Your search keyword '"Ribosome biogenesis"' showing total 45 results

1. Human nucleolar protein 7 (NOL7) is required for early pre-rRNA accumulation and pre-18S rRNA processing

Author

Mason A. McCool, Carson J. Bryant, Hannah Huang, Lisa M. Ogawa, Katherine I. Farley-Barnes, Samuel B. Sondalle, Laura Abriola, Yulia V. Surovtseva, and Susan J. Baserga

Subjects

ribosome biogenesis, pre-ribosomal rna processing, rna polymerase i, nucleolus, rrna, oncogene, tumour suppressor, Genetics, QH426-470

Abstract

The main components of the essential cellular process of eukaryotic ribosome biogenesis are highly conserved from yeast to humans. Among these, the U3 Associated Proteins (UTPs) are a small subunit processome subcomplex that coordinate the first two steps of ribosome biogenesis in transcription and pre-18S processing. While we have identified the human counterparts of most of the yeast Utps, the homologs of yeast Utp9 and Bud21 (Utp16) have remained elusive. In this study, we find that NOL7 is the likely ortholog of Bud21. Previously described as a tumour suppressor through regulation of antiangiogenic transcripts, we now show that NOL7 is required for early pre-rRNA accumulation and pre-18S rRNA processing in human cells. These roles lead to decreased protein synthesis and induction of the nucleolar stress response upon NOL7 depletion. Beyond Bud21’s nonessential role in yeast, we establish human NOL7 as an essential UTP that is necessary to maintain both early pre-rRNA levels and processing.

Published

2023

2. RNA folding and functions of RNA helicases in ribosome biogenesis

Author

Valentin Mitterer and Brigitte Pertschy

Subjects

ribosome biogenesis, rrna folding, snornas, rna helicases, Genetics, QH426-470

Abstract

Eukaryotic ribosome biogenesis involves the synthesis of ribosomal RNA (rRNA) and its stepwise folding into the unique structure present in mature ribosomes. rRNA folding starts already co-transcriptionally in the nucleolus and continues when pre-ribosomal particles further maturate in the nucleolus and upon their transit to the nucleoplasm and cytoplasm. While the approximate order of folding of rRNA subdomains is known, especially from cryo-EM structures of pre-ribosomal particles, the actual mechanisms of rRNA folding are less well understood. Both small nucleolar RNAs (snoRNAs) and proteins have been implicated in rRNA folding. snoRNAs hybridize to precursor rRNAs (pre-rRNAs) and thereby prevent premature folding of the respective rRNA elements. Ribosomal proteins (r-proteins) and ribosome assembly factors might have a similar function by binding to rRNA elements and preventing their premature folding. Besides that, a small group of ribosome assembly factors are thought to play a more active role in rRNA folding. In particular, multiple RNA helicases participate in individual ribosome assembly steps, where they are believed to coordinate RNA folding/unfolding events or the release of proteins from the rRNA. In this review, we summarize the current knowledge on mechanisms of RNA folding and on the specific function of the individual RNA helicases involved. As the yeast Saccharomyces cerevisiae is the organism in which ribosome biogenesis and the role of RNA helicases in this process is best studied, we focused our review on insights from this model organism, but also make comparisons to other organisms where applicable.

Published

2022

3. Synergistic interaction network between the snR30 RNP, Utp23, and ribosomal RNA during ribosome synthesis

Author

Timothy J. Vos and Ute Kothe

Subjects

ribosome biogenesis, rna binding, cbf5, rna–protein interaction, h/aca rna, snorna, Genetics, QH426-470

Abstract

snR30/U17 is a highly conserved H/ACA RNA that is required for maturation of the small ribosomal subunit in eukaryotes. By base-pairing to the expansion segment 6 (ES6) of 18S ribosomal RNA (rRNA), the snR30 H/ACA Ribonucleoprotein (RNP) indirectly facilitates processing of the precursor rRNA (pre-rRNA) together with other proteins such as Utp23 and other RNAs acting as ribosome assembly factors. However, the details of the molecular interaction network of snR30 and its binding partners and how these interactions contribute to pre-rRNA processing remains unknown. Here, we report the in vitro reconstitution of a Saccharomyces cerevisiae snR30 RNP and quantitative characterization of the interactions of snR30, H/ACA proteins, the Utp23 protein and ES6 of the 18S rRNA. The snR30 RNA is bound tightly by both H/ACA proteins and Utp23. We dissected the importance of different 18S rRNA regions for snR30 RNP binding and demonstrated that the snR30 complex is tightly anchored on the pre-rRNA through base-pairing to ES6 whereas other reported rRNA binding sites do not contribute to the affinity of the snR30 RNP. On its own, the ribosome assembly factor Utp23 binds in a tight, but unspecific manner to RNA. However, in complex with the snR30 RNP, Utp23 increases the affinity of the RNP for rRNA revealing synergies between snR30 RNP and Utp23 which are enhancing specificity and affinity for rRNA, respectively. Together, these findings provide mechanistic insights how the snR30 RNP and Utp23 cooperate to interact tightly and specifically with rRNA during the early stages of ribosome biogenesis.

Published

2022

4. U8 variants on the brain: a small nucleolar RNA and human disease

Author

Emily J. McFadden and Susan J. Baserga

Subjects

u8 snorna, ribosomopathy, ribosome biogenesis, labrune syndrome, leukoencephalopathy, brain calcifications and cysts, snord118, nucleolus, Genetics, QH426-470

Abstract

Small nucleolar RNAs (snoRNAs) are non-coding RNAs vital for ribosomal RNA (rRNA) maturation. The U8 snoRNA, encoded by the SNORD118 gene in humans, is an atypical C/D box snoRNA as it promotes rRNA cleavage rather than 2′–O–methylation and is unique to vertebrates. The U8 snoRNA is critical for cleavage events that produce the mature 5.8S and 28S rRNAs of the large ribosomal subunit. Unexpectedly, single nucleotide polymorphisms (SNPs) in the SNORD118 gene were recently found causal to the neurodegenerative disease leukoencephalopathy, brain calcifications, and cysts (LCC; aka Labrune syndrome), but its molecular pathogenesis is unclear. Here, we will review current knowledge on the function of the U8 snoRNA in ribosome biogenesis, and connect it to the preservation of brain function in humans as well as to its dysregulation in inherited white matter disease.

Published

2022

5. The dark side of the ribosome life cycle

Author

Sébastien Ferreira-Cerca

Subjects

ribosome, ribosome biogenesis, archaea, non-model organism, rna, Genetics, QH426-470

Abstract

Thanks to genetics, biochemistry, and structural biology many features of the ribosome´s life cycles in models of bacteria, eukaryotes, and some organelles have been revealed to near-atomic details. Collectively, these studies have provided a very detailed understanding of what are now well-established prototypes for ribosome biogenesis and function as viewed from a ‘classical’ model organisms perspective. However, very important challenges remain ahead to explore the functional and structural diversity of both ribosome biogenesis and function across the biological diversity on earth. Particularly, the ‘third domain of life’, the archaea, and also many non-model bacterial and eukaryotic organisms have been comparatively neglected. Importantly, characterizing these additional biological systems will not only offer a yet untapped window to enlighten the evolution of ribosome biogenesis and function but will also help to unravel fundamental principles of molecular adaptation of these central cellular processes.

Published

2022

6. The C-terminal tail of ribosomal protein Rps15 is engaged in cytoplasmic pre-40S maturation

Author

Ingrid Rössler, Sarah Weigl, José Fernández-Fernández, Sara Martín-Villanueva, Daniela Strauss, Ed Hurt, Jesús de la Cruz, and Brigitte Pertschy

Subjects

ribosome biogenesis, 40s ribosomal subunit, ribosomal protein, rps15/us19, yeast, chronic lymphocytic leukaemia, cll, Genetics, QH426-470

Abstract

The small ribosomal subunit protein Rps15/uS19 is involved in early nucleolar ribosome biogenesis and subsequent nuclear export of pre-40S particles to the cytoplasm. In addition, the C-terminal tail of Rps15 was suggested to play a role in mature ribosomes, namely during translation elongation. Here, we show that Rps15 not only functions in nucleolar ribosome assembly but also in cytoplasmic pre-40S maturation, which is indicated by a strong genetic interaction between Rps15 and the 40S assembly factor Ltv1. Specifically, mutations either in the globular or C-terminal domain of Rps15 when combined with the non-essential ltv1 null allele are lethal or display a strong growth defect. However, not only rps15 ltv1 double mutants but also single rps15 C-terminal deletion mutants exhibit an accumulation of the 20S pre-rRNA in the cytoplasm, indicative of a cytoplasmic pre-40S maturation defect. Since in pre-40S particles, the C-terminal tail of Rps15 is positioned between assembly factors Rio2 and Tsr1, we further tested whether Tsr1 is genetically linked to Rps15, which indeed could be demonstrated. Thus, the integrity of the Rps15 C-terminal tail plays an important role during late pre-40S maturation, perhaps in a quality control step to ensure that only 40S ribosomal subunits with functional Rps15 C-terminal tail can efficiently enter translation. As mutations in the C-terminal tail of human RPS15 have been observed in connection with chronic lymphocytic leukaemia, it is possible that apart from defects in translation, an impaired late pre-40S maturation step in the cytoplasm could also be a reason for this disease.

