1,721,016 research outputs found
Sequence-Selective Recognition of the d(GGCGCC)2 DNA Palindrome by Oligopeptide Derivatives of Mitoxantrone. Enabling for Simultaneous Targeting of the Two Guanine Bases Upstream from the Central Intercalation Site in Both Grooves and along Both Strands
No full textMolecular modelling of inhibitors of proteins involved in angiogenesis
No full textL’angiogenèse étant un processus limité dans des conditions physiologiques et un processus clé dans la croissance tumorale, elle est devenue une cible thérapeutique prometteuse. La neuropiline-1 (Np1) est un corécepteur du VEGF, qui est le facteur pro-angiogénique le mieux décrit jusqu’à présent. Dans cette thèse, nous nous intéressons à la modélisation du ligand 47, une molécule active expérimentalement, en vue de l’amarrer dans la neuropiline-1. En raison de sa flexibilité conformationnelle, ce ligand pourrait en effet adopter une conformation étendue, comme la tuftsine, un ligand naturel de Np1, ou une conformation repliée. Une étape préliminaire essentielle, avant l'exploration de la complexation du lig-47 a Np1, est l'étude de sa flexibilité conformationnelle. Il est en effet impératif de s'assurer que les interactions intra-moleculaires (conformationnelles) dans le lig-47 sont calculées a une precision comparable a celles de ses interactions intermoléculaires avec Np1. Un écueil important tient au caractère conjugue du lig-47. Les quatre fragments constitutifs de cette molecule sont tous aromatiques ou conjugues, et sont tous connectes par des atomes insaturés. [...] Nous avons, dans une première étape, construit la molécule en quatre fragments : le benzimidazole, le méthylbenzène, le benzodioxane et le carboxythiourée (CTU). Nous avons approché ces quatre fragments par une molécule d’eau afin de calibrer les rayons de Van de Waals effectifs impliqués dans les contributions d’énergies électrostatique et de répulsion. L’anisotropie ayant été assurée, nous avons cherché à reproduire la conjugaison, par la calibration des barrières de torsion V0 primaires (n=1) et binaires (n=2). Nous obtenons des accords très satisfaisants entre les courbes conformationnelles obtenues avec SIBFA et celles obtenues par des calculs de chimie quantique (QC). Nous avons ensuite effectué des minimisations de l'énergie SIBFA en partant des minima des six courbes conformationnelles. Afin d'évaluer la transférabilité de la méthode, nous avons comparé les stabilités relatives de ces minima par des calculs QC ponctuels. Or les différences d'énergie séparant le minimum « global » des minima locaux se sont avérées sous-estimées par rapport aux calculs QC. Ces résultats nous ont amenés à envisager des façons différentes de représenter le fragment CTU. La possibilité la plus évidente consiste à le séparer en deux sous-fragments amide et thioamide. Les effets de la conjugaison et de la transférabilite des multipôles et polarisabilités sont ainsi perdus mais pourraient être compensés par la prise en compte explicite de l’énergie de polarisation des fragments amide et thioamide. Avec cette approche, la recalibration des rayons effectifs a permis de préserver des accords convenables avec les calculs quantiques pour l'approche des atomes du CTU par une molécule d'eau sonde. Les courbes conformationnelles reproduisent de près les courbes QC avec une recalibration minimale. Les minima de ces courbes ont été a nouveau minimisés en SIBFA, conduisant a des structures néanmoins très proches des minima correspondants de l'approche précédente avec un CTU construit d'un seul tenant. Mais à présent, les différences d'énergie séparant le minimum global des minima locaux sont très voisine de celles trouvées en QC. De plus, l'évolution des courbes conformationnelles en fonction de la structure considérée s'est avérée régie par l'énergie de polarisation. Par ailleurs, nous avons obtenu des résultats satisfaisants lors de l’amarrage de la tuftsine dans Np1. Ces résultats s'avèrent suffisamment probants pour permettre d'envisager à présent une étude détaillée des modes d'interaction du lig-47 avec Np-1.Angiogenesis is a limited process in physiological conditions and a key process in tumor growth. Hence, it has become a promising therapeutic target. The neuropilin-1 (Np1) is a co-receptor for VEGF, which is today the best known pro-angiogenic factor. This manuscript deals with the molecular modelling of the ligand 47 (lig47), an experimentally active molecule, in order to dock it into Np1. Due to its conformational flexibility, this ligand could adopt and extended conformation such as tuftsin, a natural ligand, does in its complex with Np1, or a folded conformation. An essential preliminary step, before the exploration of the complexation of lig47 with Np1 is the study of its conformational flexibility. Indeed it must be ensured that the intramolecular (conformational) interactions are calculated with precision compared with the calculations of the interaction energies with Np1. An important issue comes from the polyconjugaison of the lig47. [...] We probed these four fragments with a water molecule in order to calibrate the effective Van der Waals radii implicated in electrostatic and repulsion contributions. Once the anisotropy was reproduced, we looked for reproducing the effect of the conjugaison on torsional barriers. We hence calibrated primary (n=1) and binary (n=2) barriers. We obtained very satisfactory agreements between