Your search keyword '"Santolini M"' showing total 43 results

1. A simple cell proliferation assay and the inflammatory protein content show significant differences in human plasmas from young and old subjects.

Author

Muraglia, A., Utyro, O., Nardini, M., Santolini, M., Ceresa, D., Agostini, V., Nencioni, A., Filaci, G., Cancedda, R., and Mastrogiacomo, M.

Published

2024

2. Performance Analysis of a 3.5 kWp CPV System with Two-axis Tracker

Author

Renzi, M., Santolini, M., and Comodi, G.

Published

2014

3. COVID-19 and beyond : a call for action and audacious solidarity to all the citizens and nations, it is humanity’s fight

Author

Auffray, C., Balling, R., Blomberg, N., Bonaldo, M. C., Boutron, B., Brahmachari, S., Bréchot, C., Cesario, A., Chen, S. -J, Clément, K., Danilenko, D., Meglio, A. D., Gelemanović, A., Goble, C., Gojobori, T., Goldman, J. D., Goldman, M., Guo, Y. -K, Heath, J., Hood, L., Hunter, P., Jin, L., Kitano, H., Knoppers, B., Lancet, D., Larue, C., Lathrop, M., Laville, M., Lindner, A. B., Magnan, A., Metspalu, A., Morin, E., Ng, L. F. P., Nicod, L., Noble, D., Nottale, L., Nowotny, H., Ochoa, T., Okeke, I. N., Oni, T., Openshaw, P., Oztürk, M., Palkonen, S., Paweska, J. T., Pison, C., Polymeropoulos, M. H., Pristipino, C., Protzer, U., Roca, J., Rozman, D., Santolini, M., Sanz, F., Scambia, G., Segal, E., Serageldin, I., Soares, M. B., Sterk, P., Sugano, S., Superti-Furga, G., Supple, D., Tegner, J., Uhlén, Mathias, Urbani, A., Valencia, A., Valentini, V., van der Werf, S., Vinciguerra, M., Wolkenhauer, O., Wouters, E., Auffray, C., Balling, R., Blomberg, N., Bonaldo, M. C., Boutron, B., Brahmachari, S., Bréchot, C., Cesario, A., Chen, S. -J, Clément, K., Danilenko, D., Meglio, A. D., Gelemanović, A., Goble, C., Gojobori, T., Goldman, J. D., Goldman, M., Guo, Y. -K, Heath, J., Hood, L., Hunter, P., Jin, L., Kitano, H., Knoppers, B., Lancet, D., Larue, C., Lathrop, M., Laville, M., Lindner, A. B., Magnan, A., Metspalu, A., Morin, E., Ng, L. F. P., Nicod, L., Noble, D., Nottale, L., Nowotny, H., Ochoa, T., Okeke, I. N., Oni, T., Openshaw, P., Oztürk, M., Palkonen, S., Paweska, J. T., Pison, C., Polymeropoulos, M. H., Pristipino, C., Protzer, U., Roca, J., Rozman, D., Santolini, M., Sanz, F., Scambia, G., Segal, E., Serageldin, I., Soares, M. B., Sterk, P., Sugano, S., Superti-Furga, G., Supple, D., Tegner, J., Uhlén, Mathias, Urbani, A., Valencia, A., Valentini, V., van der Werf, S., Vinciguerra, M., Wolkenhauer, O., and Wouters, E.

Abstract

Background: Severe acute respiratory syndrome coronavirus 2 (SARSCoV-2) belongs to a subgroup of coronaviruses rampant in bats for centuries. It caused the coronavirus disease 2019 (COVID-19) pandemic. Most patients recover, but a minority of severe cases experience acute respiratory distress or an inflammatory storm devastating many organs that can lead to patient death. The spread of SARS-CoV-2 was facilitated by the increasing intensity of air travel, urban congestion and human contact during the past decades. Until therapies and vaccines are available, tests for virus exposure, confinement and distancing measures have helped curb the pandemic. Vision: The COVID-19 pandemic calls for safeguards and remediation measures through a systemic response. Self-organizing initiatives by scientists and citizens are developing an advanced collective intelligence response to the coronavirus crisis. Their integration forms Olympiads of Solidarity and Health. Their ability to optimize our response to COVID-19 could serve as a model to trigger a global metamorphosis of our societies with far-reaching consequences for attacking fundamental challenges facing humanity in the 21st century. Mission: For COVID-19 and these other challenges, there is no alternative but action. Meeting in Paris in 2003, we set out to "rethink research to understand life and improve health." We have formed an international coalition of academia and industry ecosystems taking a systems medicine approach to understanding COVID-19 by thoroughly characterizing viruses, patients and populations during the pandemic, using openly shared tools. All results will be publicly available with no initial claims for intellectual property rights. This World Alliance for Health and Wellbeing will catalyze the creation of medical and health products such as diagnostic tests, drugs and vaccines that become common goods accessible to all, while seeking further alliances with civil society to bridge with socio-ecological an, QC 20220519

Published

2020

4. Efficiency assessment for a small heliostat solar concentration plant

Author

Renzi, M., primary, Bartolini, C. M., additional, Santolini, M., additional, and Arteconi, A., additional

Published

2014

5. Health related factors and extra-EU immigrants in Genoa (Italy)

Author

Gabutti, Giovanni, Cirigliano, F, DELLA PIETRA, P, DE ROSA, M. G., DI PIETRANTONJ, C, Flego, G, LENUZZA BERTOLOTTO, A, Santolini, M, and Sigari, G.

Published

1999

6. Efficiency assessment for a small heliostat solar concentration plant.

Author

Renzi, M., Bartolini, C. M., Santolini, M., and Arteconi, A.

Subjects

SOLAR concentrators, ENERGY consumption, HELIOSTATS, SOLAR power plants, IMAGING systems, SOLAR radiation

Abstract

In this paper, a small non-imaging focusing heliostat is presented, and an analytical model for assessing its performance is described. The main novelty of the system lies in the tracking mechanism and the mirror mount, which are based on off-the-shelf components and allow a good trade-off between accuracy and costs. The concentrator mirrors are moved by this two-axis tracking machinery to reflect the sun's rays onto a fixed target, the dimensions of which can be varied to suit the user's needs. A prototype plant to be located in central Italy was designed and simulated with a ray-tracing algorithm, and it comprises 90 heliostats for a total reflective area of 7.5 m2. The reflected solar rays are tracked taking the mechanical positioning errors of the tracking system into account. The total flux of radiation energy hitting the target was determined, and intensity distribution maps were drawn. Simulations showed that the system's optical efficiency can exceed 90% in summer, despite the tracking errors, mainly because of the smaller distance between the heliostats and the receiver. The solar concentration ratio over a receiver of 250 mm in diameter reached 80 suns with a very good uniformity. Over a 400-mm receiver, the concentrated radiation was less uniform, and the solar concentration ratio reached 50 suns, with a higher optical efficiency and collected solar radiation. The present concentration ratio is still suitable for many applications ranging from the electric power production, industrial process heat, and solar cooling. Copyright © 2014 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2015

7. Mechanical forces induce an asthma gene signature in healthy airway epithelial cells

Author

Drazen, J.M., Kho, A.T., Fredberg, J.J., Randell, S.H., Kılıç, A., Park, J.-A., Cheng, F., Tantisira, K., De Marzio, M., Mitchel, J.A., Weiss, S.T., Santolini, M., McGill, M., Sharma, A., Ameli, A., and O'Sullivan, M.J.

Subjects

3. Good health

Abstract

Bronchospasm compresses the bronchial epithelium, and this compressive stress has been implicated in asthma pathogenesis. However, the molecular mechanisms by which this compressive stress alters pathways relevant to disease are not well understood. Using air-liquid interface cultures of primary human bronchial epithelial cells derived from non-asthmatic donors and asthmatic donors, we applied a compressive stress and then used a network approach to map resulting changes in the molecular interactome. In cells from non-asthmatic donors, compression by itself was sufficient to induce inflammatory, late repair, and fibrotic pathways. Remarkably, this molecular profile of non-asthmatic cells after compression recapitulated the profile of asthmatic cells before compression. Together, these results show that even in the absence of any inflammatory stimulus, mechanical compression alone is sufficient to induce an asthma-like molecular signature.

8. Optimization of a methane expansion liquefaction cycle for small scale LNG plants

Author

Arteconi, A., Santolini, M., CARLO MARIA BARTOLINI, and Polonara, F.

