Regulation of Ribosome Biogenesis and Rna Polymerase I Transcription

Regulation of Ribosome Biogenesis and Rna Polymerase I Transcription
Author: Robert Steinbauer
Publisher: Sudwestdeutscher Verlag Fur Hochschulschriften AG
Total Pages: 148
Release: 2011-06
Genre:
ISBN: 9783838126142

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Ribosome synthesis depends on nutrient availability sensed by the target of rapamycin (TOR) signaling pathway in eukaryotic cells. TOR inactivation affects ribosome biogenesis at the level of RNA polymerase I (Pol I)-dependent transcription of ribosomal RNA (rRNA) genes, expression of ribosomal proteins (r-proteins) and ribosome biogenesis factors, pre-ribosome processing, and transport. Detailed analysis shows that upon TOR inactivation the levels of newly synthesized ribosomal subunits drop drastically before the integrity of the Pol I apparatus is severely impaired but in good correlation with a sharp decrease in r-protein production. Inhibition of translation by cycloheximide mimics the rRNA maturation defect observed immediately after TOR inactivation. Both cycloheximide addition and the depletion of individual r-proteins also reproduce TOR-dependent nucleolar entrapment of specific ribosomal precursor complexes. The conclusion could be drawn that shortage of newly synthesized r-proteins after short-term TOR inactivation is sufficient to explain most of the observed effects on ribosome production.

Emerging Concepts in Ribosome Structure, Biogenesis, and Function

Emerging Concepts in Ribosome Structure, Biogenesis, and Function
Author: Vijay Kumar
Publisher: Academic Press
Total Pages: 298
Release: 2021-09-25
Genre: Science
ISBN: 0128167343

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Ribosome biogenesis is the process of making ribosomes which are responsible for mRNA translation into proteins. It is a tightly regulated process closely linked to nearly all biochemical and cellular processes, including cell division, growth, and development. Emerging Concepts in Ribosome Structure, Biogenesis, and Function provides a synthesized overview of all the parts engaged in this process. The book begins by providing an introduction to the ribosome factory, its origin, and its evolution of translation. It then goes on to describe ribosome structure including subunits, RNA, and protein components. Ribosome biogenesis and its emergence as a frontier research area for translational potential in cancer and other diseases are also discussed. In addition, the book explores current developments in ribosome research like the emergence of ribosomopathies, how deregulation of ribosome biogenesis can impact disease mechanisms and aging, and the discovery of specialized ribosomes that have specific functions that may translate differentially with consequences on normal and pathological processes. Emerging Concepts in Ribosome Structure, Biogenesis, and Function provides fundamental coverage and emerging research on ribosomes, biogenesis, and their structure and function and is a resourceful introduction for new researchers and those engaged in interdisciplinary ribosomal research. Provides an overview of ribosome biogenesis and examines its involvement in cell transformation and cancerous growth Covers disorders related to the ribosome (ribosomopathies) and explains the significance of ribosome dysfunction in human diseases Includes commonly used methods to study ribosomes, such as polysome preparation, RNA profiling and proteomics, CryoEM, and Cell-free assays along with proper illustrations

The Nucleolus and Ribosome Biogenesis

The Nucleolus and Ribosome Biogenesis
Author: A.A. Hadjiolov
Publisher: Springer Science & Business Media
Total Pages: 281
Release: 2012-12-06
Genre: Science
ISBN: 3709187427

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The nucleolus had consistently attracted the attention of investigators in the fields of cell biology and pathology. Because of its ubiquitous presence in the nucleus of eukaryotic cells, its rapid changes during their life cycle, and its rapid response to noxious agents, this organelle has been the subject of a large number of studies. Yet, the exact function and the very reason for the existence of the nucleolus (the only large cellular structure not delimited by a membrane) remain largely unknown. The ribosomes were discovered relatively late in the study of cells, but due to their crucial involvement in the protein synthesis machinery of all living organisms, the elucidation of their structure and function quickly became one of the major goals of molecular biology. The relatively simple structure of the ribosome strengthens the hope that a full understanding of the structure and function of this organelle in molecular terms is within the reach of contemporary research~ Since each of the rRNA and protein molecules embodied in the ribosome is the product of a distinct gene, studies on the biogenesis of ribosomes expanded rapidly to become a core topic in molecular genetics.