the conformational curves obtained with SIBFA and those obtained with quantum chemistry (QC) calculations. Then we performed energy minimizations of SIBFA energy of the minima of the ix conformational curves. In order to evaluate the transferability of the method, we compared the relative stabilities of these minima with single-point QC calculations. But the differences of energy between the global minimum and local minima were underestimated in comparison with QC calculations. These results lead us to consider different ways of representing CTU. The more evident way consists in separating it in two fragments amide and thioamide. The effects of the conjugaison and the transferability of the multipoles and the polarisabilities are lost but could be compensated by the explicit consideration of the polarization energy between the amide and thioamide fragments. With this approach, the recalibration of the effective radii permitted to preserve good agreements with the QC calculations when probing the CTU by a water molecule. The conformational curves reproduce the QC curves after a minimal recalibration. The minima of these curves were then re-minimized with SIBFA, leading to structures close to those obtained with the first representation. But now, the differences of energy between the global minimum and the local minima are very close to those obtained in QC. Moreover, the evolution of the conformational curves as function of the number of the structure is ruled by the polarization energy. Otherwise, we obtained satisfactory results when we docked the tuftsin in Np1. These results will allow us to consider a detailed study of the interaction between lig47 et Np1
Rational design, synthesis, and DNA binding properties of novel sequence-selective peptidyl congeners of ametantrone
No full textNatural and synthetic compounds characterized by an anthraquinone nucleus represent an important class of anti-neoplastic agents, the mechanism of action of which is related to intercalation into DNA. Ametantrone (AM) is a synthetic 9,10-anthracenedione bearing two (hydroxyethylamino)ethylamino residues at positions 1 and 4; along with other anthraquinones and anthracyclines, it shares a polycyclic intercalating moiety and charged side chains that stabilize DNA binding. All these drugs elicit adverse side effects, which represent a challenge for antitumor chemotherapy. In the present work the structure of AM was augmented with appropriate groups that target well-defined base pairs in the major groove. These should endow AM with DNA sequence selectivity. We describe the rationale for the synthesis and the evaluation of activity of a new series of compounds in which the planar anthraquinone is conjugated at positions 1 and 4 through the side chains of AM or other bioisosteric linkers to appropriate dipeptides. The designed novel AM derivatives were shown to selectively stabilize two oligonucleotide duplexes that both have a palindromic GC-rich hexanucleotide core, but their stabilizing effects on a random DNA sequence was negligible. In the case of the most effective compound, the 1,4-bis-[Gly-(L-Lys)] derivative of AM, the experimental results confirm the predictions of earlier theoretical computations. In contrast, AM had equal stabilizing effects on all three sequences and showed no preferential binding. This novel peptide derivative can be classified as a strong binder regarding the sequences that it selectively targets, possibly opening the exploitation of less cytotoxic conjugates of AM to the targeted treatment of oncological and viral diseases
Going Beyond Counting First Authors in Author Co-citation Analysis
Full text linkThe present study examines one of the fundamental aspects of author co-citation analysis (ACA) - the way co-citation
counts are defined. Co-citation counting provides the data on which all subsequent statistical analyses and mappings
are based, and we compare ACA results based on two different types of co-citation counting - the traditional type that
only counts the first one among a cited work's authors on the one hand and a non-traditional type that takes into
account the first 5 authors of a cited work on the other hand. Results indicate that the picture produced through this non-traditional author co-citation counting contains more coherent author groups and is therefore considerably clearer. However, this picture represents fewer specialties in the research field being studied than that produced through the traditional first-author co-citation counting when the same number of top-ranked authors is selected and analyzed. Reasons for these effects are discussed
Study of inhibitors complexes with therapeutic properties : applications to metalloproteins involved in pathologies
