97 research outputs found

    PremiÚres. Les lettres au féminin en 1980

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    Le 6 mars 1980, Marguerite Yourcenar est Ă©lue Ă  l’AcadĂ©mie française. En obtenant la majoritĂ© plus une voix, elle est la premiĂšre femme en trois cent quarante-cinq ans Ă  y obtenir un fauteuil. La dĂ©cision reste cependant symbolique, comme en tĂ©moigne le propos de Jean Guitton ce jour-lĂ . Aux journalistes qui l’interrogent, il explique avec un sourire qu’il a bien entendu fait partie des opposants: l’AcadĂ©mie ayant vĂ©cu pendant trois siĂšcles sans femme, elle pouvait encore vivre trois siĂšcles ..

    Corps meurtris du roman contemporain : souffrances et accusations

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    Les corps meurtris sont rĂ©guliĂšrement au cƓur du roman contemporain : qu’ils soient le sujet mĂȘme de la narration, ou qu’ils apparaissent ponctuellement, ils dictent une Ă©criture Ă©prouvante. S’il n’est pas nouveau – les corps malades ou blessĂ©s ont de longue date fascinĂ© la littĂ©rature –, cet intĂ©rĂȘt pour la souffrance physique, est toutefois aujourd’hui symptomatique d’une volontĂ© d’exprimer et d’apprĂ©hender autrement le monde actuel, dans lequel le culte de l’apparence et de la performance, mais aussi le dĂ©veloppement du virtuel laissent peu de chance Ă  l’expression individuelle, de l’énonciation de drames intimes Ă  la formulation de problĂšmes sociaux. À travers quelques romans contemporains de langue française, l’étude de la reprĂ©sentation des corps meurtris, permettra de comprendre comment ceux-ci appuient les accusations de l’écriture contemporaine.Wounded bodies are regularly at the heart of the contemporary novel: whether they are the topic of the narrative itself or incorporated more discreetly into the text, they require a demanding style of writing. Even if this interest in physical pain is not new – sick or injured bodies have long been a fascination in literature – today it is symptomatic of a desire to express and understand more fully the contemporary world, where the cult of appearances and performance, as well as the development of virtual reality, leave little opportunity for individual expression, from the utterance of private tragedies to the wording of societal problems. Using some contemporary French and francophone novels, this study of the representation of wounded bodies allows for an understanding of how they support the accusations found in contemporary literature

    VulnĂ©rable que je suis : poĂ©tique de l’éphĂ©mĂšre chez Ali Zamir

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    Inscrites dans la rĂ©alitĂ© de la sociĂ©tĂ© comorienne, les vies vulnĂ©rables qui peuplent les romans d’Ali Zamir sont portĂ©es par une narration qui Ă©pouse la fragilitĂ© et la dĂ©tresse des personnages. Entre ignorance et folie, voix accusatrice et foisonnement verbal, la fiction mise en Ɠuvre se saisit des destins collectifs comme des existences ordinaires. Il s’agit ici de comprendre comment, roman aprĂšs roman, une singuliĂšre poĂ©tique de l’éphĂ©mĂšre en appelle au lecteur afin de rĂ©tablir la rĂ©flexion littĂ©raire Ă  l’échelle humaine.Inscribed in the reality of Comorian society, the vulnerable lives that inhabit Ali Zamir’s novels are carried by a narrative that embraces the fragility and distress of the characters. Between ignorance and madness, accusatory voice and verbal profusion, the implementing fiction grasps collective destinies like ordinary existences. It is a question here of understanding how, novel after novel, a singular poetic of ephemeral appeals to the reader in order to restore literary reflection on a human scale

