Your search keyword '"Histone variants"' showing total 834 results

1. Roles of Histone H2B, H3 and H4 Variants in Cancer Development and Prognosis.

Author

Lai, Po Man, Gong, Xiaoxiang, and Chan, Kui Ming

Subjects

*X chromosome, *CELL cycle, *GENETIC transcription regulation, *HISTONES, *CHROMATIN, *DNA repair

Abstract

Histone variants are the paralogs of core histones (H2A, H2B, H3 and H4). They are stably expressed throughout the cell cycle in a replication-independent fashion and are capable of replacing canonical counterparts under different fundamental biological processes. Variants have been shown to take part in multiple processes, including DNA damage repair, transcriptional regulation and X chromosome inactivation, with some of them even specializing in lineage-specific roles like spermatogenesis. Several reports have recently identified some unprecedented variants from different histone families and exploited their prognostic value in distinct types of cancer. Among the four classes of canonical histones, the H2A family has the greatest number of variants known to date, followed by H2B, H3 and H4. In our prior review, we focused on summarizing all 19 mammalian histone H2A variants. Here in this review, we aim to complete the full summary of the roles of mammalian histone variants from the remaining histone H2B, H3, and H4 families, along with an overview of their roles in cancer biology and their prognostic value in a clinical context. [ABSTRACT FROM AUTHOR]

Published

2024

2. Arabidopsis Histone Variant H2A.X Functions in the DNA Damage-Coupling Abscisic Acid Signaling Pathway.

Author

Guo, Peng, Wang, Tian-Jing, Wang, Shuang, Peng, Xiaoyuan, Kim, Dae Heon, and Liu, Yutong

Subjects

*DNA repair, *DOUBLE-strand DNA breaks, *PLANT hormones, *ARABIDOPSIS thaliana, *GENETIC markers, *ABSCISIC acid

Abstract

Environmental variations initiate chromatin modifications, leading to the exchange of histone subunits or the repositioning of nucleosomes. The phosphorylated histone variant H2A.X (γH2A.X) is recognized for the formation of foci that serve as established markers of DNA double-strand breaks (DSBs). Nevertheless, the precise roles of H2A.X in the cellular response to genotoxic stress and the impact of the plant hormone abscisic acid (ABA) remain incompletely understood. In this investigation, we implemented CRISPR/Cas9 technology to produce loss-of-function mutants of AtHTA3 and AtHTA5 in Arabidopsis. The phenotypes of the athta3 and athta5 single mutants were nearly identical to those of the wild-type Col-0. Nevertheless, the athta3 athta5 double mutants exhibited aberrant embryonic development, increased sensitivity to DNA damage, and higher sensitivity to ABA. The RT-qPCR analysis indicates that AtHTA3 and AtHTA5 negatively regulate the expression of AtABI3, a fundamental regulator in the ABA signaling pathway. Subsequent investigation demonstrated that AtABI3 participates in the genotoxic stress response by influencing the expression of DNA damage response genes, such as AtBRCA1, AtRAD51, and AtWEE1. Our research offers new insights into the role of H2A.X in the genotoxic and ABA responses of Arabidopsis. [ABSTRACT FROM AUTHOR]

Published

2024

3. The Function of H2A Histone Variants and Their Roles in Diseases.

Author

Yin, Xuemin, Zeng, Dong, Liao, Yingjun, Tang, Chengyuan, and Li, Ying

Subjects

*GENETIC regulation, *DNA damage, *EPIGENETICS, *GENETIC transcription, *EMBRYOLOGY, *DNA repair

Abstract

Epigenetic regulation, which is characterized by reversible and heritable genetic alterations without changing DNA sequences, has recently been increasingly studied in diseases. Histone variant regulation is an essential component of epigenetic regulation. The substitution of canonical histones by histone variants profoundly alters the local chromatin structure and modulates DNA accessibility to regulatory factors, thereby exerting a pivotal influence on gene regulation and DNA damage repair. Histone H2A variants, mainly including H2A.Z, H2A.B, macroH2A, and H2A.X, are the most abundant identified variants among all histone variants with the greatest sequence diversity. Harboring varied chromatin occupancy and structures, histone H2A variants perform distinct functions in gene transcription and DNA damage repair. They are implicated in multiple pathophysiological mechanisms and the emergence of different illnesses. Cancer, embryonic development abnormalities, neurological diseases, metabolic diseases, and heart diseases have all been linked to histone H2A variant alterations. This review focuses on the functions of H2A histone variants in mammals, including H2A.Z, H2A.B, macroH2A, and H2A.X, and their current roles in various diseases. [ABSTRACT FROM AUTHOR]

Published

2024

4. Emerging roles of plant transcriptional gene silencing under heat.

Author

Torres, José Roberto and Sanchez, Diego H.

Subjects

*PLANT gene silencing, *PLANT physiology, *NUCLEIC acids, *GENE silencing, *REGULATOR genes

Abstract

SUMMARY: Plants continuously endure unpredictable environmental fluctuations that upset their physiology, with stressful conditions negatively impacting yield and survival. As a contemporary threat of rapid progression, global warming has become one of the most menacing ecological challenges. Thus, understanding how plants integrate and respond to elevated temperatures is crucial for ensuring future crop productivity and furthering our knowledge of historical environmental acclimation and adaptation. While the canonical heat‐shock response and thermomorphogenesis have been extensively studied, evidence increasingly highlights the critical role of regulatory epigenetic mechanisms. Among these, the involvement under heat of heterochromatic suppression mediated by transcriptional gene silencing (TGS) remains the least understood. TGS refers to a multilayered metabolic machinery largely responsible for the epigenetic silencing of invasive parasitic nucleic acids and the maintenance of parental imprints. Its molecular effectors include DNA methylation, histone variants and their post‐translational modifications, and chromatin packing and remodeling. This work focuses on both established and emerging insights into the contribution of TGS to the physiology of plants under stressful high temperatures. We summarized potential roles of constitutive and facultative heterochromatin as well as the most impactful regulatory genes, highlighting events where the loss of epigenetic suppression has not yet been associated with corresponding changes in epigenetic marks. Significance Statement: High temperatures pose a major threat to plant physiology. While research has extensively focused on thermomorphogenesis and heat‐shock stress responses, the roles of epigenetic mechanisms remain relatively under‐explored. In particular, the contribution of transcriptional gene silencing (TGS) is probably the least studied. Our review highlights how canonical TGS and heterochromatin dynamics may contribute to plant heat tolerance, summarizing both established and novel insights. With this work, we aim to promote alternative avenues for eventually developing heat‐resistant crops, ultimately contributing to more sustainable agriculture under a global warming scenario. [ABSTRACT FROM AUTHOR]

Published

2024

5. Beyond the Usual Suspects: Examining the Role of Understudied Histone Variants in Breast Cancer.

Author

Dhahri, Hejer, Saintilnord, Wesley N., Chandler, Darrell, and Fondufe-Mittendorf, Yvonne N.

Subjects

*BREAST cancer, *HISTONES, *DNA folding, *REGULATOR genes, *DNA condensation, *TRANSCRIPTION factors, *BREAST, *DNA damage

Abstract

The incorporation of histone variants has structural ramifications on nucleosome dynamics and stability. Due to their unique sequences, histone variants can alter histone–histone or histone–DNA interactions, impacting the folding of DNA around the histone octamer and the overall higher-order structure of chromatin fibers. These structural modifications alter chromatin compaction and accessibility of DNA by transcription factors and other regulatory proteins to influence gene regulatory processes such as DNA damage and repair, as well as transcriptional activation or repression. Histone variants can also generate a unique interactome composed of histone chaperones and chromatin remodeling complexes. Any of these perturbations can contribute to cellular plasticity and the progression of human diseases. Here, we focus on a frequently overlooked group of histone variants lying within the four human histone gene clusters and their contribution to breast cancer. [ABSTRACT FROM AUTHOR]

Published

2024

6. Histone Variants in Neuronal Transcription and Behavioral Regulation

Author

McLean, Timothy A. B., Walters, Brandon J., Zovkic, Iva B., Saha, Ramendra N., editor, and Dudek, Serena M., editor

Published

2024

7. Histone Chaperones in Cancer

Author

Shirude, Mayur Balkrishna, Dutta, Debasree, Sharma, Siddharth, Section editor, Sobti, R. C., editor, Ganguly, Nirmal K., editor, and Kumar, Rakesh, editor

Published

2024

8. Maintenance and dynamic reprogramming of chromatin organization during development.

Author

Simon, Lauriane and Probst, Aline V.

