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14. Interleukin-7 signaling

Author

M Milacic

Subjects
Cell signaling, Hes3 signaling axis, Interleukin, General Medicine, Biology, Suppressor of cytokine signalling, Cell biology
Published
2016
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16. Exploiting Conjugate Symmetry of the Short-Time Fourier Spectrum for Speech Enhancement

Author

James Lyons, Kamil Wojcicki, M. Milacic, Anthony Phillip Stark, and Kuldip K. Paliwal

Subjects
Signal processing, Applied Mathematics, Speech recognition, Spectrum (functional analysis), Speech synthesis, computer.software_genre, Background noise, Speech enhancement, symbols.namesake, Fourier transform, Computer Science::Sound, Phase spectrum, Signal Processing, symbols, Spectrogram, Electrical and Electronic Engineering, computer, Mathematics
Abstract

Typical speech enhancement algorithms operate on the short-time magnitude spectrum, while keeping the short-time phase spectrum unchanged for synthesis. We propose a novel approach where the noisy magnitude spectrum is recombined with a changed phase spectrum to produce a modified complex spectrum. During synthesis, the low energy components of the modified complex spectrum cancel out more than the high energy components, thus reducing background noise. Using objective speech quality measures, informal subjective listening tests and spectrogram analysis, we show that the proposed method results in improved speech quality.

Published
2008
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18. A Longitudinal Control Concept For Merging Of Automated Vehicles

Author

Chang Yang, M. Milacic, and K. Kurami

Subjects
Engineering, Radar tracker, Control algorithm, Automatic control, business.industry, Control system, Control engineering, Remotely operated underwater vehicle, business, Merge (version control)
Abstract

This paper is a feasibility study of an automatic traffic merging concept for potential application to Intelligent Vehicle Highway Systems (IVHS). The authors consider a freeway entrance where on-ramp vehicles are to merge into the highway traffic by actively tracking their designated gaps. A longitudinal control system based on homing guidance is proposed and analyzed. The effectiveness of the guidance and control algorithms has been tested through computer simulations. One important feature of this method is that the controller of an on- ramp vehicle utilizes mostly the relative positional information between the vehicle and its target tap. As such infrastructure support could be minimized.

Published
2005
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19. [Value of the association of normovolemic dilution and hyperbaric oxygenation in the treatment of sudden deafness. A retrospective study]

Author

O, Zennaro, R, Dauman, A, Poisot, D, Esteben, J Y, Duclose, B, Bertrand, A M, Cros, M, Milacic, and J P, Bebear

Subjects
Adult, Male, Hemodilution, Hyperbaric Oxygenation, Adolescent, Vasodilator Agents, Hearing Loss, Sudden, Middle Aged, Prognosis, Audiometry, Vertigo, Humans, Female, Aged, Retrospective Studies
Abstract

The multiple treatments of sudden deafness shows how this pathology still remains quite unknown. The authors present a retrospective study of 87 patients treated by normovolemic hemodilution associated to hyperbaric oxygenation. They obtain a total à 60% of significant recovery (ratio between hearing gain and initial hearing loss, above 25%) and in severe hearing loss (threshold between 70 and 90 dB) 60% of good results (ratio above 50%). The importance of the initial form of audiogram and the presence of dizziness as prognostic factors is not confirmed. On the other hand, the evolution of tinnitus is correlated with the deafness and it is a supplementary means to evaluate the therapeutic efficiency. Moreover the persistence of tinnitus represents an important after effect. Sudden deafness still remains a medical emergency and the delay for carrying out any treatment should be as short as possible. On the other hand it is possible to reduce hospital stay by two sessions of hyperbaric oxygenation per day.

Published
1993

20. [Sudden deafness: a randomized comparative study of 2 administration modalities of hyperbaric oxygenotherapy combined with naftidrofuryl]

Author

R, Dauman, D, Poisot, A M, Cros, O, Zennaro, B, Bertrand, J Y, Duclos, D, Esteben, M, Milacic, C, Boudey, and J P, Bébéar

Subjects
Adult, Hemodilution, Hyperbaric Oxygenation, Audiometry, Clinical Protocols, Humans, Nafronyl, Hearing Loss, Sudden, Middle Aged
Abstract

