994 research outputs found
Unbiased, Genome-Wide In Vivo Mapping of Transcriptional Regulatory Elements Reveals Sex Differences in Chromatin Structure Associated with Sex-Specific Liver Gene Expression
We have used a simple and efficient method to identify condition-specific transcriptional regulatory sites in vivo to help elucidate the molecular basis of sex-related differences in transcription, which are widespread in mammalian tissues and affect normal physiology, drug response, inflammation, and disease. To systematically uncover transcriptional regulators responsible for these differences, we used DNase hypersensitivity analysis coupled with high-throughput sequencing to produce condition-specific maps of regulatory sites in male and female mouse livers and in livers of male mice feminized by continuous infusion of growth hormone (GH). We identified 71,264 hypersensitive sites, with 1,284 showing robust sex-related differences. Continuous GH infusion suppressed the vast majority of male-specific sites and induced a subset of female-specific sites in male livers. We also identified broad genomic regions (up to ~100 kb) showing sex-dependent hypersensitivity and similar patterns of GH responses. We found a strong association of sex-specific sites with sex-specific transcription; however, a majority of sex-specific sites were >100 kb from sex-specific genes. By analyzing sequence motifs within regulatory regions, we identified two known regulators of liver sexual dimorphism and several new candidates for further investigation. This approach can readily be applied to mapping condition-specific regulatory sites in mammalian tissues under a wide variety of physiological conditions.National Institutes of Health (U.S) ( DK33765)National Institutes of Health (U.S) (grant 577 5 P42 ES07381
Polyglutamine Expanded Huntingtin Dramatically Alters the Genome-Wide Binding of HSF1
In Huntington's disease (HD), polyglutamine expansions in the huntingtin (Htt) protein cause subtle changes in cellular functions that, over-time, lead to neurodegeneration and death. Studies have indicated that activation of the heat shock response can reduce many of the effects of mutant Htt in disease models, suggesting that the heat shock response is impaired in the disease. To understand the basis for this impairment, we have used genome-wide chromatin immunoprecipitation followed by massively parallel sequencing (ChIP-Seq) to examine the effects of mutant Htt on the master regulator of the heat shock response, HSF1. We find that, under normal conditions, HSF1 function is highly similar in cells carrying either wild-type or mutant Htt. However, polyQ-expanded Htt severely blunts the HSF1-mediated stress response. Surprisingly, we find that the HSF1 targets most affected upon stress are not directly associated with proteostasis, but with cytoskeletal binding, focal adhesion and GTPase activity. Our data raise the intriguing hypothesis that the accumulated damage from life-long impairment in these stress responses may contribute significantly to the etiology of Huntington's disease.National Institutes of Health (U.S.) (Grant R24 DK-090963)National Institutes of Health (U.S.) (Grant R01-GM089903)National Institutes of Health (U.S.) (Grant P30-ES002109)National Science Foundation (U.S.) (Award DB1-0821391
Isolated hydramnios at term gestation and the occurrence of peripartum complications
Objective: To determine if hydramnios at term gestation is an independent risk factor for poor pregnancy outcome and perinatal death. Study design: The study population consisted of 60 702 patients with singleton gestation who delivered at term (>37 weeks). Patients were classified into two groups according to the presence or the absence of hydramnios. Hydramnios was diagnosed in the presence of an amniotic fluid index greater than 25 cm or of a maximum vertical pocket of amniotic fluid of at least 8 cm or by subjective assessment. Logistic regression analysis was used to evaluate the unique contribution of hydramnios to fetal death and to perinatal and maternal morbidity. Results: The prevalence of hydramnios was 1211/60702 (2%). Patients with hydramnios had a higher incidence of complications than those with a normal amount of amniotic fluid: cesarean section (22.8 vs. 8.5%, P<0.01), antepartum death (0.6 vs. 0.2%, P<0.005), postpartum death (2.8 vs. 0.4%, P<0.01), abruptio placenta (0.9 vs, 0.3%, P<0.001), fetal distress (6.1 vs. 3.65%, P<0.0015), meconium-stained amniotic fluid (17.8 vs. 15%, P<0.001), low Apgar score at 5 min (2.95 vs. 1%, P<0.01), malpresentation (6.8 vs. 2.9%, P<0.01), clinical chorioamnionitis (0.3 vs. 0.1%, P<0.05), prolapse of cord (2.2 vs. 0.3%, P<0.01), and large-for- gestational-age infant (LGA) (23.8 vs. 8.1%, P<0.01). When adjusted for confounding variables, the presence of hydramnios remained strongly associated with perinatal mortality (odds ratio 5.5 (95% Cl 3.2-9.3)) and neonatal and maternal morbidity (odds ratios 2.1 (Cl 1.1-3.7) and 2.3 (Cl 1.9-2.7), respectively). Conclusions: (1) Hydramnios at term is an independent risk factor for perinatal death; (2) Fetal surveillance is warranted in patients with hydramnios even in the absence of other known risk factors for adverse pregnancy outcome
Boron/Calcium in planktonic foraminifera: proxy development and application to the Paleocene-Eocene boundary