Subjects

*HISTONES, *CHROMATIN, *GENETIC regulation, *GENE expression, *SOMATIC cell nuclear transfer, *POST-translational modification, *CELL cycle, *CELL differentiation

Abstract

SUMMARY: Controlled transcription of genes is critical for cell differentiation and development. Gene expression regulation therefore involves a multilayered control from nucleosome composition in histone variants and their post‐translational modifications to higher‐order folding of chromatin fibers and chromatin interactions in nuclear space. Recent technological advances have allowed gaining insight into these mechanisms, the interplay between local and higher‐order chromatin organization, and the dynamic changes that occur during stress response and developmental transitions. In this review, we will discuss chromatin organization from the nucleosome to its three‐dimensional structure in the nucleus, and consider how these different layers of organization are maintained during the cell cycle or rapidly reprogrammed during development. Significance Statement: Chromatin organization contributes to gene expression control. In this review, we examine the interplay between local and higher‐order chromatin organization and the dynamic changes that occur during stress response and developmental transitions. [ABSTRACT FROM AUTHOR]

Published

2024

9. Histone H2A variant H2A.B is enriched in transcriptionally active and replicating HSV-1 lytic chromatin.

Author

Cortes, Esteban Flores, Saddoris, Sarah M., Owens, Arryn K., Gibeault, Rebecca, Depledge, Daniel P., and Schang, Luis M.

Subjects

*CHROMATIN, *VIRAL genes, *LATENT infection, *DNA replication, *GENETIC transcription, *VIRAL DNA

Abstract

Herpes simplex virus 1 (HSV-1) transcription is restricted in latently infected neurons and the genomes are in mostly silenced chromatin, whereas all viral genes are transcribed in lytically infected cells, in which the genomes are dynamically chromatinized. Epigenetic regulation modulates HSV-1 transcription during lytic, latent, and reactivating infections but the precise mechanisms are not fully defined. Nucleosomes are dynamic: they slide, breathe, assemble, and disassemble. We and others have proposed that the most dynamic HSV-1 chromatin is transcriptionally competent, whereas the least dynamic is silenced. However, the mechanisms yielding the unusually dynamic viral chromatin remain unknown. Histone variants affect nucleosome dynamics. The dynamics of H2A, H2A.X, and macroH2A were enhanced in infected cells, whereas those of H2A.B were uniquely decreased. We constructed stably transduced cells expressing tagged histone H2A, H2A.B, macroH2A, or H2B, which assembles the H2A/H2B nucleosome dimers with all H2A variants. All H2A variants, as well as ectopic and endogenous H2B were assembled into HSV-1 chromatin evenly throughout the genome but canonical H2A was relatively depleted whereas H2A.B was enriched, particularly in the most dynamic viral chromatin. When viral transcription and DNA replication were restricted, H2A.B became as depleted from the viral chromatin through the entire genome as H2A. We propose that lytic HSV-1 nucleosomes are enriched in the dynamic variant H2A.B/H2B dimers to promote HSV-1 chromatin dynamics and transcriptional competency and conclude that the dynamics of HSV-1 chromatin are determined in part by the H2A variants. IMPORTANCE Herpes simplex virus 1 (HSV-1) transcription is epigenetically regulated during latent and lytic infections, and epigenetic inhibitors have been proposed as potential antiviral drugs to modulate latency and reactivation. However, the detailed epigenetic mechanisms of regulation of HSV-1 transcription have not been fully characterized and may differ from those regulating cellular transcription. Whereas lytic HSV-1 chromatin is unusually dynamic, latent silenced HSV-1 chromatin is not. The mechanisms resulting in the unique dynamics of the lytic chromatin remain unknown. Here we identify the enrichment of the highly dynamic histone 2A variant H2A in the most dynamic viral chromatin, which provides a mechanistic understanding of its unique dynamics. Future work to identify the mechanisms of enrichment in H2A.B on the viral chromatin may identify novel druggable epigenetic regulators that modulate HSV-1 latency and reactivation. [ABSTRACT FROM AUTHOR]

Published

2024

10. Roles of Histone H2A Variants in Cancer Development, Prognosis, and Treatment.

Author

Lai, Po Man and Chan, Kui Ming

Subjects

*NUCLEAR proteins, *CARCINOGENESIS, *GENETIC regulation, *EARLY detection of cancer, *GENETIC transcription regulation

Abstract

Histones are nuclear proteins essential for packaging genomic DNA and epigenetic gene regulation. Paralogs that can substitute core histones (H2A, H2B, H3, and H4), named histone variants, are constitutively expressed in a replication-independent manner throughout the cell cycle. With specific chaperones, they can be incorporated to chromatin to modify nucleosome stability by modulating interactions with nucleosomal DNA. This allows the regulation of essential fundamental cellular processes for instance, DNA damage repair, chromosomal segregation, and transcriptional regulation. Among all the histone families, histone H2A family has the largest number of histone variants reported to date. Each H2A variant has multiple functions apart from their primary role and some, even be further specialized to perform additional tasks in distinct lineages, such as testis specific shortH2A (sH2A). In the past decades, the discoveries of genetic alterations and mutations in genes encoding H2A variants in cancer had revealed variants' potentiality in driving carcinogenesis. In addition, there is growing evidence that H2A variants may act as novel prognostic indicators or biomarkers for both early cancer detection and therapeutic treatments. Nevertheless, no studies have ever concluded all identified variants in a single report. Here, in this review, we summarize the respective functions for all the 19 mammalian H2A variants and their roles in cancer biology whilst potentiality being used in clinical setting. [ABSTRACT FROM AUTHOR]

Published

2024

11. Roles of Histone H2B, H3 and H4 Variants in Cancer Development and Prognosis

Author

Po Man Lai, Xiaoxiang Gong, and Kui Ming Chan

Subjects

epigenetics, chromatin, histone variants, variants, cancers, H2B, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Histone variants are the paralogs of core histones (H2A, H2B, H3 and H4). They are stably expressed throughout the cell cycle in a replication-independent fashion and are capable of replacing canonical counterparts under different fundamental biological processes. Variants have been shown to take part in multiple processes, including DNA damage repair, transcriptional regulation and X chromosome inactivation, with some of them even specializing in lineage-specific roles like spermatogenesis. Several reports have recently identified some unprecedented variants from different histone families and exploited their prognostic value in distinct types of cancer. Among the four classes of canonical histones, the H2A family has the greatest number of variants known to date, followed by H2B, H3 and H4. In our prior review, we focused on summarizing all 19 mammalian histone H2A variants. Here in this review, we aim to complete the full summary of the roles of mammalian histone variants from the remaining histone H2B, H3, and H4 families, along with an overview of their roles in cancer biology and their prognostic value in a clinical context.

Published

2024

12. Diversity of H2A Histones and Their Effect on Nucleosome Structural Properties.

Author

Singhpalchevsk, L. and Shaytan, A. K.

Abstract

Histone proteins that play an important role in the chromatin dynamics and regulation of gene activity are a key epigenetic factor. They are divided into two broad classes: canonical histones and their variants. The canonical histones are expressed mainly during the S phase of the cell cycle, since they are involved in DNA packaging in the process of cell division. The histone variants are histone genes that are expressed and regulate the chromatin dynamics during the entire cell cycle. Due to the functional and species diversity, different families of variant histones are distinguished. Some proteins are characterized by minor differences from the canonical histones, while others, on the contrary, can have many important structural and functional peculiarities affecting the nucleosome stability and chromatin dynamics. In order to estimate the variability of histones of the H2A family and their effect on the nucleosome structure, we carried out a bioinformatics analysis of amino acid sequences of the H2A family histones. Clustering conducted using a UPGMA method allowed to distinguish two main subfamilies of H2A proteins: short H2A and other H2A variants that demonstrate higher conservatism of amino acid sequences. We also constructed and analyzed multiple alignments for different H2A histone subfamilies. It is important to note that the proteins of short H2A subfamily are not only the least conservative within their family, but also have the peculiarities that have a significant effect on the nucleosome structural properties. In addition, we conducted a phylogenetic analysis of short H2A histones, as a result of which the subfamilies corresponding to the H2A.B, H2A.P, H2A.Q, H2A.L variants were characterized in more detail. [ABSTRACT FROM AUTHOR]

Published

2023

13. Imaging analysis of six human histone H1 variants reveals universal enrichment of H1.2, H1.3, and H1.5 at the nuclear periphery and nucleolar H1X presence

Author

Monica Salinas-Pena, Elena Rebollo, and Albert Jordan

Subjects

histone H1, histone variants, chromatin, heterochromatin, super-resolution imaging, nucleoli, Medicine, Science, Biology (General), QH301-705.5

Abstract

Histone H1 participates in chromatin condensation and regulates nuclear processes. Human somatic cells may contain up to seven histone H1 variants, although their functional heterogeneity is not fully understood. Here, we have profiled the differential nuclear distribution of the somatic H1 repertoire in human cells through imaging techniques including super-resolution microscopy. H1 variants exhibit characteristic distribution patterns in both interphase and mitosis. H1.2, H1.3, and H1.5 are universally enriched at the nuclear periphery in all cell lines analyzed and co-localize with compacted DNA. H1.0 shows a less pronounced peripheral localization, with apparent variability among different cell lines. On the other hand, H1.4 and H1X are distributed throughout the nucleus, being H1X universally enriched in high-GC regions and abundant in the nucleoli. Interestingly, H1.4 and H1.0 show a more peripheral distribution in cell lines lacking H1.3 and H1.5. The differential distribution patterns of H1 suggest specific functionalities in organizing lamina-associated domains or nucleolar activity, which is further supported by a distinct response of H1X or phosphorylated H1.4 to the inhibition of ribosomal DNA transcription. Moreover, H1 variants depletion affects chromatin structure in a variant-specific manner. Concretely, H1.2 knock-down, either alone or combined, triggers a global chromatin decompaction. Overall, imaging has allowed us to distinguish H1 variants distribution beyond the segregation in two groups denoted by previous ChIP-Seq determinations. Our results support H1 variants heterogeneity and suggest that variant-specific functionality can be shared between different cell types.

