72 research outputs found

    Construire la territorialité à partir d'une infrastructure pour la mobilité ? L'exemple de la ligne des Alpes

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    International audienceIn this proposition we analyse the expectations stakeholders develop about territories and the different visions they have about the relationship between planning and mobility, especially concerning the regional railway system and its potential in terms of servicing metropolitan territories. We show, moreover, how the proximity between researchers and territorial stakeholders brings representations and reciprocal expectations to emerge. The proposed communication is based on an interdisciplinary action-research conducted within the pole Innovation and Mountain Territories (Labex ITEM) of the Grenoble-Alpes University in collaboration with local stakeholders (representatives of institutions, economic and associative networks, inhabitants, etc.). The research, ongoing, focuses on the role of the regional railway line Grenoble-Veynes-Gap in the construction of the Grenoble metropolis. We formulate the hypothesis that the threat of dismissing the line is bringing out more clearly the expectations and the needs of peripheral metropolitan territories in the context of the current French territorial reorganization.Afin de rĂ©flĂ©chir aux attentes que les acteurs dĂ©veloppent par rapport aux territoires, nous analysons les rapports multiples qui s’instaurent entre les diffĂ©rentes visions des acteurs autour de la relation entre territoire et mobilitĂ©, en particulier le systĂšme ferroviaire rĂ©gional et son potentiel en terme de desserte des territoires mĂ©tropolitains. Nous montrons, de plus, comment la proximitĂ© entre chercheurs et acteurs du territoire fait Ă©merger les reprĂ©sentations et les attentes rĂ©ciproques. La communication proposĂ©e s’appuie sur une recherche-action interdisciplinaire conduite au sein du Labex Innovation et territoires de montagne de l’UniversitĂ© Grenoble Alpes en collaboration avec des acteurs locaux (reprĂ©sentants des institutions, du tissu Ă©conomique et associatif, habitants, etc.). La recherche, en cours, porte sur le rĂŽle de la ligne ferroviaire rĂ©gionale Grenoble-Veynes-Gap dans la construction de la mĂ©tropole grenobloise, en formulant l’hypothĂšse que la menace de fermeture de la ligne est en train de faire Ă©merger plus nettement les attentes et les besoins des territoires mĂ©tropolitains pĂ©riphĂ©riques vis-Ă -vis de la rĂ©organisation des pĂ©rimĂštres et des pouvoirs

    Differential expression of the RTP/Drg1/Ndr1 gene product in proliferating and growth arrested cells

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    AbstractUsing a differential display method to identify differentiation-related genes in human myelomonocytic U937 cells, we cloned the cDNA of a gene identical to Drg1 and homologous to other recently discovered genes, respectively human RTP and Cap43 and mouse Ndr1 and TDD5 genes. Their open reading frames encode proteins highly conserved between mouse and man but which do not share homology with other know proteins. Conditions in which mRNAs are up-regulated suggest a role for the protein in cell growth arrest and terminal differentiation. We raised antibodies against a synthetic peptide reproducing a characteristic sequence of the putative polypeptide chain. These antibodies revealed a protein with the expected 43 kDa molecular mass, up-regulated by phorbol ester, retinoids and 1,25-(OH)2 vitamin D3 in U937 cells. It was increased in mammary carcinoma MCF-7 cells treated by retinoids and by the anti-estrogen ICI 182,780 but not by 4-hydroxytamoxifen. The mouse Drg1 homologous protein was up-regulated by retinoic acid in C2 myogenic cells. The diversity of situations in which expression of RTP/Drg1/Ndr1 has now been observed shows that it is widely distributed and up-regulated by various agents. Here we show that ligands of nuclear transcription factors involved in cell differentiation are among the inducers of this novel protein

    Drosophila Immunity: Analysis of PGRP-SB1 Expression, Enzymatic Activity and Function