9. Anti-HTLV I/II positivity in subjects at risk of HIV infection

Author

Crovari, P., Gabutti, G., Gallo, M., Guida, B., Lazzereschi, M., Piersantelli, N., Rizzo, F., and Santolini, M.

Subjects

HTLV infections -- Diagnosis, HIV infection -- Complications

Abstract

AUTHORS: P. Crovari, G. Gabutti, M. Gallo, B. Guida, M. Lazzereschi, N. Piersantelli, F. Rizzo, M. Santolini and R. Wicks. Institute of Hygiene and Preventive Medicine, Genoa University, Italy Departments [...]

Published

1992

10. An epistemology for democratic citizen science.

Author

Jaeger J, Masselot C, Greshake Tzovaras B, Senabre Hidalgo E, Haklay MM, and Santolini M

Abstract

More than ever, humanity relies on robust scientific knowledge of the world and our place within it. Unfortunately, our contemporary view of science is still suffused with outdated ideas about scientific knowledge production based on a naive kind of realism. These ideas persist among members of the public and scientists alike. They contribute to an ultra-competitive system of academic research, which sacrifices long-term productivity through an excessive obsession with short-term efficiency. Efforts to diversify this system come from a movement called democratic citizen science, which can serve as a model for scientific inquiry in general. Democratic citizen science requires an alternative theory of knowledge with a focus on the role that diversity plays in the process of discovery. Here, we present such an epistemology, based on three central philosophical pillars: perspectival realism, a naturalistic process-based epistemology, and deliberative social practices. They broaden our focus from immediate research outcomes towards cognitive and social processes which facilitate sustainable long-term productivity and scientific innovation. This marks a shift from an industrial to an ecological vision of how scientific research should be done, and how it should be assessed. At the core of this vision are research communities that are diverse, representative, and democratic., Competing Interests: We declare we have no competing interests., (© 2023 The Authors.)

Published

2023

11. Overlapping functions of SIX homeoproteins during embryonic myogenesis.

Author

Wurmser M, Madani R, Chaverot N, Backer S, Borok M, Dos Santos M, Comai G, Tajbakhsh S, Relaix F, Santolini M, Sambasivan R, Jiang R, and Maire P

Subjects

Mice, Animals, Cell Differentiation genetics, Muscle Development genetics, Gene Expression Regulation, Developmental, Muscle, Skeletal metabolism, Homeodomain Proteins metabolism, Somites metabolism

Abstract

Four SIX homeoproteins display a combinatorial expression throughout embryonic developmental myogenesis and they modulate the expression of the myogenic regulatory factors. Here, we provide a deep characterization of their role in distinct mouse developmental territories. We showed, at the hypaxial level, that the Six1:Six4 double knockout (dKO) somitic precursor cells adopt a smooth muscle fate and lose their myogenic identity. At the epaxial level, we demonstrated by the analysis of Six quadruple KO (qKO) embryos, that SIX are required for fetal myogenesis, and for the maintenance of PAX7+ progenitor cells, which differentiated prematurely and are lost by the end of fetal development in qKO embryos. Finally, we showed that Six1 and Six2 are required to establish craniofacial myogenesis by controlling the expression of Myf5. We have thus described an unknown role for SIX proteins in the control of myogenesis at different embryonic levels and refined their involvement in the genetic cascades operating at the head level and in the genesis of myogenic stem cells., Competing Interests: The authors have declared that no competing interests exist., (Copyright: © 2023 Wurmser et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.)

Published

2023

12. Community review: a robust and scalable selection system for resource allocation within open science and innovation communities.

Author

Graham CLB, Landrain TE, Vjestica A, Masselot C, Lawton E, Blondel L, Haenal L, Greshake Tzovaras B, and Santolini M

Subjects

Humans, Research Personnel, Financing, Organized, Writing

Abstract

Resource allocation is essential to selection and implementation of innovative projects in science and technology. Current "winner-take-all" models for grant applications require significant researcher time in writing extensive project proposals, and rely on the availability of a few time-saturated volunteer experts. Such processes usually carry over several months, resulting in high effective costs compared to expected benefits. We devised an agile "community review" system to allocate micro-grants for the fast prototyping of innovative solutions. Here we describe and evaluate the implementation of this community review across 147 projects from the "Just One Giant Lab's OpenCOVID19 initiative" and "Helpful Engineering" open research communities. The community review process uses granular review forms and requires the participation of grant applicants in the review process. Within a year, we organised 7 rounds of review, resulting in 614 reviews from 201 reviewers, and the attribution of 48 micro-grants of up to 4,000 euros. The system is fast, with a median process duration of 10 days, scalable, with a median of 4 reviewers per project independent of the total number of projects, and fair, with project rankings highly preserved after the synthetic removal of reviewers. Regarding potential bias introduced by involving applicants in the process, we find that review scores from both applicants and non-applicants have a similar correlation of r=0.28 with other reviews within a project, matching traditional approaches. Finally, we find that the ability of projects to apply to several rounds allows to foster the further implementation of successful early prototypes, as well as provide a pathway to constructively improve an initially failing proposal in an agile manner. Overall, this study quantitatively highlights the benefits of a frugal, community review system acting as a due diligence for rapid and agile resource allocation in open research and innovation programs, with implications for decentralised communities., Competing Interests: No competing interests were disclosed., (Copyright: © 2023 Graham CLB et al.)

Published

2023

13. Association of hospital centrality in inter-hospital patient-sharing networks with patient mortality and length of stay.

Author

Bergmark RW, Jin G, Semco RS, Santolini M, Olsen MA, and Dhand A

Subjects

United States, Humans, Retrospective Studies, Length of Stay, Inpatients, Cross-Sectional Studies, Hospitals, Hospital Mortality, Pneumonia, Heart Failure

Abstract

Objective: The interdependence of hospitals is underappreciated in patient outcomes studies. We used a network science approach to foreground this interdependence. Specifically, within two large state-based interhospital networks, we examined the relationship of a hospital's network position with in-hospital mortality and length of stay., Methods: We constructed interhospital network graphs using data from the Healthcare Cost and Utilization Project and the American Hospital Association Annual Survey for Florida (2014) and California (2011). The exposure of interest was hospital centrality, defined as weighted degree (sum of all ties to a given hospital from other hospitals). The outcomes were in-hospital mortality and length of stay with sub-analyses for four acute medical conditions: pneumonia, heart failure, ischemic stroke, myocardial infarction. We compared outcomes for each quartile of hospital centrality relative to the most central quartile (Q4), independent of patient- and hospital-level characteristics, in this retrospective cross-sectional study., Results: The inpatient cohorts had 1,246,169 patients in Florida and 1,415,728 in California. Compared to Florida's central hospitals which had an overall mortality 1.60%, peripheral hospitals had higher in-hospital mortality (1.97%, adjusted OR (95%CI): Q1 1.61 (1.37, 1.89), p<0.001). Hospitals in the middle quartiles had lower in-hospital mortality compared to central hospitals (%, adjusted OR (95% CI): Q2 1.39%, 0.79 (0.70, 0.89), p<0.001; Q3 1.33%, 0.78 (0.70, 0.87), p<0.001). Peripheral hospitals had longer lengths of stay (adjusted incidence rate ratio (95% CI): Q1 2.47 (2.44, 2.50), p<0.001). These findings were replicated in California, and in patients with heart failure and pneumonia in Florida. These results show a u-shaped distribution of outcomes based on hospital network centrality quartile., Conclusions: The position of hospitals within an inter-hospital network is associated with patient outcomes. Specifically, hospitals located in the peripheral or central positions may be most vulnerable to diminished quality outcomes due to the network. Results should be replicated with deeper clinical data., Competing Interests: The authors have declared that no competing interests exist., (Copyright: © 2023 Bergmark et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.)

Published

2023

14. Education-based grant programmes for bottom-up distance learning and project catalysis: antimicrobial resistance in Sub-Saharan Africa.

Author

Graham CLB, Akligoh H, Ori JK, Adzaho G, Salekwa L, Campbell P, Saba CKS, Landrain TE, and Santolini M

Abstract

International development and aid are often conducted through the allocation of funding determined by decisions of non-locals, especially in the west for those in the global south. In addition, such funding is often disassociated from local expertise, therefore providing little long-term developmental impact and generating distrust. This is particularly true for conservation, as well as environmental and educational programmes. We hypothesize that by granting local people the educational tools and the necessary funding to develop their own projects through the use of an applicant-driven peer-review approach, it is possible to relocalize the decision-making process to the programme participants, with the potential to generate and select more relevant projects with developmental outcomes of higher quality. Here we created an online curriculum for antimicrobial resistance (AMR) education that was followed by 89 participants across Ghana, Tanzania, Nigeria and Uganda. We then created an open research programme that facilitated the creation of eight de novo projects on AMR. Finally, we organized an applicant-driven grant round to allocate funding to the 'Neonatal Sepsis in Nigeria' project to conduct a pilot study and awareness campaign. This work opens perspectives for the design of frugal educational programmes and the funding of context-specific, community-driven projects aimed at empowering local stakeholders in the global South., Competing Interests: The authors declare no conflict of interest, (© 2023 The Authors.)