Published

2024

14. The Function of H2A Histone Variants and Their Roles in Diseases

Author

Xuemin Yin, Dong Zeng, Yingjun Liao, Chengyuan Tang, and Ying Li

Subjects

histone variants, chromatin, H2A.Z, H2A.B, macroH2A, H2A.X, Microbiology, QR1-502

Abstract

Epigenetic regulation, which is characterized by reversible and heritable genetic alterations without changing DNA sequences, has recently been increasingly studied in diseases. Histone variant regulation is an essential component of epigenetic regulation. The substitution of canonical histones by histone variants profoundly alters the local chromatin structure and modulates DNA accessibility to regulatory factors, thereby exerting a pivotal influence on gene regulation and DNA damage repair. Histone H2A variants, mainly including H2A.Z, H2A.B, macroH2A, and H2A.X, are the most abundant identified variants among all histone variants with the greatest sequence diversity. Harboring varied chromatin occupancy and structures, histone H2A variants perform distinct functions in gene transcription and DNA damage repair. They are implicated in multiple pathophysiological mechanisms and the emergence of different illnesses. Cancer, embryonic development abnormalities, neurological diseases, metabolic diseases, and heart diseases have all been linked to histone H2A variant alterations. This review focuses on the functions of H2A histone variants in mammals, including H2A.Z, H2A.B, macroH2A, and H2A.X, and their current roles in various diseases.

Published

2024

15. Arabidopsis Histone Variant H2A.X Functions in the DNA Damage-Coupling Abscisic Acid Signaling Pathway

Author

Peng Guo, Tian-Jing Wang, Shuang Wang, Xiaoyuan Peng, Dae Heon Kim, and Yutong Liu

Subjects

Arabidopsis thaliana, histone variants, genotoxic stress, ABA responses, DNA damage, CRISPR/Cas9, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Environmental variations initiate chromatin modifications, leading to the exchange of histone subunits or the repositioning of nucleosomes. The phosphorylated histone variant H2A.X (γH2A.X) is recognized for the formation of foci that serve as established markers of DNA double-strand breaks (DSBs). Nevertheless, the precise roles of H2A.X in the cellular response to genotoxic stress and the impact of the plant hormone abscisic acid (ABA) remain incompletely understood. In this investigation, we implemented CRISPR/Cas9 technology to produce loss-of-function mutants of AtHTA3 and AtHTA5 in Arabidopsis. The phenotypes of the athta3 and athta5 single mutants were nearly identical to those of the wild-type Col-0. Nevertheless, the athta3 athta5 double mutants exhibited aberrant embryonic development, increased sensitivity to DNA damage, and higher sensitivity to ABA. The RT-qPCR analysis indicates that AtHTA3 and AtHTA5 negatively regulate the expression of AtABI3, a fundamental regulator in the ABA signaling pathway. Subsequent investigation demonstrated that AtABI3 participates in the genotoxic stress response by influencing the expression of DNA damage response genes, such as AtBRCA1, AtRAD51, and AtWEE1. Our research offers new insights into the role of H2A.X in the genotoxic and ABA responses of Arabidopsis.

Published

2024

16. Beyond the Usual Suspects: Examining the Role of Understudied Histone Variants in Breast Cancer

Author

Hejer Dhahri, Wesley N. Saintilnord, Darrell Chandler, and Yvonne N. Fondufe-Mittendorf

Subjects

histone variants, onco-histones, nucleosome stability, chromatin structure, gene regulation, breast cancer, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

The incorporation of histone variants has structural ramifications on nucleosome dynamics and stability. Due to their unique sequences, histone variants can alter histone–histone or histone–DNA interactions, impacting the folding of DNA around the histone octamer and the overall higher-order structure of chromatin fibers. These structural modifications alter chromatin compaction and accessibility of DNA by transcription factors and other regulatory proteins to influence gene regulatory processes such as DNA damage and repair, as well as transcriptional activation or repression. Histone variants can also generate a unique interactome composed of histone chaperones and chromatin remodeling complexes. Any of these perturbations can contribute to cellular plasticity and the progression of human diseases. Here, we focus on a frequently overlooked group of histone variants lying within the four human histone gene clusters and their contribution to breast cancer.

Published

2024

17. Direct and cost-effective method for histone isolation from cultured mammalian cells.

Author

Batel, Anja, Polović, Mirjana, Glumac, Mateo, Gelemanović, Andrea, Šprung, Matilda, and Marinović Terzić, Ivana

Subjects

*CELL cycle, *CHROMATIN, *SOLUTION (Chemistry), *EPIGENETICS, *MASS spectrometry, *HISTONES

Abstract

Histones are an essential part of nucleosomes that regulate chromatin structure and function. Histone exchanges and modifications represent a scaffold for DNA transcription, repair, and replication. Studying histones and histone code is an important and fast-developing branch of epigenetic science. Here we propose a fast, efficient, and versatile assay for nucleosomal histone isolation from mammalian cells, without the use of acids or high salt solutions which are common for other histone isolation techniques. All components used in the protocol are common and inexpensive laboratory chemicals. The protocol has been evaluated on six commonly used cell lines and two animal tissue samples. The mild extraction conditions preserve delicate histone epigenetic changes, allowing its downstream analyses. We have demonstrated the assays' successful application during changes in the transcriptional activity of histone genes, cell cycle transitions, and DNA-damaging conditions. Histone fractions, obtained by the protocol, can be used for further applications, such as electrophoresis, immunoblot, and mass spectrometry. Therefore, the new proposed nucleosomal histone isolation method is sensitive, specific, and suitable for downstream applications of various kinds. [ABSTRACT FROM AUTHOR]

Published

2023

18. The CENP-A nucleosome: where and when it happens during the inner kinetochore's assembly.

Author

Kale, Seyit, Boopathi, Ramachandran, Belotti, Edwige, Lone, Imtiaz Nisar, Graies, Mohamed, Schröder, Maria, Petrova, Maria, Papin, Christophe, Bednar, Jan, Ugrinova, Iva, Hamiche, Ali, and Dimitrov, Stefan

Subjects

*KINETOCHORE, *SPINDLE apparatus, *CHROMATIN, *HISTONES, *CELL division, *DNA

Abstract

CENP-A nucleosomes serve as the assembly point for the kinetochores, which bind chromatin to the spindle apparatus during cell division. Human constitutive centromere-associated network (CCAN) is a 16-protein complex and is the first protein layer of the kinetochore. Only two CCAN proteins, CENP-C and CENP-N, contact the CENP-A nucleosome. Their mode of recognizing the CENP-A nucleosome has been characterized over the past decade. Three human CCAN structures have been published in the past year; slightly earlier, another model was also published for yeast. All structures point to a Y-shaped clamp that can adhere to linear and exposed DNA but not to curved and nucleosome-protected DNA. This conflicts with what we know about CENP-N's recognition of the CENP-A nucleosome. One way to reconcile these conflicting findings is via an intermediary nucleosome remodeling step between the initial recognition of the CENP-A nucleosome by CENP-C and CENP-N, and the final assembly of the remaining CCAN components that constitute the clamp. CENP-A is an essential histone variant that replaces the canonical H3 at the centromeres and marks these regions epigenetically. The CENP-A nucleosome is the specific building block of centromeric chromatin, and it is recognized by CENP-C and CENP-N, two components of the constitutive centromere-associated network (CCAN), the first protein layer of the kinetochore. Recent proposals of the yeast and human (h)CCAN structures position the assembly on exposed DNA, suggesting an elusive spatiotemporal recognition. We summarize the data on the structural organization of the CENP-A nucleosome and the binding of CENP-C and CENP-N. The latter posits an apparent contradiction in engaging the CENP-A nucleosome versus the CCAN. We propose a reconciliatory model for the assembly of CCAN on centromeric chromatin. [ABSTRACT FROM AUTHOR]