Published

2022

7. Human nucleolar protein 7 (NOL7) is required for early pre-rRNA accumulation and pre-18S rRNA processing.

Author

McCool, Mason A., Bryant, Carson J., Huang, Hannah, Ogawa, Lisa M., Farley-Barnes, Katherine I., Sondalle, Samuel B., Abriola, Laura, Surovtseva, Yulia V., and Baserga, Susan J.

Subjects

NUCLEAR proteins, RIBOSOMAL RNA, ORGANELLE formation, PROTEIN synthesis, CELL anatomy, RIBOSOMES, RIBOSOMAL proteins

Abstract

The main components of the essential cellular process of eukaryotic ribosome biogenesis are highly conserved from yeast to humans. Among these, the U3 Associated Proteins (UTPs) are a small subunit processome subcomplex that coordinate the first two steps of ribosome biogenesis in transcription and pre-18S processing. While we have identified the human counterparts of most of the yeast Utps, the homologs of yeast Utp9 and Bud21 (Utp16) have remained elusive. In this study, we find that NOL7 is the likely ortholog of Bud21. Previously described as a tumour suppressor through regulation of antiangiogenic transcripts, we now show that NOL7 is required for early pre-rRNA accumulation and pre-18S rRNA processing in human cells. These roles lead to decreased protein synthesis and induction of the nucleolar stress response upon NOL7 depletion. Beyond Bud21's nonessential role in yeast, we establish human NOL7 as an essential UTP that is necessary to maintain both early pre-rRNA levels and processing. [ABSTRACT FROM AUTHOR]

Published

2023

8. The dark side of the ribosome life cycle.

Author

Ferreira-Cerca, Sébastien

Subjects

ORGANELLE formation, RIBOSOMES, BIOLOGICAL systems, BIODIVERSITY, BIOCHEMISTRY, GENETICS

Abstract

Thanks to genetics, biochemistry, and structural biology many features of the ribosome's life cycles in models of bacteria, eukaryotes, and some organelles have been revealed to near-atomic details. Collectively, these studies have provided a very detailed understanding of what are now wellestablished prototypes for ribosome biogenesis and function as viewed from a 'classical' model organisms perspective. However, very important challenges remain ahead to explore the functional and structural diversity of both ribosome biogenesis and function across the biological diversity on earth. Particularly, the 'third domain of life', the archaea, and also many non-model bacterial and eukaryotic organisms have been comparatively neglected. Importantly, characterizing these additional biological systems will not only offer a yet untapped window to enlighten the evolution of ribosome biogenesis and function but will also help to unravel fundamental principles of molecular adaptation of these central cellular processes. [ABSTRACT FROM AUTHOR]

Published

2022

9. RNA folding and functions of RNA helicases in ribosome biogenesis.

Author

Mitterer, Valentin and Pertschy, Brigitte

Subjects

ORGANELLE formation, HELICASES, RNA, RIBOSOMAL RNA, NON-coding RNA, RIBOSOMES, RIBOSOMAL proteins

Abstract

Eukaryotic ribosome biogenesis involves the synthesis of ribosomal RNA (rRNA) and its stepwise folding into the unique structure present in mature ribosomes. rRNA folding starts already co-transcriptionally in the nucleolus and continues when pre-ribosomal particles further maturate in the nucleolus and upon their transit to the nucleoplasm and cytoplasm. While the approximate order of folding of rRNA subdomains is known, especially from cryo-EM structures of pre-ribosomal particles, the actual mechanisms of rRNA folding are less well understood. Both small nucleolar RNAs (snoRNAs) and proteins have been implicated in rRNA folding. snoRNAs hybridize to precursor rRNAs (pre-rRNAs) and thereby prevent premature folding of the respective rRNA elements. Ribosomal proteins (r-proteins) and ribosome assembly factors might have a similar function by binding to rRNA elements and preventing their premature folding. Besides that, a small group of ribosome assembly factors are thought to play a more active role in rRNA folding. In particular, multiple RNA helicases participate in individual ribosome assembly steps, where they are believed to coordinate RNA folding/unfolding events or the release of proteins from the rRNA. In this review, we summarize the current knowledge on mechanisms of RNA folding and on the specific function of the individual RNA helicases involved. As the yeast Saccharomyces cerevisiae is the organism in which ribosome biogenesis and the role of RNA helicases in this process is best studied, we focused our review on insights from this model organism, but also make comparisons to other organisms where applicable. [ABSTRACT FROM AUTHOR]

Published

2022

10. Synergistic interaction network between the snR30 RNP, Utp23, and ribosomal RNA during ribosome synthesis.

Author

Vos, Timothy J. and Kothe, Ute

Subjects

RIBOSOMAL RNA, RIBOSOMAL proteins, MOLECULAR interactions, ORGANELLE formation, SACCHAROMYCES cerevisiae, RNA

Abstract

snR30/U17 is a highly conserved H/ACA RNA that is required for maturation of the small ribosomal subunit in eukaryotes. By base-pairing to the expansion segment 6 (ES6) of 18S ribosomal RNA (rRNA), the snR30 H/ACA Ribonucleoprotein (RNP) indirectly facilitates processing of the precursor rRNA (prerRNA) together with other proteins such as Utp23 and other RNAs acting as ribosome assembly factors. However, the details of the molecular interaction network of snR30 and its binding partners and how these interactions contribute to pre-rRNA processing remains unknown. Here, we report the in vitro reconstitution of a Saccharomyces cerevisiae snR30 RNP and quantitative characterization of the interactions of snR30, H/ACA proteins, the Utp23 protein and ES6 of the 18S rRNA. The snR30 RNA is bound tightly by both H/ACA proteins and Utp23. We dissected the importance of different 18S rRNA regions for snR30 RNP binding and demonstrated that the snR30 complex is tightly anchored on the pre-rRNA through base-pairing to ES6 whereas other reported rRNA binding sites do not contribute to the affinity of the snR30 RNP. On its own, the ribosome assembly factor Utp23 binds in a tight, but unspecific manner to RNA. However, in complex with the snR30 RNP, Utp23 increases the affinity of the RNP for rRNA revealing synergies between snR30 RNP and Utp23 which are enhancing specificity and affinity for rRNA, respectively. Together, these findings provide mechanistic insights how the snR30 RNP and Utp23 cooperate to interact tightly and specifically with rRNA during the early stages of ribosome biogenesis. [ABSTRACT FROM AUTHOR]

Published

2022

11. The C-terminal tail of ribosomal protein Rps15 is engaged in cytoplasmic pre-40S maturation.

Author

Rössler, Ingrid, Weigl, Sarah, Fernández-Fernández, José, Martín-Villanueva, Sara, Strauss, Daniela, Hurt, Ed, de la Cruz, Jesús, and Pertschy, Brigitte

Subjects

ORGANELLE formation, CHRONIC leukemia, RIBOSOMES, LYMPHOCYTIC leukemia, RIBOSOMAL proteins, QUALITY control, CYTOPLASM

Abstract

The small ribosomal subunit protein Rps15/uS19 is involved in early nucleolar ribosome biogenesis and subsequent nuclear export of pre-40S particles to the cytoplasm. In addition, the C-terminal tail of Rps15 was suggested to play a role in mature ribosomes, namely during translation elongation. Here, we show that Rps15 not only functions in nucleolar ribosome assembly but also in cytoplasmic pre-40S maturation, which is indicated by a strong genetic interaction between Rps15 and the 40S assembly factor Ltv1. Specifically, mutations either in the globular or C-terminal domain of Rps15 when combined with the non-essential ltv1 null allele are lethal or display a strong growth defect. However, not only rps15 ltv1 double mutants but also single rps15 C-terminal deletion mutants exhibit an accumulation of the 20S pre-rRNA in the cytoplasm, indicative of a cytoplasmic pre-40S maturation defect. Since in pre-40S particles, the C-terminal tail of Rps15 is positioned between assembly factors Rio2 and Tsr1, we further tested whether Tsr1 is genetically linked to Rps15, which indeed could be demonstrated. Thus, the integrity of the Rps15 C-terminal tail plays an important role during late pre-40S maturation, perhaps in a quality control step to ensure that only 40S ribosomal subunits with functional Rps15 C-terminal tail can efficiently enter translation. As mutations in the C-terminal tail of human RPS15 have been observed in connection with chronic lymphocytic leukaemia, it is possible that apart from defects in translation, an impaired late pre-40S maturation step in the cytoplasm could also be a reason for this disease. [ABSTRACT FROM AUTHOR]

Published

2022

12. U8 variants on the brain: a small nucleolar RNA and human disease.

Author

McFadden, Emily J. and Baserga, Susan J.

