid sequence, *CHROMATIN, *EUKARYOTIC cells, *EPIGENOMICS
Abstract

Eukaryotic cells use chromatin marks to regulate the initiation of DNA replication. The origin recognition complex (ORC)‐associated protein ORCA plays a critical role in heterochromatin replication in mammalian cells by recruiting the initiator ORC, but the underlying mechanisms remain unclear. Here, we report crystal and cryo‐electron microscopy structures of ORCA in complex with ORC's Orc2 subunit and nucleosomes, establishing that ORCA orchestrates ternary complex assembly by simultaneously recognizing a highly conserved peptide sequence in Orc2, nucleosomal DNA, and repressive histone trimethylation marks through an aromatic cage. Unexpectedly, binding of ORCA to nucleosomes prevents chromatin array compaction in a manner that relies on H4K20 trimethylation, a histone modification critical for heterochromatin replication. We further show that ORCA is necessary and sufficient to specifically recruit ORC into chromatin condensates marked by H4K20 trimethylation, providing a paradigm for studying replication initiation in specific chromatin contexts. Collectively, our findings support a model in which ORCA not only serves as a platform for ORC recruitment to nucleosomes bearing specific histone marks but also helps establish a local chromatin environment conducive to subsequent MCM2‐7 loading. Synopsis: Eukaryotic DNA replication relies on the initiator ORC to load replicative helicases onto DNA, but how this outcome is achieved in condensed chromatin remains unclear. Biochemical and structural studies uncover a dual mechanism for how the ORC‐associated protein ORCA supports ORC during replication initiation in chromatin. Crystal and cryo‐EM structures of ORCA in complex with ORC's Orc2 subunit and nucleosomes resolve molecular details of ternary complex assembly.ORCA uses an aromatic cage in its WD40 domain to recognize repressive histone trimethylation marks, while adjacent protein regions help stabilize ORCA on nucleosomes and chromatin.ORCA recruits ORC to chromatin marked by H4K20me3 in vitro.ORCA reduces self‐association of H4K20me3‐modified but not unmodified nucleosomes and diminishes H4K20me3‐chromatin compaction.These findings support a model in which ORCA not only recruits ORC to chromatin in a histone modification‐specific manner but also reorganizes local chromatin structure in preparation for DNA replication initiation. [ABSTRACT FROM AUTHOR]

Published
2023
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3. The Origin Recognition Complex: From Origin Selection to Replication Licensing in Yeast and Humans

Author

Bik-Kwoon Tye and Yuanliang Zhai

Subjects
origin selection, replication initiation, eukaryotic DNA replication, cryoEM structures, MCM hexamers, origin recognition complex, Biology (General), QH301-705.5
Abstract

Understanding human DNA replication through the study of yeast has been an extremely fruitful journey. The minichromosome maintenance (MCM) 2–7 genes that encode the catalytic core of the eukaryotic replisome were initially identified through forward yeast genetics. The origin recognition complexes (ORC) that load the MCM hexamers at replication origins were purified from yeast extracts. We have reached an age where high-resolution cryoEM structures of yeast and human replication complexes can be compared side-by-side. Their similarities and differences are converging as alternative strategies that may deviate in detail but are shared by both species.

Published
2023
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4. A new class of disordered elements controls DNA replication through initiator self-assembly.

Author

Parker, Matthew W, Bell, Maren, Mir, Mustafa, Kao, Jonchee A, Darzacq, Xavier, Botchan, Michael R, and Berger, James M

Subjects
Chromatin, Animals, Drosophila melanogaster, Drosophila Proteins, DNA Replication, Origin Recognition Complex, Protein Multimerization, Cdc6, Cdt1, D. melanogaster, DNA replication, ORC, biochemistry, chemical biology, intrinsically disordered, phase separation, Biochemistry and Cell Biology
Abstract

The initiation of DNA replication in metazoans occurs at thousands of chromosomal sites known as origins. At each origin, the Origin Recognition Complex (ORC), Cdc6, and Cdt1 co-assemble to load the Mcm2-7 replicative helicase onto chromatin. Current replication models envisage a linear arrangement of isolated origins functioning autonomously; the extent of inter-origin organization and communication is unknown. Here, we report that the replication initiation machinery of D. melanogaster unexpectedly undergoes liquid-liquid phase separation (LLPS) upon binding DNA in vitro. We find that ORC, Cdc6, and Cdt1 contain intrinsically disordered regions (IDRs) that drive LLPS and constitute a new class of phase separating elements. Initiator IDRs are shown to regulate multiple functions, including chromosome recruitment, initiator-specific co-assembly, and Mcm2-7 loading. These data help explain how CDK activity controls replication initiation and suggest that replication programs are subject to higher-order levels of inter-origin organization.

Published
2019

5. Structural basis for the ORC1‐Cyclin A association

Author

Wang, Boxiao and Song, Jikui

Subjects
Biochemistry and Cell Biology, Biological Sciences, 2.1 Biological and endogenous factors, Aetiology, Amino Acid Motifs, Binding Sites, Crystallography, X-Ray, Cyclin A, Cyclin-Dependent Kinase 2, Humans, Hydrophobic and Hydrophilic Interactions, Models, Molecular, Origin Recognition Complex, Peptides, Protein Binding, Protein Conformation, cyclin-inhibitor complex, ORC1, Cyclin E, cell cycle regulation, Computation Theory and Mathematics, Other Information and Computing Sciences, Biophysics, Biochemistry and cell biology, Medicinal and biomolecular chemistry
Abstract

Progression of cell cycle is regulated by sequential expression of cyclins, which associate with distinct cyclin kinases to drive the transition between different cell cycle phases. The complex of Cyclin A with cyclin-dependent kinase 2 (CDK2) controls the DNA replication activity through phosphorylation of a set of chromatin factors, which critically influences the S phase transition. It has been shown that the direct interaction between the Cyclin A-CDK2 complex and origin recognition complex subunit 1 (ORC1) mediates the localization of ORC1 to centrosomes, where ORC1 inhibits cyclin E-mediated centrosome reduplication. However, the molecular basis underlying the specific recognition between ORC1 and cyclins remains elusive. Here we report the crystal structure of Cyclin A-CDK2 complex bound to a peptide derived from ORC1 at 2.54 å resolution. The structure revealed that the ORC1 peptide interacts with a hydrophobic groove, termed cyclin binding groove (CBG), of Cyclin A via a KXL motif. Distinct from other identified CBG-binding sequences, an arginine residue flanking the KXL motif of ORC1 inserts into a neighboring acidic pocket, contributing to the strong ORC1-Cyclin A association. Furthermore, structural and sequence analysis of cyclins reveals divergence on the ORC1-binding sites, which may underpin their differential ORC1-binding activities. This study provides a structural basis of the specific ORC1-cyclins recognition, with implication in development of novel inhibitors against the cyclin/CDK complexes.

Published
2019

6. Origins of DNA replication in eukaryotes.

Author

Hu, Yixin and Stillman, Bruce

Subjects
*DNA replication, *EUKARYOTIC cells, *EUKARYOTES
Abstract

Errors occurring during DNA replication can result in inaccurate replication, incomplete replication, or re-replication, resulting in genome instability that can lead to diseases such as cancer or disorders such as autism. A great deal of progress has been made toward understanding the entire process of DNA replication in eukaryotes, including the mechanism of initiation and its control. This review focuses on the current understanding of how the origin recognition complex (ORC) contributes to determining the location of replication initiation in the multiple chromosomes within eukaryotic cells, as well as methods for mapping the location and temporal patterning of DNA replication. Origin specification and configuration vary substantially between eukaryotic species and in some cases co-evolved with gene-silencing mechanisms. We discuss the possibility that centromeres and origins of DNA replication were originally derived from a common element and later separated during evolution. The initiation of DNA replication occurs at multiple sites along eukaryotic cell chromosomes. The mechanism that defines the location of these replication origins varies considerably, ranging from DNA-sequence-specific to epigenetically determined and inherited. It is possible that the origins of DNA replication and centromeres evolved from a common ancestral element. [ABSTRACT FROM AUTHOR]

Published
2023
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7. Dissection of Functional Domains of Orc1-2, the Archaeal Global DNA Damage-Responsive Regulator.