    Rational design of an orthogonal tryptophanyl nonsense suppressor tRNA

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    While a number of aminoacyl tRNA synthetase (aaRS):tRNA pairs have been engineered to alter or expand the genetic code, only the Methanococcus jannaschii tyrosyl tRNA synthetase and tRNA have been used extensively in bacteria, limiting the types and numbers of unnatural amino acids that can be utilized at any one time to expand the genetic code. In order to expand the number and type of aaRS/tRNA pairs available for engineering bacterial genetic codes, we have developed an orthogonal tryptophanyl tRNA synthetase and tRNA pair, derived from Saccharomyces cerevisiae. In the process of developing an amber suppressor tRNA, we discovered that the Escherichia coli lysyl tRNA synthetase was responsible for misacylating the initial amber suppressor version of the yeast tryptophanyl tRNA. It was discovered that modification of the G:C content of the anticodon stem and therefore reducing the structural flexibility of this stem eliminated misacylation by the E. coli lysyl tRNA synthetase, and led to the development of a functional, orthogonal suppressor pair that should prove useful for the incorporation of bulky, unnatural amino acids into the genetic code. Our results provide insight into the role of tRNA flexibility in molecular recognition and the engineering and evolution of tRNA specificity

    RloC: a wobble nucleotide-excising and zinc-responsive bacterial tRNase

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    The conserved bacterial protein RloC, a distant homologue of the tRNALys anticodon nuclease (ACNase) PrrC, is shown here to act as a wobble nucleotide-excising and Zn++-responsive tRNase. The more familiar PrrC is silenced by a genetically linked type I DNA restriction-modification (R-M) enzyme, activated by a phage anti-DNA restriction factor and counteracted by phage tRNA repair enzymes. RloC shares PrrC's ABC ATPase motifs and catalytic ACNase triad but features a distinct zinc-hook/coiled-coil insert that renders its ATPase domain similar to Rad50 and related DNA repair proteins. Geobacillus kaustophilus RloC expressed in Escherichia coli exhibited ACNase activity that differed from PrrC's in substrate preference and ability to excise the wobble nucleotide. The latter specificity could impede reversal by phage tRNA repair enzymes and account perhaps for RloC's more frequent occurrence. Mutagenesis and functional assays confirmed RloC's catalytic triad assignment and implicated its zinc hook in regulating the ACNase function. Unlike PrrC, RloC is rarely linked to a type I R-M system but other genomic attributes suggest their possible interaction in trans. As DNA damage alleviates type I DNA restriction, we further propose that these related perturbations prompt RloC to disable translation and thus ward off phage escaping DNA restriction during the recovery from DNA damage

    tRNASec is transcribed by RNA polymerase II in Trypanosoma brucei but not in humans

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    Nuclear-encoded tRNAs are universally transcribed by RNA polymerase III (Pol-III) and contain intragenic promoters. Transcription of vertebrate tRNASec however requires extragenic promoters similar to Pol-III transcribed U6 snRNA. Here, we present a comparative analysis of tRNASec transcription in humans and the parasitic protozoa Trypanosoma brucei, two evolutionary highly diverged eukaryotes. RNAi-mediated ablation of Pol-II and Pol-III as well as oligo-dT induced transcription termination show that the human tRNASec is a Pol-III transcript. In T. brucei protein-coding genes are polycistronically transcribed by Pol-II and processed by trans-splicing and polyadenylation. tRNA genes are generally clustered in between polycistrons. However, the trypanosomal tRNASec genes are embedded within a polycistron. Their transcription is sensitive to α-amanitin and RNAi-mediated ablation of Pol-II, but not of Pol-III. Ectopic expression of the tRNASec outside but not inside a polycistron requires an added external promoter. These experiments demonstrate that trypanosomal tRNASec, in contrast to its human counterpart, is transcribed by Pol-II. Synteny analysis shows that in trypanosomatids the tRNASec gene can be found in two different polycistrons, suggesting that it has evolved twice independently. Moreover, intron-encoded tRNAs are present in a number of eukaryotic genomes indicating that Pol-II transcription of tRNAs may not be restricted to trypanosomatids

    Recode-2: new design, new search tools, and many more genes

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    'Recoding' is a term used to describe non-standard read-out of the genetic code, and encompasses such phenomena as programmed ribosomal frameshifting, stop codon readthrough, selenocysteine insertion and translational bypassing. Although only a small proportion of genes utilize recoding in protein synthesis, accurate annotation of ‘recoded’ genes lags far behind annotation of 'standard' genes. In order to address this issue, provide a service to researchers in the field, and offer training data for developers of gene-annotation software, we have gathered together known cases of recoding within the Recode database. Recode-2 is an improved and updated version of the database. It provides access to detailed information on genes known to utilize translational recoding and allows complex search queries, browsing of recoding data and enhanced visualization of annotated sequence elements. At present, the Recode-2 database stores information on approximately 1500 genes that are known to utilize recoding in their expression—a factor of approximately three increase over the previous version of the database. Recode-2 is available at http://recode.ucc.i