Climate transitions on recent and geologic timescales are linked to perturbations in atmospheric carbon dioxide concentrations (pCO2). Records of ocean carbonate chemistry allow us to investigate the role of CO2 during past climate events but are limited by the availability of paleo-proxies. This thesis presents the development and calibration of Boron/Calcium (B/Ca) in planktonic foraminifera as a proxy for surface ocean carbonate chemistry from sediment traps and modern surface sediments. The B/Ca proxy is then used to reconstruct surface ocean acidification across the Paleocene-Eocene boundary (~55.8 Myr). Observations of B/Ca in the surface dwelling planktonic foraminifer Globigerinoides ruber white from the Oceanic Flux Program (OFP) sediment trap time-series located near Bermuda are used to suggest that the photosynthetic activity of symbiotic algae within the living foraminifer modify the internal pH relative to the ambient seawater, thereby influencing the B/Ca recorded in the calcitic test (Chapter Two). I hypothesize that the apparent covariance between G. ruber B/Ca and the temperature at the OFP site is due to the seasonal change in incident light affecting the symbiont activity, which can increase the internal pH during calcification from seawater by ~0.2-0.3 units. Measurements of B/Ca and δ11B in different species of planktonic foraminifera from globally distributed core-top sediments reveal that symbiotic foraminifera are offset from the theoretically predicted equilibrium with seawater (Chapter Three). I find no significant temperature effect on B/Ca and the departure from equilibrium for symbiont-bearing species is attributed to biological effects. I provide empirical calibrations for thermocline and deep-dwelling planktonic foraminifera as being primarily controlled by seawater [(〖"B(OH)" 〗_"4" ^"-" )⁄(〖"HCO" 〗_"3" ^"-" )]. Paired isotopic (δ13C, δ18O) and elemental (Mg/Ca, B/Ca) measurements are applied to reconstruct the relative timing and magnitude of environmental changes across the Paleocene-Eocene boundary, occurring ~55.8 Myr using sections from ODP Leg 174AX sites at Bass River and Ancora. Reconstructions of ocean temperature (Mg/Ca) and carbonate chemistry (δ13C and B/Ca) from planktonic foraminifera document an abrupt and significant decrease in B/Ca ratios, coincident with δ13C records and the concomitant ~6-8°C warming. The synchronous changes in all three proxies do not support the occurrence of significant precursor warming or carbon release argued elsewhere.Ph. D.Includes bibliographical referencesby Tali Lea Babil
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Evolution of low-grade glioma through intratumoral heterogeneity of the genome and epigenome
Low-grade glioma (LGG) is a diffuse and infiltrative adult brain tumor. Due to the invasive nature of the tumor, surgical resection is rarely curative. LGG often undergo malignant progression and recur as a high-grade glioblastoma (GBM). The genomic and epigenomic landscapes of these tumors, particularly at recurrence, are understudied yet clinically important. Recurrent tumors may be driven by a distinct set of genetic and epigenetic alterations than their initial tumors, yet therapeutic decisions are often made based on profiling of initial malignancies. Here we comprehensively profiled 33 LGGs and their patient-matched recurrences, including cases with 2-6 intratumoral samples, with exome sequencing to identify somatic mutations, with the Infinium 450K array to investigate DNA methylation changes, and with RNA sequencing to measure gene expression changes. We found a wide range in the degree of evolution from initial to recurrence, in terms of both somatic mutations and DNA methylation changes. Tumors treated with the alkylating chemotherapy temozolomide (TMZ) often recurred with a hypermutation phenotype that was suggestive of therapy-driven malignant progression to GBM. Therapy-associated mutational activation of the AKT-mTOR pathway was a consistent feature of these hypermutated recurrences, which promoted a new clinical trial combining the anti-tumor activity of TMZ with an mTOR inhibitor. Recurrence as GBM was associated with aberrations to cell cycle genes through convergence of both genetic and epigenetic mechanisms. Moreover, we found that the evolutionary history of a tumor is similar whether inferred from genetic or epigenetic data, suggesting co-evolution of the genome and epigenome. Finally, we identified cases in which mutations in IDH1, which are the earliest known alteration in LGG and drive gliomagenesis, were either deleted or amplified at recurrence. Mutant IDH1 reprograms the epigenome and these recurrences showed partial reversion of these epigenomic alterations. Together, these findings highlight the heterogeneity and continual evolution of LGG and emphasize the importance of studying recurrent tumors for a more complete understanding of tumor evolution and to make more informed treatment decisions
A quantitative model of transcriptional regulation reveals the influence binding location on expression