Published

2023

19. Plasmodium falciparum gametocytes display global chromatin remodelling during sexual differentiation

Author

Myriam D. Jeninga, Jingyi Tang, Shamista A. Selvarajah, Alexander G. Maier, Michael F. Duffy, and Michaela Petter

Subjects

Plasmodium falciparum, Malaria, Gametocytogenesis, Epigenome, Transcriptome, Histone variants, Biology (General), QH301-705.5

Abstract

Abstract Background The protozoan malaria parasite Plasmodium falciparum has a complex life cycle during which it needs to differentiate into multiple morphologically distinct life forms. A key process for transmission of the disease is the development of male and female gametocytes in the human blood, yet the mechanisms determining sexual dimorphism in these haploid, genetically identical sexual precursor cells remain largely unknown. To understand the epigenetic program underlying the differentiation of male and female gametocytes, we separated the two sexual forms by flow cytometry and performed RNAseq as well as comprehensive ChIPseq profiling of several histone variants and modifications. Results We show that in female gametocytes the chromatin landscape is globally remodelled with respect to genome-wide patterns and combinatorial usage of histone variants and histone modifications. We identified sex specific differences in heterochromatin distribution, implicating exported proteins and ncRNAs in sex determination. Specifically in female gametocytes, the histone variants H2A.Z/H2B.Z were highly enriched in H3K9me3-associated heterochromatin. H3K27ac occupancy correlated with stage-specific gene expression, but in contrast to asexual parasites this was unlinked to H3K4me3 co-occupancy at promoters in female gametocytes. Conclusions Collectively, we defined novel combinatorial chromatin states differentially organising the genome in gametocytes and asexual parasites and unravelled fundamental, sex-specific differences in the epigenetic code. Our chromatin maps represent an important resource for future understanding of the mechanisms driving sexual differentiation in P. falciparum.

Published

2023

20. Roles of Histone H2A Variants in Cancer Development, Prognosis, and Treatment

Author

Po Man Lai and Kui Ming Chan

Subjects

epigenetics, chromatin, histone variants, variants, cancers, H2A, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Histones are nuclear proteins essential for packaging genomic DNA and epigenetic gene regulation. Paralogs that can substitute core histones (H2A, H2B, H3, and H4), named histone variants, are constitutively expressed in a replication-independent manner throughout the cell cycle. With specific chaperones, they can be incorporated to chromatin to modify nucleosome stability by modulating interactions with nucleosomal DNA. This allows the regulation of essential fundamental cellular processes for instance, DNA damage repair, chromosomal segregation, and transcriptional regulation. Among all the histone families, histone H2A family has the largest number of histone variants reported to date. Each H2A variant has multiple functions apart from their primary role and some, even be further specialized to perform additional tasks in distinct lineages, such as testis specific shortH2A (sH2A). In the past decades, the discoveries of genetic alterations and mutations in genes encoding H2A variants in cancer had revealed variants’ potentiality in driving carcinogenesis. In addition, there is growing evidence that H2A variants may act as novel prognostic indicators or biomarkers for both early cancer detection and therapeutic treatments. Nevertheless, no studies have ever concluded all identified variants in a single report. Here, in this review, we summarize the respective functions for all the 19 mammalian H2A variants and their roles in cancer biology whilst potentiality being used in clinical setting.

Published

2024

21. Advances in biological functions and mechanisms of histone variants in plants.

Author

Xi Wu, Xu Zhang, Borong Huang, Junyou Han, and Huihui Fang

Subjects

GENETIC carriers, HISTONES, CHROMATIN, PLANT growth, PLANT development

Abstract

Nucleosome is the basic subunit of chromatin, consisting of approximately 147bp DNA wrapped around a histone octamer, containing two copies of H2A, H2B, H3 and H4. A linker histone H1 can bind nucleosomes through its conserved GH1 domain, which may promote chromatin folding into higher-order structures. Therefore, the complexity of histones act importantly for specifying chromatin and gene activities. Histone variants, encoded by separate genes and characterized by only a few amino acids differences, can affect nucleosome packaging and stability, and then modify the chromatin properties. Serving as carriers of pivotal genetic and epigenetic information, histone variants have profound significance in regulating plant growth and development, response to both biotic and abiotic stresses. At present, the biological functions of histone variants in plant have become a research hotspot. Here, we summarize recent researches on the biological functions, molecular chaperons and regulatory mechanisms of histone variants in plant, and propose some novel research directions for further study of plant histone variants research field. Our study will provide some enlightens for studying and understanding the epigenetic regulation and chromatin specialization mediated by histone variant in plant. [ABSTRACT FROM AUTHOR]

Published

2023

22. Involvement of the H3.3 Histone Variant in the Epigenetic Regulation of Gene Expression in the Nervous System, in Both Physiological and Pathological Conditions.

Author

Di Liegro, Carlo Maria, Schiera, Gabriella, Schirò, Giuseppe, and Di Liegro, Italia

Subjects

*GENETIC regulation, *EPIGENETICS, *NERVOUS system, *BASAL metabolism, *PROTEIN metabolism, *HISTONES, *CHROMATIN

Abstract

All the cells of an organism contain the same genome. However, each cell expresses only a minor fraction of its potential and, in particular, the genes encoding the proteins necessary for basal metabolism and the proteins responsible for its specific phenotype. The ability to use only the right and necessary genes involved in specific functions depends on the structural organization of the nuclear chromatin, which in turn depends on the epigenetic history of each cell, which is stored in the form of a collection of DNA and protein modifications. Among these modifications, DNA methylation and many kinds of post-translational modifications of histones play a key role in organizing the complex indexing of usable genes. In addition, non-canonical histone proteins (also known as histone variants), the synthesis of which is not directly linked with DNA replication, are used to mark specific regions of the genome. Here, we will discuss the role of the H3.3 histone variant, with particular attention to its loading into chromatin in the mammalian nervous system, both in physiological and pathological conditions. Indeed, chromatin modifications that mark cell memory seem to be of special importance for the cells involved in the complex processes of learning and memory. [ABSTRACT FROM AUTHOR]

Published

2023

23. H3.3 contributes to chromatin accessibility and transcription factor binding at promoter-proximal regulatory elements in embryonic stem cells

Author

Amanuel Tafessu, Ryan O’Hara, Sara Martire, Altair L. Dube, Purbita Saha, Vincent U. Gant, and Laura A. Banaszynski

Subjects

Histone variants, Chromatin accessibility, Transcription factor binding, Embryonic stem cells, Differentiation, Biology (General), QH301-705.5, Genetics, QH426-470

Abstract

Abstract Background The histone variant H3.3 is enriched at active regulatory elements such as promoters and enhancers in mammalian genomes. These regions are highly accessible, creating an environment that is permissive to transcription factor binding and the recruitment of transcriptional coactivators that establish a unique chromatin post-translational landscape. How H3.3 contributes to the establishment and function of chromatin states at these regions is poorly understood. Results We perform genomic analyses of features associated with active promoter chromatin in mouse embryonic stem cells (ESCs) and find evidence of subtle yet widespread promoter dysregulation in the absence of H3.3. Loss of H3.3 results in reduced chromatin accessibility and transcription factor (TF) binding at promoters of expressed genes in ESCs. Likewise, enrichment of the transcriptional coactivator p300 and downstream histone H3 acetylation at lysine 27 (H3K27ac) is reduced at promoters in the absence of H3.3, along with reduced enrichment of the acetyl lysine reader BRD4. Despite the observed chromatin dysregulation, H3.3 KO ESCs maintain transcription from ESC-specific genes. However, upon undirected differentiation, H3.3 KO cells retain footprinting of ESC-specific TF motifs and fail to generate footprints of lineage-specific TF motifs, in line with their diminished capacity to differentiate. Conclusions H3.3 facilitates DNA accessibility, transcription factor binding, and histone post-translational modification at active promoters. While H3.3 is not required for maintaining transcription in ESCs, it does promote de novo transcription factor binding which may contribute to the dysregulation of cellular differentiation in the absence of H3.3.