Hyperbaric oxygen therapy is one of the numerous therapies which have been proposed in the management of sudden deafness. It is presumptuous to claim the efficiency of any treatment in a pathology where both the origin and the actual rate of spontaneous recovery are unknown. The grounds of therapies are therefore empirical but the need of urgent therapy is dictated by ethics. This study compares the effects of hyperbaric oxygen therapy in two groups of patients; according ot their order in randomization the subjects were treated either at a rate of 1 session or 2 sessions per day. Hyperbaric oxygen therapy was associated with infusion of Naftidrofuryl to counteract the vasoconstrictive effect of increased oxygen pressure in blood. Steroids were also administered simultaneously to avoid, for the same reasons, cerebral oedema. Normovolemic hemodilution (Dauman et al. 1983) was systemically performed in all the patients preliminarily to hyperbaric oxygen therapy, in order to reduce the haematocrit and thus facilitate blood supply. The efficiency and the side effects were similar in the two groups, provided that some principles in the selection and the monitoring of the patients were respected. The rate of 2 sessions of hyperbaric oxygen therapy per day has obvious advantages in view of health policy, but it requires the hospitalization of the patient and should be restricted to the younger subjects.

Published
1993

24. [Normovolemic hemodilution in the treatment of sudden deafness]

Author

A M, Cros, R, Dauman, D, Esteben, M, Milacic, D, Dogimont, and C, Boudey

Subjects
Adult, Male, Hemodilution, Hematocrit, Humans, Female, Hearing Loss, Sudden, Middle Aged, Hearing Loss, Aged
Abstract

After the apparition of a sudden deafness, 45 patients (22 men and 23 women, with a mean age of 44 +/- 14.9 years) were treated with normovolaemic haemodilution performed with dextran 60. They were placed into 4 groups depending on their hearing loss: total loss: 10 cases; severe loss: 90 to 70 db. 13 cases; moderates loss: 65 to 40 db, 14 cases, slight loss: less than or equal to 35 db, 8 cases. The mean time between the onset of the hearing loss and treatment was 9.3 +/- 12.4 days. The initial mean haematocrit was 44.8 +/- 3.8% and mean haematocrit after haemodilution was 33.1 +/- 2.8%. For 51% of the patients, an almost total recovery was obtained. In 15.5% of cases, recovery was between 25 to 50% of the hearing loss, and in 33.3% of the patients recovery was negligible. We did not find any relationship between hearing recovery and initial haematocrit. The best results were obtained in the group of patients treated early. Hearing gain was significatively better if delay in starting treatment was less than 7 days. There was a relationship between the initial hearing loss and the final recuperation. These results suggested that haemodilution increased labyrinth microcirculation and oxygenation of the cochlear sensory cells, reversing the ischaemic insult to these cells.

Published
1986

26. A Comparative Occlusal and Cephalometric Study of Dental and Skeletal Anteroposterior Relationships

Author

M. Milacic and M. Markovic

Subjects
Male, Cephalometry, business.industry, Dentistry, General Medicine, Facial Bones, Models, Dental, stomatognathic diseases, Jaw Relation Record, Child, Preschool, Humans, Medicine, Female, Child, business, Tooth, Malocclusion
Abstract

Anteroposterior dental relationships (Class I, II or III) were assessed from study plaster models and skeletal relationships were determined on the basis of the ANB angle of 585 orthodontic patients. It was found that there was no agreement between dental and skeletal anteroposterior relationships in about 25 per cent of the cases investigated.

Published
1983
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27. The Reactome Pathway Knowledgebase 2024.

Author

Milacic M, Beavers D, Conley P, Gong C, Gillespie M, Griss J, Haw R, Jassal B, Matthews L, May B, Petryszak R, Ragueneau E, Rothfels K, Sevilla C, Shamovsky V, Stephan R, Tiwari K, Varusai T, Weiser J, Wright A, Wu G, Stein L, Hermjakob H, and D'Eustachio P

Subjects
Humans, Proteome genetics, Knowledge Bases, Metabolic Networks and Pathways genetics, Signal Transduction
Abstract

The Reactome Knowledgebase (https://reactome.org), an Elixir and GCBR core biological data resource, provides manually curated molecular details of a broad range of normal and disease-related biological processes. Processes are annotated as an ordered network of molecular transformations in a single consistent data model. Reactome thus functions both as a digital archive of manually curated human biological processes and as a tool for discovering functional relationships in data such as gene expression profiles or somatic mutation catalogs from tumor cells. Here we review progress towards annotation of the entire human proteome, targeted annotation of disease-causing genetic variants of proteins and of small-molecule drugs in a pathway context, and towards supporting explicit annotation of cell- and tissue-specific pathways. Finally, we briefly discuss issues involved in making Reactome more fully interoperable with other related resources such as the Gene Ontology and maintaining the resulting community resource network., (© The Author(s) 2023. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published
2024
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28. Using the Reactome Database.

