1,351 research outputs found

    Special Issue on “fruit metabolism and metabolomics”

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    Over the past 10 years, knowledge about several aspects of fruit metabolism has been greatly improved. Notably, high-throughput metabolomic technologies have allowed quantifying metabolite levels across various biological processes, and identifying the genes that underly fruit development and ripening. This Special Issue is designed to exemplify the current use of metabolomics studies of temperate and tropical fruit for basic research as well as practical applications. It includes articles about different aspects of fruit biochemical phenotyping, fruit metabolism before and after harvest, including primary and specialized metabolisms, and bioactive compounds involved in growth and environmental responses. The effect of genotype, stages of development or fruit tissue on metabolomic profiles and corresponding metabolism regulations are addressed, as well as the combination of other omics with metabolomics for fruit metabolism studies. © 2020 by the authors. Licensee MDPI, Basel, Switzerland.partly funded by MetaboHUB (ANR‐11‐INBS‐0010) and PHENOME (ANR‐11‐ INBS‐0012) French Agence Nationale de la Recherche projects. S.O. was parcially supported by grants RTI2018‐ 099797‐B‐100 (Ministerio de ciencia, InnovaciĂłn y Universidades, Spain) and UMA18‐DEDERJA‐179 (ConsejerĂ­a de EconomĂ­a, Conocimiento, Empresas y Universidades, Junta de AndalucĂ­a, Spain).Peer reviewe

    Special Issue on “fruit metabolism and metabolomics”

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    Over the past 10 years, knowledge about several aspects of fruit metabolism has been greatly improved. Notably, high-throughput metabolomic technologies have allowed quantifying metabolite levels across various biological processes, and identifying the genes that underly fruit development and ripening. This Special Issue is designed to exemplify the current use of metabolomics studies of temperate and tropical fruit for basic research as well as practical applications. It includes articles about different aspects of fruit biochemical phenotyping, fruit metabolism before and after harvest, including primary and specialized metabolisms, and bioactive compounds involved in growth and environmental responses. The effect of genotype, stages of development or fruit tissue on metabolomic profiles and corresponding metabolism regulations are addressed, as well as the combination of other omics with metabolomics for fruit metabolism studies. © 2020 by the authors. Licensee MDPI, Basel, Switzerland.partly funded by MetaboHUB (ANR‐11‐INBS‐0010) and PHENOME (ANR‐11‐ INBS‐0012) French Agence Nationale de la Recherche projects. S.O. was parcially supported by grants RTI2018‐ 099797‐B‐100 (Ministerio de ciencia, InnovaciĂłn y Universidades, Spain) and UMA18‐DEDERJA‐179 (ConsejerĂ­a de EconomĂ­a, Conocimiento, Empresas y Universidades, Junta de AndalucĂ­a, Spain).Peer reviewe

    Dense Optical Tracking: Connecting the Dots

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    Recent approaches to point tracking are able to recover the trajectory of any scene point through a large portion of a video despite the presence of occlusions. They are, however, too slow in practice to track every point observed in a single frame in a reasonable amount of time. This paper introduces DOT, a novel, simple and efficient method for solving this problem. It first extracts a small set of tracks from key regions at motion boundaries using an off-the-shelf point tracking algorithm. Given source and target frames, DOT then computes rough initial estimates of a dense flow field and visibility mask through nearest-neighbor interpolation, before refining them using a learnable optical flow estimator that explicitly handles occlusions and can be trained on synthetic data with ground-truth correspondences. We show that DOT is significantly more accurate than current optical flow techniques, outperforms sophisticated "universal" trackers like OmniMotion, and is on par with, or better than, the best point tracking algorithms like CoTracker while being at least two orders of magnitude faster. Quantitative and qualitative experiments with synthetic and real videos validate the promise of the proposed approach. Code, data, and videos showcasing the capabilities of our approach are available in the project webpage: https://16lemoing.github.io/dot .Comment: Accepted to CVPR 202

    Modeling Carbon Export Out of Mature Peach Leaves

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    Reseña de Kaufmant, Marie-EugĂ©nie, «Le cheval au thĂ©Ăątre dans l’Espagne du SiĂšcle d’Or. Fondements idĂ©ologiques et mĂ©canismes d’une poĂ©tique dans la comedia nueva», Binges, Éditions Orbis Tertius, 2018, 576 pp. ISBN: 978-2-36783-113-8