Subjects

NON-coding RNA, RIBOSOMAL RNA, LEUKOENCEPHALOPATHIES, ORGANELLE formation, SINGLE nucleotide polymorphisms, RIBOSOMES

Abstract

Small nucleolar RNAs (snoRNAs) are non-coding RNAs vital for ribosomal RNA (rRNA) maturation. The U8 snoRNA, encoded by the SNORD118 gene in humans, is an atypical C/D box snoRNA as it promotes rRNA cleavage rather than 2'-O-methylation and is unique to vertebrates. The U8 snoRNA is critical for cleavage events that produce the mature 5.8S and 28S rRNAs of the large ribosomal subunit. Unexpectedly, single nucleotide polymorphisms (SNPs) in the SNORD118 gene were recently found causal to the neurodegenerative disease leukoencephalopathy, brain calcifications, and cysts (LCC; aka Labrune syndrome), but its molecular pathogenesis is unclear. Here, we will review current knowledge on the function of the U8 snoRNA in ribosome biogenesis, and connect it to the preservation of brain function in humans as well as to its dysregulation in inherited white matter disease. [ABSTRACT FROM AUTHOR]

Published

2022

13. In vitro dimerization of human RIO2 kinase.

Author

Maurice, Frédérique, Pérébaskine, Natacha, Thore, Stéphane, and Fribourg, Sébastien

Abstract

RIO proteins form a conserved family of atypical protein kinases. RIO2 is a serine/threonine protein kinase/ATPase involved in pre-40S ribosomal maturation. Current crystal structures of archaeal and fungal Rio2 proteins report a monomeric form of the protein. Here, we describe three atomic structures of the human RIO2 kinase showing that it forms a homodimer in vitro. Upon self-association, each protomer ATP-binding pocket is partially remodelled and found in an apostate. The homodimerization is mediated by key residues previously shown to be responsible for ATP binding and catalysis. This unusual in vitro protein kinase dimer reveals an intricate mechanism where identical residues are involved in substrate binding and oligomeric state formation. We speculate that such an oligomeric state might be formed also in vivo and might function in maintaining the protein in an inactive state and could be employed during import. [ABSTRACT FROM AUTHOR]

Published

2019

14. The human RNA helicase DHX37 is required for release of the U3 snoRNP from pre-ribosomal particles.

Author

Choudhury, Priyanka, Hackert, Philipp, Memet, Indira, Sloan, Katherine E., and Bohnsack, Markus T.

Abstract

Ribosome synthesis is an essential cellular process, and perturbation of human ribosome production is linked to cancer and genetic diseases termed ribosomopathies. During their assembly, pre-ribosomal particles undergo numerous structural rearrangements, which establish the architecture present in mature complexes and serve as key checkpoints, ensuring the fidelity of ribosome biogenesis. RNA helicases are essential mediators of such remodelling events and here, we demonstrate that the DEAH-box RNA helicase DHX37 is required for maturation of the small ribosomal subunit in human cells. Our data reveal that the presence of DHX37 in early pre-ribosomal particles is monitored by a quality control pathway and that failure to recruit DHX37 leads to pre-rRNA degradation. Using an in vivo crosslinking approach, we show that DHX37 binds directly to the U3 small nucleolar RNA (snoRNA) and demonstrate that the catalytic activity of the helicase is required for dissociation of the U3 snoRNA from pre-ribosomal complexes. This is an important event during ribosome assembly as it enables formation of the central pseudoknot structure of the small ribosomal subunit. We identify UTP14A as a direct interaction partner of DHX37 and our data suggest that UTP14A can act as a cofactor that stimulates the activity of the helicase in the context of U3 snoRNA release. [ABSTRACT FROM AUTHOR]

Published

2019

15. The role of OncoSnoRNAs and Ribosomal RNA 2’-O-methylation in Cancer

Author

Elena S. Martens-Uzunova, Daniela Barros-Silva, Denis L. J. Lafontaine, Guido Jenster, Jonathan Klavert, and Carmen Jerónimo

Subjects

Methyltransferase, cancer prognostics, Ribosome biogenesis, Review, Biology, Methylation, Ribosome, cancer biomarker, cancer therapeutics, SDG 3 - Good Health and Well-being, Neoplasms, Protein biosynthesis, ribosomal RNA 2’-O-methylation, Animals, Humans, RNA, Small Nucleolar, RNA Processing, Post-Transcriptional, Small nucleolar RNA, Molecular Biology, Fibrillarin, cancer diagnostics, Cell Biology, Ribosomal RNA, Cell biology, box C/D snoRNA, RNA, Ribosomal, Ribosomes

Abstract

Ribosomes are essential nanomachines responsible for all protein production in cells. Ribosome biogenesis and function are energy costly processes, they are tightly regulated to match cellular needs. In cancer, major pathways that control ribosome biogenesis and function are often deregulated to ensure cell survival and to accommodate the continuous proliferation of tumour cells. Ribosomal RNAs (rRNAs) are abundantly modified with 2'-O-methylation (Nm, ribomethylation) being one of the most common modifications. In eukaryotic ribosomes, ribomethylation is performed by the methyltransferase Fibrillarin guided by box C/D small nucleolar RNAs (snoRNAs). Accumulating evidences indicate that snoRNA expression and ribosome methylation profiles are altered in cancer. Here we review our current knowledge on differential snoRNA expression and rRNA 2ʹ-O methylation in the context of human malignancies, and discuss the consequences and opportunities for cancer diagnostics, prognostics, and therapeutics.

Published

2021

16. Efficient fractionation and analysis of ribosome assembly intermediates in human cells

Author

Russell T. Sapio, Blanca Nieto, Dimitri G. Pestov, Sonia G. Gaspar, Mercedes Dosil, Laura Clavaín, Xosé R. Bustelo, Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Instituto Nacional de Salud (España), Junta de Castilla y León, Asociación Española Contra el Cáncer, Fundación 'la Caixa', Fundación Memoria de D. Samuel Solorzano Barruso, Universidad de Salamanca, Banco Santander, Ministerio de Educación, Cultura y Deporte (España), and European Commission

Subjects

Ribosomal Proteins, Affinity matrix, Human ribosome synthesis, pre-rRNA maturation, Preribosome, Nucleolus, Mutant, preribosomes, Ribosome biogenesis, Biology, Ribosome, Ribosome assembly, Technical Report, RNA Precursors, Humans, Molecular Biology, Technical Paper, Cell Biology, HCT116 Cells, Cell biology, Preribosomes, RNA, Ribosomal, Pre-rRNA maturation, Extraction methods, ribosome assembly, Ribosomes, Cell Nucleolus, HeLa Cells

Abstract

© 2021 The Author(s)., Biochemical studies of the human ribosome synthesis pathway have been hindered by technical difficulties in obtaining intact preribosomal complexes from internal regions of the nucleolus. Here we provide a detailed description of an extraction method that enables efficient detection, isolation, and characterization of nucleolar preribosomes containing large pre-rRNA species. The three-step Preribosome Sequential Extraction (PSE) protocol preserves the integrity of early preribosomal complexes and yields preparations amenable to biochemical analyses from low amounts of starting material. We validate this procedure through the detection of specific trans-acting factors and pre-rRNAs in the extracted preribosomes using affinity matrix pull-downs and sedimentation assays. In addition, we describe the application of the PSE method for monitoring cellular levels of ribosome-free 5S RNP complexes as an indicator of ribosome biogenesis stress. Our optimized experimental procedures will facilitate studies of human ribosome biogenesis in normal, mutant and stressed-cell scenarios, including the characterization of candidate ribosome biogenesis factors, preribosome interactors under specific physiological conditions or effects of drugs on ribosome maturation., This work was supported by the Spanish Ministry of Science and Innovation [BFU2017-88192-P to MD][RTI2018-096481-B-100 to XRB]; the National Institutes of Health [R03CA246009 to DGP]; the Castilla-León autonomous government [CSI252P18 and CSI145P2 to XRB]; the Spanish Association against Cancer [GC16173472GARC to XRB]; “la Caixa” Banking Foundation [HR20-00164 to XRB]; and the Samuel Solórzano Foundation [FS/36-2017 to MD]. BN has been supported by a predoctoral contract sponsored by the University of Salamanca and Santander Bank, SGG by a predoctoral FPU contract of the Spanish Ministry of Education, Culture and Sports, and LC by a predoctoral contract from the Spanish Association against Cancer. The Centro de Investigación del Cáncer is supported by the Programa de Apoyo a Planes Estratégicos de Investigación de Estructuras de Investigación de Excelencia of the Ministry of Education of the Castilla-León Government (CLC-2017-01). Both the Spanish and Castilla-León government-associated funding is partially supported by the European Regional Development Fund.