Author

Liu, Xiaotong, Sun, Mengmeng, Xu, Ruyi, Shen, Yulong, Huang, Qihong, Feng, Xu, and She, Qunxin

Subjects
*DNA-binding proteins, *CELL death inhibition, *MUTANT proteins, *DNA repair, *DNA
Abstract

Orc1-2 is a non-initiator ortholog of archaeal/eukaryotic Orc1 proteins, which functions as a global regulator in DNA damage-responsive (DDR) expression. As for Orc1 initiators, the DDR regulator harbors an AAA+ ATPase domain, an Initiator-Specific Motif (ISM) and a winged-helix (wH) DNA-binding domain, which are also organized in a similar fashion. To investigate how Orc1-2 mediates the DDR regulation, the orc1-2 mutants inactivating each of these functional domains were constructed with Saccharolobus islandicus and genetically characterized. We found that disruption of each functional domain completely abolished the DDR regulation in these orc1-2 mutants. Strikingly, inactivation of ATP hydrolysis of Orc1-2 rendered an inviable mutant. However, the cell lethality can be suppressed by the deficiency of the DNA binding in the same protein, and it occurs independent of any DNA damage signal. Mutant Orc1-2 proteins were then obtained and investigated for DNA-binding in vitro. This revealed that both the AAA+ ATPase and the wH domains are involved in DNA-binding, where ISM and R381R383 in wH are responsible for specific DNA binding. We further show that Orc1-2 regulation occurs in two distinct steps: (a) eliciting cell division inhibition at a low Orc1-2 content, and this regulation is switched on by ATP binding and turned off by ATP hydrolysis; any failure in turning off the regulation leads to growth inhibition and cell death; (b) activation of the expression of DDR gene encoding DNA repair proteins at an elevated level of Orc1-2. [ABSTRACT FROM AUTHOR]

Published
2022
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8. Conformational control and DNA-binding mechanism of the metazoan origin recognition complex

Author

Bleichert, Franziska, Leitner, Alexander, Aebersold, Ruedi, Botchan, Michael R, and Berger, James M

Subjects
1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, Animals, Cell Cycle Proteins, DNA, Drosophila Proteins, Drosophila melanogaster, Humans, Minichromosome Maintenance Proteins, Nuclear Proteins, Origin Recognition Complex, origin recognition complex, DNA replication, initiators, AAA(+) ATPase, helicase loading, AAA+ ATPase
Abstract

In eukaryotes, the heterohexameric origin recognition complex (ORC) coordinates replication onset by facilitating the recruitment and loading of the minichromosome maintenance 2-7 (Mcm2-7) replicative helicase onto DNA to license origins. Drosophila ORC can adopt an autoinhibited configuration that is predicted to prevent Mcm2-7 loading; how the complex is activated and whether other ORC homologs can assume this state are not known. Using chemical cross-linking and mass spectrometry, biochemical assays, and electron microscopy (EM), we show that the autoinhibited state of Drosophila ORC is populated in solution, and that human ORC can also adopt this form. ATP binding to ORC supports a transition from the autoinhibited state to an active configuration, enabling the nucleotide-dependent association of ORC with both DNA and Cdc6. An unstructured N-terminal region adjacent to the conserved ATPase domain of Orc1 is shown to be required for high-affinity ORC-DNA interactions, but not for activation. ORC optimally binds DNA duplexes longer than the predicted footprint of the ORC ATPases associated with a variety of cellular activities (AAA+) and winged-helix (WH) folds; cryo-EM analysis of Drosophila ORC bound to DNA and Cdc6 indicates that ORC contacts DNA outside of its central core region, bending the DNA away from its central DNA-binding channel. Our findings indicate that ORC autoinhibition may be common to metazoans and that ORC-Cdc6 remodels origin DNA before Mcm2-7 recruitment and loading.

Published
2018

9. Expression and Clinical Significance of Origin Recognition Complex Subunit 6 in Breast Cancer – A Comprehensive Bioinformatics Analysis

Author

Chen S, Jin Z, Xin L, Lv L, Zhang X, Gong Y, and Liu J

Subjects
origin recognition complex, breast cancer, prognostic biomarker, nomogram, gene set enrichment analysis, immune infiltration, Medicine (General), R5-920
Abstract

Shaohua Chen,1,2 Ziyao Jin,3 Linfeng Xin,4 Lv Lv,2 Xuemei Zhang,3 Yizhen Gong,5 Jianlun Liu1 1Department of Breast Surgery, Guangxi Medical University Cancer Hospital, Nangning, People’s Republic of China; 2Department of Breast and Thyroid Surgery, Affiliated Hospital of Guilin Medical University, Guilin, People’s Republic of China; 3Department of Pathology, Affiliated Hospital of Guilin Medical University, Guilin, People’s Republic of China; 4Clinical Medicine, Guilin Medical University, Guilin, People’s Republic of China; 5Department of Gastrointestinal Surgery, Guangxi Medical University Cancer Hospital, Nangning, People’s Republic of ChinaCorrespondence: Jianlun Liu Email 631228181@qq.comObjective: We aimed to investigate the expression, diagnostic and prognostic values, and potential molecular mechanisms of the origin recognition complex (ORC) in breast cancer (BC).Methods: Kaplan–Meier estimation was used to assess the prognostic value of ORC genes, and Oncomine, TCGA, GEO and ULCAN databases were used to analyze their expression in BC. Wilcoxon rank-sum tests were used to evaluate the relationship between ORC gene expression levels and BC clinicopathological features. Receiver operating characteristic (ROC) curves were used to assess the diagnostic value of ORC genes in BC. Survival analysis was performed using Kaplan–Meier estimation and Cox regression. A nomogram was constructed to predict 1-, 3-, and 5-year survival probabilities in BC. Gene set enrichment analysis (GSEA) and immune infiltration were used to investigate potential molecular mechanisms of the ORC.Results: ORC1L and ORC6L were highly expressed in BC compared with healthy tissue, while ORC5L expression patterns were inconsistent; no significant differences in ORC2L, ORC3L or ORC4L expression were observed between BC and healthy tissues. ORC1L and ORC6L expression levels were significantly correlated with age, tumor (T) stage and molecular subtype; ORC5L expression was significantly correlated with age and number of nearby lymph nodes with cancer (N stage). ORC6L expression had the highest diagnostic value in BC and was an independent prognostic factor for poor overall survival (OS). ORC6L may be involved in cell cycle progression and may regulate cancer signaling pathways, including NF-κB, P53, and WNT, in BC. ORC6L expression was also associated with immune infiltration.Conclusion: ORC1L and ORC6L are highly expressed in BC; ORC6L has a high diagnostic value and is an independent prognostic factor for poor OS. ORC6L may be involved in the initiation and progression of BC by regulating cell cycle progression, promoting cancer signaling pathway activation, and influencing tumor immune cell infiltration.Keywords: origin recognition complex, breast cancer, prognostic biomarker, nomogram, gene set enrichment analysis, immune infiltration

Published
2021

10. Origin recognition complex harbors an intrinsic nucleosome remodeling activity.

Author

Sai Li, Wasserman, Michael R., Yurieva, Olga, Lu Bai, O’Donnell, Michael E., and Shixin Liu

Subjects
*DNA replication, *HARBORS, *HISTONES, *CHROMATIN, *DNA sequencing
Abstract

Eukaryotic DNA replication is initiated at multiple chromosomal sites known as origins of replication that are specifically recognized by the origin recognition complex (ORC) containing multiple ATPase sites. In budding yeast, ORC binds to specific DNA sequences known as autonomously replicating sequences (ARSs) that are mostly nucleosome depleted. However, nucleosomes may still inhibit the licensing of some origins by occluding ORC binding and subsequent MCM helicase loading. Using purified proteins and single-molecule visualization, we find here that the ORC can eject histones from a nucleosome in an ATP-dependent manner. The ORC selectively evicts H2A-H2B dimers but leaves the (H3-H4)2 tetramer on DNA. It also discriminates canonical H2A from the H2A.Z variant, evicting the former while retaining the latter. Finally, the bromo-adjacent homology (BAH) domain of the Orc1 subunit is essential for ORC-mediated histone eviction. These findings suggest that the ORC is a bona fide nucleosome remodeler that functions to create a local chromatin environment optimal for origin activity. [ABSTRACT FROM AUTHOR]

Published
2022
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11. The DNA replication protein Orc1 from the yeast Torulaspora delbrueckii is required for heterochromatin formation but not as a silencer-binding protein.