Published

2023

15. Network-based response module comprised of gene expression biomarkers predicts response to infliximab at treatment initiation in ulcerative colitis.

Author

Ghiassian SD, Voitalov I, Withers JB, Santolini M, Saleh A, and Akmaev VR

Subjects

Antibodies, Monoclonal therapeutic use, Biomarkers metabolism, Cohort Studies, Humans, Infliximab genetics, Infliximab therapeutic use, Transcriptome, Treatment Outcome, Colitis, Ulcerative drug therapy, Colitis, Ulcerative genetics

Abstract

This cross-cohort study aimed to (1) determine a network-based molecular signature that predicts the likelihood of inadequate response to the tumor necrosis factor-ɑ inhibitor (TNFi) therapy, infliximab, in ulcerative colitis (UC) patients, and (2) address biomarker irreproducibility across different cohort studies. Whole-transcriptome microarray data were derived from biopsies of affected colon tissue from 2 cohorts of infliximab-treated UC patients (training N = 24 and validation N = 22). Response was defined as endoscopic and histologic healing at 4-6 weeks and 8 weeks, respectively. From the training cohort, genes with RNA expression that significantly correlated with clinical response outcomes were mapped onto the Human Interactome network map of protein-protein interactions to identify a largest connected component (LCC) of proteins indicative of infliximab response status in UC. Expression levels of transcripts within the LCC were fed into a probabilistic neural network model to generate a classifier that predicts inadequate response to infliximab. A classifier predictive of inadequate response to infliximab was generated and tested in a cross-cohort, blinded fashion; the AUC was 0.83 and inadequate response was predicted with a 100% positive predictive value and 64% sensitivity. Genes separately identified from the 2 cohorts that correlated with response to infliximab appeared distinct but mapped onto the same network region of the Human Interactome, reflecting a common underlying biology of response among UC patients. Cross-cohort validation of a classifier predictive of infliximab response status in UC patients indicates that a molecular signature of non-response to TNFi therapies is present in patients' baseline gene expression data. The goal is to develop a diagnostic test that predicts which patients will have an inadequate response to targeted therapies and define new targets and pathways for therapeutic development., (Copyright © 2022 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2022

16. Quantifying the rise and fall of scientific fields.

Author

Singh CK, Barme E, Ward R, Tupikina L, and Santolini M

Subjects

Physics, Research Design, Publications, Writing

Abstract

Science advances by pushing the boundaries of the adjacent possible. While the global scientific enterprise grows at an exponential pace, at the mesoscopic level the exploration and exploitation of research ideas are reflected through the rise and fall of research fields. The empirical literature has largely studied such dynamics on a case-by-case basis, with a focus on explaining how and why communities of knowledge production evolve. Although fields rise and fall on different temporal and population scales, they are generally argued to pass through a common set of evolutionary stages. To understand the social processes that drive these stages beyond case studies, we need a way to quantify and compare different fields on the same terms. In this paper we develop techniques for identifying common patterns in the evolution of scientific fields and demonstrate their usefulness using 1.5 million preprints from the arXiv repository covering 175 research fields spanning Physics, Mathematics, Computer Science, Quantitative Biology and Quantitative Finance. We show that fields consistently follow a rise and fall pattern captured by a two parameters right-tailed Gumbel temporal distribution. We introduce a field-specific re-scaled time and explore the generic properties shared by articles and authors at the creation, adoption, peak, and decay evolutionary phases. We find that the early phase of a field is characterized by disruptive works mixing of cognitively distant fields written by small teams of interdisciplinary authors, while late phases exhibit the role of specialized, large teams building on the previous works in the field. This method provides foundations to quantitatively explore the generic patterns underlying the evolution of research fields in science, with general implications in innovation studies., Competing Interests: The commercial affiliation does not alter our adherence to PLOS ONE policies on sharing data and materials.

Published

2022

17. Retraction notice to "Network-based response module comprised of gene expression biomarkers predicts response to infliximab at treatment initiation in ulcerative colitis" Translational Research 239C (2021) 35-43.

Author

Akmaev VR, Ghiassian SD, Withers JB, Santolini M, and Saleh A

Published

2022

18. Implementing the Co-Immune Open Innovation Program to Address Vaccination Hesitancy and Access to Vaccines: Retrospective Study.

Author

Masselot C, Greshake Tzovaras B, Graham CLB, Finnegan G, Jeyaram R, Vitali I, Landrain T, and Santolini M

Abstract

Background: The rise of major complex public health problems, such as vaccination hesitancy and access to vaccination, requires innovative, open, and transdisciplinary approaches. Yet, institutional silos and lack of participation on the part of nonacademic citizens in the design of solutions hamper efforts to meet these challenges. Against this background, new solutions have been explored, with participatory research, citizen science, hackathons, and challenge-based approaches being applied in the context of public health., Objective: Our aim was to develop a program for creating citizen science and open innovation projects that address the contemporary challenges of vaccination in France and around the globe., Methods: We designed and implemented Co-Immune, a program created to tackle the question of vaccination hesitancy and access to vaccination through an online and offline challenge-based open innovation approach. The program was run on the open science platform Just One Giant Lab., Results: Over a 6-month period, the Co-Immune program gathered 234 participants of diverse backgrounds and 13 partners from the public and private sectors. The program comprised 10 events to facilitate the creation of 20 new projects, as well as the continuation of two existing projects, to address the issues of vaccination hesitancy and access, ranging from app development and data mining to analysis and game design. In an open framework, the projects made their data, code, and solutions publicly available., Conclusions: Co-Immune highlights how open innovation approaches and online platforms can help to gather and coordinate noninstitutional communities in a rapid, distributed, and global way toward solving public health issues. Such initiatives can lead to the production and transfer of knowledge, creating novel solutions in the public health sector. The example of Co-Immune contributes to paving the way for organizations and individuals to collaboratively tackle future global challenges., (©Camille Masselot, Bastian Greshake Tzovaras, Chris L B Graham, Gary Finnegan, Rathin Jeyaram, Isabelle Vitali, Thomas Landrain, Marc Santolini. Originally published in Journal of Participatory Medicine (https://jopm.jmir.org), 21.01.2022.)

Published

2022

19. RETRACTED: Network-based response module comprised of gene expression biomarkers predicts response to infliximab at treatment initiation in ulcerative colitis.

Author

Ghiassian SD, Withers JB, Santolini M, Saleh A, and Akmaev VR

Subjects

Area Under Curve, Biomarkers, Case-Control Studies, Colitis, Ulcerative metabolism, Gastrointestinal Agents therapeutic use, Humans, Intestinal Mucosa drug effects, Protein Interaction Maps genetics, Reproducibility of Results, Treatment Outcome, Colitis, Ulcerative drug therapy, Colitis, Ulcerative genetics, Gene Expression drug effects, Infliximab therapeutic use

Abstract

This article has been retracted: please see Elsevier Policy on Article Withdrawal (https://www.elsevier.com/about/our-business/policies/article-withdrawal). This article has been retracted at the request of the authors after consulting with the Editors. During a follow-up study, the authors regretfully discovered that the microarray probe-to-gene mapping was incorrect. Although the methodology and primary findings remain the same, the identity of the biomarker genes are incorrect as a result of this honest mistake. The extent of the changes to correct this information necessitated the publication of a corrected version of this article: https://doi.org/10.1016/j.trsl.2022.03.006., (Copyright © 2021 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2022

20. Detection of Spatiotemporal Clusters of COVID-19-Associated Symptoms and Prevention Using a Participatory Surveillance App: Protocol for the @choum Study.