Published

2021

17. RNA-Seq employing a novel rRNA depletion strategy reveals a rich repertoire of snoRNAs in Euglena gracilis including box C/D and Ψ-guide RNAs targeting the modification of rRNA extremities.

Author

Moore, Ashley N., McWatters, David C., Hudson, Andrew J., and Russell, Anthony G.

Abstract

Previous mRNA transcriptome studies of Euglena gracilis have shown that this organism possesses a large and diverse complement of protein coding genes; however, the study of non-coding RNA classes has been limited. The natural extensive fragmentation of the E. gracilis large subunit ribosomal RNA presents additional barriers to the identification of non-coding RNAs as size-selected small RNA libraries will be dominated by rRNA sequences. In this study we have developed a strategy to significantly reduce rRNA amplification prior to RNA-Seq analysis thereby producing a ncRNA library allowing for the identification of many new E. gracilis small RNAs. Library analysis reveals 113 unique new small nucleolar (sno) RNAs and a large collection of snoRNA isoforms, as well as the first significant collection of nuclear tRNAs in this organism. A 3′ end AGAUGN consensus motif and conserved structural features can now be defined for E. gracilis pseudouridine guide RNAs. snoRNAs of both classes were identified that target modification of the 3′ extremities of rRNAs utilizing predicted base-pairing interactions with internally transcribed spacers (ITS), providing insight into the timing of steps in rRNA maturation. Cumulatively, this represents the most comprehensive analysis of small ncRNAs in Euglena gracilis to date. [ABSTRACT FROM AUTHOR]

Published

2018

18. Multiple Puf proteins regulate the stability of ribosome biogenesis transcripts.

Author

Fischer, Anthony D. and Olivas, Wendy M.

Abstract

Cells must make careful use of the resources available to them. A key area of cellular regulation involves the biogenesis of ribosomes. Transcriptional regulation of ribosome biogenesis factor genes through alterations in histone acetylation has been well studied. This work identifies a post-transcriptional mechanism of ribosome biogenesis regulation by Puf protein control of mRNA stability. Puf proteins are eukaryotic mRNA binding proteins that play regulatory roles in mRNA degradation and translation via association with specific conserved elements in the 3ʹ untranslated region (UTR) of target mRNAs and with degradation and translation factors. We demonstrate that several ribosome biogenesis factor mRNAs in Saccharomyces cerevisiae containing a canonical Puf4p element in their 3ʹ UTRs are destabilized by Puf2p, Puf4, and Puf5p, yet stabilized by Puf1p and Puf3p. In the absence of all Puf proteins, these ribosome biogenesis mRNAs are destabilized by a secondary mechanism involving the same 3ʹ UTR element. Unlike other targets of Puf4p regulation, the decay of these transcripts is not altered by carbon source. Overexpression of Puf4p results in delayed ribosomal RNA processing and altered ribosomal subunit trafficking. These results represent a novel role for Puf proteins in yeast as regulators of ribosome biogenesis transcript stability. [ABSTRACT FROM AUTHOR]

Published

2018

19. Domain definition and interaction mapping for the endonuclease complex hNob1/hPno1.

Author

Raoelijaona, Finaritra, Thore, Stéphane, and Fribourg, Sébastien

Abstract

Ribosome biogenesis requires a variety of trans-acting factors in order to produce functional ribosomal subunits. In human cells, the complex formed by the proteins hNob1 and hPno1 is crucial to the site 3 cleavage occurring at the 3ʹ-end of 18S pre-rRNA. However, the properties and activity of this complex are still poorly understood. We present here a detailed characterization of hNob1 organization and its interaction with hPno1. We redefine the boundaries of the endonuclease PIN domain present in hNob1 and we further delineate the precise interacting modules required for complex formation in hNob1 and hPno1. Altogether, our data contributes to a better understanding of the complex biology required during the site 3 cleavage step in ribosome biogenesis. [ABSTRACT FROM AUTHOR]

Published

2018

20. Insights into remodeling events during eukaryotic large ribosomal subunit assembly provided by high resolution cryo-EM structures.

Author

Biedka, Stephanie, Wu, Shan, LaPeruta, Amber J., Gao, Ning, and Woolford, John L.

Abstract

Ribosomes are responsible for translating the genome, in the form of mRNA, into the proteome in all organisms. Biogenesis of ribosomes in eukaryotes is a complex process involving numerous remodeling events driven in part by the concerted actions of hundreds of protein assembly factors. A major challenge in studying eukaryotic ribosome assembly has, until recently, been a lack of structural data to facilitate understanding of the conformational and compositional changes the pre-ribosome undergoes during its construction. Cryo-electron microscopy (cryo-EM) has begun filling these gaps; recent advances in cryo-EM have enabled the determination of several high resolution pre-ribosome structures. This review focuses mainly on lessons learned from the study of pre-60S particles purified from yeast using the assembly factor Nog2 as bait. These Nog2 particles provide insight into many aspects of nuclear stages of 60S subunit assembly, including construction of major 60S subunit functional centers and processing of the ITS2 spacer RNA. [ABSTRACT FROM PUBLISHER]

Published

2017

21. LARP1 isoform expression in human cancer cell lines

Author

Sarah Bonham, Josephine Morris, Martin Fellermeyer, Roman Fischer, Andrew D Beggs, Joanne D. Stockton, James Chettle, Pia Neubert, Hagen Schwenzer, Sarah P. Blagden, and Mai Abdel Mouti

Subjects

Gene isoform, alternative protein isoforms, Ribosome biogenesis, RNA-binding protein, Biology, Autoantigens, LARP1, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, medicine, cancer, Humans, Protein Isoforms, Amino Acid Sequence, Gene Silencing, RNA Binding Proteins, Promoter Regions, Genetic, Molecular Biology, 030304 developmental biology, 0303 health sciences, Cancer, RNA-Binding Proteins, Cell Biology, DNA Methylation, medicine.disease, In vitro, Cell biology, Gene Expression Regulation, Neoplastic, Alternative Splicing, Ribonucleoproteins, Cell culture, Organ Specificity, 030220 oncology & carcinogenesis, Multigene Family, Cancer cell, RNA, Research Article, Research Paper, Protein Binding

Abstract

LARP1 is an oncogenic RNA-binding protein required for ribosome biogenesis and cancer cell survival. From published in vitro studies, there is disparity over which of two different LARP1 protein isoforms (termed the long LI-LARP1 and short SI-LARP1) is the canonical. Here, after conducting a series of biochemical and cellular assays, we conclude that LI-LARP1 (NM_033551.3 > NP_056130.2) is the dominantly expressed form. We observe that SI-LARP1 (NM_015315.5> NP_056130.2) is epigenetically repressed and that this repression is evolutionarily conserved in all but a small subclade of mammalian species. As with other LARP family members, there are multiple potential LARP1 mRNA isoforms that appear to be censored within the nucleus. The capacity of the cell to modulate splicing and expression of these apparently ‘redundant’ mRNAs hints at contextually specific mechanisms of LARP1 expression.