Author

Maria, Haniam and Rusche, Laura N.

Subjects
*PROTEINS, *CHROMOSOMES, *BINDING sites, *DNA, *GENETIC mutation, *YEAST, *GENES, *SACCHAROMYCES
Abstract

To understand the process by which new protein functions emerge, we examined how the yeast heterochromatin protein Sir3 arose through gene duplication from the conserved DNA replication protein Orc1. Orc1 is a subunit of the origin recognition complex (ORC), which marks origins of DNA replication. In Saccharomyces cerevisiae, Orc1 also promotes heterochromatin assembly by recruiting the structural proteins Sir1-4 to silencer DNA. In contrast, the paralog of Orc1, Sir3, is a nucleosome-binding protein that spreads across heterochromatic loci in conjunction with other Sir proteins. We previously found that a nonduplicated Orc1 from the yeast Kluyveromyces lactis behaved like ScSir3 but did not have a silencer-binding function like ScOrc1. Moreover, K. lactis lacks Sir1, the protein that interacts directly with ScOrc1 at the silencer. Here, we examined whether the emergence of Sir1 coincided with Orc1 acting as a silencer-binding protein. In the nonduplicated species Torulaspora delbrueckii, which has an ortholog of Sir1 (TdKos3), we found that TdOrc1 spreads across heterochromatic loci independently of ORC, as ScSir3 and KlOrc1 do. This spreading is dependent on the nucleosome binding BAH domain of Orc1 and on Sir2 and Kos3. However, TdOrc1 does not have a silencer-binding function: T. delbrueckii silencers do not require ORC-binding sites to function, and Orc1 and Kos3 do not appear to interact. Instead, Orc1 and Kos3 both spread across heterochromatic loci with other Sir proteins. Thus, Orc1 and Sir1/Kos3 originally had different roles in heterochromatin formation than they do now in S. cerevisiae. [ABSTRACT FROM AUTHOR]

Published
2022
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12. Genome sequence of an extremely halophilic archaeon isolated from Permian Period halite, Salado Formation in New Mexico, USA: Halobacterium sp. strain NMX12-1.

Author

Soto L, DasSarma P, Anton BP, Vincze T, Verma I, Eralp B, Powers DW, Dozier BL, Roberts RJ, and DasSarma S

Abstract

Halobacterium sp. strain NMX12-1, an extremely halophilic Archaeon, was isolated from 250 million-year-old Salado Formation salt crystal in Carlsbad, New Mexico. Single-molecule real-time sequencing revealed a 3.2-Mbp genome with a 2.6-Mbp chromosome and five plasmids (234, 211, 119, 21, and 1.6-kbp). The GC-rich genome encodes an acidic proteome, characteristic of Haloarchaea.

Published
2024
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13. Four decades of Eukaryotic DNA replication: From yeast genetics to high-resolution cryo-EM structures of the replisome.

Author

Tye BK

Subjects
History, 20th Century, History, 21st Century, Cryoelectron Microscopy methods, DNA Replication, Saccharomyces cerevisiae genetics, Saccharomyces cerevisiae metabolism
Abstract

I had my eyes set on DNA replication research when I took my first molecular biology course in graduate school. My election to the National Academy of Sciences came just when I was retiring from active research. It gives me an opportunity to reflect on my personal journey in eukaryotic DNA replication research, which started as a thought experiment and culminated in witnessing the determination of the cryoelectron microscopic structure of the yeast replisome in the act of transferring histone-encoded epigenetic information at the replication fork. I would like to dedicate this inaugural article to my talented trainees and valuable collaborators in gratitude for the joy they gave me in this journey. I also want to thank my mentors who instilled in me the purpose of science. I hope junior scientists will not be disheartened by the marathon nature of research, but mindful enough to integrate and pause for other equally fun and meaningful activities of life into the marathon., Competing Interests: Competing interests statement:The author declares no competing interest.

Published
2024
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14. A Meier-Gorlin Syndrome Mutation Impairs the ORC1-Nucleosome Association

Author

Zhang, Wei, Sankaran, Saumya, Gozani, Or, and Song, Jikui

Subjects
Genetics, 2.1 Biological and endogenous factors, Aetiology, Congenital Microtia, DNA, Electrophoretic Mobility Shift Assay, Growth Disorders, Humans, Micrognathism, Mutation, Nucleosomes, Origin Recognition Complex, Patella, Chemical Sciences, Biological Sciences, Organic Chemistry
Abstract

Recent studies have identified several genetic mutations within the BAH domain of human Origin Recognition Complex subunit 1 (hORC1BAH), including the R105Q mutation, implicated in Meier-Gorlin Syndrome (MGS). However, the pathological role of the hORC1 R105Q mutation remains unclear. In this study, we have investigated the interactions of the hORC1BAH domain with histone H4K20me2, DNA, and the nucleosome core particle labeled with H4Kc20me2, a chemical analog of H4K20me2. Our study revealed a nucleosomal DNA binding site for hORC1BAH. The R105Q mutation reduces the hORC1BAH-DNA binding affinity, leading to impaired hORC1BAH-nucleosome interaction, which likely influences DNA replication initiation and MGS pathogenesis. This study provides an etiologic link between the hORC1 R105Q mutation and MGS.

Published
2015

15. Reports Outline Bioinformatics Study Results from Shanghai Jiao Tong University School of Medicine (Origin recognition complex 6 overexpression promotes growth of glioma cells).

Abstract

A recent study conducted by researchers at Shanghai Jiao Tong University School of Medicine explored the expression patterns, biological functions, and underlying mechanisms associated with ORC6 (origin recognition complex 6) in glioma, a type of brain tumor. The study found that ORC6 expression was significantly increased in human glioma tissues and correlated with poorer overall survival and higher tumor grade. Depleting ORC6 in glioma cells decreased cell viability and proliferation, disrupted cell cycle progression and mobility, and triggered apoptosis, while enhancing ORC6 expression augmented malignant behaviors. The study suggests that ORC6 may be a promising therapeutic target for glioma treatment. [Extracted from the article]

Published
2024

16. Dissection of Functional Domains of Orc1-2, the Archaeal Global DNA Damage-Responsive Regulator

Author

Xiaotong Liu, Mengmeng Sun, Ruyi Xu, Yulong Shen, Qihong Huang, Xu Feng, and Qunxin She

Subjects
origin recognition complex, DNA damage response, AAA+ ATPase, winged-helix domain, archaea, global regulator, Biology (General), QH301-705.5, Chemistry, QD1-999
Abstract

Orc1-2 is a non-initiator ortholog of archaeal/eukaryotic Orc1 proteins, which functions as a global regulator in DNA damage-responsive (DDR) expression. As for Orc1 initiators, the DDR regulator harbors an AAA+ ATPase domain, an Initiator-Specific Motif (ISM) and a winged-helix (wH) DNA-binding domain, which are also organized in a similar fashion. To investigate how Orc1-2 mediates the DDR regulation, the orc1-2 mutants inactivating each of these functional domains were constructed with Saccharolobus islandicus and genetically characterized. We found that disruption of each functional domain completely abolished the DDR regulation in these orc1-2 mutants. Strikingly, inactivation of ATP hydrolysis of Orc1-2 rendered an inviable mutant. However, the cell lethality can be suppressed by the deficiency of the DNA binding in the same protein, and it occurs independent of any DNA damage signal. Mutant Orc1-2 proteins were then obtained and investigated for DNA-binding in vitro. This revealed that both the AAA+ ATPase and the wH domains are involved in DNA-binding, where ISM and R381R383 in wH are responsible for specific DNA binding. We further show that Orc1-2 regulation occurs in two distinct steps: (a) eliciting cell division inhibition at a low Orc1-2 content, and this regulation is switched on by ATP binding and turned off by ATP hydrolysis; any failure in turning off the regulation leads to growth inhibition and cell death; (b) activation of the expression of DDR gene encoding DNA repair proteins at an elevated level of Orc1-2.