Author

De Ridder D, Loizeau AJ, Sandoval JL, Ehrler F, Perrier M, Ritch A, Violot G, Santolini M, Greshake Tzovaras B, Stringhini S, Kaiser L, Pradeau JF, Joost S, and Guessous I

Abstract

Background: The early detection of clusters of infectious diseases such as the SARS-CoV-2-related COVID-19 disease can promote timely testing recommendation compliance and help to prevent disease outbreaks. Prior research revealed the potential of COVID-19 participatory syndromic surveillance systems to complement traditional surveillance systems. However, most existing systems did not integrate geographic information at a local scale, which could improve the management of the SARS-CoV-2 pandemic., Objective: The aim of this study is to detect active and emerging spatiotemporal clusters of COVID-19-associated symptoms, and to examine (a posteriori) the association between the clusters' characteristics and sociodemographic and environmental determinants., Methods: This report presents the methodology and development of the @choum (English: "achoo") study, evaluating an epidemiological digital surveillance tool to detect and prevent clusters of individuals (target sample size, N=5000), aged 18 years or above, with COVID-19-associated symptoms living and/or working in the canton of Geneva, Switzerland. The tool is a 5-minute survey integrated into a free and secure mobile app (CoronApp-HUG). Participants are enrolled through a comprehensive communication campaign conducted throughout the 12-month data collection phase. Participants register to the tool by providing electronic informed consent and nonsensitive information (gender, age, geographically masked addresses). Symptomatic participants can then report COVID-19-associated symptoms at their onset (eg, symptoms type, test date) by tapping on the @choum button. Those who have not yet been tested are offered the possibility to be informed on their cluster status (information returned by daily automated clustering analysis). At each participation step, participants are redirected to the official COVID-19 recommendations websites. Geospatial clustering analyses are performed using the modified space-time density-based spatial clustering of applications with noise (MST-DBSCAN) algorithm., Results: The study began on September 1, 2020, and will be completed on February 28, 2022. Multiple tests performed at various time points throughout the 5-month preparation phase have helped to improve the tool's user experience and the accuracy of the clustering analyses. A 1-month pilot study performed among 38 pharmacists working in 7 Geneva-based pharmacies confirmed the proper functioning of the tool. Since the tool's launch to the entire population of Geneva on February 11, 2021, data are being collected and clusters are being carefully monitored. The primary study outcomes are expected to be published in mid-2022., Conclusions: The @choum study evaluates an innovative participatory epidemiological digital surveillance tool to detect and prevent clusters of COVID-19-associated symptoms. @choum collects precise geographic information while protecting the user's privacy by using geomasking methods. By providing an evidence base to inform citizens and local authorities on areas potentially facing a high COVID-19 burden, the tool supports the targeted allocation of public health resources and promotes testing., International Registered Report Identifier (irrid): DERR1-10.2196/30444., (©David De Ridder, Andrea Jutta Loizeau, José Luis Sandoval, Frédéric Ehrler, Myriam Perrier, Albert Ritch, Guillemette Violot, Marc Santolini, Bastian Greshake Tzovaras, Silvia Stringhini, Laurent Kaiser, Jean-François Pradeau, Stéphane Joost, Idris Guessous. Originally published in JMIR Research Protocols (https://www.researchprotocols.org), 06.10.2021.)

Published

2021

21. Proteomic Analysis Uncovers Measles Virus Protein C Interaction With p65-iASPP Protein Complex.

Author

Meignié A, Combredet C, Santolini M, Kovács IA, Douché T, Gianetto QG, Eun H, Matondo M, Jacob Y, Grailhe R, Tangy F, and Komarova AV

Subjects

Animals, Cell Death, Cell Line, Chlorocebus aethiops, Host-Pathogen Interactions, Humans, Intracellular Signaling Peptides and Proteins genetics, Measles virus genetics, Measles virus physiology, Protein Interaction Maps, Proteomics, Repressor Proteins genetics, Transcription Factor RelA genetics, Tumor Suppressor Protein p53 genetics, Tumor Suppressor Protein p53 metabolism, Viral Nonstructural Proteins genetics, Virus Replication, Intracellular Signaling Peptides and Proteins metabolism, Repressor Proteins metabolism, Transcription Factor RelA metabolism, Viral Nonstructural Proteins metabolism

Abstract

Viruses manipulate the central machineries of host cells to their advantage. They prevent host cell antiviral responses to create a favorable environment for their survival and propagation. Measles virus (MV) encodes two nonstructural proteins MV-V and MV-C known to counteract the host interferon response and to regulate cell death pathways. Several molecular mechanisms underlining MV-V regulation of innate immunity and cell death pathways have been proposed, whereas MV-C host-interacting proteins are less studied. We suggest that some cellular factors that are controlled by MV-C protein during viral replication could be components of innate immunity and the cell death pathways. To determine which host factors are targeted by MV-C, we captured both direct and indirect host-interacting proteins of MV-C protein. For this, we used a strategy based on recombinant viruses expressing tagged viral proteins followed by affinity purification and a bottom-up mass spectrometry analysis. From the list of host proteins specifically interacting with MV-C protein in different cell lines, we selected the host targets that belong to immunity and cell death pathways for further validation. Direct protein interaction partners of MV-C were determined by applying protein complementation assay and the bioluminescence resonance energy transfer approach. As a result, we found that MV-C protein specifically interacts with p65-iASPP protein complex that controls both cell death and innate immunity pathways and evaluated the significance of these host factors on virus replication., Competing Interests: Conflict of interest The authors declare no competing interests., (Copyright © 2021 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2021

22. Mechanical forces induce an asthma gene signature in healthy airway epithelial cells.

Author

Kılıç A, Ameli A, Park JA, Kho AT, Tantisira K, Santolini M, Cheng F, Mitchel JA, McGill M, O'Sullivan MJ, De Marzio M, Sharma A, Randell SH, Drazen JM, Fredberg JJ, and Weiss ST

Subjects

Epithelial Cells pathology, Humans, Airway Remodeling physiology, Asthma genetics, Bronchi pathology, Epithelial Cells metabolism, Gene Expression, Stress, Mechanical

Abstract

Bronchospasm compresses the bronchial epithelium, and this compressive stress has been implicated in asthma pathogenesis. However, the molecular mechanisms by which this compressive stress alters pathways relevant to disease are not well understood. Using air-liquid interface cultures of primary human bronchial epithelial cells derived from non-asthmatic donors and asthmatic donors, we applied a compressive stress and then used a network approach to map resulting changes in the molecular interactome. In cells from non-asthmatic donors, compression by itself was sufficient to induce inflammatory, late repair, and fibrotic pathways. Remarkably, this molecular profile of non-asthmatic cells after compression recapitulated the profile of asthmatic cells before compression. Together, these results show that even in the absence of any inflammatory stimulus, mechanical compression alone is sufficient to induce an asthma-like molecular signature.

Published

2020

23. Integration of Molecular Interactome and Targeted Interaction Analysis to Identify a COPD Disease Network Module.

Author

Sharma A, Kitsak M, Cho MH, Ameli A, Zhou X, Jiang Z, Crapo JD, Beaty TH, Menche J, Bakke PS, Santolini M, and Silverman EK

Subjects

Female, Genome-Wide Association Study, Humans, Male, Databases, Genetic, GTPase-Activating Proteins genetics, GTPase-Activating Proteins metabolism, Genetic Loci, Genetic Predisposition to Disease, Pulmonary Disease, Chronic Obstructive genetics, Pulmonary Disease, Chronic Obstructive metabolism

Abstract

The polygenic nature of complex diseases offers potential opportunities to utilize network-based approaches that leverage the comprehensive set of protein-protein interactions (the human interactome) to identify new genes of interest and relevant biological pathways. However, the incompleteness of the current human interactome prevents it from reaching its full potential to extract network-based knowledge from gene discovery efforts, such as genome-wide association studies, for complex diseases like chronic obstructive pulmonary disease (COPD). Here, we provide a framework that integrates the existing human interactome information with experimental protein-protein interaction data for FAM13A, one of the most highly associated genetic loci to COPD, to find a more comprehensive disease network module. We identified an initial disease network neighborhood by applying a random-walk method. Next, we developed a network-based closeness approach (C AB ) that revealed 9 out of 96 FAM13A interacting partners identified by affinity purification assays were significantly close to the initial network neighborhood. Moreover, compared to a similar method (local radiality), the C AB approach predicts low-degree genes as potential candidates. The candidates identified by the network-based closeness approach were combined with the initial network neighborhood to build a comprehensive disease network module (163 genes) that was enriched with genes differentially expressed between controls and COPD subjects in alveolar macrophages, lung tissue, sputum, blood, and bronchial brushing datasets. Overall, we demonstrate an approach to find disease-related network components using new laboratory data to overcome incompleteness of the current interactome.