Non-coding RNAs and Cancer

Non-coding RNAs and Cancer
Author: Muller Fabbri
Publisher: Springer Science & Business Media
Total Pages: 287
Release: 2013-10-28
Genre: Medical
ISBN: 1461484448

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The discovery of microRNAs and its role as gene expression regulators in human carcinogenesis represents one of the most important scientific achievements of the last decade. More recently, other non-coding RNAs have been discovered and its implications in cancer are emerging as well, suggesting a broader than anticipated involvement of the non-coding genome in cancer. Moreover, completely new and unexpected functions for microRNAs are being revealed, leading to the identification of new anticancer molecular targets. This book represents a comprehensive guide on non-coding RNAs and cancer, spanning from its role as cancer biomarkers, to providing the most useful bioinformatic tools, to presenting some of the most relevant discoveries, which indicates how these fascinating molecules act as fine orchestrators of cancer biology.

Ribosome Biogenesis

Ribosome Biogenesis
Author: Karl-Dieter Entian
Publisher: Springer Nature
Total Pages: 287
Release: 2022-07-07
Genre: Medical
ISBN: 1071625012

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This Open Access volume provides comprehensive reviews and describes the latest techniques to study eukaryotic ribosome biogenesis. For more than 50 years ribosomes are a major research topic. Our knowledge about ribosome biogenesis and function such as transcription, mRNA modification, and translation was the sine qua non for developing the powerful RNA-based vaccines against RNA-viruses causing the world-threatening Covid-19 pandemia. The chapters in this book are organized into six parts. Part One discusses a comparative survey about the unity and diversity of ribosome biogenesis in pro- and eukaryotic cells. Part Two deals with the genomic organization of eukaryotic rDNA and the role of RNA polymerase I in ribosomal RNA transcription. Part Three explores in vitro methods to study RNA polymerase I structure and its function, and Part Four analyzes the nucleo-cytoplasmic transport of assembled ribosomes and RNP complexes. Part Five covers modifications that increase the complexity of rRNAs, and Part Six provides readers with a review of eukaryotic translation and - for the first time - describes a new method to analyze translation in vitro. Written in the highly successful Methods in Molecular Biology series format, chapters include introductions to their respective topics, lists of the necessary materials and reagents, step-by-step, readily reproducible laboratory protocols, and tips on troubleshooting and avoiding known pitfalls. Cutting-edge and comprehensive, Ribosome Biogenesis: Methods and Protocols is a valuable resource for scientists and researchers interested in learning more about the increasing importance of in vitro RNA-technologies.

Relative Roles of UBF and RRN3 in the Transcription of the Ribosomal RNA Genes and Ribosome Biogenesis Determined Using in Vivo Mouse Models

Relative Roles of UBF and RRN3 in the Transcription of the Ribosomal RNA Genes and Ribosome Biogenesis Determined Using in Vivo Mouse Models
Author: Chelsea Herdman
Publisher:
Total Pages: 177
Release: 2017
Genre:
ISBN:

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Ribosome biogenesis, or the synthesis of ribosomes, is an important cell process occurring in the nucleolus that utilizes transcription by all three nuclear RNA polymerases. The initial and rate-limiting step is the transcription of the catalytic ribosomal RNAs 28S, 18S and 5.8S in the form of a precursor ribosomal RNA (pre-rRNA/47S) by RNA polymerase I (RPI, also known as Pol1 and POLR1). RPI has a dedicated set of basal factors responsible for its activation. These are the architectural factor UBF, the TBP containing factor SL1, the initiation factor RRN3, and the termination factor TTF1. Ribosomal RNA synthesis is tightly regulated and accounts for 30-50% of total gene transcription. As such, this process is linked to cell growth, transformation, proliferation and the actions of tumour suppressors and oncogenes. Notably, UBF and RRN3 are activated by many of the same growth signaling pathways. The human and mouse haploid genome contain ~200 copies of the ribosomal RNA genes, the ribosomal DNA (rDNA). These ribosomal DNA copies are arranged in tandem repeats on the short arms of acrocentric chromosomes. Interestingly, only a fraction of the rDNA copies are active, and a significant number are epigenetically silenced and heterochromatic. The reason for having so many copies and their regulation in vivo by silencing is not yet understood, though it has been connected with genome stability. This thesis presents the analysis of the in vivo requirements for UBF and RRN3 in rRNA transcription and rDNA chromatin structure. We had previously analyzed the loss of UBF in mouse embryonic fibroblasts using tamoxifen-dependent conditional knockout. As we wanted to compare the loss of RRN3 in a similar model, we re-analyzed the RRN3 knockout mice and created cell lines as was performed for the UBF knockout. Importantly, we find that RRN3 is essential for preimplantation and its loss arrests development at E3.5, contrary to previous work that showed a late E9.5 developmental arrest. Using mouse embryonic fibroblast (MEF) cell lines conditional for UBF or RRN3, we found that the loss of either factor prevented RPI transcription. However, we found that UBF was essential for the recruitment of the other RPI transcription factors and the formation of the preinitiation complex, as well as to maintain an open rDNA chromatin structure, while RRN3 was required only for RPI recruitment. These studies allowed us to identify an upstream boundary element on the rDNA formed of H2A.Z, TTF1, CTCF and activating histone marks, which is independent of RPI activity. We also found that UBF loss, but not RRN3 loss, led to a synchronous and massive p53-independent apoptosis, specifically in oncogenically transformed cells. This strongly suggests that drug targeting UBF could be a viable cancer treatment. Finally, we have observed that the rDNA activity status in pluripotent cells differs from that of differentiated cells. Embryonic stem cells (ESCs) were also generated from the mice conditional for UBF and RRN3. Preliminary results indicate that, unlike somatic cells, all the rRNA genes in these and other pluripotent cell lines are potentially active. This makes ESCs and their differentiation an ideal model in which to study the establishment of rDNA silencing and the role of UBF and/or RRN3 in this process. Together these data define the in vivo roles of UBF and RRN3 in ribosomal RNA transcription and suggest mechanisms by which they maintain rDNA integrity and may drive cell differentiation.