Understanding the mechanistic basis of transcriptional regulation has been a central focus of molecular biology since its inception. New high-throughput chromatin immunoprecipitation experiments have revealed that most regulatory proteins bind thousands of sites in mammalian genomes. However, the functional significance of these binding sites remains unclear. We present a quantitative model of transcriptional regulation that suggests the contribution of each binding site to tissue-specific gene expression depends strongly on its position relative to the transcription start site. For three cell types, we show that, by considering binding position, it is possible to predict relative expression levels between cell types with an accuracy approaching the level of agreement between different experimental platforms. Our model suggests that, for the transcription factors profiled in these cell types, a regulatory site's influence on expression falls off almost linearly with distance from the transcription start site in a 10 kilobase range. Binding to both evolutionarily conserved and non-conserved sequences contributes significantly to transcriptional regulation. Our approach also reveals the quantitative, tissue-specific role of individual proteins in activating or repressing transcription. These results suggest that regulator binding position plays a previously unappreciated role in influencing expression and blurs the classical distinction between proximal promoter and distal binding events
Use of commercial off-the-shelf digital cameras for scientific data acquisition and scene-specific color calibration
Author Manuscript. Published in final edited form as: J Opt Soc Am A Opt Image Sci Vis. 2014 February 1; 31(2): 312–321
Direct Recruitment of Polycomb Repressive Complex 1 to Chromatin by Core Binding Transcription Factors
Polycomb repressive complexes (PRCs) play key roles in developmental epigenetic regulation. Yet the mechanisms that target PRCs to specific loci in mammalian cells remain incompletely understood. In this study we show that Bmi1, a core component of Polycomb Repressive Complex 1 (PRC1), binds directly to the Runx1/CBFβ transcription factor complex. Genome-wide studies in megakaryocytic cells demonstrate significant chromatin occupancy overlap between the PRC1 core component Ring1b and Runx1/CBFβ and functional regulation of a considerable fraction of commonly bound genes. Bmi1/Ring1b and Runx1/CBFβ deficiencies generate partial phenocopies of one another in vivo. We also show that Ring1b occupies key Runx1 binding sites in primary murine thymocytes and that this occurs via PRC2-independent mechanisms. Genetic depletion of Runx1 results in reduced Ring1b binding at these sites in vivo. These findings provide evidence for site-specific PRC1 chromatin recruitment by core binding transcription factors in mammalian cells.National Institutes of Health (U.S.) (Grant U54-CA112967)National Institutes of Health (U.S.) (Grant R01-GM089903)National Science Foundation (U.S.) (Award DB1-0821391)National Institutes of Health (U.S.) (P30-ES002109
Pengaruh Pola Asuh Demokratis Orangtua Terhadap Karakter Remaja Kristen di HKI Sitali-tali Rahut Bosi Pangaribuan Tahun 2020
Abstrak:Penelitian ini bertujuan untuk mengetahui terdapat tidaknya Pengaruh Pola Asuh Demokratis Orangtua Terhadap Karakter Remaja Kristen di HKI Sitali-tali Rahut Bosi Pangaribuan Tahun 2020, dengan hipotesis terdapat pengaruh yang positif dan signifikan antara Pola Asuh Demokratis Orangtua terhadap Karakter Remaja Kristen di HKI Sitali-tali Rahut Bosi Pangaribuan Tahun 2020. Penelitian ini menggunakan pendekatan kuantitatif deskriptif, dengan populasi seluruh remaja di HKI Sitali-tali Rahut Bosi Pangaribuan yang berjumlah 41 orang dengan sampel berjumlah 41 orang. Data dikumpulkan dengan angket tertutup sebanyak 38 item yang disusun oleh penulis berdasarkan indikator variabel sesuai teori ahli. Uji coba angket dilakukan kepada 30 remaja yang bukan responden penelitian, dan telah diuji validitas dan reliabilitasnya. Hasil analisis data menunjukkan bahwa terdapat pengaruh yang positif dan signifikan antara Pola Asuh Demokratis Orangtua terhadap Karakter Remaja Kristen di HKI Sitali-tali Rahut Bosi Pangaribuan Tahun 2020 dengan koefisien determinasi (r2) = 37,94% dan uji signifikan pengaruh diperoleh FhitungFtabel sebesar 23,354,08, artinya Ho ditolak dan Ha diterima.Kata kunci: pola asuh demokratis, karakter Abstract:This study aims to determine whether there is an influence of parental democratic parenting on Christian adolescent characters in HKI Sitali-Tali Rahut Bosi Pangaribuan in 2020, with the hypothesis that there is a positive and significant influence between parental democratic parenting on Christian adolescent characters in HKI Sitali- Tali Rahut Bosi Pangaribuan in 2020. This research uses a descriptive quantitative approach, with a population of all adolescents in HKI Sitali-Tali Rahut Bosi Pangaribuan totaling 41 people with a sample of 41 people. Data were collected using a closed questionnaire of 38 items compiled by the author based on variable indicators according to expert theory. Questionnaire trials were conducted on 30 adolescents who were not research respondents, and their validity and reliability had been tested. The results of the data analysis show that there is a positive and significant influence between Parents' Democratic Parenting Patterns on the Character of Christian Adolescents in HKI Sitali-Tali Rahut Bosi Pangaribuan in 2020 with a coefficient of determination (r2) = 37.94% and a significant test of influence obtained Fcount Ftable of 23.35 4.08, meaning that Ha is rejected and Ha is accepted.Keywords: democratic parenting, characte
Copyright, contratto e accesso alla conoscenza: un’analisi comparata = Copyright, contract and access to knowledge: a comparative analysis.