Published

2018

24. The Ca 2+ transient as a feedback sensor controlling cardiomyocyte ionic conductances in mouse populations.

Author

Rees CM, Yang JH, Santolini M, Lusis AJ, Weiss JN, and Karma A

Subjects

Animals, Cells, Cultured, Heart Ventricles cytology, Mice, Myocardial Contraction, Patch-Clamp Techniques, Calcium metabolism, Cations metabolism, Ion Channels metabolism, Myocytes, Cardiac physiology, Potassium metabolism

Abstract

Conductances of ion channels and transporters controlling cardiac excitation may vary in a population of subjects with different cardiac gene expression patterns. However, the amount of variability and its origin are not quantitatively known. We propose a new conceptual approach to predict this variability that consists of finding combinations of conductances generating a normal intracellular Ca 2+ transient without any constraint on the action potential. Furthermore, we validate experimentally its predictions using the Hybrid Mouse Diversity Panel, a model system of genetically diverse mouse strains that allows us to quantify inter-subject versus intra-subject variability. The method predicts that conductances of inward Ca 2+ and outward K + currents compensate each other to generate a normal Ca 2+ transient in good quantitative agreement with current measurements in ventricular myocytes from hearts of different isogenic strains. Our results suggest that a feedback mechanism sensing the aggregate Ca 2+ transient of the heart suffices to regulate ionic conductances., Competing Interests: CR, JY, MS, AL, JW, AK No competing interests declared, (© 2018, Rees et al.)

Published

2018

25. Predicting perturbation patterns from the topology of biological networks.

Author

Santolini M and Barabási AL

Subjects

Bacteria genetics, Bacteria metabolism, Chemotaxis physiology, Gene Expression Regulation, Bacterial physiology, Models, Biological

Abstract

High-throughput technologies, offering an unprecedented wealth of quantitative data underlying the makeup of living systems, are changing biology. Notably, the systematic mapping of the relationships between biochemical entities has fueled the rapid development of network biology, offering a suitable framework to describe disease phenotypes and predict potential drug targets. However, our ability to develop accurate dynamical models remains limited, due in part to the limited knowledge of the kinetic parameters underlying these interactions. Here, we explore the degree to which we can make reasonably accurate predictions in the absence of the kinetic parameters. We find that simple dynamically agnostic models are sufficient to recover the strength and sign of the biochemical perturbation patterns observed in 87 biological models for which the underlying kinetics are known. Surprisingly, a simple distance-based model achieves 65% accuracy. We show that this predictive power is robust to topological and kinetic parameter perturbations, and we identify key network properties that can increase up to 80% the recovery rate of the true perturbation patterns. We validate our approach using experimental data on the chemotactic pathway in bacteria, finding that a network model of perturbation spreading predicts with ∼80% accuracy the directionality of gene expression and phenotype changes in knock-out and overproduction experiments. These findings show that the steady advances in mapping out the topology of biochemical interaction networks opens avenues for accurate perturbation spread modeling, with direct implications for medicine and drug development., Competing Interests: The authors declare no conflict of interest.

Published

2018

26. Controllability in an islet specific regulatory network identifies the transcriptional factor NFATC4, which regulates Type 2 Diabetes associated genes.

Author

Sharma A, Halu A, Decano JL, Padi M, Liu YY, Prasad RB, Fadista J, Santolini M, Menche J, Weiss ST, Vidal M, Silverman EK, Aikawa M, Barabási AL, Groop L, and Loscalzo J

Abstract

Probing the dynamic control features of biological networks represents a new frontier in capturing the dysregulated pathways in complex diseases. Here, using patient samples obtained from a pancreatic islet transplantation program, we constructed a tissue-specific gene regulatory network and used the control centrality (Cc) concept to identify the high control centrality (HiCc) pathways, which might serve as key pathobiological pathways for Type 2 Diabetes (T2D). We found that HiCc pathway genes were significantly enriched with modest GWAS p -values in the DIAbetes Genetics Replication And Meta-analysis (DIAGRAM) study. We identified variants regulating gene expression (expression quantitative loci, eQTL) of HiCc pathway genes in islet samples. These eQTL genes showed higher levels of differential expression compared to non-eQTL genes in low, medium, and high glucose concentrations in rat islets. Among genes with highly significant eQTL evidence, NFATC4 belonged to four HiCc pathways. We asked if the expressions of T2D-associated candidate genes from GWAS and literature are regulated by Nfatc4 in rat islets. Extensive in vitro silencing of Nfatc4 in rat islet cells displayed reduced expression of 16, and increased expression of four putative downstream T2D genes. Overall, our approach uncovers the mechanistic connection of NFATC4 with downstream targets including a previously unknown one, TCF7L2, and establishes the HiCc pathways' relationship to T2D., Competing Interests: In the past three years, E.K.S. received honoraria and consulting fees from Merck, grant support and consulting fees from GlaxoSmithKline, and honoraria and travel support from Novartis. J.L. discloses a relevant conflict for his founder’s role with Scipher, Inc. (a network medicine company).

Published

2018

27. A systems immunology approach identifies the collective impact of 5 miRs in Th2 inflammation.

Author

Kılıç A, Santolini M, Nakano T, Schiller M, Teranishi M, Gellert P, Ponomareva Y, Braun T, Uchida S, Weiss ST, Sharma A, and Renz H

Subjects

Animals, Asthma immunology, Asthma pathology, Bronchoalveolar Lavage Fluid cytology, Bronchoalveolar Lavage Fluid immunology, Disease Models, Animal, Female, Gene Expression Profiling, Gene Regulatory Networks immunology, Humans, Inflammation immunology, Inflammation pathology, Lung cytology, Lung immunology, Lung pathology, Mice, Mice, Inbred BALB C, Ovalbumin administration & dosage, Ovalbumin immunology, Primary Cell Culture, Protein Interaction Maps immunology, Systems Biology methods, Th2 Cells metabolism, Asthma genetics, Gene Expression Regulation immunology, Inflammation genetics, MicroRNAs metabolism, Th2 Cells immunology

Abstract

Allergic asthma is a chronic inflammatory disease dominated by a CD4+ T helper 2 (Th2) cell signature. The immune response amplifies in self-enforcing loops, promoting Th2-driven cellular immunity and leaving the host unable to terminate inflammation. Posttranscriptional mechanisms, including microRNAs (miRs), are pivotal in maintaining immune homeostasis. Since an altered expression of various miRs has been associated with T cell-driven diseases, including asthma, we hypothesized that miRs control mechanisms ensuring Th2 stability and maintenance in the lung. We isolated murine CD4+ Th2 cells from allergic inflamed lungs and profiled gene and miR expression. Instead of focusing on the magnitude of miR differential expression, here we addressed the secondary consequences for the set of molecular interactions in the cell, the interactome. We developed the Impact of Differential Expression Across Layers, a network-based algorithm to prioritize disease-relevant miRs based on the central role of their targets in the molecular interactome. This method identified 5 Th2-related miRs (mir27b, mir206, mir106b, mir203, and mir23b) whose antagonization led to a sharp reduction of the Th2 phenotype. Overall, a systems biology tool was developed and validated, highlighting the role of miRs in Th2-driven immune response. This result offers potentially novel approaches for therapeutic interventions.

Published

2018

28. A personalized, multiomics approach identifies genes involved in cardiac hypertrophy and heart failure.

Author

Santolini M, Romay MC, Yukhtman CL, Rau CD, Ren S, Saucerman JJ, Wang JJ, Weiss JN, Wang Y, Lusis AJ, and Karma A

Abstract

A traditional approach to investigate the genetic basis of complex diseases is to identify genes with a global change in expression between diseased and healthy individuals. However, population heterogeneity may undermine the effort to uncover genes with significant but individual contribution to the spectrum of disease phenotypes within a population. Here we investigate individual changes of gene expression when inducing hypertrophy and heart failure in 100 + strains of genetically distinct mice from the Hybrid Mouse Diversity Panel (HMDP). We find that genes whose expression fold-change correlates in a statistically significant way with the severity of the disease are either up or down-regulated across strains, and therefore missed by a traditional population-wide analysis of differential gene expression. Furthermore, those "fold-change" genes are enriched in human cardiac disease genes and form a dense co-regulated module strongly interacting with the cardiac hypertrophic signaling network in the human interactome. We validate our approach by showing that the knockdown of Hes1 , predicted as a strong candidate, induces a dramatic reduction of hypertrophy by 80-90% in neonatal rat ventricular myocytes. Our results demonstrate that individualized approaches are crucial to identify genes underlying complex diseases as well as to develop personalized therapies., Competing Interests: The authors declare no competing financial interests.

