A Model-Driven Quantitative Analysis of Retrotransposon Distributions in the Human Genome

Andrea Riba; Maria Rita Fumagalli; Michele Caselle; Matteo Osella

doi:10.1093/gbe/evaa201

A Model-Driven Quantitative Analysis of Retrotransposon Distributions in the Human Genome

Genome Biology and Evolution ◽

10.1093/gbe/evaa201 ◽

2020 ◽

Vol 12 (11) ◽

pp. 2045-2059

Author(s):

Andrea Riba ◽

Maria Rita Fumagalli ◽

Michele Caselle ◽

Matteo Osella

Keyword(s):

Human Genome ◽

Dna Sequences ◽

Statistical Physics ◽

Evolutionary Dynamics ◽

Analytical Framework ◽

Host Genome ◽

Model Driven ◽

Random Placement ◽

Evolution Of Mammals

Abstract Retrotransposons, DNA sequences capable of creating copies of themselves, compose about half of the human genome and played a central role in the evolution of mammals. Their current position in the host genome is the result of the retrotranscription process and of the following host genome evolution. We apply a model from statistical physics to show that the genomic distribution of the two most populated classes of retrotransposons in human deviates from random placement, and that this deviation increases with time. The time dependence suggests a major role of the host genome dynamics in shaping the current retrotransposon distributions. Focusing on a neutral scenario, we show that a simple model based on random placement followed by genome expansion and sequence duplications can reproduce the empirical retrotransposon distributions, even though more complex and possibly selective mechanisms can have contributed. Besides the inherent interest in understanding the origin of current retrotransposon distributions, this work sets a general analytical framework to analyze quantitatively the effects of genome evolutionary dynamics on the distribution of genomic elements.

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Genomic duplications shaped current retrotransposon position distribution in human

10.1101/819284 ◽

2019 ◽

Cited By ~ 1

Author(s):

Andrea Riba ◽

Maria Rita Fumagalli ◽

Michele Caselle ◽

Matteo Osella

Keyword(s):

Dna Sequences ◽

Statistical Physics ◽

Evolutionary Dynamics ◽

Analytical Framework ◽

Host Genome ◽

Current Position ◽

Genomic Distribution ◽

Random Placement ◽

Evolution Of Mammals

Retrotransposons, DNA sequences capable of creating copies of themselves, compose about half of the human genome and played a central role in the evolution of mammals. Their current position in the host genome is the result of the retrotranscription process and of the following host genome evolution. We apply a model from statistical physics to show that the genomic distribution of the two most populated classes of retrotransposons in human deviates from random placement, and that this deviation increases with time. The time dependence suggests a major role of the host genome dynamics in shaping the current retrotransposon distributions. In fact, these distributions can be explained by a stochastic process of random placement due to retrotranscription followed by genome expansion and sequence duplications. Besides the inherent interest in understanding the origin of current retrotransposon distributions, this work sets a general analytical framework to analyze quantitatively the effects of genome evolutionary dynamics on the distribution of genomic elements.

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DNA methylation in satellite repeats disorders

Essays in Biochemistry ◽

10.1042/ebc20190028 ◽

2019 ◽

Vol 63 (6) ◽

pp. 757-771 ◽

Cited By ~ 4

Author(s):

Claire Francastel ◽

Frédérique Magdinier

Keyword(s):

Dna Methylation ◽

Human Genome ◽

Repetitive Dna ◽

Dna Sequences ◽

Satellite Repeats ◽

Tremendous Progress ◽

Genes Encoding ◽

Dna Elements ◽

Near Future

Abstract Despite the tremendous progress made in recent years in assembling the human genome, tandemly repeated DNA elements remain poorly characterized. These sequences account for the vast majority of methylated sites in the human genome and their methylated state is necessary for this repetitive DNA to function properly and to maintain genome integrity. Furthermore, recent advances highlight the emerging role of these sequences in regulating the functions of the human genome and its variability during evolution, among individuals, or in disease susceptibility. In addition, a number of inherited rare diseases are directly linked to the alteration of some of these repetitive DNA sequences, either through changes in the organization or size of the tandem repeat arrays or through mutations in genes encoding chromatin modifiers involved in the epigenetic regulation of these elements. Although largely overlooked so far in the functional annotation of the human genome, satellite elements play key roles in its architectural and topological organization. This includes functions as boundary elements delimitating functional domains or assembly of repressive nuclear compartments, with local or distal impact on gene expression. Thus, the consideration of satellite repeats organization and their associated epigenetic landmarks, including DNA methylation (DNAme), will become unavoidable in the near future to fully decipher human phenotypes and associated diseases.