Author

Rothfels K, Milacic M, Matthews L, Haw R, Sevilla C, Gillespie M, Stephan R, Gong C, Ragueneau E, May B, Shamovsky V, Wright A, Weiser J, Beavers D, Conley P, Tiwari K, Jassal B, Griss J, Senff-Ribeiro A, Brunson T, Petryszak R, Hermjakob H, D'Eustachio P, Wu G, and Stein L

Subjects
Humans, Animals, Mice, Rats, Databases, Protein, Proteins metabolism, Signal Transduction, Metabolic Networks and Pathways, Zebrafish metabolism
Abstract

Pathway databases provide descriptions of the roles of proteins, nucleic acids, lipids, carbohydrates, and other molecular entities within their biological cellular contexts. Pathway-centric views of these roles may allow for the discovery of unexpected functional relationships in data such as gene expression profiles and somatic mutation catalogues from tumor cells. For this reason, there is a high demand for high-quality pathway databases and their associated tools. The Reactome project (a collaboration between the Ontario Institute for Cancer Research, New York University Langone Health, the European Bioinformatics Institute, and Oregon Health & Science University) is one such pathway database. Reactome collects detailed information on biological pathways and processes in humans from the primary literature. Reactome content is manually curated, expert-authored, and peer-reviewed and spans the gamut from simple intermediate metabolism to signaling pathways and complex cellular events. This information is supplemented with likely orthologous molecular reactions in mouse, rat, zebrafish, worm, and other model organisms. © 2023 The Authors. Current Protocols published by Wiley Periodicals LLC. Basic Protocol 1: Browsing a Reactome pathway Basic Protocol 2: Exploring Reactome annotations of disease and drugs Basic Protocol 3: Finding the pathways involving a gene or protein Alternate Protocol 1: Finding the pathways involving a gene or protein using UniProtKB (SwissProt), Ensembl, or Entrez gene identifier Alternate Protocol 2: Using advanced search Basic Protocol 4: Using the Reactome pathway analysis tool to identify statistically overrepresented pathways Basic Protocol 5: Using the Reactome pathway analysis tool to overlay expression data onto Reactome pathway diagrams Basic Protocol 6: Comparing inferred model organism and human pathways using the Species Comparison tool Basic Protocol 7: Comparing tissue-specific expression using the Tissue Distribution tool., (© 2023 The Authors. Current Protocols published by Wiley Periodicals LLC.)

Published
2023
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29. The reactome pathway knowledgebase 2022.

Author

Gillespie M, Jassal B, Stephan R, Milacic M, Rothfels K, Senff-Ribeiro A, Griss J, Sevilla C, Matthews L, Gong C, Deng C, Varusai T, Ragueneau E, Haider Y, May B, Shamovsky V, Weiser J, Brunson T, Sanati N, Beckman L, Shao X, Fabregat A, Sidiropoulos K, Murillo J, Viteri G, Cook J, Shorser S, Bader G, Demir E, Sander C, Haw R, Wu G, Stein L, Hermjakob H, and D'Eustachio P

Subjects
COVID-19 metabolism, Data Curation, Genome, Human, Host-Pathogen Interactions, Humans, Proteins genetics, Signal Transduction, Software, Antiviral Agents pharmacology, Knowledge Bases, Proteins metabolism
Abstract

The Reactome Knowledgebase (https://reactome.org), an Elixir core resource, provides manually curated molecular details across a broad range of physiological and pathological biological processes in humans, including both hereditary and acquired disease processes. The processes are annotated as an ordered network of molecular transformations in a single consistent data model. Reactome thus functions both as a digital archive of manually curated human biological processes and as a tool for discovering functional relationships in data such as gene expression profiles or somatic mutation catalogs from tumor cells. Recent curation work has expanded our annotations of normal and disease-associated signaling processes and of the drugs that target them, in particular infections caused by the SARS-CoV-1 and SARS-CoV-2 coronaviruses and the host response to infection. New tools support better simultaneous analysis of high-throughput data from multiple sources and the placement of understudied ('dark') proteins from analyzed datasets in the context of Reactome's manually curated pathways., (© The Author(s) 2021. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published
2022
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30. The reactome pathway knowledgebase.