    The Acute Phase Protein Serum Amyloid A Induces Lipolysis and Inflammation in Human Adipocytes through Distinct Pathways

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    Background: The acute phase response (APR) is characterized by alterations in lipid and glucose metabolism leading to an increased delivery of energy substrates. In adipocytes, there is a coordinated decrease in Free Fatty acids (FFAs) and glucose storage, in addition to an increase in FFAs mobilization. Serum Amyloid A (SAA) is an acute phase protein mainly associated with High Density Lipoproteins (HDL). We hypothesized that enrichment of HDL with SAA, during the APR, could be implicated in the metabolic changes occurring in adipocytes. Methodology/Principal Findings: In vitro differentiated human adipocytes (hMADS) were treated with SAA enriched HDL or recombinant SAA and the metabolic phenotype of the cells analyzed. In hMADS, SAA induces an increased lipolysis through an ERK dependent pathway. At the molecular level, SAA represses PPARc2, C/EBPa and SREBP-1c gene expression, three transcription factors involved in adipocyte differentiation or lipid synthesis. In addition, the activation of the NF-kB pathway by SAA leads to the induction of pro-inflammatory cytokines and chemokines, as in the case of immune cells. These latter findings were replicated in freshly isolated mature human adipocytes. Conclusions/Significance: Besides its well-characterized role in cholesterol metabolism, SAA has direct metabolic effects on human adipocytes. These metabolic changes could be at least partly responsible for alterations of adipocyte metabolism observed during the APR as well as during pathophysiological conditions such as obesity and conditions leading to insuli

    Complete Genome Sequence of Mycoplasma suis and Insights into Its Biology and Adaption to an Erythrocyte Niche

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    Mycoplasma suis, the causative agent of porcine infectious anemia, has never been cultured in vitro and mechanisms by which it causes disease are poorly understood. Thus, the objective herein was to use whole genome sequencing and analysis of M. suis to define pathogenicity mechanisms and biochemical pathways. M. suis was harvested from the blood of an experimentally infected pig. Following DNA extraction and construction of a paired end library, whole-genome sequencing was performed using GS-FLX (454) and Titanium chemistry. Reads on paired-end constructs were assembled using GS De Novo Assembler and gaps closed by primer walking; assembly was validated by PFGE. Glimmer and Manatee Annotation Engine were used to predict and annotate protein-coding sequences (CDS). The M. suis genome consists of a single, 742,431 bp chromosome with low G+C content of 31.1%. A total of 844 CDS, 3 single copies, unlinked rRNA genes and 32 tRNAs were identified. Gene homologies and GC skew graph show that M. suis has a typical Mollicutes oriC. The predicted metabolic pathway is concise, showing evidence of adaptation to blood environment. M. suis is a glycolytic species, obtaining energy through sugars fermentation and ATP-synthase. The pentose-phosphate pathway, metabolism of cofactors and vitamins, pyruvate dehydrogenase and NAD+ kinase are missing. Thus, ribose, NADH, NADPH and coenzyme A are possibly essential for its growth. M. suis can generate purines from hypoxanthine, which is secreted by RBCs, and cytidine nucleotides from uracil. Toxins orthologs were not identified. We suggest that M. suis may cause disease by scavenging and competing for host' nutrients, leading to decreased life-span of RBCs. In summary, genome analysis shows that M. suis is dependent on host cell metabolism and this characteristic is likely to be linked to its pathogenicity. The prediction of essential nutrients will aid the development of in vitro cultivation systems