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    Reseña de Kaufmant, Marie-EugĂ©nie, Le cheval au thĂ©Ăątre dans l’Espagne du SiĂšcle d’Or. Fondements idĂ©ologiques et mĂ©canismes d’une poĂ©tique dans la comedia nueva, Binges, Éditions Orbis Tertius, 2018, 576 pp. ISBN: 978-2-36783-113-

    Phenotypic and fine genetic characterization of the D locus controlling fruit acidity in peach

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    <p>Abstract</p> <p>Background</p> <p>Acidity is an essential component of the organoleptic quality of fleshy fruits. However, in these fruits, the physiological and molecular mechanisms that control fruit acidity remain unclear. In peach the <it>D </it>locus controls fruit acidity; low-acidity is determined by the dominant allele. Using a peach progeny of 208 F<sub>2 </sub>trees, the <it>D </it>locus was mapped to the proximal end of linkage group 5 and co-localized with major QTLs involved in the control of fruit pH, titratable acidity and organic acid concentration and small QTLs for sugar concentration. To investigate the molecular basis of fruit acidity in peach we initiated the map-based cloning of the <it>D </it>locus.</p> <p>Results</p> <p>In order to generate a high-resolution linkage map in the vicinity of the <it>D </it>locus, 1,024 AFLP primer combinations were screened using DNA of bulked acid and low-acid segregants. We also screened a segregating population of 1,718 individuals for chromosomal recombination events linked to the <it>D </it>locus and identified 308 individuals with recombination events close to <it>D</it>. Using these recombinant individuals we delimited the <it>D </it>locus to a genetic interval of 0.4 cM. We also constructed a peach BAC library of 52,000 clones with a mean insert size of 90 kb. The screening of the BAC library with markers tightly linked to <it>D </it>locus indicated that 1 cM corresponds to 250 kb at the vicinity of the <it>D </it>locus.</p> <p>Conclusion</p> <p>In the present work we presented the first high-resolution genetic map of <it>D </it>locus in peach. We also constructed a peach BAC library of approximately 15ïżœïżœ genome equivalent. This fine genetic and physical characterization of the <it>D </it>locus is the first step towards the isolation of the gene(s) underlying fruit acidity in peach.</p

    Dame Kobold (1920) de Hugo von Hofmannsthal et son modÚle : La dama duende (1629) de Pedro Calderón de la Barca