Author

Jassal B, Matthews L, Viteri G, Gong C, Lorente P, Fabregat A, Sidiropoulos K, Cook J, Gillespie M, Haw R, Loney F, May B, Milacic M, Rothfels K, Sevilla C, Shamovsky V, Shorser S, Varusai T, Weiser J, Wu G, Stein L, Hermjakob H, and D'Eustachio P

Subjects
Genome, Human, Humans, Metabolic Networks and Pathways, Protein Interaction Maps, Signal Transduction, Databases, Chemical, Databases, Pharmaceutical, Knowledge Bases, Software
Abstract

The Reactome Knowledgebase (https://reactome.org) provides molecular details of signal transduction, transport, DNA replication, metabolism and other cellular processes as an ordered network of molecular transformations in a single consistent data model, an extended version of a classic metabolic map. Reactome functions both as an archive of biological processes and as a tool for discovering functional relationships in data such as gene expression profiles or somatic mutation catalogs from tumor cells. To extend our ability to annotate human disease processes, we have implemented a new drug class and have used it initially to annotate drugs relevant to cardiovascular disease. Our annotation model depends on external domain experts to identify new areas for annotation and to review new content. New web pages facilitate recruitment of community experts and allow those who have contributed to Reactome to identify their contributions and link them to their ORCID records. To improve visualization of our content, we have implemented a new tool to automatically lay out the components of individual reactions with multiple options for downloading the reaction diagrams and associated data, and a new display of our event hierarchy that will facilitate visual interpretation of pathway analysis results., (© The Author(s) 2019. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published
2020
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31. Reactome and ORCID-fine-grained credit attribution for community curation.

Author

Viteri G, Matthews L, Varusai T, Gillespie M, Milacic M, Cook J, Weiser J, Shorser S, Sidiropoulos K, Fabregat A, Haw R, Wu G, Stein L, D'Eustachio P, and Hermjakob H

Subjects
User-Computer Interface, Data Curation, Signal Transduction
Abstract

Reactome is a manually curated, open-source, open-data knowledge base of biomolecular pathways. Reactome has always provided clear credit attribution for authors, curators and reviewers through fine-grained annotation of all three roles at the reaction and pathway level. These data are visible in the web interface and provided through the various data download formats. To enhance visibility and credit attribution for the work of authors, curators and reviewers, and to provide additional opportunities for Reactome community engagement, we have implemented key changes to Reactome: contributor names are now fully searchable in the web interface, and contributors can 'claim' their contributions to their ORCID profile with a few clicks. In addition, we are reaching out to domain experts to request their help in reviewing and editing Reactome pathways through a new 'Contribution' section, highlighting pathways which are awaiting community review. Database URL: https://reactome.org., (© The Author(s) 2019. Published by Oxford University Press.)

Published
2019
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32. The Reactome Pathway Knowledgebase.

Author

Fabregat A, Jupe S, Matthews L, Sidiropoulos K, Gillespie M, Garapati P, Haw R, Jassal B, Korninger F, May B, Milacic M, Roca CD, Rothfels K, Sevilla C, Shamovsky V, Shorser S, Varusai T, Viteri G, Weiser J, Wu G, Stein L, Hermjakob H, and D'Eustachio P

Subjects
Computer Graphics, Databases, Chemical, Databases, Protein, Humans, Internet, Molecular Sequence Annotation, Signal Transduction, User-Computer Interface, Knowledge Bases, Metabolic Networks and Pathways
Abstract

The Reactome Knowledgebase (https://reactome.org) provides molecular details of signal transduction, transport, DNA replication, metabolism, and other cellular processes as an ordered network of molecular transformations-an extended version of a classic metabolic map, in a single consistent data model. Reactome functions both as an archive of biological processes and as a tool for discovering unexpected functional relationships in data such as gene expression profiles or somatic mutation catalogues from tumor cells. To support the continued brisk growth in the size and complexity of Reactome, we have implemented a graph database, improved performance of data analysis tools, and designed new data structures and strategies to boost diagram viewer performance. To make our website more accessible to human users, we have improved pathway display and navigation by implementing interactive Enhanced High Level Diagrams (EHLDs) with an associated icon library, and subpathway highlighting and zooming, in a simplified and reorganized web site with adaptive design. To encourage re-use of our content, we have enabled export of pathway diagrams as 'PowerPoint' files., (© The Author(s) 2017. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published
2018
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33. Overview of the interactive task in BioCreative V.