No full textLes fonctions catalytiques de l'intégrase (IN) du Virus de l'Immunodéficience humaine (VIH-1) sont strictement nécessaires pour l'intégration du génome viral dans les cellules hôtes. Aujourd'hui, trois inhibiteurs anti-IN appartenant à la famille des dikétoacides sont utilisés en thérapie : le raltegravir, l'elvitegravir et le dolutegravir. Cependant, les patients traités par ces médicaments développent des mutations de résistance. Dans ce travail, nous cherchons à mieux comprendre le mécanisme d'interaction de ces drogues avec l'ADN viral. Ce travail a également contribué à la conception de molécules qui devraient être dotées d'une affinité augmentée pour l'ADN, permettant de surmonter le problème de la résistance virale. La compréhension du mécanisme d'inhibition de IN s'est poursuivie par l'étude de deux anticorps monoclonaux anti-K159 (peptide 147-175 du coeur catalytique de IN), 4C6 et 4F4. Les résultats montrent que les anticorps reconnaissent leurs épitopes dans l'IN. D'autre part, du fait de son implication dans de nombreuses étapes du cycle du VIH-1, nous ciblons la protéine 7 de la nucléocapside (NCp7). Pour ce faire, nous avons étudié la structure de nos systèmes (NCp7 et NCp7-ADN) et nous avons pu déterminer les interactions clés responsables de la structuration, ainsi que des fonctions, de ces systèmes. Dans un second temps, nous avons évalué les interactions de NCp7 avec un inhibiteur éjecteur de zinc (C247) de la famille des thioesters. Enfin, sur le plan méthodologique, nous avons raffiné dans le potentiel SIBFA (Sum of Interaction Between Fragments Ab initio computed) la représentation des doublets libres de type sp et sp2 dans les molécules conjuguées.The catalytic functions of integrase (IN) of Human Immunodeficiency Virus (HIV-1) are strictly necessary for the integration of the viral genome into the host cells. To this day, three anti-IN inhibitors belonging to the diketoacids are used in therapy: raltegravir, elvitegravir and dolutegravir. However, under treatments with these drugs, patients develop resistance mutations. In this work, we seek to better understand the interaction of the three drugs with viral DNA. This work also contributed to the design of novel molecules. These should be endowed with increased DNA binding affinities as a step towards overcoming viral resistance. The understanding of the inhibition mechanism of IN was pursued by the study of two monoclonal antibodies, 4F4 and 4C6, which are directed against sequence 147-175 of the catalytic core of HIV-1 IN, a peptide denoted K159. The results show that the antibodies recognize their epitopes in IN. We also aim to target an HIV-1 nucleocaspid protein NCp7 involved in many stages of the viral cycle. We have thus studied the structure of NCp7 and its viral DNA complex. We were able to determine the interactions responsible for the structuring and thus the functions of these complexes. Then, we evaluated the interactions of NCp7 with an inhibitor of the thioester family, C247, which acts as a zinc ejector. Finally, from the methodological standpoint, we have refined in SIBFA (Sum of Interaction Between Fragments Ab initio computed) the representation of the sp2 and sp lone pairs in conjugated molecules
Variations on the Author
Full text link“Variations on the Author” discusses two of Eduardo Coutinho’s recent films (Um Dia na Vida, from 2010, and Últimas Conversas, posthumously released in 2015) and their contribution to the general question of documentary authorship. The director’s filmography is characterized by a consistent yet self-effacing form of authorial self-inscription: Coutinho often features as an interviewer that rather than express opinions propels discourses; an interviewer that is good at listening. This mode of self-inscription characterizes him as an author who is not expressive but who is nonetheless markedly present on the screen. In Um Dia na Vida, however, Coutinho is completely absent form the image, while Últimas Conversas, on the contrary, includes a confessional prologue that moves the director from the margins to the center of his films. This article examines the ways in which these works stand out in the filmography of a director who offers new insights into the notion of cinematic authorship
Appropriate Similarity Measures for Author Cocitation Analysis
Full text linkWe provide a number of new insights into the methodological discussion about author cocitation analysis. We first argue that the use of the Pearson correlation for measuring the similarity between authors’ cocitation profiles is not very satisfactory. We then discuss what kind of similarity measures may be used as an alternative to the Pearson correlation. We consider three similarity measures in particular. One is the well-known cosine. The other two similarity measures have not been used before in the bibliometric literature. Finally, we show by means of an example that our findings have a high practical relevance.information science;Pearson correlation;cosine;similarity measure;author cocitation analysis
Dispelling the Myths Behind First-author Citation Counts
Full text linkWe conducted a full-scale evaluative citation analysis study of scholars in the XML research field to explore just how different from each other author rankings resulting from different citation counting methods actually are, and to demonstrate the capability of emerging data and tools on the Web in supporting more realistic citation counting methods. Our results contest some common arguments for the continued
use of first-author citation counts in the evaluation of scholars, such as high correlations between author rankings by first-author citation counts and other citation
counting methods, and high costs of using more realistic citation counting methods that are not well-supported by the ISI databases. It is argued that increasingly available digital full text research papers make it possible for citation analysis studies to go beyond what the ISI databases have directly supported and to employ more
sophisticated methods
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