Published
2022
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20. The human origin recognition complex is essential for pre-RC assembly, mitosis, and maintenance of nuclear structure

Author

Hsiang-Chen Chou, Kuhulika Bhalla, Osama EL Demerdesh, Olaf Klingbeil, Kaarina Hanington, Sergey Aganezov, Peter Andrews, Habeeb Alsudani, Kenneth Chang, Christopher R Vakoc, Michael C Schatz, W Richard McCombie, and Bruce Stillman

Subjects
initiation of DNA replication, origin recognition complex, CDC6, pre-replicative complex, mitosis, CRISPR-Cas9 gene editing, Medicine, Science, Biology (General), QH301-705.5
Abstract

The origin recognition complex (ORC) cooperates with CDC6, MCM2-7, and CDT1 to form pre-RC complexes at origins of DNA replication. Here, using tiling-sgRNA CRISPR screens, we report that each subunit of ORC and CDC6 is essential in human cells. Using an auxin-inducible degradation system, we created stable cell lines capable of ablating ORC2 rapidly, revealing multiple cell division cycle phenotypes. The primary defects in the absence of ORC2 were cells encountering difficulty in initiating DNA replication or progressing through the cell division cycle due to reduced MCM2-7 loading onto chromatin in G1 phase. The nuclei of ORC2-deficient cells were also large, with decompacted heterochromatin. Some ORC2-deficient cells that completed DNA replication entered into, but never exited mitosis. ORC1 knockout cells also demonstrated extremely slow cell proliferation and abnormal cell and nuclear morphology. Thus, ORC proteins and CDC6 are indispensable for normal cellular proliferation and contribute to nuclear organization.

Published
2021
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21. A Meier-Gorlin syndrome mutation in a conserved C-terminal helix of Orc6 impedes origin recognition complex formation.

Author

Bleichert, Franziska, Balasov, Maxim, Chesnokov, Igor, Nogales, Eva, Botchan, Michael R, and Berger, James M

Subjects
Patella, Animals, Humans, Drosophila, Micrognathism, Growth Disorders, Microscopy, Electron, Mutation, Origin Recognition Complex, Congenital Microtia, D. melanogaster, DNA replication, Human, Meier-Gorlin syndrome, ORC, S. cerevisiae, origin licensing, origin recognition complex, Microscopy, Electron, Biochemistry and Cell Biology
Abstract

In eukaryotes, DNA replication requires the origin recognition complex (ORC), a six-subunit assembly that promotes replisome formation on chromosomal origins. Despite extant homology between certain subunits, the degree of structural and organizational overlap between budding yeast and metazoan ORC has been unclear. Using 3D electron microscopy, we determined the subunit organization of metazoan ORC, revealing that it adopts a global architecture very similar to the budding yeast complex. Bioinformatic analysis extends this conservation to Orc6, a subunit of somewhat enigmatic function. Unexpectedly, a mutation in the Orc6 C-terminus linked to Meier-Gorlin syndrome, a dwarfism disorder, impedes proper recruitment of Orc6 into ORC; biochemical studies reveal that this region of Orc6 associates with a previously uncharacterized domain of Orc3 and is required for ORC function and MCM2-7 loading in vivo. Together, our results suggest that Meier-Gorlin syndrome mutations in Orc6 impair the formation of ORC hexamers, interfering with appropriate ORC functions. DOI:http://dx.doi.org/10.7554/eLife.00882.001.

Published
2013

22. Humanizing the yeast origin recognition complex.

Author

Lee, Clare S. K., Cheung, Ming Fung, Li, Jinsen, Zhao, Yongqian, Lam, Wai Hei, Ho, Vincy, Rohs, Remo, Zhai, Yuanliang, Leung, Danny, and Tye, Bik-Kwoon

Subjects
YEAST, DNA insertion elements, BIOLOGICAL evolution, ORIGIN recognition complex, DNA replication, BINDING sites
Abstract

The Origin Recognition Complex (ORC) is an evolutionarily conserved six-subunit protein complex that binds specific sites at many locations to coordinately replicate the entire eukaryote genome. Though highly conserved in structure, ORC's selectivity for replication origins has diverged tremendously between yeasts and humans to adapt to vastly different life cycles. In this work, we demonstrate that the selectivity determinant of ORC for DNA binding lies in a 19-amino acid insertion helix in the Orc4 subunit, which is present in yeast but absent in human. Removal of this motif from Orc4 transforms the yeast ORC, which selects origins based on base-specific binding at defined locations, into one whose selectivity is dictated by chromatin landscape and afforded with plasticity, as reported for human. Notably, the altered yeast ORC has acquired an affinity for regions near transcriptional start sites (TSSs), which the human ORC also favors. In most model yeast species the Origin Recognition Complex (ORC) binds defined and species-specific base sequences while in humans what determines the binding appears to be more complex. Here the authors reveal that the yeast's ORC complex binding specificity is dependent on a 19-amino acid insertion helix in the Orc4 subunit which is lost in human. [ABSTRACT FROM AUTHOR]

Published
2021
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23. An androgen receptor-based signature to predict prognosis and identification of ORC1 as a therapeutical target for prostate adenocarcinoma.

Author

Li L, Chen D, Chen X, Zhu J, Bao W, Li C, Miao F, and Feng R

Subjects
Male, Humans, Receptors, Androgen genetics, Prostate metabolism, Drug Resistance, Neoplasm genetics, Origin Recognition Complex, Prostatic Neoplasms, Castration-Resistant drug therapy, Adenocarcinoma drug therapy, Benzamides, Nitriles, Phenylthiohydantoin
Abstract

Background: Aberrant activation of androgen receptor (AR) signaling plays a crucial role in the progression of prostate adenocarcinoma (PRAD) and contributes significantly to the development of enzalutamide resistance. In this study, we aimed to identify a novel AR-driven signature that can predict prognosis and endows potentially reveal novel therapeutic targets for PRAD., Methods: The Seurat package was used to preprocess the single-cell RNA sequencing (scRNA-seq). Differentially expressed genes were visualized using limma and pheamap packages. LASSO and multi-variate Cox regression models were established using glmnet package. The package "Consensus Cluster Plus" was utilized to perform the consensus clustering analysis. The biological roles of origin recognition complex subunit 1 (ORC1) in PRAD were determined by gain- and loss-of-function studies in vitro and in vivo ., Result: We characterized the scRNA-seq data from GSE99795 and identified 10 AR-associated genes (ARGs). The ARGs model was trained and validated in internal and external cohorts. The ARGs were identified as an independent hazard factor in PRAD and correlated with clinical risk characteristics. In addition, the ARGs were found to be correlated with somatic tumor mutation burden (TMB) levels. Two groups that have distinct prognostic and molecular features were identified through consensus clustering analysis. ORC1 was identified as a critical target among these ARGs, and it ORC1 promoted proliferation and stem-like properties of PRAD cells. Chromatin immunoprecipitation (ChIP)-qPCR assay confirmed that AR could directly bind the promoter of ORC1. Activated AR/ORC1 axis contributed to enzalutamide resistance, and targeting ORC1 rendered PRAD cells more susceptible to enzalutamide., Conclusions: This study defines an AR-driven signature that AR activates ORC1 expressions to promote PRAD progression and enzalutamide resistance, which may provide novel targets for PRAD treatment., Competing Interests: All authors declare that they have no competing interests., (© 2024 Li et al.)

Published
2024
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24. The Enigmatic Conservation of a Rap1 Binding Site in the Saccharomyces cerevisiae HMR-E Silencer

Author

Teytelman, Leonid, Nishimura, Erin A Osborne, Özaydin, Bilge, Eisen, Michael B, and Rine, Jasper

Subjects
Biological Sciences, Genetics, Human Genome, Generic health relevance, Binding Sites, DNA-Binding Proteins, Gene Silencing, Genes, Fungal, Genetic Loci, Origin Recognition Complex, Saccharomyces cerevisiae, Saccharomyces cerevisiae Proteins, Shelterin Complex, Telomere-Binding Proteins, Transcription Factors, silencing, sensu stricto, Rap1, genomics, transcription factors, Biochemistry and cell biology, Statistics
Abstract

Silencing at the HMR and HML loci in Saccharomyces cerevisiae requires recruitment of Sir proteins to the HML and HMR silencers. The silencers are regulatory sites flanking both loci and consisting of binding sites for the Rap1, Abf1, and ORC proteins, each of which also functions at hundreds of sites throughout the genome in processes unrelated to silencing. Interestingly, the sequence of the binding site for Rap1 at the silencers is distinct from the genome-wide binding profile of Rap1, being a weaker match to the consensus, and indeed is bound with low affinity relative to the consensus sequence. Remarkably, this low-affinity Rap1 binding site variant was conserved among silencers of the sensu stricto Saccharomyces species, maintained as a poor match to the Rap1 genome-wide consensus sequence in all of them. We tested multiple predictions about the possible role of this binding-site variant in silencing by substituting the native Rap1 binding site at the HMR-E silencer with the genome-wide consensus sequence for Rap1. Contrary to the predictions from the current models of Rap1, we found no influence of the Rap1 binding site version on the kinetics of establishing silencing, nor on the maintenance of silencing, nor the extent of silencing. We further explored implications of these findings with regard to prevention of ectopic silencing, and deduced that the selective pressure for the unprecedented conservation of this binding site variant may not be related to silencing.