Published

2018

29. Selective cysteine modification of metal-free human metallothionein 1a and its isolated domain fragments: Solution structural properties revealed via ESI-MS.

Author

Irvine GW, Santolini M, and Stillman MJ

Subjects

Cysteine chemistry, Cysteine metabolism, Humans, Hydrogen-Ion Concentration, Mass Spectrometry, Metallothionein genetics, Metallothionein metabolism, Protein Domains, Metallothionein chemistry, Protein Folding, Protein Processing, Post-Translational

Abstract

Human metallothionein 1a, a protein with two cysteine-rich metal-binding domains (α with 11 Cys and β with 9), was analyzed in its metal-free form by selective, covalent Cys modification coupled with ESI-MS. The modification profiles of the isolated β- and α-fragments reacted with p-benzoquinone (Bq), N-ethylmalemide (NEM) and iodoacetamide (IAM) were compared with the full length protein using ESI-mass spectral data to follow the reaction pathway. Under denaturing conditions at low pH, the reaction profile with each modifier followed pathways that resulted in stochastic, Normal distributions of species whose maxima was equal to the mol. eq. of modifier added. Our interpretation of modification at this pH is that reaction with the cysteines is unimpeded when the full protein or those of its isolated domains are denatured. At neutral pH, where the protein is expected to be folded in a more compact structure, there is a difference in the larger Bq and NEM modification, whose reaction profiles indicate a cooperative pattern. The reaction profile with IAM under native conditions follows a similar stochastic distribution as at low pH, suggesting that this modifier is small enough to access the cysteines unimpeded by the compact structure. The data emphasize the utility of residue modification coupled with electrospray ionization mass spectrometry for the study of protein structure., (© 2017 The Protein Society.)

Published

2017

30. Systems Genetics Approach Identifies Gene Pathways and Adamts2 as Drivers of Isoproterenol-Induced Cardiac Hypertrophy and Cardiomyopathy in Mice.

Author

Rau CD, Romay MC, Tuteryan M, Wang JJ, Santolini M, Ren S, Karma A, Weiss JN, Wang Y, and Lusis AJ

Subjects

ADAMTS Proteins physiology, Animals, Cardiomegaly chemically induced, Cardiomyopathies genetics, Cardiomyopathies metabolism, Cardiomyopathies physiopathology, Cardiotonic Agents adverse effects, Catecholamines adverse effects, Gene Expression Regulation drug effects, Gene Regulatory Networks genetics, Heart Failure genetics, Heart Ventricles metabolism, Isoproterenol pharmacology, Mice, Mice, Inbred Strains genetics, Myocardium metabolism, Myocytes, Cardiac metabolism, Signal Transduction drug effects, Ventricular Remodeling genetics, ADAMTS Proteins genetics, Cardiomegaly genetics, Systems Biology methods

Abstract

We previously reported a genetic analysis of heart failure traits in a population of inbred mouse strains treated with isoproterenol to mimic catecholamine-driven cardiac hypertrophy. Here, we apply a co-expression network algorithm, wMICA, to perform a systems-level analysis of left ventricular transcriptomes from these mice. We describe the features of the overall network but focus on a module identified in treated hearts that is strongly related to cardiac hypertrophy and pathological remodeling. Using the causal modeling algorithm NEO, we identified the gene Adamts2 as a putative regulator of this module and validated the predictive value of NEO using small interfering RNA-mediated knockdown in neonatal rat ventricular myocytes. Adamts2 silencing regulated the expression of the genes residing within the module and impaired isoproterenol-induced cellular hypertrophy. Our results provide a view of higher order interactions in heart failure with potential for diagnostic and therapeutic insights., (Copyright © 2017 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2017

31. Early pregnancy vitamin D status and risk of preeclampsia.

Author

Mirzakhani H, Litonjua AA, McElrath TF, O'Connor G, Lee-Parritz A, Iverson R, Macones G, Strunk RC, Bacharier LB, Zeiger R, Hollis BW, Handy DE, Sharma A, Laranjo N, Carey V, Qiu W, Santolini M, Liu S, Chhabra D, Enquobahrie DA, Williams MA, Loscalzo J, and Weiss ST

Subjects

Adolescent, Adult, Female, Humans, Incidence, Pre-Eclampsia blood, Pre-Eclampsia epidemiology, Pregnancy, Risk Factors, Vitamin D administration & dosage, Vitamin D pharmacokinetics, Dietary Supplements, Pre-Eclampsia prevention & control, Pregnancy Trimester, First blood, Pregnancy Trimester, Third blood, Vitamin D analogs & derivatives

Abstract

Background: Low vitamin D status in pregnancy was proposed as a risk factor of preeclampsia., Methods: We assessed the effect of vitamin D supplementation (4,400 vs. 400 IU/day), initiated early in pregnancy (10-18 weeks), on the development of preeclampsia. The effects of serum vitamin D (25-hydroxyvitamin D [25OHD]) levels on preeclampsia incidence at trial entry and in the third trimester (32-38 weeks) were studied. We also conducted a nested case-control study of 157 women to investigate peripheral blood vitamin D-associated gene expression profiles at 10 to 18 weeks in 47 participants who developed preeclampsia., Results: Of 881 women randomized, outcome data were available for 816, with 67 (8.2%) developing preeclampsia. There was no significant difference between treatment (N = 408) or control (N = 408) groups in the incidence of preeclampsia (8.08% vs. 8.33%, respectively; relative risk: 0.97; 95% CI, 0.61-1.53). However, in a cohort analysis and after adjustment for confounders, a significant effect of sufficient vitamin D status (25OHD ≥30 ng/ml) was observed in both early and late pregnancy compared with insufficient levels (25OHD <30 ng/ml) (adjusted odds ratio, 0.28; 95% CI, 0.10-0.96). Differential expression of 348 vitamin D-associated genes (158 upregulated) was found in peripheral blood of women who developed preeclampsia (FDR <0.05 in the Vitamin D Antenatal Asthma Reduction Trial [VDAART]; P < 0.05 in a replication cohort). Functional enrichment and network analyses of this vitamin D-associated gene set suggests several highly functional modules related to systematic inflammatory and immune responses, including some nodes with a high degree of connectivity., Conclusions: Vitamin D supplementation initiated in weeks 10-18 of pregnancy did not reduce preeclampsia incidence in the intention-to-treat paradigm. However, vitamin D levels of 30 ng/ml or higher at trial entry and in late pregnancy were associated with a lower risk of preeclampsia. Differentially expressed vitamin D-associated transcriptomes implicated the emergence of an early pregnancy, distinctive immune response in women who went on to develop preeclampsia., Trial Registration: ClinicalTrials.gov NCT00920621., Funding: Quebec Breast Cancer Foundation and Genome Canada Innovation Network. This trial was funded by the National Heart, Lung, and Blood Institute. For details see Acknowledgments., Competing Interests: The authors have declared that no conflict of interest exists.

Published

2016

32. MyoD reprogramming requires Six1 and Six4 homeoproteins: genome-wide cis-regulatory module analysis.

Author

Santolini M, Sakakibara I, Gauthier M, Ribas-Aulinas F, Takahashi H, Sawasaki T, Mouly V, Concordet JP, Defossez PA, Hakim V, and Maire P

Subjects

Animals, Base Sequence, Binding Sites genetics, Cells, Cultured, Chromatin Immunoprecipitation, Embryo, Mammalian cytology, Fibroblasts metabolism, Homeodomain Proteins genetics, Humans, Luciferases metabolism, Mice, Knockout, Muscle Development genetics, Mutation genetics, Nuclear Proteins metabolism, Nucleotide Motifs genetics, Reproducibility of Results, Trans-Activators genetics, Transcription Factors metabolism, Cellular Reprogramming genetics, Genome, Homeodomain Proteins metabolism, MyoD Protein metabolism, Regulatory Sequences, Nucleic Acid genetics, Trans-Activators metabolism