Published

2023

24. Epigenetic Mechanisms: DNA Methylation and Histone Protein Modification

Author

Gagnidze, Khatuna, Pfaff, Donald W., Pfaff, Donald W., editor, Volkow, Nora D., editor, and Rubenstein, John L., editor

Published

2022

25. Inhibition of HIST1H2AB suppresses the proliferation of lung adenocarcinoma.

Author

Chai, Xiaojun, Wang, Guangxue, Hong, Xuan, Feng, Minghao, Wang, He, Liu, Fabing, Yao, Wei, Zhu, Dongyi, and Li, Qinchuan

Abstract

Background: Lung adenocarcinoma is one of the common causes of cancer‐related deaths worldwide. Histone cluster 1 H2A family member b (HIST1H2AB) is a member of the histone H2A family. Bioinformatic analyses have revealed that HIST1H2AB is highly expressed in some cancers and might be an oncogene. However, information on the function of HIST1H2AB in lung adenocarcinoma is limited. Methods: The expression of HIST1H2AB was analyzed in normal lung, lung adenocarcinoma and paracancerous tissues from The Cancer Genome Atlas (TCGA) database and immunohistochemistry staining. It was further verified in the relative cell lines using real‐time quantitative polymerase chain reaction (RT‐qPCR). When the adenocarcinoma cells lines (A549 and H1299) were successfully transfected with shHIST1H2AB or an empty plasmid packaged into a lentivirus, cell proliferation was detected using Celigo fluorescence cell‐counting, colony formation and annexin V‐allophycocyanin assays. Twenty nude mice were subcutaneously injected with A549 cells transfected with shHIST1H2AB or empty plasmid; the tumor size was recorded on day 25 and then measured every 3 days thereafter. The final tumor weight was measured on day 37. Significantly differentially expressed genes were analyzed using a human gene expression array. Furthermore, the potentially relevant genes were verified using RT‐qPCR and western blotting. Results: HIST1H2AB was highly expressed in lung adenocarcinoma tissues from TCGA database and immunohistochemistry staining. Similar results were seen in the lung adenocarcinoma cells. When the cells were successfully transfected with shHIST1H2AB or an empty plasmid, downregulation of HIST1H2AB inhibited the growth and promoted the apoptosis of lung adenocarcinoma cells. The xenograft results suggested that HIST1H2AB downregulation delayed tumor growth and reduced tumor weight. Moreover, interferon signaling pathway and four genes (HMGB1, FOXM1, F2RL1 and SLC4A7) might be regulated by HIST1H2AB in the development of lung adenocarcinoma as indicated through gene expression array, RT‐qPCR and western blotting analyses. Conclusions: HIST1H2AB acts as an oncogenic protein and HIST1H2AB inhibition suppresses the proliferation of lung adenocarcinoma cells. It may be a novel target for lung adenocarcinoma therapy. [ABSTRACT FROM AUTHOR]

Published

2023

26. Plasmodium falciparum gametocytes display global chromatin remodelling during sexual differentiation.

Author

Jeninga, Myriam D., Tang, Jingyi, Selvarajah, Shamista A., Maier, Alexander G., Duffy, Michael F., and Petter, Michaela

Subjects

*SEX differentiation (Embryology), *GERM cells, *PLASMODIUM falciparum, *CHROMATIN, *LIFE cycles (Biology), *HAPLOIDY, *HISTONES, *EPIGENOMICS, *GENETIC sex determination

Abstract

Background: The protozoan malaria parasite Plasmodium falciparum has a complex life cycle during which it needs to differentiate into multiple morphologically distinct life forms. A key process for transmission of the disease is the development of male and female gametocytes in the human blood, yet the mechanisms determining sexual dimorphism in these haploid, genetically identical sexual precursor cells remain largely unknown. To understand the epigenetic program underlying the differentiation of male and female gametocytes, we separated the two sexual forms by flow cytometry and performed RNAseq as well as comprehensive ChIPseq profiling of several histone variants and modifications. Results: We show that in female gametocytes the chromatin landscape is globally remodelled with respect to genome-wide patterns and combinatorial usage of histone variants and histone modifications. We identified sex specific differences in heterochromatin distribution, implicating exported proteins and ncRNAs in sex determination. Specifically in female gametocytes, the histone variants H2A.Z/H2B.Z were highly enriched in H3K9me3-associated heterochromatin. H3K27ac occupancy correlated with stage-specific gene expression, but in contrast to asexual parasites this was unlinked to H3K4me3 co-occupancy at promoters in female gametocytes. Conclusions: Collectively, we defined novel combinatorial chromatin states differentially organising the genome in gametocytes and asexual parasites and unravelled fundamental, sex-specific differences in the epigenetic code. Our chromatin maps represent an important resource for future understanding of the mechanisms driving sexual differentiation in P. falciparum. [ABSTRACT FROM AUTHOR]

Published

2023

27. Histone variant-specific post-translational modifications.

Author

Joseph, Faith M. and Young, Nicolas L.

Subjects

*HISTONES, *POST-translational modification, *CHROMATIN, *CELL differentiation, *APPROPRIATE technology, *LOCUS (Genetics)

Abstract

Post-translational modifications (PTMs) of histones play a key role in DNA-based processes and contribute to cell differentiation and gene function by adding an extra layer of regulation. Variations in histone sequences within each family of histones expands the chromatin repertoire and provide further mechanisms for regulation and signaling. While variants are known to be present in certain genomic loci and carry out important functions, much remains unknown about variant-specific PTMs and their role in regulating chromatin. This ambiguity is in part due to the limited technologies and appropriate reagents to identify and quantitate variant-specific PTMs. Nonetheless, histone variants are an integral portion of the chromatin system and the understanding of their modifications and resolving how PTMs function differently on specific variants is paramount to the advancement of the field. Here we review the current knowledge on post-translational modifications specific to histone variants, with an emphasis on well-characterized PTMs of known function. While not every possible PTM is addressed, we present key variant-specific PTMs and what is known about their function and mechanisms in convenient reference tables. [ABSTRACT FROM AUTHOR]

Published

2023

28. Histone variants in archaea – An undiscovered country.

Author

Stevens, Kathryn M. and Warnecke, Tobias

Subjects

*ARCHAEBACTERIA, *HISTONES, *EUKARYOTES, *CHROMATIN, *BIOLOGY, *GENOMES

Abstract

Exchanging core histones in the nucleosome for paralogous variants can have important functional ramifications. Many of these variants, and their physiological roles, have been characterized in exquisite detail in model eukaryotes, including humans. In comparison, our knowledge of histone biology in archaea remains rudimentary. This is true in particular for our knowledge of histone variants. Many archaea encode several histone genes that differ in sequence, but do these paralogs make distinct, adaptive contributions to genome organization and regulation in a manner comparable to eukaryotes? Below, we review what we know about histone variants in archaea at the level of structure, regulation, and evolution. In all areas, our knowledge pales when compared to the wealth of insight that has been gathered for eukaryotes. Recent findings, however, provide tantalizing glimpses into a rich and largely undiscovered country that is at times familiar and eukaryote-like and at times strange and uniquely archaeal. We sketch a preliminary roadmap for further exploration of this country; an undertaking that may ultimately shed light not only on chromatin biology in archaea but also on the origin of histone-based chromatin in eukaryotes. [ABSTRACT FROM AUTHOR]

Published

2023

29. The ins and outs of CENP-A: Chromatin dynamics of the centromere-specific histone.

Author

Stirpe, Alessandro and Heun, Patrick

Subjects

*CHROMATIN, *CENTROMERE, *DNA repair, *CHROMOSOMES, *ANEUPLOIDY, *CHROMOSOME segregation

Abstract

Centromeres are highly specialised chromosome domains defined by the presence of an epigenetic mark, the specific histone H3 variant called CENP-A (centromere protein A). They constitute the genomic regions on which kinetochores form and when defective cause segregation defects that can lead to aneuploidy and cancer. Here, we discuss how CENP-A is established and maintained to propagate centromere identity while subjected to dynamic chromatin remodelling during essential cellular processes like DNA repair, replication, and transcription. We highlight parallels and identify conserved mechanisms between different model organism with a particular focus on 1) the establishment of CENP-A at centromeres, 2) CENP-A maintenance during transcription and replication, and 3) the mechanisms that help preventing CENP-A localization at non-centromeric sites. We then give examples of how timely loading of new CENP-A to the centromere, maintenance of old CENP-A during S-phase and transcription, and removal of CENP-A at non-centromeric sites are coordinated and controlled by an intricate network of factors whose identity is slowly being unravelled. [ABSTRACT FROM AUTHOR]

Published

2023

30. Evolution, structure and function of divergent macroH2A1 splice isoforms.

Author

Guberovic, Iva, Farkas, Marina, Corujo, David, and Buschbeck, Marcus

Subjects

*ALTERNATIVE RNA splicing, *GENETIC regulation, *GENETIC engineering, *LIGAND binding (Biochemistry), *GENETIC transcription regulation, *HISTONES

Abstract

The replacement of replication-coupled histones with non-canonical histone variants provides chromatin with additional properties and contributes to the plasticity of the epigenome. MacroH2A histone variants are counterparts of the replication-coupled histone H2A. They are characterized by a unique tripartite structure, consisting of a histone fold, an unstructured linker, and a globular macrodomain. MacroH2A1.1 and macroH2A1.2 are the result of alternative splicing of the MACROH2A1 gene and can have opposing biological functions. Here, we discuss the structural differences between the macrodomains of the two isoforms, resulting in differential ligand binding. We further discuss how this modulates gene regulation by the two isoforms, in cases resulting in opposing role of macroH2A1.1 and macroH2A1.2 in development and differentiation. Finally, we share recent insight in the evolution of macroH2As. Taken together, in this review, we aim to discuss in unprecedented detail distinct properties and functions of the fascinating macroH2A1 splice isoforms. [ABSTRACT FROM AUTHOR]

Published

2023

31. Spotlight on histone H2A variants: From B to X to Z.

Author

Herchenröther, Andreas, Wunderlich, Tim M., Lan, Jie, and Hake, Sandra B.