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    Peptidoglycan is an essential and specific component of the bacterial cell wall and therefore is an ideal recognition signature for the immune system. Peptidoglycan recognition proteins (PGRPs) are conserved from insects to mammals and able to bind PGN (non-catalytic PGRPs) and, in some cases, to efficiently degrade it (catalytic PGRPs). In Drosophila, several non-catalytic PGRPs function as selective peptidoglycan receptors upstream of the Toll and Imd pathways, the two major signalling cascades regulating the systemic production of antimicrobial peptides. Recognition PGRPs specifically activate the Toll pathway in response to Lys-type peptidoglycan found in most Gram-positive bacteria and the Imd pathway in response to DAP-type peptidoglycan encountered in Gram-positive bacilli-type bacteria and in Gram-negative bacteria. Catalytic PGRPs on the other hand can potentially reduce the level of immune activation by scavenging peptidoglycan. In accordance with this, PGRP-LB and PGRP-SC1A/B/2 have been shown to act as negative regulators of the Imd pathway. In this study, we report a biochemical and genetic analysis of PGRP-SB1, a catalytic PGRP. Our data show that PGRP-SB1 is abundantly secreted into the hemolymph following Imd pathway activation in the fat body, and exhibits an enzymatic activity towards DAP-type polymeric peptidoglycan. We have generated a PGRP-SB1/2 null mutant by homologous recombination, but its thorough phenotypic analysis did not reveal any immune function, suggesting a subtle role or redundancy of PGRP-SB1/2 with other molecules. Possible immune functions of PGRP-SB1 are discussed

    Short Term Evolution of a Highly Transmissible Methicillin-Resistant Staphylococcus aureus Clone (ST228) in a Tertiary Care Hospital

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    Staphylococcus aureus is recognized as one of the major human pathogens and is by far one of the most common nosocomial organisms. The genetic basis for the emergence of highly epidemic strains remains mysterious. Studying the microevolution of the different clones of S. aureus is essential for identifying the forces driving pathogen emergence and spread. The aim of the present study was to determine the genetic changes characterizing a lineage belonging to the South German clone (ST228) that spread over ten years in a tertiary care hospital in Switzerland. For this reason, we compared the whole genome of eight isolates recovered between 2001 and 2008 at the Lausanne hospital. The genetic comparison of these isolates revealed that their genomes are extremely closely related. Yet, a few more important genetic changes, such as the replacement of a plasmid, the loss of large fragments of DNA, or the insertion of transposases, were observed. These transfers of mobile genetic elements shaped the evolution of the ST228 lineage that spread within the Lausanne hospital. Nevertheless, although the strains analyzed differed in their dynamics, we have not been able to link a particular genetic element with spreading success. Finally, the present study showed that new sequencing technologies improve considerably the quality and quantity of information obtained for a single strain; but this information is still difficult to interpret and important investments are required for the technology to become accessible for routine investigations

    A 4-Year Retrospective Analysis of Salivary Gland Cytopathology Using the Milan System for Reporting Salivary Gland Cytology and Ancillary Studies

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    The cytopathology of salivary glands presents major challenges due to the heterogeneity of benign and malignant neoplasms, which is reflected in the large range of WHO 2017 Classifications. Fine needle aspiration (FNA) of salivary gland tumours is still the favoured initial approach as it results in good sensitivity and specificity. The Milan System for Reporting Salivary Gland Cytopathology (MSRSGC) was published in 2018 and comprises seven categories. We report results from a 4-year retrospective analysis of 328 salivary gland FNAs which were reviewed and classified according to the MSRSGC. We assess the risk of neoplasm, the risk of malignancy and the contribution of ancillary studies to the diagnosis. Benign neoplasms were the most frequent diagnosis (44.2%). Malignant and suspicious for malignancy were identified in 11.3% and 4.9% of diagnosed cases, respectively. Histopathological analysis after surgery was available for 216 (65.8%) of the cases. All malignant cases were confirmed post-surgery, and 68.8% of suspicious for malignancy were confirmed as malignant tumours. Immunocytochemistry was informative in 72.3% of cases. Immunocytochemistry and FISH provided the definitive diagnosis in 23.7% and 33% of cases, respectively. In conclusion, the MSRSGC is more effective when specific features of neoplasms can be identified. Ancillary studies help to further characterise salivary gland tumours and thereby increase the accuracy of MSRSGC
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