Abstract

Myogenic regulatory factors of the MyoD family have the ability to reprogram differentiated cells toward a myogenic fate. In this study, we demonstrate that Six1 or Six4 are required for the reprogramming by MyoD of mouse embryonic fibroblasts (MEFs). Using microarray experiments, we found 761 genes under the control of both Six and MyoD. Using MyoD ChIPseq data and a genome-wide search for Six1/4 MEF3 binding sites, we found significant co-localization of binding sites for MyoD and Six proteins on over a thousand mouse genomic DNA regions. The combination of both datasets yielded 82 genes which are synergistically activated by Six and MyoD, with 96 associated MyoD+MEF3 putative cis-regulatory modules (CRMs). Fourteen out of 19 of the CRMs that we tested demonstrated in Luciferase assays a synergistic action also observed for their cognate gene. We searched putative binding sites on these CRMs using available databases and de novo search of conserved motifs and demonstrated that the Six/MyoD synergistic activation takes place in a feedforward way. It involves the recruitment of these two families of transcription factors to their targets, together with partner transcription factors, encoded by genes that are themselves activated by Six and MyoD, including Mef2, Pbx-Meis and EBF., (© The Author(s) 2016. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published

2016

33. Six1 homeoprotein drives myofiber type IIA specialization in soleus muscle.

Author

Sakakibara I, Wurmser M, Dos Santos M, Santolini M, Ducommun S, Davaze R, Guernec A, Sakamoto K, and Maire P

Subjects

Animals, Calcium metabolism, Gene Deletion, Gene Regulatory Networks, Glycolysis, Homeodomain Proteins genetics, Male, Mice, Muscle Fibers, Skeletal cytology, Myosin Heavy Chains genetics, Myosin Heavy Chains metabolism, Phenotype, Transcriptome, Homeodomain Proteins metabolism, Muscle Fibers, Skeletal metabolism

Abstract

Background: Adult skeletal muscles are composed of slow and fast myofiber subtypes which each express selective genes required for their specific contractile and metabolic activity. Six homeoproteins are transcription factors regulating muscle cell fate through activation of myogenic regulatory factors and driving fast-type gene expression during embryogenesis., Results: We show here that Six1 protein accumulates more robustly in the nuclei of adult fast-type muscles than in adult slow-type muscles, this specific enrichment takes place during perinatal growth. Deletion of Six1 in soleus impaired fast-type myofiber specialization during perinatal development, resulting in a slow phenotype and a complete lack of Myosin heavy chain 2A (MyHCIIA) expression. Global transcriptomic analysis of wild-type and Six1 mutant myofibers identified the gene networks controlled by Six1 in adult soleus muscle. This analysis showed that Six1 is required for the expression of numerous genes encoding fast-type sarcomeric proteins, glycolytic enzymes and controlling intracellular calcium homeostasis. Parvalbumin, a key player of calcium buffering, in particular, is a direct target of Six1 in the adult myofiber., Conclusions: This analysis revealed that Six1 controls distinct aspects of adult muscle physiology in vivo, and acts as a main determinant of fast-fiber type acquisition and maintenance.

Published

2016

34. Safety and tolerability of 13-valent pneumococcal conjugate vaccine in the elderly.

Author

Durando P, Rosselli R, Cremonesi I, Orsi A, Albanese E, Barberis I, Paganino C, Trucchi C, Martini M, Marensi L, Turello V, Study Group TL, Bregante A, Cacciani R, Iudici R, La Marca D, Pedano L, Petrucci AF, Santolini M, Sbisà V, and Zacconi M

Subjects

Aged, Aged, 80 and over, Drug-Related Side Effects and Adverse Reactions pathology, Fatigue chemically induced, Fatigue epidemiology, Female, Headache chemically induced, Headache epidemiology, Humans, Italy, Male, Pain chemically induced, Pain epidemiology, Pneumococcal Vaccines administration & dosage, Drug-Related Side Effects and Adverse Reactions epidemiology

Abstract

Background: In September 2011 the European Medical Agency authorized the use of 13-valent pneumococcal conjugate vaccine (PCV13) in adults aged ≥50 years. The same occurred in the US in December 2011 when the Food and Drug Administration approved the use of PCV13 in the same target age-group with indication for the prevention of invasive pneumococcal diseases and community acquired pneumonia sustained by the serotypes contained in the vaccine. The Liguria Region, in Italy, implemented in 2013 an active and free of charge immunization strategy with PCV13 among adults affected by specific risk conditions and the elderly aged ≥70 years., Methods: An observational study was performed in order to assess the safety and tolerability of PCV13 among elderly dwelling in the metropolitan area of Genoa, the capital city of Liguria Region. Eligible subjects, who received PCV13 following the public health immunization campaign at the Local Health Unit 3 of Genoa, provided a written informed consent to take part in the study. Eight-hundred-seventy-one subjects were enrolled between October 2013 and May 2014: all were monitored by qualified healthcare personnel for at least 30 min after vaccination at the outpatient clinics, in order to assess any possible sudden reaction. The occurrence of a series of local and systemic solicited reactions and of any unsolicited Adverse Events (AEs) was monitored using a self-administered clinical diary and by regular phone contacts up to 14 and 21 d following immunization, respectively. Moreover, a 6-months follow-up following vaccination was planned in order to monitor Severe Adverse Events (SAEs)., Results: No sudden reaction occurred in vaccinees at the outpatient clinics. Pain (27.4%) was the most frequent reaction reported by subjects at the injection site, while new muscle pain (13.6%), fatigue (10.7%), and headache (9.9%) resulted the most common systemic reactions. Rates of the main reactions reported in this on-field study resulted generally lower than those registered in clinical trials performed in the elderly. The incidence of fever (2.2%) following vaccination was low at values superimposable to that reported in previous studies., Conclusion: This observational study showed a good safety and tolerability of PCV13 among the elderly in routine clinical practice further confirming the evidence coming from clinical trials in the same age-group.

Published

2015

35. A general pairwise interaction model provides an accurate description of in vivo transcription factor binding sites.

Author

Santolini M, Mora T, and Hakim V

Subjects

Animals, Base Sequence, Binding Sites genetics, Cells, Cultured, Drosophila melanogaster, Mice, Molecular Sequence Data, Position-Specific Scoring Matrices, Protein Binding, Algorithms, Computational Biology methods, Models, Theoretical, Response Elements, Transcription Factors metabolism

Abstract

The identification of transcription factor binding sites (TFBSs) on genomic DNA is of crucial importance for understanding and predicting regulatory elements in gene networks. TFBS motifs are commonly described by Position Weight Matrices (PWMs), in which each DNA base pair contributes independently to the transcription factor (TF) binding. However, this description ignores correlations between nucleotides at different positions, and is generally inaccurate: analysing fly and mouse in vivo ChIPseq data, we show that in most cases the PWM model fails to reproduce the observed statistics of TFBSs. To overcome this issue, we introduce the pairwise interaction model (PIM), a generalization of the PWM model. The model is based on the principle of maximum entropy and explicitly describes pairwise correlations between nucleotides at different positions, while being otherwise as unconstrained as possible. It is mathematically equivalent to considering a TF-DNA binding energy that depends additively on each nucleotide identity at all positions in the TFBS, like the PWM model, but also additively on pairs of nucleotides. We find that the PIM significantly improves over the PWM model, and even provides an optimal description of TFBS statistics within statistical noise. The PIM generalizes previous approaches to interdependent positions: it accounts for co-variation of two or more base pairs, and predicts secondary motifs, while outperforming multiple-motif models consisting of mixtures of PWMs. We analyse the structure of pairwise interactions between nucleotides, and find that they are sparse and dominantly located between consecutive base pairs in the flanking region of TFBS. Nonetheless, interactions between pairs of non-consecutive nucleotides are found to play a significant role in the obtained accurate description of TFBS statistics. The PIM is computationally tractable, and provides a general framework that should be useful for describing and predicting TFBSs beyond PWMs.