Subjects

*HISTONES, *DNA structure, *CHROMOSOMES, *DNA repair, *CHROMATIN, *DNA

Abstract

Chromatin, the functional organization of DNA with histone proteins in eukaryotic nuclei, is the tightly-regulated template for several biological processes, such as transcription, replication, DNA damage repair, chromosome stability and sister chromatid segregation. In order to achieve a reversible control of local chromatin structure and DNA accessibility, various interconnected mechanisms have evolved. One of such processes includes the deposition of functionally-diverse variants of histone proteins into nucleosomes, the building blocks of chromatin. Among core histones, the family of H2A histone variants exhibits the largest number of members and highest sequence-divergence. In this short review, we report and discuss recent discoveries concerning the biological functions of the animal histone variants H2A.B, H2A.X and H2A.Z and how dysregulation or mutation of the latter impacts the development of disease. [ABSTRACT FROM AUTHOR]

Published

2023

32. Seminars in cell and development biology on histone variants remodelers of H2A variants associated with heterochromatin.

Author

Berger, Frédéric, Muegge, Kathrin, and Richards, Eric J.

Subjects

*DEVELOPMENTAL biology, *HETEROCHROMATIN, *CHROMATIN, *SEMINARS, *GENOMES, *CYTOLOGY

Abstract

Variants of the histone H2A occupy distinct locations in the genome. There is relatively little known about the mechanisms responsible for deposition of specific H2A variants. Notable exceptions are chromatin remodelers that control the dynamics of H2A.Z at promoters. Here we review the steps that identified the role of a specific class of chromatin remodelers, including LSH and DDM1 that deposit the variants macroH2A in mammals and H2A.W in plants, respectively. The function of these remodelers in heterochromatin is discussed together with their multiple roles in genome stability. [ABSTRACT FROM AUTHOR]

Published

2023

33. Post-Translational Modifications of Histone Variants in the Absence and Presence of a Methionine-Depleting Enzyme in Normal and Cancer Cells.

Author

Montalbano, Serena, Raboni, Samanta, Sidoli, Simone, Mozzarelli, Andrea, Bettati, Stefano, and Buschini, Annamaria

Subjects

*ENZYME analysis, *NUCLEAR proteins, *METHIONINE, *LYASES, *DNA methylation, *AMINES, *HISTONES, *MASS spectrometry, *TUMORS, *CELL lines, *EPITHELIAL cells, *EPIGENOMICS, *PEPTIDES, *CELL death

Abstract

Simple Summary: Cancer cells exhibit unique metabolic properties, including a high requirement for methionine. However, the mechanism that explains how cancer cells suffer from the absence of methionine more significantly than healthy cells remains elusive. Methionine is essential for epigenetic reprogramming of cells, both at the DNA level and for post-translation histone code modification. The post-translational modifications of histone variants (hPTMs) in normal and cancer cells were characterized by mass-spectrometry in the absence and presence of methionine gamma-lyase (MGL), a bacterial enzyme that degrades methionine and inhibits the growth of cancer cells. Results indicate a complex pattern of PTMs on histone variants and striking differences between normal and cancer cells that might help in the understanding of the molecular mechanisms triggered by methionine depletion and in the fine-tuning of MGL-based cancer therapy. Methionine is an essential amino acid involved in the formation of polyamines and a precursor metabolite for DNA and protein methylation. The dependence of cancer cells on methionine has triggered extensive investigations aimed at its targeting for cancer therapy, including the exploitation as a therapeutic tool of methionine γ-lyase (MGL), a bacterial enzyme that degrades methionine, capable of inhibiting cancer cells growth due to methionine starvation. We have exploited the high-resolution power of mass spectrometry to compare the effects of reduced availability of the methyl donor SAM, induced by MGL treatment, on the post-translational modifications of the histone tails in normal Hs27 and cancer HT-29 cells. In the absence of MGL, our analysis detected a three-fold higher relative abundance of trimethylated K25 of H1.4 in HT-29 than Hs27 cells, and a complex pattern of methylated, unmethylated and acetylated peptides in H2 and H3.3. In the presence of MGL, in HT-29, the peptide H2A1_4_11 is predominantly unmodified with mono-methylated K5 increasing upon treatment, whereas in Hs27 cells, H2A1_4_11 is monomethylated at K5 and K9 with these marks decreasing upon treatment. The time dependence of the effects of MGL-mediated methionine depletion on PTMs of histone variants in HT-29 cancer cells was also monitored. Overall, our present data on histone variants H1, H2A, H2B as well as H3.3 integrated with our previous studies on histones H3 and H4, shed light on the epigenetic modifications associated with methionine starvation and associated cancer cell death. [ABSTRACT FROM AUTHOR]

Published

2023

34. Hydrozoan sperm-specific SPKK motif-containing histone H2B variants stabilise chromatin with limited compaction.

Author

Török, Anna, Browne, Martin J. G., Vilar, Jordina C., Patwal, Indu, DuBuc, Timothy Q., Febrimarsa, Atcheson, Erwan, Frank, Uri, Gornik, Sebastian G., and Flaus, Andrew

Subjects

*BASIC proteins, *CHROMATIN, *NUCLEAR proteins, *COMPACTING, *CELL cycle, *HISTONES

Abstract

Many animals achieve sperm chromatin compaction and stabilisation by replacing canonical histones with sperm nuclear basic proteins (SNBPs) such as protamines during spermatogenesis. Hydrozoan cnidarians and echinoid sea urchins lack protamines and have evolved a distinctive family of sperm-specific histone H2Bs (spH2Bs) with extended N termini rich in SPK(K/R) motifs. Echinoid sperm packaging is regulated by spH2Bs. Their sperm is negatively buoyant and fertilises on the sea floor. Hydroid cnidarians undertake broadcast spawning but their sperm properties are poorly characterised. We show that Hydractinia echinata and H. symbiolongicarpus sperm chromatin possesses higher stability than somatic chromatin, with reduced accessibility to transposase Tn5 integration and to endonucleases in vitro. In contrast, nuclear dimensions are only moderately reduced in mature Hydractinia sperm. Ectopic expression of spH2B in the background of H2B.1 knockdown results in downregulation of global transcription and cell cycle arrest in embryos, without altering their nuclear density. Taken together, SPKK-containing spH2B variants act to stabilise chromatin and silence transcription in Hydractinia sperm with only limited chromatin compaction. We suggest that spH2Bs could contribute to sperm buoyancy as a reproductive adaptation. [ABSTRACT FROM AUTHOR]

Published

2023

35. Chromatin-based DNA replication initiation regulation in eukaryotes

Author

Hao, Lei, Fang, Ruixin, and Long, Haizhen

Published

2023

36. Nuclear envelope, chromatin organizers, histones, and DNA: The many achilles heels exploited across cancers

Author

A. K. Balaji, Santam Saha, Shruti Deshpande, Darshini Poola, and Kundan Sengupta

Subjects

lamins, heterochromatin, genome organization, nuclear envelope, oncohistones, histone variants, Biology (General), QH301-705.5

Abstract

In eukaryotic cells, the genome is organized in the form of chromatin composed of DNA and histones that organize and regulate gene expression. The dysregulation of chromatin remodeling, including the aberrant incorporation of histone variants and their consequent post-translational modifications, is prevalent across cancers. Additionally, nuclear envelope proteins are often deregulated in cancers, which impacts the 3D organization of the genome. Altered nuclear morphology, genome organization, and gene expression are defining features of cancers. With advances in single-cell sequencing, imaging technologies, and high-end data mining approaches, we are now at the forefront of designing appropriate small molecules to selectively inhibit the growth and proliferation of cancer cells in a genome- and epigenome-specific manner. Here, we review recent advances and the emerging significance of aberrations in nuclear envelope proteins, histone variants, and oncohistones in deregulating chromatin organization and gene expression in oncogenesis.

Published

2022

37. H2A.Z's 'social' network: functional partners of an enigmatic histone variant.

Author

Kreienbaum, Carlotta, Paasche, Lena W., and Hake, Sandra B.

