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Philippe Gilot

Researcher at Pasteur Institute

Publications -  13
Citations -  624

Philippe Gilot is an academic researcher from Pasteur Institute. The author has contributed to research in topics: Listeria monocytogenes & Mycobacterium tuberculosis. The author has an hindex of 9, co-authored 12 publications receiving 598 citations.

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The ATP binding cassette (ABC) transport systems of Mycobacterium tuberculosis

TL;DR: The inventory and assembly of the typical subunits of the ABC transporters encoded by the complete genome of Mycobacterium tuberculosis found that there is an under-representation of the importers in M. tuberculosis, which may reflect the capacity of this bacterium to synthesize many essential compounds and to grow in the presence of few external nutrients.
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Serotyping and esterase typing for analysis of Listeria monocytogenes populations recovered from foodstuffs and from human patients with listeriosis in Belgium.

TL;DR: The secretion of the virulence determinant phosphatidylinositol-specific phospholipase C and the pathogenicity level of strains in immunocompromised mice could not explain the unequal distribution of esterase types.
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Listeria monocytogenes possesses adhesins for fibronectin.

TL;DR: The binding of L. monocytogenes to fibronectin adds to the number of molecules to which the bacterium is able to adhere and emphasizes the complexity of host-pathogen interactions.
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Specific Identification of Listeria welshimeri and Listeria monocytogenes by PCR Assays Targeting a Gene Encoding a Fibronectin-Binding Protein

TL;DR: A L. welshimeri DNA fragment cloned and sequenced homologous to the previously described fibronectin-binding protein-encoding gene (fbp) of Listeria monocytogenes expresses a 24.8-kDa protein that binds to human fibronsectin.
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Cloning, sequencing and characterisation of a Listeria monocytogenes gene encoding a fibronectin-binding protein.

TL;DR: Restriction endonuclease-PCR showed that the fbp gene displays a degree of allelic variation among isolates of L. monocytogenes, whereas the corresponding amplified fragment ofL.