Il processo di digitalizzazione e lo sviluppo dei media, stravolgendo il paradigma tradizionale del copyright/diritto d’autore conducono a reazioni opposte. Da un lato, estendendo in vario modo l’ampiezza dell’esclusiva autorale favoriscono l’adozione di regole restrittive di accesso e uso dei contenuti; dall’altro, alimentano le logiche di condivisione, specie in alcune aree di produzione del sapere.
Il contratto, pur mutata la propria natura nella dimensione digitale, rappresenta la prima leva per l’affermazione di tali divergenti dinamiche, che, in entrambe le direzioni, riguardano anche la circolazione della conoscenza scientifica. Nel senso dell’apertura, lo strumento negoziale consente di perseguire i principi affermati dal movimento dell’Open Access (OA), abbattendo le barriere economiche e giuridiche all’accesso e utilizzo dei contenuti.
Dal deposito e pubblicazione su archivi istituzionali e disciplinari di opere transitate già attraverso i canali editoriali convenzionali, comunemente definita green road, alla pubblicazione su riviste ad accesso aperto, gold road, il fenomeno si sviluppa dal basso verso l’alto grazie alle dichiarazioni di principio e alle norme informali che hanno sin ora guidato le comunità accademiche nell’affermazione dell’OA. Di recente, tuttavia, i principi dell’OA sono oggetto di attenzione da parte del decisore pubblico che, pur timidamente, ne “impone” l’attuazione a tutte le comunità accademiche. Eppure, il diritto formale non sembra da solo sufficiente: è soltanto il primo tassello di una disciplina organica tesa a definire regole e incentivi per la produzione e la disseminazione della conoscenza scientifica, allo scopo di bilanciare la libertà “accademica” con il diritto di accesso alla conoscenza. = ENGLISH VERSION = Along with a comparative perspective that takes account of the U.S. and Italian law, this work aims to explore the interface between copyright and contract lae in publishing process.
In the current publishing environment, contracts and technology play a dominant role in the exploitation of copyrighted works. Publishers are granted by assignment of all copyright rights to reproduce and publish the work, but also to exercise control over its contents through technological protection measures. At the same time, mass digitization allows libraries and other organizations to make contents available online, which it entails a redefinition of the traditional publishing process and introduces new players to the scene (e.g., Google Books).
Hence, technology proves to be a powerful instrument for the spread of knowledge and it is on this pattern that Open Access (OA) is rapidly gaining ground.
Mostly based on a bottom-up approach that is on soft law, institutional policies and contracts, OA designs a new legal environment targeting the objectives of free accessibility, further distribution, and proper archiving of publications. These aims can be achieved through the creation of new open access business models to publish on OA journals (gold road) or to self-archive in institutional or disciplinary repositories works that have been originally published in conventional journals (green road).
However, in order for OA to be fully developed it is necessary to devise a principled and feasible approach to the dissemination of scholarly works against the current social, economic and legal background.
Indeed, the importance of OA is steadily recognized by legislators who integrate OA provisions into their legal system. This is an innovation of great significance, which was first fostered in the USA, and then extended in some European countries such as Italy and Germany in the European framework. Nevertheless, considering the different law systems, the formal law need to be combined with national strategies and institutional policies providing adequate incentives to the authors, while also promoting academic freedom and the right to knowledge access
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