Subjects

*GENETIC regulation, *CELL cycle regulation, *POST-translational modification, *GENE expression, *AMINO acids, *TRANSCRIPTION factors

Abstract

The histone variant H2A.Z has been extensively studied to understand its manifold DNA-based functions. In the past years, researchers identified its specific binding partners, the 'H2A.Z interactome', that convey H2A.Z-dependent chromatin changes. Here, we summarize the latest findings regarding vertebrate H2A.Z-associated factors and focus on their roles in gene activation and repression, cell cycle regulation, (neuro)development, and tumorigenesis. Additionally, we demonstrate how protein–protein interactions and post-translational histone modifications can fine-tune the complex interplay of H2A.Z-regulated gene expression. Last, we review the most recent results on interactors of the two isoforms H2A.Z.1 and H2A.Z.2.1, which differ in only three amino acids, and focus on cancer-associated mutations of H2A and H2A.Z, which reveal fascinating insights into the functional importance of such minuscule changes. H2A.Z is involved in gene activation and repression, partly through interaction with post-translational modification (PTM) writer and eraser complexes (directly or through mediators). Focusing on PTMs with regard to the histone code hypothesis and the H2A.Z interactome will shed light on H2A.Z's multitude of functions. More studies display distinct functions for H2A.Z.1 and H2A.Z.2.1 partly through specific interactors, even though they only differ in three amino acids. Focusing on how their binding specificity is achieved will highlight the importance of every amino acid. H2A.Z and its interactors [e.g., PWWP Domain Containing 2A (PWWP2A) and ZNF512B] are emerging as novel regulators in early development and neurodevelopment, associate with diseases as well as cancer development, and offer new therapeutic potential. [ABSTRACT FROM AUTHOR]

Published

2022

38. The histone H3 variant H3.3 regulates gene body DNA methylation in Arabidopsis thaliana

Author

Wollmann, Heike, Stroud, Hume, Yelagandula, Ramesh, Tarutani, Yoshiaki, Jiang, Danhua, Jing, Li, Jamge, Bhagyshree, Takeuchi, Hidenori, Holec, Sarah, Nie, Xin, Kakutani, Tetsuji, Jacobsen, Steven E, and Berger, Frédéric

Subjects

Plant Biology, Biological Sciences, Genetics, Human Genome, Prevention, Biotechnology, Underpinning research, 1.1 Normal biological development and functioning, Generic health relevance, Arabidopsis, Arabidopsis Proteins, Chromatin, DNA (Cytosine-5-)-Methyltransferases, DNA Methylation, DNA, Plant, Epigenesis, Genetic, Genome, Plant, Histones, Plant Proteins, Transcription, Genetic, H3.3, Histone variants, H2A.Z, Linker histone H1, DNA methylation, Environmental Sciences, Information and Computing Sciences, Bioinformatics

Abstract

BackgroundGene bodies of vertebrates and flowering plants are occupied by the histone variant H3.3 and DNA methylation. The origin and significance of these profiles remain largely unknown. DNA methylation and H3.3 enrichment profiles over gene bodies are correlated and both have a similar dependence on gene transcription levels. This suggests a mechanistic link between H3.3 and gene body methylation.ResultsWe engineered an H3.3 knockdown in Arabidopsis thaliana and observed transcription reduction that predominantly affects genes responsive to environmental cues. When H3.3 levels are reduced, gene bodies show a loss of DNA methylation correlated with transcription levels. To study the origin of changes in DNA methylation profiles when H3.3 levels are reduced, we examined genome-wide distributions of several histone H3 marks, H2A.Z, and linker histone H1. We report that in the absence of H3.3, H1 distribution increases in gene bodies in a transcription-dependent manner.ConclusionsWe propose that H3.3 prevents recruitment of H1, inhibiting H1's promotion of chromatin folding that restricts access to DNA methyltransferases responsible for gene body methylation. Thus, gene body methylation is likely shaped by H3.3 dynamics in conjunction with transcriptional activity.

Published

2017

39. H2A-H2B Histone Dimer Plasticity and Its Functional Implications.

Author

Kniazeva, Anastasiia S., Armeev, Grigoriy A., and Shaytan, Alexey K.

Subjects

*MOLECULAR dynamics, *AMINO acid sequence, *POST-translational modification, *HISTONES, *CHROMATIN

Abstract

The protein core of the nucleosome is composed of an H3-H4 histone tetramer and two H2A-H2B histone dimers. The tetramer organizes the central 60 DNA bp, while H2A-H2B dimers lock the flanking DNA segments. Being positioned at the sides of the nucleosome, H2A-H2B dimers stabilize the overall structure of the nucleosome and modulate its dynamics, such as DNA unwrapping, sliding, etc. Such modulation at the epigenetic level is achieved through post-translational modifications and the incorporation of histone variants. However, the detailed connection between the sequence of H2A-H2B histones and their structure, dynamics and implications for nucleosome functioning remains elusive. In this work, we present a detailed study of H2A-H2B dimer dynamics in the free form and in the context of nucleosomes via atomistic molecular dynamics simulations (based on X. laevis histones). We supplement simulation results by comparative analysis of information in the structural databases. Particularly, we describe a major dynamical mode corresponding to the bending movement of the longest H2A and H2B α-helices. This overall bending dynamics of the H2A-H2B dimer were found to be modulated by its interactions with DNA, H3-H4 tetramer, the presence of DNA twist-defects with nucleosomal DNA and the amino acid sequence of histones. Taken together, our results shed new light on the dynamical mechanisms of nucleosome functioning, such as nucleosome sliding, DNA-unwrapping and their epigenetic modulation. [ABSTRACT FROM AUTHOR]

Published

2022

40. H3.3 contributes to chromatin accessibility and transcription factor binding at promoter-proximal regulatory elements in embryonic stem cells

Author

Tafessu, Amanuel, O’Hara, Ryan, Martire, Sara, Dube, Altair L., Saha, Purbita, Gant, Vincent U., and Banaszynski, Laura A.

Published

2023

41. Genes and Chromatin

Author

Carlberg, Carsten, Molnár, Ferdinand, Carlberg, Carsten, and Molnár, Ferdinand

Published

2020

42. Histones and their chaperones: Adaptive remodelers of an ever-changing chromatinic landscape

Author

Karla Torres-Arciga, Manuel Flores-León, Samuel Ruiz-Pérez, Magalli Trujillo-Pineda, Rodrigo González-Barrios, and Luis A. Herrera

Subjects

epigenetics, histone variants, transposons, aging, syndromes, chromatin remodeling, Genetics, QH426-470

Abstract

Chromatin maintenance and remodeling are processes that take place alongside DNA repair, replication, or transcription to ensure the survival and adaptability of a cell. The environment and the needs of the cell dictate how chromatin is remodeled; particularly where and which histones are deposited, thus changing the canonical histone array to regulate chromatin structure and gene expression. Chromatin is highly dynamic, and histone variants and their chaperones play a crucial role in maintaining the epigenetic regulation at different genomic regions. Despite the large number of histone variants reported to date, studies on their roles in physiological processes and pathologies are emerging but continue to be scarce. Here, we present recent advances in the research on histone variants and their chaperones, with a focus on their importance in molecular mechanisms such as replication, transcription, and DNA damage repair. Additionally, we discuss the emerging role they have in transposable element regulation, aging, and chromatin remodeling syndromes. Finally, we describe currently used methods and their limitations in the study of these proteins and highlight the importance of improving the experimental approaches to further understand this epigenetic machinery.

Published

2022

43. Erratum: Breaking the aging epigenetic barrier

Author

Frontiers Production Office

Subjects

senescence, histone variants, chromatin dynamics, cancer, nucleosomes, Biology (General), QH301-705.5

Published

2022

44. Involvement of the H3.3 Histone Variant in the Epigenetic Regulation of Gene Expression in the Nervous System, in Both Physiological and Pathological Conditions

Author

Carlo Maria Di Liegro, Gabriella Schiera, Giuseppe Schirò, and Italia Di Liegro

Subjects

histone variants, H3.3 histone, histone post-translational modifications (PTMs), epigenetic modification of gene expression in brain development and function, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

All the cells of an organism contain the same genome. However, each cell expresses only a minor fraction of its potential and, in particular, the genes encoding the proteins necessary for basal metabolism and the proteins responsible for its specific phenotype. The ability to use only the right and necessary genes involved in specific functions depends on the structural organization of the nuclear chromatin, which in turn depends on the epigenetic history of each cell, which is stored in the form of a collection of DNA and protein modifications. Among these modifications, DNA methylation and many kinds of post-translational modifications of histones play a key role in organizing the complex indexing of usable genes. In addition, non-canonical histone proteins (also known as histone variants), the synthesis of which is not directly linked with DNA replication, are used to mark specific regions of the genome. Here, we will discuss the role of the H3.3 histone variant, with particular attention to its loading into chromatin in the mammalian nervous system, both in physiological and pathological conditions. Indeed, chromatin modifications that mark cell memory seem to be of special importance for the cells involved in the complex processes of learning and memory.