Author

Wang Q, S Abdul S, Almeida L, Ananiadou S, Balderas-Martínez YI, Batista-Navarro R, Campos D, Chilton L, Chou HJ, Contreras G, Cooper L, Dai HJ, Ferrell B, Fluck J, Gama-Castro S, George N, Gkoutos G, Irin AK, Jensen LJ, Jimenez S, Jue TR, Keseler I, Madan S, Matos S, McQuilton P, Milacic M, Mort M, Natarajan J, Pafilis E, Pereira E, Rao S, Rinaldi F, Rothfels K, Salgado D, Silva RM, Singh O, Stefancsik R, Su CH, Subramani S, Tadepally HD, Tsaprouni L, Vasilevsky N, Wang X, Chatr-Aryamontri A, Laulederkind SJ, Matis-Mitchell S, McEntyre J, Orchard S, Pundir S, Rodriguez-Esteban R, Van Auken K, Lu Z, Schaeffer M, Wu CH, Hirschman L, and Arighi CN

Subjects
Data Curation methods, Data Mining methods, Electronic Data Processing methods
Abstract

Fully automated text mining (TM) systems promote efficient literature searching, retrieval, and review but are not sufficient to produce ready-to-consume curated documents. These systems are not meant to replace biocurators, but instead to assist them in one or more literature curation steps. To do so, the user interface is an important aspect that needs to be considered for tool adoption. The BioCreative Interactive task (IAT) is a track designed for exploring user-system interactions, promoting development of useful TM tools, and providing a communication channel between the biocuration and the TM communities. In BioCreative V, the IAT track followed a format similar to previous interactive tracks, where the utility and usability of TM tools, as well as the generation of use cases, have been the focal points. The proposed curation tasks are user-centric and formally evaluated by biocurators. In BioCreative V IAT, seven TM systems and 43 biocurators participated. Two levels of user participation were offered to broaden curator involvement and obtain more feedback on usability aspects. The full level participation involved training on the system, curation of a set of documents with and without TM assistance, tracking of time-on-task, and completion of a user survey. The partial level participation was designed to focus on usability aspects of the interface and not the performance per se In this case, biocurators navigated the system by performing pre-designed tasks and then were asked whether they were able to achieve the task and the level of difficulty in completing the task. In this manuscript, we describe the development of the interactive task, from planning to execution and discuss major findings for the systems tested.Database URL: http://www.biocreative.org., (Published by Oxford University Press 2016. This work is written by US Government employees and is in the public domain in the US.)

Published
2016
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34. MET network in PubMed: a text-mined network visualization and curation system.

Author

Dai HJ, Su CH, Lai PT, Huang MS, Jonnagaddala J, Rose Jue T, Rao S, Chou HJ, Milacic M, Singh O, Syed-Abdul S, and Hsu WL

Subjects
Data Curation, User-Computer Interface, Computational Biology methods, Data Mining methods, PubMed, Software
Abstract

Metastasis is the dissemination of a cancer/tumor from one organ to another, and it is the most dangerous stage during cancer progression, causing more than 90% of cancer deaths. Improving the understanding of the complicated cellular mechanisms underlying metastasis requires investigations of the signaling pathways. To this end, we developed a METastasis (MET) network visualization and curation tool to assist metastasis researchers retrieve network information of interest while browsing through the large volume of studies in PubMed. MET can recognize relations among genes, cancers, tissues and organs of metastasis mentioned in the literature through text-mining techniques, and then produce a visualization of all mined relations in a metastasis network. To facilitate the curation process, MET is developed as a browser extension that allows curators to review and edit concepts and relations related to metastasis directly in PubMed. PubMed users can also view the metastatic networks integrated from the large collection of research papers directly through MET. For the BioCreative 2015 interactive track (IAT), a curation task was proposed to curate metastatic networks among PubMed abstracts. Six curators participated in the proposed task and a post-IAT task, curating 963 unique metastatic relations from 174 PubMed abstracts using MET.Database URL: http://btm.tmu.edu.tw/metastasisway., (© The Author(s) 2016. Published by Oxford University Press.)

Published
2016
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35. The Reactome pathway Knowledgebase.