Published

2020

22. Sgd1 is an MIF4G domain-containing cofactor of the RNA helicase Fal1 and associates with the 5’ domain of the 18S rRNA sequence

Author

Jimena Davila Gallesio, Philipp Hackert, Katherine E. Bohnsack, and Markus T. Bohnsack

Subjects

Models, Molecular, RNA helicase, Saccharomyces cerevisiae Proteins, Protein Conformation, Ribosome biogenesis, Saccharomyces cerevisiae, Biology, Ribosome, 18S ribosomal RNA, 03 medical and health sciences, 0302 clinical medicine, Protein Domains, RNA, Ribosomal, 18S, Binding site, Molecular Biology, 030304 developmental biology, 0303 health sciences, Binding Sites, RNA, Nuclear Proteins, RNA-Binding Proteins, Cell Biology, Ribosomal RNA, small nucleolar RNA (snoRNA), RNA Helicase A, Cell biology, MIF4G domain, ribosome, 030220 oncology & carcinogenesis, Nucleic Acid Conformation, Biogenesis, SSU processome, Research Paper, Protein Binding

Abstract

Assembly of eukaryotic ribosomal subunits is a complex and dynamic process involving the action of more than 200 trans-acting assembly factors. Although recent cryo-electron microscopy structures have provided information on architecture of several pre-ribosomal particles and the binding sites of many AFs, the RNA and protein interactions of many other AFs not captured in these snapshots still remain elusive. RNA helicases are key regulators of structural rearrangements within pre-ribosomal complexes and here we have analysed the eIF4A-like RNA helicase Fal1 and its putative cofactor Sgd1. Our data show that these proteins interact directly via the MIF4G domain of Sgd1 and that the MIF4G domain of Sgd1 stimulates the catalytic activity of Fal1 in vitro. The catalytic activity of Fal1, and the interaction between Fal1 and Sgd1, are required for efficient pre-rRNA processing at the A0, A1 and A2 sites. Furthermore, Sgd1 co-purifies the early small subunit biogenesis factors Lcp5 and Rok1, suggesting that the Fal1-Sgd1 complex likely functions within the SSU processome. In vivo crosslinking data reveal that Sgd1 binds to helix H12 of the 18S rRNA sequence and we further demonstrate that this interaction is formed by the C-terminal region of the protein, which is essential for its function in ribosome biogenesis.

Published

2020

23. Proteome distribution between nucleoplasm and nucleolus and its relation to ribosome biogenesis in Arabidopsis thaliana.

Author

Palm, Denise, Simm, Stefan, Darm, Katrin, Weis, Benjamin L., Ruprecht, Maike, Schleiff, Enrico, and Scharf, Christian

Published

2016

24. The cytoplasmic mRNA degradation factor Pat1 is required for rRNA processing.

Author

Muppavarapu, Mridula, Huch, Susanne, and Nissan, Tracy

Published

2016

25. The human RNA helicase DHX37 is required for release of the U3 snoRNP from pre-ribosomal particles

Author

Indira Memet, Philipp Hackert, Katherine E. Sloan, Markus T. Bohnsack, and Priyanka Choudhury

Subjects

RNA helicase, Ribosome biogenesis, ribosome biogenesis, snoRNA, Ribosome, Catalysis, Ribosome assembly, DEAD-box RNA Helicases, 03 medical and health sciences, 0302 clinical medicine, Ribonucleoproteins, Small Nucleolar, Cell Line, Tumor, Humans, RNA, Small Nucleolar, Small nucleolar RNA, RNA Processing, Post-Transcriptional, Molecular Biology, 030304 developmental biology, protein cofactor, 0303 health sciences, biology, Helicase, Cell Biology, Ribosomal RNA, RNA Helicase A, Cell biology, ribosome, RNA processing, 030220 oncology & carcinogenesis, biology.protein, Pseudoknot, Ribosomes, Research Paper, Protein Binding

Abstract

Ribosome synthesis is an essential cellular process, and perturbation of human ribosome production is linked to cancer and genetic diseases termed ribosomopathies. During their assembly, pre-ribosomal particles undergo numerous structural rearrangements, which establish the architecture present in mature complexes and serve as key checkpoints, ensuring the fidelity of ribosome biogenesis. RNA helicases are essential mediators of such remodelling events and here, we demonstrate that the DEAH-box RNA helicase DHX37 is required for maturation of the small ribosomal subunit in human cells. Our data reveal that the presence of DHX37 in early pre-ribosomal particles is monitored by a quality control pathway and that failure to recruit DHX37 leads to pre-rRNA degradation. Using an in vivo crosslinking approach, we show that DHX37 binds directly to the U3 small nucleolar RNA (snoRNA) and demonstrate that the catalytic activity of the helicase is required for dissociation of the U3 snoRNA from pre-ribosomal complexes. This is an important event during ribosome assembly as it enables formation of the central pseudoknot structure of the small ribosomal subunit. We identify UTP14A as a direct interaction partner of DHX37 and our data suggest that UTP14A can act as a cofactor that stimulates the activity of the helicase in the context of U3 snoRNA release.

Published

2018

26. Immature large ribosomal subunits containing the 7S pre-rRNA can engage in translation in Saccharomyces cerevisiae.

Author

Rodríguez-Galán, Olga, García-Gómez, Juan J, Kressler, Dieter, and de la Cruz, Jesús

Published

2015

27. The RNA recognition motif of NIFK is required for rRNA maturation during cell cycle progression.

Author

Pan, Wen-An, Tsai, Hsin-Yue, Wang, Shun-Chang, Hsiao, Michael, Wu, Pei-Yu, and Tsai, Ming-Daw

Published

2015

28. Contributions of transcription and mRNA decay to gene expression dynamics of fission yeast in response to oxidative stress.

Author

Marguerat, Samuel, Lawler, Katherine, Brazma, Alvis, and Bähler, Jürg

Published

2014

29. The DExD box ATPase DDX55 is recruited to domain IV of the 28S ribosomal RNA by its C-terminal region

Author

Jens Kretschmer, Markus T. Bohnsack, Katherine E. Bohnsack, Priyanka Choudhury, and Philipp Hackert

Subjects

RNA helicase, RNA-protein interaction, Ribosome biogenesis, Ribosome, DEAD-box RNA Helicases, 03 medical and health sciences, 0302 clinical medicine, RNA, Transfer, RNA-Protein Interaction, 28S ribosomal RNA, RNA, Ribosomal, 28S, RNA Precursors, Humans, RNA, Small Nucleolar, ATPase, Protein Interaction Domains and Motifs, Amino Acid Sequence, RNA, Messenger, Binding site, Molecular Biology, 030304 developmental biology, 0303 health sciences, Binding Sites, Organelle Biogenesis, ribonucleoprotein complex (RNP), biology, Base Sequence, Sequence Homology, Amino Acid, RNA, Helicase, Cell Biology, RNA Helicase A, Recombinant Proteins, Cell biology, MicroRNAs, HEK293 Cells, ribosome, 030220 oncology & carcinogenesis, Protein Biosynthesis, biology.protein, Nucleic Acid Conformation, RNA, Long Noncoding, Ribosomes, Sequence Alignment, HeLa Cells, Protein Binding, Research Article, Research Paper

Abstract

RNA helicases contribute to diverse aspects of RNA metabolism through their functions in re-arranging RNA structures. Identification of the remodelling targets of RNA helicases is a critical step in elucidating their cellular functions. Here, we show that, in contrast to many other ribosome biogenesis factors, the DExD box ATPase DDX55 predominantly localizes to the nucleoplasm and we identify a nuclear localization signal within the C-terminal region of the protein. DDX55 associates with pre-ribosomal subunits in human cells and is required for maturation of large subunit pre-rRNAs. Interestingly, in vitro analyses show that DDX55 selectively associates with double-stranded RNA substrates, which also stimulate its ATPase activity, and our data suggest that the C-terminal region of DDX55 contributes to this substrate specificity. The C-terminal region of DDX55 is also necessary for recruitment of the helicase to pre-ribosomes and, using in vivo crosslinking, we reveal a binding site for DDX55 in helix H62 of the 28S ribosomal RNA. Taken together, these data highlight the importance of the C-terminal region of DDX55 in substrate specificity and recruitment, and identify domain IV as a potential remodelling target of DDX55 during LSU biogenesis.