Published
2012

25. The BAH domain of ORC1 links H4K20me2 to DNA replication licensing and Meier–Gorlin syndrome

Author

Kuo, Alex J, Song, Jikui, Cheung, Peggie, Ishibe-Murakami, Satoko, Yamazoe, Sayumi, Chen, James K, Patel, Dinshaw J, and Gozani, Or

Subjects
Biological Sciences, Genetics, Human Society, Animals, Carrier Proteins, Cell Cycle, Cell Line, Chromatin, Congenital Microtia, Crystallography, X-Ray, DNA Replication, Disease Models, Animal, Dwarfism, Ear, Growth Disorders, Histones, Humans, Lysine, Methylation, Micrognathism, Models, Molecular, Origin Recognition Complex, Patella, Protein Structure, Tertiary, Replication Origin, Zebrafish, Zebrafish Proteins, General Science & Technology
Abstract

The recognition of distinctly modified histones by specialized 'effector' proteins constitutes a key mechanism for transducing molecular events at chromatin to biological outcomes. Effector proteins influence DNA-templated processes, including transcription, DNA recombination and DNA repair; however, no effector functions have yet been identified within the mammalian machinery that regulate DNA replication. Here we show that ORC1--a component of ORC (origin of replication complex), which mediates pre-DNA replication licensing--contains a bromo adjacent homology (BAH) domain that specifically recognizes histone H4 dimethylated at lysine 20 (H4K20me2). Recognition of H4K20me2 is a property common to BAH domains present within diverse metazoan ORC1 proteins. Structural studies reveal that the specificity of the BAH domain for H4K20me2 is mediated by a dynamic aromatic dimethyl-lysine-binding cage and multiple intermolecular contacts involving the bound peptide. H4K20me2 is enriched at replication origins, and abrogating ORC1 recognition of H4K20me2 in cells impairs ORC1 occupancy at replication origins, ORC chromatin loading and cell-cycle progression. Mutation of the ORC1 BAH domain has been implicated in the aetiology of Meier-Gorlin syndrome (MGS), a form of primordial dwarfism, and ORC1 depletion in zebrafish results in an MGS-like phenotype. We find that wild-type human ORC1, but not ORC1-H4K20me2-binding mutants, rescues the growth retardation of orc1 morphants. Moreover, zebrafish depleted of H4K20me2 have diminished body size, mirroring the phenotype of orc1 morphants. Together, our results identify the BAH domain as a novel methyl-lysine-binding module, thereby establishing the first direct link between histone methylation and the metazoan DNA replication machinery, and defining a pivotal aetiological role for the canonical H4K20me2 mark, via ORC1, in primordial dwarfism.

Published
2012

26. The dynamic nature of the human origin recognition complex revealed through five cryoEM structures.

Author

Jaremko, Matt J., Kin Fan On, Thomas, Dennis R., Stillman, Bruce, and Joshua-Tor, Leemor

Subjects
*HUMAN origins, *DNA replication, *DNA helicases, *CELL cycle proteins, *ORIGIN recognition complex, *DNA
Abstract

Genome replication is initiated from specific origin sites established by dynamic events. The Origin Recognition Complex (ORC) is necessary for orchestrating the initiation process by binding to origin DNA, recruiting CDC6, and assembling the MCM replicative helicase on DNA. Here we report five cryoEM structures of the human ORC (HsORC) that illustrate the native flexibility of the complex. The absence of ORC1 revealed a compact, stable complex of ORC2-5. Introduction of ORC1 opens the complex into several dynamic conformations. Two structures revealed dynamic movements of the ORC1 AAA+ and ORC2 winged-helix domains that likely impact DNA incorporation into the ORC core. Additional twist and pinch motions were observed in an open ORC conformation revealing a hinge at the ORC5-ORC3 interface that may facilitate ORC binding to DNA. Finally, a structure of ORC was determined with endogenous DNA bound in the core revealing important differences between human and yeast origin recognition. [ABSTRACT FROM AUTHOR]

Published
2020
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27. Structural mechanism of helicase loading onto replication origin DNA by ORC-Cdc6.

Author

Zuanning Yuan, Schneider, Sarah, Dodd, Thomas, Riera, Alberto, Lin Bai, Chunli Yan, Magdalou, Indiana, Ivanov, Ivaylo, Stillman, Bruce, Huilin Li, and Speck, Christian

Subjects
*DNA replication, *DNA helicases, *DNA
Abstract

DNA replication origins serve as sites of replicative helicase loading. In all eukaryotes, the six-subunit origin recognition complex (Orc1-6; ORC) recognizes the replication origin. During late M-phase of the cell-cycle, Cdc6 binds to ORC and the ORC–Cdc6 complex loads in a multistep reaction and, with the help of Cdt1, the core Mcm2-7 helicase onto DNA. A key intermediate is the ORC–Cdc6–Cdt1–Mcm2-7 (OCCM) complex in which DNA has been already inserted into the central channel of Mcm2-7. Until now, it has been unclear how the origin DNA is guided by ORC–Cdc6 and inserted into the Mcm2-7 hexamer. Here, we truncated the C-terminal winged-helix-domain (WHD) of Mcm6 to slow down the loading reaction, thereby capturing two loading intermediates prior to DNA insertion in budding yeast. In "semi-attached OCCM," the Mcm3 and Mcm7 WHDs latch onto ORC–Cdc6 while the main body of the Mcm2-7 hexamer is not connected. In "pre-insertion OCCM," the main body of Mcm2-7 docks onto ORC–Cdc6, and the origin DNA is bent and positioned adjacent to the open DNA entry gate, poised for insertion, at the Mcm2–Mcm5 interface. We used molecular simulations to reveal the dynamic transition from preloading conformers to the loaded conformers in which the loading of Mcm2-7 on DNA is complete and the DNA entry gate is fully closed. Our work provides multiple molecular insights into a key event of eukaryotic DNA replication. [ABSTRACT FROM AUTHOR]

Published
2020
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28. Origin Recognition Complex (ORC) Evolution Is Influenced by Global Gene Duplication/Loss Patterns in Eukaryotic Genomes.

Author

Ocaña-Pallarès, Eduard, Vergara, Zaida, Desvoyes, Bénédicte, Tejada-Jimenez, Manuel, Romero-Jurado, Ainoa, Galván, Aurora, Fernández, Emilio, Ruiz-Trillo, Iñaki, and Gutierrez, Crisanto

Subjects
*EUKARYOTIC genomes, *CHROMOSOME duplication, *GENOME size, *CHLAMYDOMONAS reinhardtii, *ORIGIN recognition complex
Abstract

The conservation of orthologs of most subunits of the origin recognition complex (ORC) has served to propose that the whole complex is common to all eukaryotes. However, various uncertainties have arisen concerning ORC subunit composition in a variety of lineages. Also, it is unclear whether the ancestral diversification of ORC in eukaryotes was accompanied by the neofunctionalization of some subunits, for example, role of ORC1 in centriole homeostasis. We have addressed these questions by reconstructing the distribution and evolutionary history of ORC1-5/CDC6 in a taxon-rich eukaryotic data set. First, we identified ORC subunits previously undetected in divergent lineages, which allowed us to propose a series of parsimonious scenarios for the origin of this multiprotein complex. Contrary to previous expectations, we found a global tendency in eukaryotes to increase or decrease the number of subunits as a consequence of genome duplications or streamlining, respectively. Interestingly, parasites show significantly lower number of subunits than free-living eukaryotes, especially those with the lowest genome size and gene content metrics. We also investigated the evolutionary origin of the ORC1 role in centriole homeostasis mediated by the PACT region in human cells. In particular, we tested the consequences of reducing ORC1 levels in the centriole-containing green alga Chlamydomonas reinhardtii. We found that the proportion of centrioles to flagella and nuclei was not dramatically affected. This, together with the PACT region not being significantly more conserved in centriole-bearing eukaryotes, supports the notion that this neofunctionalization of ORC1 would be a recent acquisition rather than an ancestral eukaryotic feature. [ABSTRACT FROM AUTHOR]