Author

Fabregat A, Sidiropoulos K, Garapati P, Gillespie M, Hausmann K, Haw R, Jassal B, Jupe S, Korninger F, McKay S, Matthews L, May B, Milacic M, Rothfels K, Shamovsky V, Webber M, Weiser J, Williams M, Wu G, Stein L, Hermjakob H, and D'Eustachio P

Subjects
Gene Expression, Humans, Knowledge Bases, Proteins metabolism, Signal Transduction, Software, Databases, Chemical, Metabolic Networks and Pathways
Abstract

The Reactome Knowledgebase (www.reactome.org) provides molecular details of signal transduction, transport, DNA replication, metabolism and other cellular processes as an ordered network of molecular transformations-an extended version of a classic metabolic map, in a single consistent data model. Reactome functions both as an archive of biological processes and as a tool for discovering unexpected functional relationships in data such as gene expression pattern surveys or somatic mutation catalogues from tumour cells. Over the last two years we redeveloped major components of the Reactome web interface to improve usability, responsiveness and data visualization. A new pathway diagram viewer provides a faster, clearer interface and smooth zooming from the entire reaction network to the details of individual reactions. Tool performance for analysis of user datasets has been substantially improved, now generating detailed results for genome-wide expression datasets within seconds. The analysis module can now be accessed through a RESTFul interface, facilitating its inclusion in third party applications. A new overview module allows the visualization of analysis results on a genome-wide Reactome pathway hierarchy using a single screen page. The search interface now provides auto-completion as well as a faceted search to narrow result lists efficiently., (© The Author(s) 2015. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published
2016
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36. The Reactome pathway knowledgebase.

Author

Croft D, Mundo AF, Haw R, Milacic M, Weiser J, Wu G, Caudy M, Garapati P, Gillespie M, Kamdar MR, Jassal B, Jupe S, Matthews L, May B, Palatnik S, Rothfels K, Shamovsky V, Song H, Williams M, Birney E, Hermjakob H, Stein L, and D'Eustachio P

Subjects
Disease, Humans, Internet, Knowledge Bases, Metabolic Networks and Pathways, Databases, Protein, Proteins metabolism
Abstract

Reactome (http://www.reactome.org) is a manually curated open-source open-data resource of human pathways and reactions. The current version 46 describes 7088 human proteins (34% of the predicted human proteome), participating in 6744 reactions based on data extracted from 15 107 research publications with PubMed links. The Reactome Web site and analysis tool set have been completely redesigned to increase speed, flexibility and user friendliness. The data model has been extended to support annotation of disease processes due to infectious agents and to mutation.

Published
2014
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37. Annotating cancer variants and anti-cancer therapeutics in reactome.

Author

Milacic M, Haw R, Rothfels K, Wu G, Croft D, Hermjakob H, D'Eustachio P, and Stein L

Abstract

Reactome describes biological pathways as chemical reactions that closely mirror the actual physical interactions that occur in the cell. Recent extensions of our data model accommodate the annotation of cancer and other disease processes. First, we have extended our class of protein modifications to accommodate annotation of changes in amino acid sequence and the formation of fusion proteins to describe the proteins involved in disease processes. Second, we have added a disease attribute to reaction, pathway, and physical entity classes that uses disease ontology terms. To support the graphical representation of "cancer" pathways, we have adapted our Pathway Browser to display disease variants and events in a way that allows comparison with the wild type pathway, and shows connections between perturbations in cancer and other biological pathways. The curation of pathways associated with cancer, coupled with our efforts to create other disease-specific pathways, will interoperate with our existing pathway and network analysis tools. Using the Epidermal Growth Factor Receptor (EGFR) signaling pathway as an example, we show how Reactome annotates and presents the altered biological behavior of EGFR variants due to their altered kinase and ligand-binding properties, and the mode of action and specificity of anti-cancer therapeutics.

Published
2012
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38. [Value of the association of normovolemic dilution and hyperbaric oxygenation in the treatment of sudden deafness. A retrospective study].