Published

2020

30. Auxiliary domains of the HrpB bacterial DExH-box helicase shape its RNA preferences

Author

Karl Perron, Stéphane Hausmann, Verena Ducret, Johan Geiser, Martina Valentini, and Oscar Vadas

Subjects

Models, Molecular, RNA helicase, Protein Conformation, Ribosome biogenesis, RNA-binding protein, RNA-binding proteins, DEAD-box RNA Helicases, 03 medical and health sciences, Structure-Activity Relationship, 0302 clinical medicine, Bacterial Proteins, ATPase, Protein Interaction Domains and Motifs, Amino Acid Sequence, HDX-MS, Molecular Biology, 030304 developmental biology, Ribonucleoprotein, Sequence Deletion, ddc:616, Adenosine Triphosphatases, 0303 health sciences, Binding Sites, biology, Helicase, RNA, Cell Biology, RNA Helicase A, Cell biology, ddc:580, Phenotype, 030220 oncology & carcinogenesis, RNA splicing, Mutation, Pseudomonas aeruginosa, biology.protein, DExH-box, Function (biology), Protein Binding, Research Paper

Abstract

RNA helicases are fundamental players in RNA metabolism: they remodel RNA secondary structures and arrange ribonucleoprotein complexes. While DExH-box RNA helicases function in ribosome biogenesis and splicing in eukaryotes, information is scarce about bacterial homologs. HrpB is the only bacterial DExH-box protein whose structure is solved. Besides the catalytic core, HrpB possesses three accessory domains, conserved in all DExH-box helicases, plus a unique C-terminal extension (CTE). The function of these auxiliary domains remains unknown. Here, we characterize genetically and biochemically Pseudomonas aeruginosa HrpB homolog. We reveal that the auxiliary domains shape HrpB RNA preferences, affecting RNA species recognition and catalytic activity. We show that, among several types of RNAs, the single-stranded poly(A) and the highly structured MS2 RNA strongly stimulate HrpB ATPase activity. In addition, deleting the CTE affects only stimulation by structured RNAs like MS2 and rRNAs, while deletion of accessory domains results in gain of poly(U)-dependent activity. Finally, using hydrogen-deuterium exchange, we dissect the molecular details of HrpB interaction with poly(A) and MS2 RNAs. The catalytic core interacts with both RNAs, triggering a conformational change that reorients HrpB. Regions within the accessory domains and CTE are, instead, specifically responsive to MS2. Altogether, we demonstrate that in bacteria, like in eukaryotes, DExH-box helicase auxiliary domains are indispensable for RNA handling., Graphical Abstract

Published

2020

31. Domain definition and interaction mapping for the endonuclease complex hNob1/hPno1

Author

Finaritra Raoelijaona, Sébastien Fribourg, Stéphane Thore, Acides Nucléiques : Régulations Naturelle et Artificielle (ARNA), Université de Bordeaux (UB)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS), This work was funded by ANR grant (ANR Blanc 2010 grant RIBOPRE40S (ANR-10-BLAN-1224) and RIBOMAN ANR-16-CE11-0029 to S.F.), the INSERM and the University of Bordeaux., ANR-10-BLAN-1224,RIBOPRE40S,Analyse structurale et fonctionnelle du processus de maturation des précurseurs de la petite sous-unité ribosomique eucaryote(2010), and ANR-16-CE11-0029,RIBOMAN,Une approche intégrative de la biogenèse des ribosomes(2016)

Subjects

Models, Molecular, 0301 basic medicine, pre-rRNA, Ribosome biogenesis, Computational biology, Biology, Brief Communication, Cleavage (embryo), endonuclease, Domain definition, PIN domain, 03 medical and health sciences, Endonuclease, Protein Domains, Catalytic Domain, Protein Interaction Mapping, Humans, [SDV.BBM.BC]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biochemistry [q-bio.BM], Molecular Biology, Binding Sites, Sequence Homology, Amino Acid, Nuclear Proteins, RNA-Binding Proteins, Cell Biology, Ribosomal RNA, KH domain, 030104 developmental biology, Amino Acid Substitution, biology.protein, Endonuclease complex, zinc ribbon

Abstract

International audience; Ribosome biogenesis requires a variety of trans-acting factors in order to produce functional ribosomal subunits. In human cells, the complex formed by the proteins hNob1 and hPno1 is crucial to the site 3 cleavage occurring at the 3'-end of 18S pre-rRNA. However, the properties and activity of this complex are still poorly understood. We present here a detailed characterization of hNob1 organization and its interaction with hPno1. We redefine the boundaries of the endonuclease PIN domain present in hNob1 and we further delineate the precise interacting modules required for complex formation in hNob1 and hPno1. Altogether, our data contributes to a better understanding of the complex biology required during the site 3 cleavage step in ribosome biogenesis.

Published

2018

32. RNA helicases.

Author

Owttrim, George W.

Published

2013

33. Human RioK3 is a novel component of cytoplasmic pre-40S pre-ribosomal particles.

Author

Baumas, Kamila, Soudet, Julien, Caizergues-Ferrer, Michele, Faubladier, Marlene, Yves, Henry, and Mougin, Annie

Published

2012

34. The nucleolar protein Nop19p interacts preferentially with Utp25p and Dhr2p and is essential for the production of the 40S ribosomal subunit in Saccharomyces cerevisiae.

Author

Choque, Elodie, Marcellin, Marlène, Burlet-Schiltz, Odile, Gadal, Olivier, and Dez, Christophe

Published

2011

35. Nop6, a component of 90S pre-ribosomal particles, is required for 40S ribosomal subunit biogenesis in Saccharomyces cerevisiae.

Author

García-Gómez, Juan José, Babiano, Reyes, Lebaron, Simon, Froment, Carine, Monsarrat, Bernard, Henry, Yves, and de la Cruz, Jesús

Published

2011

36. Insights into remodeling events during eukaryotic large ribosomal subunit assembly provided by high resolution cryo-EM structures

Author

Stephanie Biedka, Ning Gao, Shan Wu, Amber LaPeruta, and John L. Woolford

Subjects

0301 basic medicine, Models, Molecular, Saccharomyces cerevisiae Proteins, Protein Conformation, Ribosome biogenesis, ribosome biogenesis, Saccharomyces cerevisiae, Biology, Ribosome, GTP Phosphohydrolases, 03 medical and health sciences, Large ribosomal subunit, DNA, Ribosomal Spacer, Molecular Biology, remodeling, high resolution cryo-EM, Eukaryotic Large Ribosomal Subunit, Cryoelectron Microscopy, RNA, Cell Biology, Ribosome Subunits, Large, Eukaryotic, Cell biology, 030104 developmental biology, Point Of View, Protein Biosynthesis, Proteome, Assembly intermediates, Protein Multimerization, Eukaryotic Ribosome, Biogenesis

Abstract

Ribosomes are responsible for translating the genome, in the form of mRNA, into the proteome in all organisms. Biogenesis of ribosomes in eukaryotes is a complex process involving numerous remodeling events driven in part by the concerted actions of hundreds of protein assembly factors. A major challenge in studying eukaryotic ribosome assembly has, until recently, been a lack of structural data to facilitate understanding of the conformational and compositional changes the pre-ribosome undergoes during its construction. Cryo-electron microscopy (cryo-EM) has begun filling these gaps; recent advances in cryo-EM have enabled the determination of several high resolution pre-ribosome structures. This review focuses mainly on lessons learned from the study of pre-60S particles purified from yeast using the assembly factor Nog2 as bait. These Nog2 particles provide insight into many aspects of nuclear stages of 60S subunit assembly, including construction of major 60S subunit functional centers and processing of the ITS2 spacer RNA.

Published

2017

37. Multiple Puf proteins regulate the stability of ribosome biogenesis transcripts

Author

Anthony D. Fischer and Wendy M. Olivas

Subjects

0301 basic medicine, Untranslated region, Saccharomyces cerevisiae Proteins, RNA Stability, Ribosome biogenesis, ribosome biogenesis, Saccharomyces cerevisiae, Puf proteins, Biology, yeast, Ribosome, Mrna decay, 03 medical and health sciences, Pumilio, Gene Expression Regulation, Fungal, Transcriptional regulation, mRNA stability, RNA Processing, Post-Transcriptional, Molecular Biology, 3' Untranslated Regions, Messenger RNA, Binding Sites, RNA-Binding Proteins, Translation (biology), Cell Biology, Ribosomal RNA, 3ʹ UTR, Cell biology, 030104 developmental biology, Ribosomes, Biogenesis, Research Paper

Abstract

Cells must make careful use of the resources available to them. A key area of cellular regulation involves the biogenesis of ribosomes. Transcriptional regulation of ribosome biogenesis factor genes through alterations in histone acetylation has been well studied. This work identifies a post-transcriptional mechanism of ribosome biogenesis regulation by Puf protein control of mRNA stability. Puf proteins are eukaryotic mRNA binding proteins that play regulatory roles in mRNA degradation and translation via association with specific conserved elements in the 3ʹ untranslated region (UTR) of target mRNAs and with degradation and translation factors. We demonstrate that several ribosome biogenesis factor mRNAs in Saccharomyces cerevisiae containing a canonical Puf4p element in their 3ʹ UTRs are destabilized by Puf2p, Puf4, and Puf5p, yet stabilized by Puf1p and Puf3p. In the absence of all Puf proteins, these ribosome biogenesis mRNAs are destabilized by a secondary mechanism involving the same 3ʹ UTR element. Unlike other targets of Puf4p regulation, the decay of these transcripts is not altered by carbon source. Overexpression of Puf4p results in delayed ribosomal RNA processing and altered ribosomal subunit trafficking. These results represent a novel role for Puf proteins in yeast as regulators of ribosome biogenesis transcript stability.