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    Le thĂ©Ăątre du SiĂšcle d’or espagnol a fascinĂ© les dramaturges autrichiens, parmi lesquels Hofmannsthal. Celui-ci Ă©crit en 1920 Dame Kobold d’aprĂšs la traduction allemande de Johann Diederich Gries de La dama duende (1629) de CalderĂłn. Respectant l’intrigue et l’ancrage spatio-temporel de la piĂšce espagnole, il s’en Ă©loigne grĂące Ă  la modernitĂ© de sa langue et par des dĂ©crochages qui l’amĂšnent Ă  dĂ©velopper la dimension Ɠdipienne des relations entre les personnages. Ces dĂ©crochages finissent par dĂ©boucher sur une significative modification revenant Ă  affirmer la nĂ©cessitĂ© de la foi en l’autre pour arriver Ă  une vraie rencontre amoureuse. Cette modification s’inscrit dans une rĂ©flexion sur la masculinitĂ© et la fĂ©minitĂ©. La fidĂ©litĂ© novatrice de Hofmannsthal lui permet ainsi de dĂ©montrer l’atemporalitĂ© du texte caldĂ©ronien, puisque La dama duende porte en germe l’histoire de Dame Kobold, celle d’un Homme qui devient pleinement Homme en rencontrant une Femme, et d’une Femme qui devient pleinement Femme en rencontrant un Homme.Das Theater des spanischen Goldenen Zeitalters faszinierte österreichische BĂŒhnenautoren, unter ihnen Hofmannsthal. 1920 schreibt er Dame Kobold. Quelle seiner Inspiration ist Johann Diederich Gries‘ deutsche Übersetzung des TheaterstĂŒcks La dama duende (1629) von Calderon. Dabei hĂ€lt er an der Handlung und der rĂ€umlich-zeitlichen Verankerung des spanischen Vorbilds fest, entfernt sich aber durch seine moderne Sprache und Sinnverschiebungen, die die Dimension ödipaler Beziehungen der Personen untereinander zur Geltung bringt. Durch diese Verschiebungen gibt er dem TheaterstĂŒck einen entscheidend umgewandelten Sinn, nĂ€mlich den, dass der Glaube an den anderen notwendig ist, damit es zu einer wahren Liebesbegegnung und Liebesbeziehung kommen kann. Dieses Umwandeln steht im Rahmen des Nachdenkens ĂŒber MĂ€nnlichkeit und Weiblichkeit. Diese erneuernde Art, dem ursprĂŒnglichen Text treu zu bleiben, gibt Hofmannsthal die Möglichkeit zu zeigen, dass der Text von Calderon ĂŒber seine Zeit hinausgeht, da La dama duende schon den Keim zu Dame Kobold in sich birgt, den Keim zu der Geschichte eines Mannes, der ein wahrer Mann wird, indem er eine Frau wahrhaft liebt, und zu der Geschichte einer Frau, die zu einer wahren Frau wird, indem sie einen Mann wahrhaft liebt.Austrian dramatists were fascinated by the Spanish Siglo de Oro drama. Among them was Hofmannsthal, who wrote Dame Kobold in 1920, a rewriting of Johann Diederich Gries’s German translation of La dama duende (CalderĂłn, 1629). Keeping in mind the plot and the spatiotemporal foundations of the Spanish play, he moves away from it thanks to the modernity of his writing and distance from the original text, which leads him to develop the Oedipal dimension of the relationships between the characters. This distance eventually reaches a significant modification, affirming the necessity of faith in the other in order to achieve a real love encounter. This modification is part of a reflexion about masculinity and femininity. Hofmannsthal’s innovative faithfulness allows him to demonstrate the timelesness of the Calderonian text, as La dama duende contains the seeds of the story of Dame Kobold, the story of a Man who becomes fully a Man when he meets a Woman, and the one of a Woman who becomes fully a Woman when she meets a Man

    Response to highly active antiretroviral therapy among severely immuno-compromised HIV-infected patients in Cambodia.

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    BACKGROUND: HAART efficacy was evaluated in a real-life setting in Phnom Penh (MĂ©decins Sans FrontiĂšres programme) among severely immuno-compromised patients. METHODS: Factors associated with mortality and immune reconstitution were identified using Cox proportional hazards and logistic regression models, respectively. RESULTS: From July 2001 to April 2005, 1735 patients initiated HAART, with median CD4 cell count of 20 (inter-quartile range, 6-78) cells/microl. Mortality at 2 years increased as the CD4 cell count at HAART initiation decreased, (4.4, 4.5, 7.5 and 24.7% in patients with CD4 cell count > 100, 51-100, 21-50 and < or = 20 cells/microl, respectively; P < 10). Cotrimoxazole and fluconazole prophylaxis were protective against mortality as long as CD4 cell counts remained < or = 200 and < or = 100 cells/microl, respectively. The proportion of patients with successful immune reconstitution (CD4 cell gain > 100 cells/microl at 6 months) was 46.3%; it was lower in patients with previous ART exposure [odds ratio (OR), 0.16; 95% confidence interval (CI), 0.05-0.45] and patients developing a new opportunistic infection/immune reconstitution infection syndromes (OR, 0.71; 95% CI, 0.52-0.98). Similar efficacy was found between the stavudine-lamivudine-nevirapine fixed dose combination and the combination stavudine-lamivudine-efavirenz in terms of mortality and successful immune reconstitution. No surrogate markers for CD4 cell change could be identified among total lymphocyte count, haemoglobin, weight and body mass index. CONCLUSION: Although CD4 cell count-stratified mortality rates were similar to those observed in industrialized countries for patients with CD4 cell count > 50 cells/microl, patients with CD4 cell count < or = 20 cells/microl posed a real challenge to clinicians. Widespread voluntary HIV testing and counselling should be encouraged to allow HAART initiation before the development of severe immuno-suppression
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