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Role of Transcriptional Read-Through in PRE Activity in Drosophila melanogaster

Acta Naturae ◽

10.32607/20758251-2016-8-2-79-86 ◽

2016 ◽

Vol 8 (2) ◽

pp. 79-86 ◽

Cited By ~ 3

Author(s):

P. V. Elizar’ev ◽

D. V. Lomaev ◽

D. A. Chetverina ◽

P. G. Georgiev ◽

M. M. Erokhin

Keyword(s):

Dna Sequences ◽

Cell Types ◽

Transcription Terminator ◽

Response Elements ◽

Polycomb Response Elements ◽

The Individual ◽

Multicellular Organisms ◽

Different Cell Types ◽

Main Factor

Maintenance of the individual patterns of gene expression in different cell types is required for the differentiation and development of multicellular organisms. Expression of many genes is controlled by Polycomb (PcG) and Trithorax (TrxG) group proteins that act through association with chromatin. PcG/TrxG are assembled on the DNA sequences termed PREs (Polycomb Response Elements), the activity of which can be modulated and switched from repression to activation. In this study, we analyzed the influence of transcriptional read-through on PRE activity switch mediated by the yeast activator GAL4. We show that a transcription terminator inserted between the promoter and PRE doesnt prevent switching of PRE activity from repression to activation. We demonstrate that, independently of PRE orientation, high levels of transcription fail to dislodge PcG/TrxG proteins from PRE in the absence of a terminator. Thus, transcription is not the main factor required for PRE activity switch.

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Human Herpesvirus 8 DNA Sequences in Pemphigus: The Role of the Virus in Oncogenic and Autoimmune Manifestations

Archives of Dermatology ◽

10.1001/archderm.134.6.751 ◽

1998 ◽

Vol 134 (6) ◽

pp. 751-751 ◽

Cited By ~ 5

Author(s):

K. J. Smith

Keyword(s):

Dna Sequences ◽

Human Herpesvirus ◽

Human Herpesvirus 8 ◽

Herpesvirus 8

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The role of pathogen genomics in assessing tick-borne pathogen evolutionary dynamics

10.1603/ice.2016.105334 ◽

2016 ◽

Author(s):

Giovanna Carpi

Keyword(s):

Evolutionary Dynamics

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Non-pharmacological Strategies Against Systemic Inflammation: Molecular Basis and Clinical Evidence

Current Pharmaceutical Design ◽

10.2174/1381612826666200403122600 ◽

2020 ◽

Vol 26 (22) ◽

pp. 2620-2629 ◽

Cited By ~ 2

Author(s):

Rita Del Pinto ◽

Davide Pietropaoli ◽

Annalisa Monaco ◽

Giovambattista Desideri ◽

Claudio Ferri ◽

...

Keyword(s):

Human Genome ◽

Systemic Inflammation ◽

Clinical Evidence ◽

Metabolic Diseases ◽

Lifestyle Changes ◽

Common Denominator ◽

Active Lifestyle ◽

Systemic Impact ◽

Public Health Strategies

Systemic inflammation is a common denominator to a variety of cardiovascular (CV) and non-CV diseases and relative risk factors, including hypertension and its control, metabolic diseases, rheumatic disorders, and those affecting the gastrointestinal tract. Besides medications, a non-pharmacological approach encompassing lifestyle changes and other complementary measures is mentioned in several updated guidelines on the management of these conditions. We performed an updated narrative review on the mechanisms behind the systemic impact of inflammation and the role of non-pharmacological, complementary measures centered on lowering systemic phlogosis for preserving or restoring a good global health. The central role of genetics in shaping the immune response is discussed in conjunction with that of the microbiome, highlighting the interdependence and mutual influences between the human genome and microbial integrity, diversity, and functions. Several plausible strategies to modulate inflammation and restore balanced crosstalk between the human genome and the microbiome are then recapitulated, including dietary measures, active lifestyle, and other potential approaches to manipulate the resident microbial community. To date, evidence from high-quality human studies is sparse to allow the unconditioned inclusion of understudied, though plausible solutions against inflammation into public health strategies for global wellness. This gap claims further focused, well-designed research targeted at unravelling the mechanisms behind future personalized medicine.