Published

2023

45. Unraveling the Role of Histone Variant CENP-A and Chaperone HJURP Expression in Thymic Epithelial Neoplasms.

Author

Levidou, Georgia, Palamaris, Konstantinos, Sykaras, Alexandros G., Andreadakis, Georgios, Masaoutis, Christos, Theochari, Irene, Korkolopoulou, Penelope, Rontogianni, Dimitra, and Theocharis, Stamatios

Subjects

*HISTONES, *CENTROMERE, *HOLLIDAY junctions, *GENE expression profiling, *EPITHELIAL tumors, *PROGNOSIS, *TUMORS, *OVERALL survival

Abstract

Background: Recent advances demonstrate the role of chromatin regulators, including histone variants and histone chaperones, in cancer initiation and progression. Methods: Histone H3K4me3, histone variant centromere protein (CENP-A) and histone chaperones Holliday junction recognition protein (HJURP) as well as DAXX expression were examined immunohistochemically in 95 thymic epithelial tumor (TET) specimens. Our results were compared with the expression profile of DAXX, HJURP and CENP-A in gene expression profiling interactive analysis (GEPIA2). Results: The lymphocyte-poor B3- and C-type TETs were more frequently DAXX negative (p = 0.043). B3 and C-Type TETs showed higher cytoplasmic and nuclear CENP-A (p = 0.007 and p = 0.002) and higher cytoplasmic HJURP H-score (p < 0.001). Higher nuclear CENP-A and cytoplasmic HJURP expression was associated with advanced Masaoka–Koga stage (p = 0.048 and p < 0.001). A positive correlation between HJURP and CENP-A was also observed. The presence of cytoplasmic CENP-A expression was correlated with a favorable overall survival (p = 0.03). CENP-A overexpression in survival analysis of TCGA TETs showed similar results. H3K4me3 expression was not associated with any clinicopathological parameters. Conclusions: Our results suggest a significant interaction between CENP-A and HJURP in TETs. Moreover, we confirmed the presence of a cytoplasmic CENP-A immunolocalization, suggesting also a possible favorable prognostic value of this specific immunostaining pattern. [ABSTRACT FROM AUTHOR]

Published

2022

46. Localization of Epigenetic Markers in Leishmania Chromatin.

Author

McDonald, Jacquelyn R., Jensen, Bryan C., Sur, Aakash, Wong, Iris L. K., Beverley, Stephen M., and Myler, Peter J.

Subjects

CHROMATIN, RNA polymerases, EPIGENETICS, LEISHMANIA, CHROMOSOME segregation, DNA replication, CENTROMERE

Abstract

Eukaryotes use histone variants and post-translation modifications (PTMs), as well as DNA base modifications, to regulate DNA replication/repair, chromosome condensation, and gene expression. Despite the unusual organization of their protein-coding genes into large polycistronic transcription units (PTUs), trypanosomatid parasites also employ a "histone code" to control these processes, but the details of this epigenetic code are poorly understood. Here, we present the results of experiments designed to elucidate the distribution of histone variants and PTMs over the chromatin landscape of Leishmania tarentolae. These experiments show that two histone variants (H2A.Z and H2B.V) and three histone H3 PTMs (H3K4me3, H3K16ac, and H3K76me3) are enriched at transcription start sites (TSSs); while a histone variant (H3.V) and the trypanosomatid-specific hyper-modified DNA base J are located at transcription termination sites (TTSs). Reduced nucleosome density was observed at all TTSs and TSSs for RNA genes transcribed by RNA polymerases I (RNAPI) or RNAPIII; as well as (to a lesser extent) at TSSs for the PTUs transcribed by RNAPII. Several PTMs (H3K4me3, H3K16ac H3K20me2 and H3K36me3) and base J were enriched at centromeres, while H3K50ac was specifically associated with the periphery of these centromeric sequences. These findings significantly expand our knowledge of the epigenetic markers associated with transcription, DNA replication and/or chromosome segregation in these early diverging eukaryotes and will hopefully lay the groundwork for future studies to elucidate how they control these fundamental processes. [ABSTRACT FROM AUTHOR]

Published

2022

47. Transmission of chromatin states across generations in C. elegans.

Author

Özdemir, Isa and Steiner, Florian A.

Abstract

Epigenetic inheritance refers to the transmission of phenotypes across generations without affecting the genomic DNA sequence. Even though it has been documented in many species in fungi, animals and plants, the mechanisms underlying epigenetic inheritance are not fully uncovered. Epialleles, the heritable units of epigenetic information, can take the form of several biomolecules, including histones and their post-translational modifications (PTMs). Here, we review the recent advances in the understanding of the transmission of histone variants and histone PTM patterns across generations in C. elegans. We provide a general overview of the intergenerational and transgenerational inheritance of histone PTMs and their modifiers and discuss the interplay among different histone PTMs. We also evaluate soma-germ line communication and its impact on the inheritance of epigenetic traits. [ABSTRACT FROM AUTHOR]

Published

2022

48. Histone dynamics during DNA replication stress

Author

Chia-Ling Hsu, Shin Yen Chong, Chia-Yeh Lin, and Cheng-Fu Kao

Subjects

Replication stress, Genome instability, Histone dynamics, Histone modifications, Histone variants, Medicine

Abstract

Abstract Accurate and complete replication of the genome is essential not only for genome stability but also for cell viability. However, cells face constant threats to the replication process, such as spontaneous DNA modifications and DNA lesions from endogenous and external sources. Any obstacle that slows down replication forks or perturbs replication dynamics is generally considered to be a form of replication stress, and the past decade has seen numerous advances in our understanding of how cells respond to and resolve such challenges. Furthermore, recent studies have also uncovered links between defects in replication stress responses and genome instability or various diseases, such as cancer. Because replication stress takes place in the context of chromatin, histone dynamics play key roles in modulating fork progression and replication stress responses. Here, we summarize the current understanding of histone dynamics in replication stress, highlighting recent advances in the characterization of fork-protective mechanisms.

Published

2021

49. CENP-A Modifications on Ser68 and Lys124 Are Dispensable for Establishment, Maintenance, and Long-Term Function of Human Centromeres

Author

Fachinetti, Daniele, Logsdon, Glennis A, Abdullah, Amira, Selzer, Evan B, Cleveland, Don W, and Black, Ben E

Subjects

Biochemistry and Cell Biology, Biological Sciences, Genetics, Cancer, Underpinning research, 1.1 Normal biological development and functioning, Generic health relevance, Autoantigens, Cell Line, Centromere, Centromere Protein A, Chromosomal Proteins, Non-Histone, Genetic Loci, Humans, Lysine, Protein Processing, Post-Translational, Serine, CENP-A, CRISPR, auxin, centromere, chromatin assembly, epigenetics, histone, histone variants, kinetochore, mitosis, Medical and Health Sciences, Developmental Biology, Biochemistry and cell biology

Abstract

CENP-A is a histone H3 variant key to epigenetic specification of mammalian centromeres. Using transient overexpression of CENP-A mutants, two recent reports in Developmental Cell proposed essential centromere functions for post-translational modifications of human CENP-A. Phosphorylation at Ser68 was proposed to have an essential role in CENP-A deposition at centromeres. Blockage of ubiquitination at Lys124 was proposed to abrogate localization of CENP-A to the centromere. Following gene inactivation and replacement in human cells, we demonstrate that CENP-A mutants that cannot be phosphorylated at Ser68 or ubiquitinated at Lys124 assemble efficiently at centromeres during G1, mediate early events in centromere establishment at an ectopic chromosomal locus, and maintain centromere function indefinitely. Thus, neither Ser68 nor Lys124 post-translational modification is essential for long-term centromere identity, propagation, cell-cycle-dependent deposition, maintenance, function, or mediation of early steps in centromere establishment.

Published

2017

50. Breaking the aging epigenetic barrier

Author

Sweta Sikder, Ganesan Arunkumar, Daniël P. Melters, and Yamini Dalal

Subjects

senescence, histone variants, chromatin dynamics, cancer, nucleosomes, Biology (General), QH301-705.5

Abstract

Aging is an inexorable event occurring universally for all organisms characterized by the progressive loss of cell function. However, less is known about the key events occurring inside the nucleus in the process of aging. The advent of chromosome capture techniques and extensive modern sequencing technologies have illuminated a rather dynamic structure of chromatin inside the nucleus. As cells advance along their life cycle, chromatin condensation states alter which leads to a different epigenetic landscape, correlated with modified gene expression. The exact factors mediating these changes in the chromatin structure and function remain elusive in the context of aging cells. The accumulation of DNA damage, reactive oxygen species and loss of genomic integrity as cells cease to divide can contribute to a tumor stimulating environment. In this review, we focus on genomic and epigenomic changes occurring in an aged cell which can contribute to age-related tumor formation.

Published

2022