Published
2020
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30. The origin recognition core complex regulates dendrite and spine development in postmitotic neurons

Author

Huang, Zhen, Zang, Keling, and Reichardt, Louis F

Subjects
Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Neurosciences, Genetics, Underpinning research, 1.1 Normal biological development and functioning, Adenosine Triphosphatases, Amino Acid Motifs, Animals, Cell Membrane, DNA Replication, Dendritic Spines, Gene Expression Regulation, Mice, Mitosis, Mutant Proteins, Origin Recognition Complex, Protein Subunits, Pseudopodia, RNA, Messenger, Rats, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences
Abstract

The origin recognition complex (ORC) ensures exactly one round of genome replication per cell cycle through acting as a molecular switch that precisely controls the assembly, firing, and inactivation of the replication initiation machinery. Recent data indicate that it may also coordinate the processes of mitosis and cytokinesis and ensure the proper distribution of replicated genome to daughter cells. We have found that the ORC core subunits are highly expressed in the nervous system. They are selectively localized to the neuronal somatodendritic compartment and enriched in the membrane fraction. siRNA knockdown of ORC subunits dramatically reduced dendritic branch formation and severely impeded dendritic spine emergence. Expression of ORC ATPase motif mutants enhanced the branching of dendritic arbors. The ORC core complex thus appears to have a novel role in regulating dendrite and dendritic spine development in postmitotic neurons.

Published
2005

32. DNA replication licensing and human cell proliferation.

Author

Stoeber, Kai, Tlsty, Thea D, Happerfield, Lisa, Thomas, Geraldine A, Romanov, Sergei, Bobrow, Lynda, Williams, E Dillwyn, and Williams, Gareth H

Subjects
Biochemistry and Cell Biology, Biological Sciences, Genetics, Cancer, Breast Cancer, 1.1 Normal biological development and functioning, Aetiology, Underpinning research, 2.1 Biological and endogenous factors, Generic health relevance, Animals, Cell Cycle, Cell Cycle Proteins, Cell Differentiation, Cell Division, Cell Line, Cell-Free System, Cellular Senescence, DNA Replication, DNA-Binding Proteins, Fluorescent Antibody Technique, G1 Phase, HeLa Cells, Humans, Mice, Microscopy, Confocal, Minichromosome Maintenance Complex Component 2, Nuclear Proteins, Origin Recognition Complex, Schizosaccharomyces pombe Proteins, Hela Cells, Non-programmatic, Medical and Health Sciences, Developmental Biology, Biochemistry and cell biology
Abstract

The convergence point of growth regulatory pathways that control cell proliferation is the initiation of genome replication, the core of which is the assembly of pre-replicative complexes resulting in chromatin being "licensed" for DNA replication in the subsequent S phase. We have analysed regulation of the pre-replicative complex proteins ORC, Cdc6, and MCM in cycling and non-proliferating quiescent, differentiated and replicative senescent human cells. Moreover, a human cell-free DNA replication system has been exploited to study the replicative capacity of nuclei and cytosolic extracts prepared from these cells. These studies demonstrate that downregulation of the Cdc6 and MCM constituents of the replication initiation pathway is a common downstream mechanism for loss of proliferative capacity in human cells. Furthermore, analysis of MCM protein expression in self-renewing, stable and permanent human tissues shows that the three classes of tissue have developed very different growth control strategies with respect to replication licensing. Notably, in breast tissue we found striking differences between the proportion of mammary acinar cells that express MCM proteins and those labelled with conventional proliferation markers, raising the intriguing possibility that progenitor cells of some tissues are held in a prolonged G1 phase or "in-cycle arrest". We conclude that biomarkers for replication-licensed cells detect, in addition to actively proliferating cells, cells with growth potential, a concept that has major implications for developmental and cancer biology.

Published
2001

33. The Origin Recognition Complex: From Origin Selection to Replication Licensing in Yeast and Humans.

Author

Tye BK and Zhai Y

Abstract

Understanding human DNA replication through the study of yeast has been an extremely fruitful journey. The minichromosome maintenance (MCM) 2-7 genes that encode the catalytic core of the eukaryotic replisome were initially identified through forward yeast genetics. The origin recognition complexes (ORC) that load the MCM hexamers at replication origins were purified from yeast extracts. We have reached an age where high-resolution cryoEM structures of yeast and human replication complexes can be compared side-by-side. Their similarities and differences are converging as alternative strategies that may deviate in detail but are shared by both species.

Published
2023
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34. Investigation of the Interaction of Human Origin Recognition Complex Subunit 1 with G-Quadruplex DNAs of Human c-myc Promoter and Telomere Regions

Author

Afaf Eladl, Yudai Yamaoki, Shoko Hoshina, Haruka Horinouchi, Keiko Kondo, Shou Waga, Takashi Nagata, and Masato Katahira

Subjects
origin recognition complex, G-quadruplex, DNA replication, replication origin, NMR, structure, Biology (General), QH301-705.5, Chemistry, QD1-999
Abstract

Origin recognition complex (ORC) binds to replication origins in eukaryotic DNAs and plays an important role in replication. Although yeast ORC is known to sequence-specifically bind to a replication origin, how human ORC recognizes a replication origin remains unknown. Previous genome-wide studies revealed that guanine (G)-rich sequences, potentially forming G-quadruplex (G4) structures, are present in most replication origins in human cells. We previously suggested that the region comprising residues 413–511 of human ORC subunit 1, hORC1413–511, binds preferentially to G-rich DNAs, which form a G4 structure in the absence of hORC1413–511. Here, we investigated the interaction of hORC1413-511 with various G-rich DNAs derived from human c-myc promoter and telomere regions. Fluorescence anisotropy revealed that hORC1413–511 binds preferentially to DNAs that have G4 structures over ones having double-stranded structures. Importantly, circular dichroism (CD) and nuclear magnetic resonance (NMR) showed that those G-rich DNAs retain the G4 structures even after binding with hORC1413–511. NMR chemical shift perturbation analyses revealed that the external G-tetrad planes of the G4 structures are the primary binding sites for hORC1413–511. The present study suggests that human ORC1 may recognize replication origins through the G4 structure.

Published
2021
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35. Replication of the Plant Genome

Author

Gutierrez, Crisanto, Sequeira-Mendes, Joana, Aragüez, Irene, Tester, Mark, Series editor, Jorgensen, Richard, Series editor, and Howell, Stephen H., editor

Published
2014
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37. Specific basic patch‐dependent multimerization of Saccharomyces cerevisiae ORC on single‐stranded DNA promotes ATP hydrolysis.

Author

Kawakami, Hironori, Muraoka, Ryuya, Ohashi, Eiji, Kawabata, Kenta, Kanamoto, Shota, Chichibu, Takeaki, Tsurimoto, Toshiki, and Katayama, Tsutomu

Subjects
*DNA replication, *SINGLE-stranded DNA, *SACCHAROMYCES cerevisiae, *ADENINE nucleotides, *EUKARYOTIC cells, *HYDROLYSIS, *DNA
Abstract

Replication initiation at specific genomic loci dictates precise duplication and inheritance of genetic information. In eukaryotic cells, ATP‐bound origin recognition complexes (ORCs) stably bind to double‐stranded (ds) DNA origins to recruit the replicative helicase onto the origin DNA. To achieve these processes, an essential region of the origin DNA must be recognized by the eukaryotic origin sensor (EOS) basic patch within the disordered domain of the largest ORC subunit, Orc1. Although ORC also binds single‐stranded (ss) DNA in an EOS‐independent manner, it is unknown whether EOS regulates ORC on ssDNA. We found that, in budding yeast, ORC multimerizes on ssDNA in vitro independently of adenine nucleotides. We also found that the ORC multimers form in an EOS‐dependent manner and stimulate the ORC ATPase activity. An analysis of genomics data supported the idea that ORC‐ssDNA binding occurs in vivo at specific genomic loci outside of replication origins. These results suggest that EOS function is differentiated by ORC‐bound ssDNA, which promotes ORC self‐assembly and ATP hydrolysis. These mechanisms could modulate ORC activity at specific genomic loci and could be conserved among eukaryotes. [ABSTRACT FROM AUTHOR]

Published
2019
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38. NMR characterization of the structure of the intrinsically disordered region of human origin recognition complex subunit 1, hORC1, and of its interaction with G-quadruplex DNAs.