    The Father's game : the narrator-father in contemporary french novel

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    Rares sont les occasions pour le pĂšre de faire entendre sa voix dans le roman français contemporain. Alors que le rĂ©cit de filiation a pris une ampleur sans prĂ©cĂ©dent dĂšs les annĂ©es 1980, offrant aux fils et aux filles la possibilitĂ© de questionner leur ascendance, la figure paternelle est de longue date sommĂ©e de garder le silence. Le fait n’est pas nouveau : la littĂ©rature fut Ă  maintes reprises le tĂ©moin d’une paternitĂ© tenue Ă  distance de l’intimitĂ© familiale, victime de l’image tenace d’un patriarche, autoritaire et injuste, progressivement dĂ©possĂ©dĂ©e de ses pouvoirs par l’Histoire. À l’approche du XXIe siĂšcle cependant, les sciences humaines manifestent un intĂ©rĂȘt soudain pour le sujet ; considĂ©rant le silence du pĂšre, la sociologie, la psychologie, l’histoire mais aussi la littĂ©rature s’interrogent : quelle place, quel rĂŽle et finalement quelle identitĂ© doivent ĂȘtre aujourd’hui accordĂ©s au pĂšre ? Parmi la rumeur grandissante, le principal intĂ©ressĂ©, pressĂ© de questions, peine Ă  se hisser sur le devant de la scĂšne pour prendre la parole. Il convient dĂšs lors de prĂȘter attention Ă  l’exception du pĂšre-narrateur et d’enquĂȘter sur les modalitĂ©s d’une telle Ă©mergence dans le roman contemporain. L’analyse appuyĂ©e sur un corpus de romans de quatre Ă©crivains – Philippe Forest, Laurent Mauvignier, GisĂšle Fournier et Sylvie Gracia –, mĂȘlant Ă©crits fictifs et autobiographiques, a permis de dĂ©finir les caractĂ©ristiques d’un phĂ©nomĂšne inĂ©dit introduisant une rĂ©flexion nouvelle sur la paternitĂ©, en ce qu’elle rĂ©pond de l’incertitude de l’individu contemporain, mais aussi de la paternitĂ© littĂ©raire et des enjeux de l’écriture contemporaine. L’étude pose pour cela dans un premier temps les contextes historiques et gĂ©nĂ©riques de la paternitĂ© en confrontant les points de vue proposĂ©s par les sciences humaines et ceux rĂ©sultant de l’approche littĂ©raire. La structure de la narration paternelle est ensuite observĂ©e de maniĂšre Ă  comprendre comment advient la parole du pĂšre et le fonctionnement spĂ©cifique de celle-ci. Enfin la derniĂšre partie s’attarde sur la singularitĂ© de la voix paternelle et sur ce qui, visant Ă  rendre compte du rĂ©el, s’apparente Ă  un jeu littĂ©raire sans fin, entraĂźnant cĂŽte Ă  cĂŽte, Ă©crivain, personnages et lecteur.In the contemporary French novel, the father has few opportunities to be heard. While there have been an increasing number of stories about filiation since the 1980's, giving sons and daughters the possibility of questioning their ancestry, the father figure remains silent. Nothing is new here: literature often shows the father being kept away from the private sphere of family life, the father being a victim of the enduring patriarchal image and of his lost authority. At the turn of the 21st century, however, the humanities and social sciences suddenly began to take an interest in the topic. Looking at the father's silence, sociology, psychology, history, and also literature ask the question: what place, what role, and, in the end, what identity should be given to the father? In the midst of this growing discussion, the key player pressed by questions struggles to make his way into the foreground and take the floor. If eventually he introduces himself as a narrator, this should be noted and the forms of such an emergence in the contemporary novel should be investigated. An analysis based on the novels of four writers – Philippe Forest, Laurent Mauvignier, GisĂšle Fournier et Sylvie Gracia – blending fictional and autobiographical works, allows us to define the features of an unprecedented phenomenon leading to new ideas about being a father today in terms of how it reflects the uncertainty of the individual in society, and also about the authorship of the work (“paternity”) and its issues in contemporary writing. This study first lays out historical and generic contexts of fatherhood by addressing the points of view offered by the social sciences and those derived from the literary approach. The structure of the paternal narration is then observed in such a way to allow an understanding of what's behind the father's words and how they work. Finally, the last chapter focuses on the singularity of the paternal voice and on that which, attempting to take account of reality, lends itself to an endless literary game, carrying away author, characters, and reader
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