Author

Zennaro O, Dauman R, Poisot A, Esteben D, Duclose JY, Bertrand B, Cros AM, Milacic M, and Bebear JP

Subjects
Adolescent, Adult, Aged, Audiometry, Female, Hearing Loss, Sudden complications, Humans, Male, Middle Aged, Prognosis, Retrospective Studies, Vasodilator Agents therapeutic use, Vertigo etiology, Hearing Loss, Sudden therapy, Hemodilution methods, Hyperbaric Oxygenation
Abstract

The multiple treatments of sudden deafness shows how this pathology still remains quite unknown. The authors present a retrospective study of 87 patients treated by normovolemic hemodilution associated to hyperbaric oxygenation. They obtain a total à 60% of significant recovery (ratio between hearing gain and initial hearing loss, above 25%) and in severe hearing loss (threshold between 70 and 90 dB) 60% of good results (ratio above 50%). The importance of the initial form of audiogram and the presence of dizziness as prognostic factors is not confirmed. On the other hand, the evolution of tinnitus is correlated with the deafness and it is a supplementary means to evaluate the therapeutic efficiency. Moreover the persistence of tinnitus represents an important after effect. Sudden deafness still remains a medical emergency and the delay for carrying out any treatment should be as short as possible. On the other hand it is possible to reduce hospital stay by two sessions of hyperbaric oxygenation per day.

Published
1993

39. [Sudden deafness: a randomized comparative study of 2 administration modalities of hyperbaric oxygenotherapy combined with naftidrofuryl].

Author

Dauman R, Poisot D, Cros AM, Zennaro O, Bertrand B, Duclos JY, Esteben D, Milacic M, Boudey C, and Bébéar JP

Subjects
Adult, Audiometry, Clinical Protocols, Hemodilution methods, Humans, Middle Aged, Hearing Loss, Sudden therapy, Hyperbaric Oxygenation, Nafronyl therapeutic use
Abstract

Hyperbaric oxygen therapy is one of the numerous therapies which have been proposed in the management of sudden deafness. It is presumptuous to claim the efficiency of any treatment in a pathology where both the origin and the actual rate of spontaneous recovery are unknown. The grounds of therapies are therefore empirical but the need of urgent therapy is dictated by ethics. This study compares the effects of hyperbaric oxygen therapy in two groups of patients; according ot their order in randomization the subjects were treated either at a rate of 1 session or 2 sessions per day. Hyperbaric oxygen therapy was associated with infusion of Naftidrofuryl to counteract the vasoconstrictive effect of increased oxygen pressure in blood. Steroids were also administered simultaneously to avoid, for the same reasons, cerebral oedema. Normovolemic hemodilution (Dauman et al. 1983) was systemically performed in all the patients preliminarily to hyperbaric oxygen therapy, in order to reduce the haematocrit and thus facilitate blood supply. The efficiency and the side effects were similar in the two groups, provided that some principles in the selection and the monitoring of the patients were respected. The rate of 2 sessions of hyperbaric oxygen therapy per day has obvious advantages in view of health policy, but it requires the hospitalization of the patient and should be restricted to the younger subjects.

Published
1993

41. [Normovolemic hemodilution in the treatment of sudden deafness].

Author

Cros AM, Dauman R, Esteben D, Milacic M, Dogimont D, and Boudey C

Subjects
Adult, Aged, Female, Hearing Loss blood, Hearing Loss therapy, Hearing Loss, Sudden blood, Hematocrit, Humans, Male, Middle Aged, Hearing Loss, Sudden therapy, Hemodilution methods
Abstract

After the apparition of a sudden deafness, 45 patients (22 men and 23 women, with a mean age of 44 +/- 14.9 years) were treated with normovolaemic haemodilution performed with dextran 60. They were placed into 4 groups depending on their hearing loss: total loss: 10 cases; severe loss: 90 to 70 db. 13 cases; moderates loss: 65 to 40 db, 14 cases, slight loss: less than or equal to 35 db, 8 cases. The mean time between the onset of the hearing loss and treatment was 9.3 +/- 12.4 days. The initial mean haematocrit was 44.8 +/- 3.8% and mean haematocrit after haemodilution was 33.1 +/- 2.8%. For 51% of the patients, an almost total recovery was obtained. In 15.5% of cases, recovery was between 25 to 50% of the hearing loss, and in 33.3% of the patients recovery was negligible. We did not find any relationship between hearing recovery and initial haematocrit. The best results were obtained in the group of patients treated early. Hearing gain was significatively better if delay in starting treatment was less than 7 days. There was a relationship between the initial hearing loss and the final recuperation. These results suggested that haemodilution increased labyrinth microcirculation and oxygenation of the cochlear sensory cells, reversing the ischaemic insult to these cells.

Published
1986
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