The Nucleolus

The Nucleolus
Author: Mark O. J. Olson
Publisher: Springer Science & Business Media
Total Pages: 434
Release: 2011-09-15
Genre: Science
ISBN: 1461405149

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Within the past two decades, extraordinary new functions for the nucleolus have begun to appear, giving the field a new vitality and generating renewed excitement and interest. These new discoveries include both newly-discovered functions and aspects of its conventional role. The Nucleolus is divided into three parts: nucleolar structure and organization, the role of the nucleolus in ribosome biogenesis, and novel functions of the nucleolus.

Transcription of Ribosomal RNA Genes by Eukaryotic RNA Polymerase I

Transcription of Ribosomal RNA Genes by Eukaryotic RNA Polymerase I
Author: Marvin R. Paule
Publisher: Springer
Total Pages: 350
Release: 1998-10-06
Genre: Medical
ISBN:

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The mechanism by which ribosomal RNA is synthesized has been a topic of intensive research for nearly 30 years. In 1981 the first in vitro transcription system for ribosomal RNA from a eukaryote - mouse ascites cells - was reported, followed rapidly by similar systems in a variety of other eukaryotes, all revealed by a relatively small number of research groups. This monograph is the first to bring together the results and opinions of all these groups. Though it unavoidably emphasizes the common features of ribosomal RNA transcription between species, the species specificity of the process and nucleolar dominance and its possible mechanism(s) are also discussed.

Ubiquitin-mediated Regulation of RNA Polymerase I in Saccharomyces Cerevisiae

Ubiquitin-mediated Regulation of RNA Polymerase I in Saccharomyces Cerevisiae
Author: Sabrina Kamran
Publisher:
Total Pages: 95
Release: 2019
Genre:
ISBN:

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Ribosomes are key cellular components ensuring that cells correctly synthesize their protein cohort. Dysregulation of this process can lead to improper cell growth and is linked to the progression of several types of cancers, making understanding of this process of great interest to both researchers and clinicians. Ribosome biogenesis, the process by which ribosomes are produced, is largely controlled by regulating the rate-limiting step of rDNA transcription by RNA Polymerase I, which transcribes three of the four ribosomal RNAs within the cell. Although rDNA transcription is highly regulated by post-translational modifications in response to changing environmental conditions, little is known of how RNA Polymerase I activity is regulated. Our previous research identified a novel role for ubiquitin-mediated regulation of RNA Polymerase I in ribosome biogenesis. We discovered that ubiquitination of Rpa190, the largest subunit of RNA polymerase I, regulates growth and is modulated by the deubiquitinating enzyme Ubp10. This thesis explores the details of Rpa190 ubiquitination and provides an understanding of how ubiquitination regulates rDNA transcription using both genetic and pharmacological approaches. First, it identifies how ubiquitination of Rpa190 modulates active rDNA transcription. It also identifies the SCF[superscript]Grr1 complex as a potential upstream ubiquitin pathway that regulates ribosome biogenesis. Second, it identifies that the ubiquitination of Rpa190 likely serves as the physiological axis affected by the pharmacology of BMH-21, a novel small molecule being considered for use as an anti-cancer therapeutic.