Author

Eladl, Afaf, Yamaoki, Yudai, Kamba, Keisuke, Hoshina, Shoko, Horinouchi, Haruka, Kondo, Keiko, Waga, Shou, Nagata, Takashi, and Katahira, Masato

Subjects
*QUADRUPLEX nucleic acids, *DNA replication, *HUMAN origins, *LYSINE, *NUCLEAR magnetic resonance, *MAGNETIC circular dichroism, *DNA
Abstract

Human origin recognition complex (hORC) binds to the DNA replication origin and then initiates DNA replication. However, hORC does not exhibit DNA sequence-specificity and how hORC recognizes the replication origin on genomic DNA remains elusive. Previously, we found that hORC recognizes G-quadruplex structures potentially formed near the replication origin. Then, we showed that hORC subunit 1 (hORC1) preferentially binds to G-quadruplex DNAs using a hORC1 construct comprising residues 413 to 511 (hORC1413−511). Here, we investigate the structural characteristics of hORC1413−511 in its free and complex forms with G-quadruplex DNAs. Circular dichroism and nuclear magnetic resonance (NMR) spectroscopic studies indicated that hORC1413−511 is disordered except for a short α-helical region in both the free and complex forms. NMR chemical shift perturbation (CSP) analysis suggested that basic residues, arginines and lysines, and polar residues, serines and threonines, are involved in the G-quadruplex DNA binding. Then, this was confirmed by mutation analysis. Interestingly, CSP analysis indicated that hORC1413−511 binds to both parallel- and (3 + 1)-type G-quadruplex DNAs using the same residues, and thereby in the same manner. Our study suggests that hORC1 uses its intrinsically disordered G-quadruplex binding region to recognize parallel-type and (3 + 1)-type G-quadruplex structures at replication origin. • hORC1 binds to G-quadruplex (G4) DNAs. • The G4 DNA-binding region of hORC1, hORC1413−511, is intrinsically disordered. • hORC1413−511 remains disordered upon binding to G4 DNAs. • Interaction of basic and polar residues of hORC1413−511 with G4 DNAs is suggested. • hORC1413−511 binds to both parallel and (3 + 1)-type G4s in the same manner. [ABSTRACT FROM AUTHOR]

Published
2023
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39. The consequences of differential origin licensing dynamics in distinct chromatin environments

Author

Jeremy E. Purvis, Liu Mei, Song E, Katarzyna M. Kedziora, and Cook Jg

Subjects
DNA Replication, Euchromatin, Minichromosome Maintenance Proteins, DNA damage, Chemistry, Heterochromatin, Cell Cycle, DNA replication, Origin Recognition Complex, Cell Cycle Proteins, Replication Origin, Cell cycle, Genome, Chromatin, Cell biology, Eukaryotic Cells, Gene duplication, Genetics, Animals, Humans
Abstract

Eukaryotic chromosomes contain regions of varying accessibility, yet DNA replication factors must access all regions. The first replication step is loading MCM complexes to license replication origins during the G1 cell cycle phase. It is not yet known how mammalian MCM complexes are adequately distributed to both accessible euchromatin regions and less accessible heterochromatin regions. To address this question, we combined time-lapse live-cell imaging with immunofluorescence imaging of single human cells to quantify the relative rates of MCM loading in euchromatin and heterochromatin throughout G1. We report here that MCM loading in euchromatin is faster than that in heterochromatin in early G1, but surprisingly, heterochromatin loading accelerates relative to euchromatin loading in middle and late G1. This differential acceleration allows both chromatin types to begin S phase with similar concentrations of loaded MCM. The different loading dynamics require ORCA-dependent differences in origin recognition complex distribution. A consequence of heterochromatin licensing dynamics is that cells experiencing a truncated G1 phase from premature cyclin E expression enter S phase with underlicensed heterochromatin, and DNA damage accumulates preferentially in heterochromatin in the subsequent S/G2 phase. Thus, G1 length is critical for sufficient MCM loading, particularly in heterochromatin, to ensure complete genome duplication and to maintain genome stability.In this study the authors have, for the first time, quantified DNA replication origin licensing dynamics and distribution in single cells at subnuclear resolution. The cell cycle and DNA replication fields have long appreciated that origin licensing is both absolutely essential for replication and that licensing is strictly confined to G1 phase. The biochemical process of origin licensing- which is the DNA loading of MCM complexes- is known in considerable detail. What has never been explored in any system, is the dynamics of origin licensing itself. Here the authors define the dynamics of human MCM loading at different times within G1 in both euchromatin and heterochromatin, and explore the consequences of those dynamics for genome stability.

Published
2022

41. Sulfolobus islandicus Employs Orc1-2-Mediated DNA Damage Response in Defense against Infection by SSV2

Author

Shaoying Wang, Qunxin She, and Li Huang

Subjects
DNA Repair, Ultraviolet Rays, Immunology, Origin Recognition Complex, Virus Replication, Microbiology, 4-Nitroquinoline-1-oxide, Sulfolobus, Virus-Cell Interactions, Gene Expression Regulation, Virology, Insect Science, Fuselloviridae, DNA Damage
Abstract

All living organisms have evolved DNA damage response (DDR) strategies in coping with threats to the integrity of their genome. In response to DNA damage, Sulfolobus islandicus activates its DDR network in which Orc1-2, an ortholog of the archaeal Orc1/Cdc6 superfamily proteins, plays a central regulatory role. Here, we show that pretreatment with UV irradiation reduced virus genome replication in S. islandicus infected with the fusellovirus SSV2. Like treatment with UV or the DNA-damaging agent 4-nitroquinoline-1-oxide (NQO), infection with SSV2 facilitated the expression of orc1-2 and significantly raised the cellular level of Orc1-2. The inhibitory effect of UV irradiation on the virus DNA level was no longer apparent in the infected culture of an S. islandicus orc1-2 deletion mutant strain. On the other hand, the overexpression of orc1-2 decreased virus genomic DNA by ~10(2)-fold compared to that in the parent strain. Furthermore, as part of the Orc1-2-mediated DDR response genes for homologous recombination repair (HRR), cell aggregation and intercellular DNA transfer were upregulated, whereas genes for cell division were downregulated. However, the HRR pathway remained functional in host inhibition of SSV2 genome replication in the absence of UpsA, a subunit of pili essential for intercellular DNA transfer. In agreement with this finding, lack of the general transcriptional activator TFB3, which controls the expression of the ups genes, only moderately affected SSV2 genome replication. Our results demonstrate that infection of S. islandicus by SSV2 triggers the host DDR pathway that, in return, suppresses virus genome replication. IMPORTANCE Extremophiles thrive in harsh habitats and thus often face a daunting challenge to the integrity of their genome. How these organisms respond to virus infection when their genome is damaged remains unclear. We found that the thermophilic archaeon Sulfolobus islandicus became more inhibitory to genome replication of the virus SSV2 after preinfection UV irradiation than without the pretreatment. On the other hand, like treatment with UV or other DNA-damaging agents, infection of S. islandicus by SSV2 triggers the activation of Orc1-2-mediated DNA damage response, including the activation of homologous recombination repair, cell aggregation and DNA import, and the repression of cell division. The inhibitory effect of pretreatment with UV irradiation on SSV2 genome replication was no longer observed in an S. islandicus mutant lacking Orc1-2. Our results suggest that DNA damage response is employed by S. islandicus as a strategy to defend against virus infection.