Published

2014

36. Imogene: identification of motifs and cis-regulatory modules underlying gene co-regulation.

Author

Rouault H, Santolini M, Schweisguth F, and Hakim V

Subjects

Algorithms, Animals, Binding Sites, Data Interpretation, Statistical, Drosophila genetics, Gene Expression Regulation, Developmental, Humans, Mice, Nucleotide Motifs, Rats, Transcription Factors metabolism, Gene Expression Regulation, Regulatory Elements, Transcriptional, Software

Abstract

Cis-regulatory modules (CRMs) and motifs play a central role in tissue and condition-specific gene expression. Here we present Imogene, an ensemble of statistical tools that we have developed to facilitate their identification and implemented in a publicly available software. Starting from a small training set of mammalian or fly CRMs that drive similar gene expression profiles, Imogene determines de novo cis-regulatory motifs that underlie this co-expression. It can then predict on a genome-wide scale other CRMs with a regulatory potential similar to the training set. Imogene bypasses the need of large datasets for statistical analyses by making central use of the information provided by the sequenced genomes of multiple species, based on the developed statistical tools and explicit models for transcription factor binding site evolution. We test Imogene on characterized tissue-specific mouse developmental CRMs. Its ability to identify CRMs with the same specificity based on its de novo created motifs is comparable to that of previously evaluated 'motif-blind' methods. We further show, both in flies and in mammals, that Imogene de novo generated motifs are sufficient to discriminate CRMs related to different developmental programs. Notably, purely relying on sequence data, Imogene performs as well in this discrimination task as a previously reported learning algorithm based on Chromatin Immunoprecipitation (ChIP) data for multiple transcription factors at multiple developmental stages., (© The Author(s) 2014. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published

2014

37. Six homeoproteins and a Iinc-RNA at the fast MYH locus lock fast myofiber terminal phenotype.

Author

Sakakibara I, Santolini M, Ferry A, Hakim V, and Maire P

Subjects

Animals, Cloning, Molecular, Enhancer Elements, Genetic, Extracellular Matrix Proteins genetics, Gene Expression Regulation, Developmental, Homeodomain Proteins metabolism, Mice, Knockout, Muscle, Skeletal growth & development, Protein-Lysine 6-Oxidase genetics, Homeodomain Proteins genetics, Muscle Contraction genetics, Myosin Heavy Chains genetics, RNA, Long Noncoding genetics

Abstract

Thousands of long intergenic non-coding RNAs (lincRNAs) are encoded by the mammalian genome. However, the function of most of these lincRNAs has not been identified in vivo. Here, we demonstrate a role for a novel lincRNA, linc-MYH, in adult fast-type myofiber specialization. Fast myosin heavy chain (MYH) genes and linc-MYH share a common enhancer, located in the fast MYH gene locus and regulated by Six1 homeoproteins. linc-MYH in nuclei of fast-type myofibers prevents slow-type and enhances fast-type gene expression. Functional fast-sarcomeric unit formation is achieved by the coordinate expression of fast MYHs and linc-MYH, under the control of a common Six-bound enhancer.

Published

2014

38. Genome-wide analyses of Shavenbaby target genes reveals distinct features of enhancer organization.

Author

Menoret D, Santolini M, Fernandes I, Spokony R, Zanet J, Gonzalez I, Latapie Y, Ferrer P, Rouault H, White KP, Besse P, Hakim V, Aerts S, Payre F, and Plaza S

Subjects

Animals, Binding Sites, Computational Biology, DNA-Binding Proteins metabolism, Drosophila Proteins metabolism, Drosophila melanogaster growth & development, Drosophila melanogaster metabolism, Embryo, Nonmammalian, Molecular Sequence Annotation, Molecular Sequence Data, Nucleotide Motifs, Protein Binding, Transcription Factors metabolism, Trichomes growth & development, Trichomes metabolism, DNA-Binding Proteins genetics, Drosophila Proteins genetics, Drosophila melanogaster genetics, Enhancer Elements, Genetic, Gene Expression Regulation, Developmental, Genome, Transcription Factors genetics, Trichomes genetics

Abstract

Background: Developmental programs are implemented by regulatory interactions between Transcription Factors (TFs) and their target genes, which remain poorly understood. While recent studies have focused on regulatory cascades of TFs that govern early development, little is known about how the ultimate effectors of cell differentiation are selected and controlled. We addressed this question during late Drosophila embryogenesis, when the finely tuned expression of the TF Ovo/Shavenbaby (Svb) triggers the morphological differentiation of epidermal trichomes., Results: We defined a sizeable set of genes downstream of Svb and used in vivo assays to delineate 14 enhancers driving their specific expression in trichome cells. Coupling computational modeling to functional dissection, we investigated the regulatory logic of these enhancers. Extending the repertoire of epidermal effectors using genome-wide approaches showed that the regulatory models learned from this first sample are representative of the whole set of trichome enhancers. These enhancers harbor remarkable features with respect to their functional architectures, including a weak or non-existent clustering of Svb binding sites. The in vivo function of each site relies on its intimate context, notably the flanking nucleotides. Two additional cis-regulatory motifs, present in a broad diversity of composition and positioning among trichome enhancers, critically contribute to enhancer activity., Conclusions: Our results show that Svb directly regulates a large set of terminal effectors of the remodeling of epidermal cells. Further, these data reveal that trichome formation is underpinned by unexpectedly diverse modes of regulation, providing fresh insights into the functional architecture of enhancers governing a terminal differentiation program.

Published

2013

39. Six homeoproteins directly activate Myod expression in the gene regulatory networks that control early myogenesis.

Author

Relaix F, Demignon J, Laclef C, Pujol J, Santolini M, Niro C, Lagha M, Rocancourt D, Buckingham M, and Maire P

Subjects

Animals, Gene Regulatory Networks, Transcription Factors genetics, Homeodomain Proteins genetics, Muscle Development

Abstract

In mammals, several genetic pathways have been characterized that govern engagement of multipotent embryonic progenitors into the myogenic program through the control of the key myogenic regulatory gene Myod. Here we demonstrate the involvement of Six homeoproteins. We first targeted into a Pax3 allele a sequence encoding a negative form of Six4 that binds DNA but cannot interact with essential Eya co-factors. The resulting embryos present hypoplasic skeletal muscles and impaired Myod activation in the trunk in the absence of Myf5/Mrf4. At the axial level, we further show that Myod is still expressed in compound Six1/Six4:Pax3 but not in Six1/Six4:Myf5 triple mutant embryos, demonstrating that Six1/4 participates in the Pax3-Myod genetic pathway. Myod expression and head myogenesis is preserved in Six1/Six4:Myf5 triple mutant embryos, illustrating that upstream regulators of Myod in different embryonic territories are distinct. We show that Myod regulatory regions are directly controlled by Six proteins and that, in the absence of Six1 and Six4, Six2 can compensate., Competing Interests: The authors have declared that no competing interests exist.

Published

2013

40. Epidemiology of HBV and HDV infections in a rural area of Central African Republic.

Author

Crovari P, Santolini M, Bandettini R, Bonanni P, Branca P, and Coppola RC

Subjects

Adolescent, Adult, Age Factors, Central African Republic epidemiology, Female, Hepatitis B complications, Hepatitis B Antibodies blood, Hepatitis B Surface Antigens blood, Hepatitis D complications, Humans, Immunoglobulin M analysis, Male, Middle Aged, Prevalence, Hepatitis B epidemiology, Hepatitis D epidemiology, Rural Population

Published

1991

41. [Ulcerative colitis and Crohn's disease of the colon. Diagnostic validity of the various disciplines].

Author

Berti Riboli E, Reboa G, Terrizzi A, Aste H, Lapertosa G, and Santolini ME

Subjects

Humans, Methods, Colitis, Ulcerative diagnosis, Colonic Diseases diagnosis, Crohn Disease diagnosis

Published

1978

42. [Cooking meat in microwave ovens does not cause formation of mutagenic substances].

Author

Sirtori C, Paganuzzi M, Lombardo C, Ruzzon T, Santolini M, Dutto P, Lapide M, and Chiola S

Subjects

Animals, Cattle, Cooking, Food Handling, Meat radiation effects, Microwaves, Mutagens biosynthesis

Abstract

Unlabelled: During the cooking process of meat, mutagenic and/or carcinogenic substances can be formed that can induce tumours of the gastro-intestinal tract or of other organs in the rat. The formation of these substances is proportionate to the cooking time, the cooking surface and the quantity of fats contained in meat. A comparison is made between beef cooked on a grid where the temperature reaches 200 degrees C, and cooked in a microwave oven (Cuocorapido Candy 500 CL, frequency 2450 Mhz) where the temperature does not exceed 100 degrees C. Mutagenic substances were extracted by the Commoner technique and mutagenic activity was assayed with the Ames test., Results: no mutagenic activity was demonstrated in the extracts of meat cooked in microwave ovens, while mutagenic activity was clearly demonstrated in the extracts of meat cooked on a grid.

Published

1983

43. 'Nonsecretory' multiple myeloma. Report of a case.

Author

Indiveri F, Barabino A, Santolini ME, and Santolini B

Subjects

Bence Jones Protein biosynthesis, Bone Marrow Examination, Female, Humans, Immunoelectrophoresis, Melphalan therapeutic use, Multiple Myeloma diagnostic imaging, Multiple Myeloma metabolism, Plasmacytoma diagnosis, Plasmacytoma drug therapy, Radiography, Ribs pathology, Skull diagnostic imaging, Multiple Myeloma immunology, Myeloma Proteins biosynthesis

Published

1974