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Landscape resistance constrains hybridization across contact zones in a reproductively and morphologically polymorphic salamander

Scientific Reports ◽

10.1038/s41598-021-88349-7 ◽

2021 ◽

Vol 11 (1) ◽

Author(s):

Guillermo Velo-Antón ◽

André Lourenço ◽

Pedro Galán ◽

Alfredo Nicieza ◽

Pedro Tarroso

Keyword(s):

Contact Zone ◽

Environmental Heterogeneity ◽

Evolutionary Dynamics ◽

Morphological Differentiation ◽

Phenotypic Traits ◽

Hybrid Zones ◽

Landscape Resistance ◽

Phenotypic Differentiation ◽

Contact Zones

AbstractExplicitly accounting for phenotypic differentiation together with environmental heterogeneity is crucial to understand the evolutionary dynamics in hybrid zones. Species showing intra-specific variation in phenotypic traits that meet across environmentally heterogeneous regions constitute excellent natural settings to study the role of phenotypic differentiation and environmental factors in shaping the spatial extent and patterns of admixture in hybrid zones. We studied three environmentally distinct contact zones where morphologically and reproductively divergent subspecies of Salamandra salamandra co-occur: the pueriparous S. s. bernardezi that is mostly parapatric to its three larviparous subspecies neighbours. We used a landscape genetics framework to: (i) characterise the spatial location and extent of each contact zone; (ii) assess patterns of introgression and hybridization between subspecies pairs; and (iii) examine the role of environmental heterogeneity in the evolutionary dynamics of hybrid zones. We found high levels of introgression between parity modes, and between distinct phenotypes, thus demonstrating the evolution to pueriparity alone or morphological differentiation do not lead to reproductive isolation between these highly divergent S. salamandra morphotypes. However, we detected substantial variation in patterns of hybridization across contact zones, being lower in the contact zone located on a topographically complex area. We highlight the importance of accounting for spatial environmental heterogeneity when studying evolutionary dynamics of hybrid zones.

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Parasites in Antarctic krill guts inferred from DNA sequences

Antarctic Science ◽

10.1017/s0954102018000469 ◽

2019 ◽

Vol 31 (1) ◽

pp. 16-22 ◽

Cited By ~ 2

Author(s):

Alison C. Cleary ◽

Maria C. Casas ◽

Edward G. Durbin ◽

Jaime Gómez-Gutiérrez

Keyword(s):

Dna Sequences ◽

High Frequency ◽

Dna Analysis ◽

Antarctic Krill ◽

Euphausia Superba ◽

Gut Contents ◽

The West ◽

West Antarctic ◽

Wide Range

AbstractThe keystone role of Antarctic krill,Euphausia superbaDana, in Southern Ocean ecosystems, means it is essential to understand the factors controlling their abundance and secondary production. One such factor that remains poorly known is the role of parasites. A recent study of krill diet using DNA analysis of gut contents provided a snapshot of the parasites present within 170E. superbaguts in a small area along the West Antarctic Peninsula. These parasites includedMetschnikowiaspp. fungi,Haptoglossasp. peronosporomycetes,LankesteriaandParalecudinaspp. apicomplexa,Stegophorussp. nematodes, andPseudocolliniaspp. ciliates. Of these parasites,Metschnikowiaspp. fungi andPseudocolliniaspp. ciliates had previously been observed inE. superba, as had other genera of apicomplexans, though notLankesteriaandParalecudina.In contrast, nematodes had previously only been observed in eggs ofE. superba, and there are no literature reports of peronosporomycetes in euphausiids.Pseudocolliniaspp., parasitoids which obligately kill their host, were the most frequently observed infection, with a prevalence of 12%. The wide range of observed parasites and the relatively high frequency of infections suggest parasites may play a more important role than previously acknowledged inE. superbaecology and population dynamics.