Published
2022

47. Genomic analysis finds no evidence of canonical eukaryotic DNA processing complexes in a free-living protist

Author

Dayana E. Salas-Leiva, Bruce A. Curtis, Zhenzhen Yi, Martin Kolisko, Shelby K Williams, Jon Jerlström-Hultqvist, Joan Salas-Leiva, Lucie Gallot-Lavallée, Geert J. P. L. Kops, John M. Archibald, Alastair G. B. Simpson, Andrew J. Roger, Eelco C. Tromer, Cell Biochemistry, Salas-Leiva, Dayana E [0000-0003-2356-3351], Tromer, Eelco C [0000-0003-3540-7727], Curtis, Bruce A [0000-0001-6729-2173], Jerlström-Hultqvist, Jon [0000-0002-7992-7970], Kolisko, Martin [0000-0003-0600-1867], Yi, Zhenzhen [0000-0002-0693-9989], Salas-Leiva, Joan S [0000-0002-4141-140X], Gallot-Lavallée, Lucie [0000-0001-6763-3388], Williams, Shelby K [0000-0001-7005-5208], Kops, Geert JPL [0000-0003-3555-5295], Archibald, John M [0000-0001-7255-780X], Simpson, Alastair GB [0000-0002-4133-1709], Roger, Andrew J [0000-0003-1370-9820], Apollo - University of Cambridge Repository, Hubrecht Institute for Developmental Biology and Stem Cell Research, Salas-Leiva, Dayana E. [0000-0003-2356-3351], Tromer, Eelco C. [0000-0003-3540-7727], Curtis, Bruce A. [0000-0001-6729-2173], Salas-Leiva, Joan S. [0000-0002-4141-140X], Williams, Shelby K. [0000-0001-7005-5208], Kops, Geert J. P. L. [0000-0003-3555-5295], Archibald, John M. [0000-0001-7255-780X], Simpson, Alastair G. B. [0000-0002-4133-1709], and Roger, Andrew J. [0000-0003-1370-9820]

Subjects
Metamonad, 631/181, Evolution, Science, General Physics and Astronomy, Sequence assembly, Eukaryotic DNA replication, 45/23, Biology, medicine.disease_cause, Microbiology, General Biochemistry, Genetics and Molecular Biology, Article, Eukaryotic Cells/metabolism, chemistry.chemical_compound, medicine, DNA/metabolism, Animals, Parasites, 631/326, 49/91, Comparative genomics, Multidisciplinary, Genome, Kinetochore, Protist, Eukaryota, Proteins, General Chemistry, DNA, Genomics, biology.organism_classification, Biological Evolution, Parasites/genetics, Eukaryota/genetics, Eukaryotic Cells, chemistry, Evolutionary biology, FOS: Biological sciences, Proteins/genetics, Origin recognition complex
Abstract

Funder: Canadian Institutes of Health Research (Grant: FRN-142349) Natural Sciences and Engineering Research Council of Canada (Grant: RGPIN 05871-2014), Cells replicate and segregate their DNA with precision. Previous studies showed that these regulated cell-cycle processes were present in the last eukaryotic common ancestor and that their core molecular parts are conserved across eukaryotes. However, some metamonad parasites have secondarily lost components of the DNA processing and segregation apparatuses. To clarify the evolutionary history of these systems in these unusual eukaryotes, we generated a genome assembly for the free-living metamonad Carpediemonas membranifera and carried out a comparative genomics analysis. Here, we show that parasitic and free-living metamonads harbor an incomplete set of proteins for processing and segregating DNA. Unexpectedly, Carpediemonas species are further streamlined, lacking the origin recognition complex, Cdc6 and most structural kinetochore subunits. Carpediemonas species are thus the first known eukaryotes that appear to lack this suite of conserved complexes, suggesting that they likely rely on yet-to-be-discovered or alternative mechanisms to carry out these fundamental processes.

Published
2021

49. Origin recognition complex subunit 1(ORC1) is a potential biomarker and therapeutic target in cancer.

Author

Wu L, Chen H, and Yang C

Subjects
Humans, Biomarkers, Cell Cycle Proteins, Clinical Relevance, Databases, Factual, Nuclear Proteins, Prognosis, Neoplasms diagnosis, Neoplasms genetics, Origin Recognition Complex
Abstract

Background: The origin recognition complex 1 (ORC1) is a large subunit of the origin recognition complex and acts as the master subunit of the precoding complex., Objective: To explore potential function and clinical significance of ORC1 in cancers., Methods: The expression level of ORC1 in different types of tumor tissues and matched normal tissues were detected by The Cancer Genome Atlas (TCGA) and validated by datasets from the gene expression omnibus (GEO) database. The association between ORC1 expression and infiltration levels of immune cell was analyzed. ORC1 and its co-expression genes were subjected to enrichment analysis to explore potential mechanisms in cancers, and the protein-protein interaction (PPI) network was constructed. Finally, the expression of ORC1 in tumor tissue and adjacent tissue was verified by immunohistochemistry (IHC)., Results: ORC1 was highly expressed in the majority of tumors, and the expression level of ORC1 was associated with the pathological stages of ACC, LUAD, OV and SKCM. ORC1 was closely related with poor prognosis in ACC, LIHC, PAAD, READ and THCA. ORC1 in ACC and KICH was positively correlated with the infiltration level of immune cells while it was negatively correlated with the infiltration level of immune cells in THYM. Co-expression network analysis showed that CDCA3, GSG2, KIF2C, NCAPH and PLK1 were positively correlated with ORC1 in cancer, and enrichment analysis showed a correlation with cytosol, ATP binding and cell division. The expression of ORC1 in UCEC and KICH was higher than that in the adjacent tissues., Conclusion: ORC1 over-expressed in most tumors and could be severed as a novel biomarker for diagnosis. This study revealed that ORC1 might inhibit tumor immunity and might be a potential therapeutic target in cancers., (© 2023. BioMed Central Ltd., part of Springer Nature.)

Published
2023
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50. Multi-omics analysis reveals the involvement of origin recognition complex subunit 6 in tumor immune regulation and malignant progression.

Author

Zhu J, Chen Q, Zeng L, Gao H, Wu T, He Y, Xu J, Pang J, Peng J, Deng Y, Han Y, and Yi W

Subjects
Humans, Immunosuppressive Agents, Multiomics, Tumor Microenvironment, Carcinoma, Hepatocellular genetics, Glioma genetics, Liver Neoplasms genetics, Origin Recognition Complex
Abstract

Background: Origin recognition complex 6 ( ORC6 ) is one of the six highly conserved subunit proteins required for DNA replication and is essential for maintaining genome stability during cell division. Recent research shows that ORC6 regulates the advancement of multiple cancers; however, it remains unclear what regulatory impact it has on the tumor immune microenvironment., Methods: Unpaired Wilcoxon rank sum and signed rank tests were used to analyze the differences in the expression of ORC6 in normal tissues and corresponding tumor tissues. Multiple online databases have evaluated the genetic alterations, protein expression and localization, and clinical relevance of ORC6 . To evaluate the potential prognostic impact and diagnostic significance of ORC6 expression, we carried out log-rank, univariate Cox regression, and receiver operating characteristic curve analysis. The ICGC-LIRI-JP cohort, CGGA-301 cohort, CGGA-325 cohort, CGGA-693 cohort, and GSE13041 cohort were used for external validation of the study findings. The associations between ORC6 expression and immune cell infiltration, immune checkpoint expression, and immunotherapy cohorts was further analyzed. To explore the functional and signaling pathways related to ORC6 expression, gene set enrichment analysis was performed. To clarify the expression and function of ORC6 in hepatocellular carcinoma (LIHC) and glioma, we conducted in vitro experiments., Results: Expression of ORC6 is upregulated in the majority of cancer types and is associated with poor patient prognosis, notably in cases of LIHC and gliomas. In addition, ORC6 may be involved in multiple signaling pathways related to cancer progression and immune regulation. High expression of ORC6 correlates with an immunosuppressive state in the tumor microenvironment. The results of further immunotherapy cohort analysis suggested that patients in the ORC6 high-expression group benefited from immunotherapy. Inhibiting ORC6 expression suppressed the proliferative and migratory abilities of LIHC and glioma cells., Conclusion: High expression of ORC6 may be used as a biomarker to predict the poor prognosis of most tumor patients. The high expression of ORC6 may be involved in the regulation of the tumor immunosuppressive environment, and it is expected to become a molecular target for inhibiting tumor progression., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Zhu, Chen, Zeng, Gao, Wu, He, Xu, Pang, Peng, Deng, Han and Yi.)

Published
2023
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