Published

2018

38. A new layer of rRNA regulation by small interference RNAs and the nuclear RNAi pathway

Author

Xuezhu Feng, Yun Wang, Shouhong Guang, Xufei Zhou, and Xiangyang Chen

Subjects

0301 basic medicine, Small interfering RNA, Active Transport, Cell Nucleus, Arabidopsis, Ribosome biogenesis, RNA-binding protein, Biology, Ribosome, 03 medical and health sciences, RNA interference, RNA Precursors, Animals, Homeostasis, RNA, Small Interfering, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Molecular Biology, Point of View, Genetics, Cell Nucleus, Neurospora crassa, RNA, RNA-Binding Proteins, Cell Biology, Argonaute, Ribosomal RNA, Protein Transport, 030104 developmental biology, RNA, Ribosomal, Exoribonucleases, RNA Interference, Ribosomes, Protein Binding

Abstract

Ribosome biogenesis drives cell growth and proliferation, but mechanisms that modulate this process remain poorly understood. For a long time, small rRNA sequences have been widely treated as non-specific degradation products and neglected as garbage sequences. Recently, we identified a new class of antisense ribosomal siRNAs (risiRNAs) that downregulate pre-rRNA through the nuclear RNAi pathway in C. elegans. risiRNAs exhibit sequence characteristics similar to 22G RNA while complement to 18S and 26S rRNA. risiRNAs elicit the translocation of the nuclear Argonaute protein NRDE-3 from the cytoplasm to nucleus and nucleolus, in which the risiRNA/NRDE complex binds to pre-rRNA and silences rRNA expression. Interestingly, when C. elegans is exposed to environmental stimuli, such as cold shock and ultraviolet illumination, risiRNAs accumulate and further turn on the nuclear RNAi-mediated gene silencing pathway. risiRNA may act in a quality control mechanism of rRNA homeostasis. When the exoribonuclease SUSI-1(ceDis3L2) is mutated, risiRNAs are dramatically increased. In this Point of View article, we will summarize our understanding of the small antisense ribosomal siRNAs in a variety of organisms, especially C. elegans, and their possible roles in the quality control mechanism of rRNA homeostasis.

Published

2017

39. The CshA DEAD-box RNA helicase is important for quorum sensing control in Staphylococcus aureus

Author

Stella Oun, Peter Redder, Myriam Girard, Patrick Linder, Caroline Giraud, Anna-Rita Corvaglia, Jean-Philippe Didier, Jacques Schrenzel, Patrice Francois, and Elena Buttazzoni

Subjects

Staphylococcus aureus, RNA helicase, DEAD box, RNA Stability, Ribosome biogenesis, Biology, degradosome, Bacterial degradosome, Hemolysis, Microbiology, DEAD-box RNA Helicases, 03 medical and health sciences, Bacterial Proteins, Molecular Biology, Gene, 030304 developmental biology, ddc:616, Adenosine Triphosphatases, 2. Zero hunger, 0303 health sciences, 030306 microbiology, quorum sensing, RNA, Cell Biology, RNA Helicase A, Enzyme Activation, Quorum sensing, Phenotype, Biofilms, Mutation, Trans-Activators, Degradosome, Research Paper

Abstract

DEAD-box RNA helicases are present in almost all living organisms and participate in various processes of RNA metabolism. Bacterial proteins of this large family were shown to be required for translation initiation, ribosome biogenesis and RNA decay. The latter is primordial for rapid adaptation to changing environmental conditions. In particular, the RhlB RNA helicase from E. coli was shown to assist the bacterial degradosome machinery. Recently, the CshA DEAD-box proteins from Bacillus subtilis and Staphylococcus aureus were shown to interact with proteins that are believed to form the degradosome. S. aureus can cause life-threatening disease, with particular concern focusing on biofilm formation on catheters and prosthetic devices, since in this form the bacteria are almost impossible to eradicate both by the immune system and antibiotic treatment. This persistent state relies on the expression of surface encoded proteins that allow attachment to various surfaces, and contrasts with the dispersal mode of growth that relies on the secretion of proteins such as hemolysins and proteases. The switch between these two states is mainly mediated by the Staphylococcal cell density sensing system encoded by agr. We show that inactivation of the cshA DEAD-box gene results in dysregulation of biofilm formation and hemolysis through modulation of agr mRNA stability. Importantly, inactivation of the agrA gene in the cshA mutant background reverses the defect, indicating that cshA is genetically upstream of agr and that a delicate balance of agr mRNA abundance mediated through stability control by CshA is critical for proper expression of virulence factors.

Published

2013

40. Proteome distribution between nucleoplasm and nucleolus and its relation to ribosome biogenesis in Arabidopsis thaliana

Author

Benjamin L. Weis, Maike Ruprecht, Denise Palm, Enrico Schleiff, Stefan Simm, Christian Scharf, and Katrin Darm

Subjects

0301 basic medicine, Proteome, Nucleolus, Arabidopsis, Ribosome biogenesis, Biology, Ribosome, 03 medical and health sciences, Ribosomal protein, Phosphorylation, RRNA processing, Molecular Biology, Cells, Cultured, Plant Proteins, Nucleoplasm, food and beverages, Acetylation, Cell Biology, Molecular biology, Cell biology, 030104 developmental biology, Cytoplasm, Ribosomes, Cell Nucleolus, Research Paper

Abstract

Ribosome biogenesis is an essential process initiated in the nucleolus. In eukaryotes, multiple ribosome biogenesis factors (RBFs) can be found in the nucleolus, the nucleus and in the cytoplasm. They act in processing, folding and modification of the pre-ribosomal (r)RNAs, incorporation of ribosomal proteins (RPs), export of pre-ribosomal particles to the cytoplasm, and quality control mechanisms. Ribosome biogenesis is best established for Saccharomyces cerevisiae. Plant ortholog assignment to yeast RBFs revealed the absence of about 30% of the yeast RBFs in plants. In turn, few plant specific proteins have been identified by biochemical experiments to act in plant ribosome biogenesis. Nevertheless, a complete inventory of plant RBFs has not been established yet. We analyzed the proteome of the nucleus and nucleolus of Arabidopsis thaliana and the post-translational modifications of these proteins. We identified 1602 proteins in the nucleolar and 2544 proteins in the nuclear fraction with an overlap of 1429 proteins. For a randomly selected set of proteins identified by the proteomic approach we confirmed the localization inferred from the proteomics data by the localization of GFP fusion proteins. We assigned the identified proteins to various complexes and functions and found about 519 plant proteins that have a potential to act as a RBFs, but which have not been experimentally characterized yet. Last, we compared the distribution of RBFs and RPs in the various fractions with the distribution established for yeast.

Published

2016

41. Contributions of transcription and mRNA decay to gene expression dynamics of fission yeast in response to oxidative stress

Author

Samuel, Marguerat, Katherine, Lawler, Alvis, Brazma, and Jürg, Bähler

Subjects

Ribosomal Proteins, Transcription, Genetic, RNA Stability, Adaptation, Biological, ribosome biogenesis, Regulatory Sequences, Ribonucleic Acid, Models, Biological, mRNA turnover, post-transcriptional control, Gene Expression Regulation, Fungal, Schizosaccharomyces, Atf1, Cluster Analysis, Position-Specific Scoring Matrices, oxidative stress, RNA, Messenger, Nucleotide Motifs, Activating Transcription Factor 1, Gene Expression Profiling, mathematical modeling, Phosphoproteins, fission yeast, Schizosaccharomyces pombe Proteins, RNA Polymerase II, Transcriptome, gene regulation, Research Paper

Abstract

The cooperation of transcriptional and post-transcriptional levels of control to shape gene regulation is only partially understood. Here we show that a combination of two simple and non-invasive genomic techniques, coupled with kinetic mathematical modeling, affords insight into the intricate dynamics of RNA regulation in response to oxidative stress in the fission yeast Schizosaccharomyces pombe. This study reveals a dominant role of transcriptional regulation in response to stress, but also points to the first minutes after stress induction as a critical time when the coordinated control of mRNA turnover can support the control of transcription for rapid gene regulation. In addition, we uncover specialized gene expression strategies associated with distinct functional gene groups, such as simultaneous transcriptional repression and mRNA destabilization for genes encoding ribosomal proteins, delayed mRNA destabilization with varying contribution of transcription for ribosome biogenesis genes, dominant roles of mRNA stabilization for genes functioning in protein degradation, and adjustment of both transcription and mRNA turnover during the adaptation to stress. We also show that genes regulated independently of the bZIP transcription factor Atf1p are predominantly controlled by mRNA turnover, and identify putative cis-regulatory sequences that are associated with different gene expression strategies during the stress response. This study highlights the intricate and multi-faceted interplay between transcription and RNA turnover during the dynamic regulatory response to stress.