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Agricultural Policy Networks of the Republic of Ireland and Northern Ireland

Political Studies ◽

10.1111/j.1467-9248.1995.tb01725.x ◽

1995 ◽

Vol 43 (4) ◽

pp. 664-682 ◽

Cited By ~ 14

Author(s):

Neil Collins

Keyword(s):

Northern Ireland ◽

Agricultural Policy ◽

Policy Making ◽

Analytical Framework ◽

Policy Networks ◽

Republic Of Ireland ◽

European Literature ◽

The Republic

This paper provides an analytical framework within which to understand the contrasting way farmers' interests are aggregated and articulated in Northern Ireland and the Republic of Ireland. The analysis draws on the dominant European literature on state-farmer relations which emphasizes the role of policy networks and explores whether the concepts of pluralism or corporatism best characterize policy making in the two states.

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Assessment of the Role of Activator Protein-1 on Transcription of the Mouse Steroidogenic Acute Regulatory Protein Gene

Molecular Endocrinology ◽

10.1210/me.2003-0223 ◽

2004 ◽

Vol 18 (3) ◽

pp. 558-573 ◽

Cited By ~ 52

Author(s):

Pulak R. Manna ◽

Darrell W. Eubank ◽

Douglas M. Stocco

Keyword(s):

Binding Site ◽

Gene Transcription ◽

Dna Sequences ◽

Regulatory Protein ◽

Activator Protein 1 ◽

Transcriptional Responses ◽

Activator Protein ◽

Steroidogenic Acute Regulatory ◽

Star Gene

Abstract cAMP-dependent mechanisms regulate the steroidogenic acute regulatory (StAR) protein even though its promoter lacks a consensus cAMP response-element (CRE, TGACGTCA). Transcriptional regulation of the StAR gene has been demonstrated to involve combinations of DNA sequences that provide recognition motifs for sequence-specific transcription factors. We recently identified and characterized three canonical 5′-CRE half-sites within the cAMP-responsive region (−151/−1 bp) of the mouse StAR gene. Among these CRE elements, the CRE2 half-site is analogous (TGACTGA) to an activator protein-1 (AP-1) sequence [TGA(C/G)TCA]; therefore, the role of the AP-1 transcription factor was explored in StAR gene transcription. Mutation in the AP-1 element demonstrated an approximately 50% decrease in StAR reporter activity. Using EMSA, oligonucleotide probes containing an AP-1 binding site were found to specifically bind to nuclear proteins obtained from mouse MA-10 Leydig and Y-1 adrenocortical tumor cells. The integrity of the sequence-specific AP-1 element in StAR gene transcription was assessed using the AP-1 family members, Fos (c-Fos, Fra-1, Fra-2, and Fos B) and Jun (c-Jun, Jun B, and Jun D), which demonstrated the involvement of Fos and Jun in StAR gene transcription to varying degrees. Disruption of the AP-1 binding site reversed the transcriptional responses seen with Fos and Jun. EMSA studies utilizing antibodies specific to Fos and Jun demonstrated the involvement of several AP-1 family proteins. Functional assessment of Fos and Jun was further demonstrated by transfecting antisense c-Fos, Fra-1, and dominant negative forms of Fos (A-Fos) and c-Jun (TAM-67) into MA-10 cells, which significantly (P < 0.01) repressed transcription of the StAR gene. Mutation of the AP-1 site in combination with mutations in other cis-elements resulted in a further decrease of StAR promoter activity, demonstrating a functional cooperation between these factors. Mammalian two-hybrid assays revealed high-affinity protein-protein interactions between c-Fos and c-Jun with steroidogenic factor 1, GATA-4, and CCAAT/enhancer binding protein-β. These findings demonstrate that Fos and Jun can bind to the TGACTGA element in the StAR promoter and provide novel insights into the mechanisms regulating StAR gene transcription.

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