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Featured researches published by C. Mirre.


Development Genes and Evolution | 1987

Haemocytes accumulate collagen transcripts during Drosophila melanogaster metamorphosis

Bernard Knibiehler; C. Mirre; Jean Pierre Cecchini; Yannick Le Parco

SummaryWe report a direct examination of the expression of one collagen gene (DCg1) during Drosophila melanogaster metamorphosis, based on data from in situ hybridization. The transcripts of this gene, thought to encode a basement membrane type IV collagen, are mainly accumulated during ecdysis in wandering haemocytes. Our results demonstrate that haemocytes contribute to extracellular matrix deposition and seem to perform a fibroblastic function during Drosophila development.


Experimental Cell Research | 1986

Stage and tissue-specific expression of a collagen gene during Drosophila melanogaster development☆

Y. Le Parco; Bernard Knibiehler; Jean-Pierre Cecchini; C. Mirre

Based on data from developmental RNA profiles and in situ hybridization, we report a direct examination of the expression of one collagen gene (Dcg1) during drosophila melanogaster life cycle. These studies show, for the first time, that the expression of a collagen gene is both differential and tissue-specific during the course of development. Moreover, they demonstrate that the connective tissues in Drosophila do contain a collagen type synthesized by mesodermal tissues. Indeed the accumulation of Dcg1 transcripts was located mainly within the second instar fat bodies, the third instar lymph glands, and over adepithelial cells associated with third instar imaginal discs. In addition, these results seem to confirm the interpretation that wandering hemocytes released by the lymph glands could contribute in extracellular matrix composition in some tissues in the larva.


Insect Biochemistry | 1989

DCg1 αIV collagen chain of Drosophila melanogaster is synthesized during embryonic organogenesis by mesenchymal cells and is deposited in muscle basement membranes

Yannick Le Parco; AndréLe Bivic; Bernard Knibiehler; C. Mirre; Jean-Pierre Cecchini

Abstract We report the purification and characterization of three sequence-specific polyclonal antibodies raised against specific portions of the Drosophila αIV collagen chain produced from the gene DCg1. These antibodies were used for immunolocalization experiments on tissue sections from embryonic organogenesis stages (13–17) and first larval stages. This analysis was paralleled by in situ hybridization experiments with a labeled fragment of the gene DCg1. We demonstrated that, by late embryogenesis, the DCg1 αIV chain was synthesized by individual mesoblasts and deposited in basement membranes of skeletal and visceral muscles. These sites of αIV collagen deposition were the same, by first and second instars, but the protein was then synthesized by fat body cells. Our results were reminiscent of those obtained for vertebrate in vitro myogenesis, they suggested, moreover, a tissue-specific composition of basement membranes in Drosophila melanogaster .


Mechanisms of Development | 1990

Collagen type IV of Drosophila is stockpiled in the growing oocyte and differentially located during early stages of embryogenesis

Bernard Knibiehler; C. Mirre; Y. Le Parco

We have developed and characterized a battery of specific polyclonal antibodies directed against specific portions of the alpha-chain of collagen type IV synthesized in Drosophila by the gene DCg1. Here, we describe the use of these antibodies together with in situ hybridization experiments in an attempt to study the expression and localization of collagen type IV during Drosophila oogenesis and early embryogenesis. The results clearly demonstrate that DCg1 is maternally expressed by follicle cells and that the collagen type IV chain produced is stockpiled in the growing oocyte. During the gastrulation stages, this component of Drosophila basement membranes concentrated on cells involved in the gradual invaginations leading to morphogenetic furrows. The presence of collagen type IV, which is an RGD-bearing molecule, during early stages of Drosophila development is discussed in comparison with the crucial, active role its vertebrate counterpart is supposed to play in morphogenetic processes.


Journal of Cell Science | 1993

GPI-anchored proteins associate to form microdomains during their intracellular transport in Caco-2 cells.

Martine Garcia; C. Mirre; Andrea Quaroni; H. Reggio; A. Le Bivic


American Journal of Physiology-cell Physiology | 1996

Detergent-resistant membrane microdomains from Caco-2 cells do not contain caveolin

C. Mirre; Laure Monlauzeur; Martine Garcia; A. Le Bivic


Journal of Cell Science | 1997

Human syntaxin 3 is localized apically in human intestinal cells

Lionel Breuza; C. Mirre; P. Chavrier; A. Le Bivic


Development | 1988

De novo expression of a type IV collagen gene in Drosophila embryos is restricted to mesodermal derivatives and occurs at germ band shortening

C. Mirre; Jean-Pierre Cecchini; Y. Le Parco; Bernard Knibiehler


FEBS Journal | 1987

Evidence for a type-IV-related collagen in Drosophila melanogaster. Evolutionary constancy of the carboxyl-terminal noncollagenous domain.

Jean-Pierre Cecchini; Bernard Knibiehler; C. Mirre; Yannick Le Parco


Journal of Neuroscience Research | 1992

Collagen IV is present in the developing CNS during Drosophila neurogenesis

C. Mirre; Y. Le Parco; Bernard Knibiehler

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Bernard Knibiehler

Centre national de la recherche scientifique

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Jean-Pierre Cecchini

Centre national de la recherche scientifique

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Yannick Le Parco

Centre national de la recherche scientifique

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Y. Le Parco

Centre national de la recherche scientifique

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AndréLe Bivic

Centre national de la recherche scientifique

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Bernard Knihiehler

Centre national de la recherche scientifique

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