Published

2014

42. RNA helicases: diverse roles in prokaryotic response to abiotic stress

Author

George W. Owttrim

Subjects

Riboswitch, Small RNA, RNA helicase, abiotic stress, ribosome biogenesis, Review, Biology, prokaryotes, Stress, Physiological, DEAD-box proteins, Molecular Biology, cold-adapted degradosome, RNA, cytoskeleton compartmentalization, Cell Biology, Non-coding RNA, RNA Helicase A, Cell biology, Cold Temperature, Prokaryotic Cells, RNA editing, eIF4A, Protein Biosynthesis, Degradosome, Ribosomes, RNA Helicases

Abstract

Similar to proteins, RNA molecules must fold into the correct conformation and associate with protein complexes in order to be functional within a cell. RNA helicases rearrange RNA secondary structure and RNA-protein interactions in an ATP-dependent reaction, performing crucial functions in all aspects of RNA metabolism. In prokaryotes, RNA helicase activity is associated with roles in housekeeping functions including RNA turnover, ribosome biogenesis, translation and small RNA metabolism. In addition, RNA helicase expression and/or activity are frequently altered during cellular response to abiotic stress, implying they perform defined roles during cellular adaptation to changes in the growth environment. Specifically, RNA helicases contribute to the formation of cold-adapted ribosomes and RNA degradosomes, implying a role in alleviation of RNA secondary structure stabilization at low temperature. A common emerging theme involves RNA helicases acting as scaffolds for protein-protein interaction and functioning as molecular clamps, holding RNA-protein complexes in specific conformations. This review highlights recent advances in DEAD-box RNA helicase association with cellular response to abiotic stress in prokaryotes.

Published

2012

43. Human RioK3 is a novel component of cytoplasmic pre-40S pre-ribosomal particles

Author

Kamila Baumas, Marlène Faubladier, Yves Henry, Michèle Caizergues-Ferrer, Julien Soudet, Annie Mougin, Laboratoire de biologie moléculaire eucaryote (LBME), Université Toulouse III - Paul Sabatier (UT3), Université Fédérale Toulouse Midi-Pyrénées-Université Fédérale Toulouse Midi-Pyrénées-Centre National de la Recherche Scientifique (CNRS)-Centre de Biologie Intégrative (CBI), and Université Fédérale Toulouse Midi-Pyrénées-Université Fédérale Toulouse Midi-Pyrénées-Centre National de la Recherche Scientifique (CNRS)-Centre National de la Recherche Scientifique (CNRS)

Subjects

Cytoplasm, Amino Acid Motifs, Molecular Sequence Data, ribosome biogenesis, Biology, Protein Serine-Threonine Kinases, Rio protein, 03 medical and health sciences, 5S ribosomal RNA, 0302 clinical medicine, Ribosomal protein, Large ribosomal subunit, RNA Precursors, RNA, Ribosomal, 18S, Humans, Eukaryotic Small Ribosomal Subunit, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Amino Acid Sequence, HeLa cells, Molecular Biology, 030304 developmental biology, 50S, Ribosome Subunits, Small, Eukaryotic, 0303 health sciences, Eukaryotic Large Ribosomal Subunit, Cell Biology, Ribosomal RNA, Biochemistry, 030220 oncology & carcinogenesis, pre-40S pre-ribosomal particle, Eukaryotic Ribosome, Sequence Alignment, Protein Binding, Research Paper

Abstract

International audience; Maturation of the 40S ribosomal subunit precursors in mammals mobilizes several non-ribosomal proteins, including the atypical protein kinase RioK2. Here, we have investigated the involvement of another member of the RIO kinase family, RioK3, in human ribosome biogenesis. RioK3 is a cytoplasmic protein that does not seem to shuttle between nucleus and cytoplasm via a Crm1-dependent mechanism as does RioK2 and which sediments with cytoplasmic 40S ribosomal particles in a sucrose gradient. When the small ribosomal subunit biogenesis is impaired by depletion of either rpS15, rpS19 or RioK2, a concomitant decrease in the amount of RioK3 is observed. Surprisingly, we observed a dramatic and specific increase in the levels of RioK3 when the biogenesis of the large ribosomal subunit is impaired. A fraction of RioK3 is associated with the non ribosomal pre-40S particle components hLtv1 and hEnp1 as well as with the 18S-E pre-rRNA indicating that it belongs to a bona fide cytoplasmic pre-40S particle. Finally, RioK3 depletion leads to an increase in the levels of the 21S rRNA precursor in the 18S rRNA production pathway. Altogether, our results strongly suggest that RioK3 is a novel cytoplasmic component of pre-40S pre-ribosomal particle(s) in human cells, required for normal processing of the 21S pre-rRNA.

Published

2012

44. RNA helicases: diverse roles in prokaryotic response to abiotic stress.

Author

Owttrim GW

Subjects

Cold Temperature, Prokaryotic Cells metabolism, Protein Biosynthesis physiology, RNA metabolism, RNA Helicases chemistry, Ribosomes metabolism, Stress, Physiological, RNA Helicases metabolism

Abstract

Similar to proteins, RNA molecules must fold into the correct conformation and associate with protein complexes in order to be functional within a cell. RNA helicases rearrange RNA secondary structure and RNA-protein interactions in an ATP-dependent reaction, performing crucial functions in all aspects of RNA metabolism. In prokaryotes, RNA helicase activity is associated with roles in housekeeping functions including RNA turnover, ribosome biogenesis, translation and small RNA metabolism. In addition, RNA helicase expression and/or activity are frequently altered during cellular response to abiotic stress, implying they perform defined roles during cellular adaptation to changes in the growth environment. Specifically, RNA helicases contribute to the formation of cold-adapted ribosomes and RNA degradosomes, implying a role in alleviation of RNA secondary structure stabilization at low temperature. A common emerging theme involves RNA helicases acting as scaffolds for protein-protein interaction and functioning as molecular clamps, holding RNA-protein complexes in specific conformations. This review highlights recent advances in DEAD-box RNA helicase association with cellular response to abiotic stress in prokaryotes.

Published

2013

45. [Untitled]

Subjects

0303 health sciences, Ribosome biogenesis, RNA-binding protein, Cell Biology, Methylation, Ribosomal RNA, Biology, Ribosome, Cell biology, 03 medical and health sciences, 0302 clinical medicine, RNA-Protein Interaction, 030220 oncology & carcinogenesis, Molecular Biology, PIN domain, Biogenesis, 030304 developmental biology

Abstract

Ribosome production is an essential cellular process involving a plethora of trans-acting factors, such as nucleases, methyltransferases, RNA helicases and kinases that catalyse key maturation steps. Precise temporal and spatial regulation of such enzymes is essential to ensure accurate and efficient subunit assembly. Here, we focus on the maturation of the 3' end of the 18S rRNA in human cells. We reveal that human RIO2 is an active kinase that phosphorylates both itself and the rRNA methyltransferase DIM1 in vitro. In contrast to yeast, our data confirm that human DIM1 predominantly acts in the nucleus and we further demonstrate that the 21S pre-rRNA is the main target for DIM1-catalysed methylation. We show that the PIN domain of the endonuclease NOB1 is required for site 3 cleavage, while the zinc ribbon domain is essential for pre-40S recruitment. Furthermore, we also demonstrate that NOB1, PNO1 and DIM1 bind to a region of the pre-rRNA encompassing the 3' end of 18S and the start of ITS1, in vitro. Interestingly, NOB1 is present in the cell at higher levels than other pre-40S factors. We provide evidence that NOB1 is multimeric within the cell and show that NOB1 multimerisation is lost when ribosome biogenesis is blocked. Taken together, our data indicate a dynamic interplay of key factors associated with the 3' end of the 18S rRNA during human pre-40S biogenesis and highlight potential mechanisms by which this process can be regulated.