Delphine Gerbod
Pasteur Institute
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Featured researches published by Delphine Gerbod.
Journal of Clinical Microbiology | 2005
Christophe Noël; Fabienne Dufernez; Delphine Gerbod; Virginia P. Edgcomb; Pilar Delgado-Viscogliosi; L. C. Ho; Mulkit Singh; René Wintjens; Mitchell L. Sogin; Monique Capron; Raymond J. Pierce; Lionel Zenner; Eric Viscogliosi
ABSTRACT Small-subunit (SSU) rRNA gene sequences were obtained by PCR from 12 Blastocystis isolates from humans, rats, and reptiles for which elongation factor 1α (EF-1α) gene sequences are already available. These new sequences were analyzed by the Bayesian method in a broad phylogeny including, for the first time, all Blastocystis sequences available in the databases. Phylogenetic trees identified seven well-resolved groups plus several discrete lineages that could represent newly defined clades. Comparative analysis of SSU rRNA- and EF-1α-based trees obtained by maximum-likelihood methods from a restricted sampling (13 isolates) revealed overall agreement between the two phylogenies. In spite of their morphological similarity, sequence divergence among Blastocystis isolates reflected considerable genetic diversity that could be correlated with the existence of potentially ≥12 different species within the genus. Based on this analysis and previous PCR-based genotype classification data, six of these major groups might consist of Blastocystis isolates from both humans and other animal hosts, confirming the low host specificity of Blastocystis. Our results also strongly suggest the existence of numerous zoonotic isolates with frequent animal-to-human and human-to-animal transmissions and of a large potential reservoir in animals for infections in humans.
Molecular and Biochemical Parasitology | 2003
Christophe Noël; Corinne Peyronnet; Delphine Gerbod; Virginia P. Edgcomb; Pilar Delgado-Viscogliosi; Mitchell L. Sogin; Monique Capron; Eric Viscogliosi; Lionel Zenner
In conclusion, the present study confirms that genetic diversity exists among Blastocystis organisms isolated from different hosts and suggests that more than one species of Blastocystis infect humans. The possibility of cross-contamination between animals and humans exists, and the data suggest a low host specificity of these microorganisms. Thus, if Blastocystis isolated from animals are capable of infecting humans, the number of animals found to be infected with Blastocystis could represent a large potential reservoir for infection of humans.
Journal of Eukaryotic Microbiology | 2001
Delphine Gerbod; Virginia P. Edgcomb; Christophe Noël; Lionel Zenner; René Wintjens; Pilar Delgado-Viscogliosi; Michael Holder; Mitchell L. Sogin; Eric Viscogliosi
Abstract The phylogenetic position of the trichomonad, Histomonas meleagridis was determined by analysis of small subunit rRNAs. Molecular trees including all identified parabasalid sequences available in data bases were inferred by distance, parsimony, and likelihood methods. All reveal a close relationship between H. meleagridis, and Dientamoeba fragilis. Moreover, small subunit rRNAs of both amoeboid species have a reduced G + C content and increased chain length relative to other parabasalids. Finally, the rRNA genes from H. meleagridis and D. fragilis share a recent common ancestor with Tritrichomonas foetus, which exhibits a more developed cytoskeleton. This indicates that Histomonas and Dientamoeba secondarily lost most of the typical trichomonad cytoskeletal structures and hence, do not represent primitive morphologies. A global phylogeny of parabasalids revealed significant discrepancies with morphology-based classifications, such as the polyphyly of most of the parabasalid families and classes included in our study.
Journal of Biological Chemistry | 2004
René Wintjens; Christophe Noël; Alex C.W. May; Delphine Gerbod; Fabienne Dufernez; Monique Capron; Eric Viscogliosi; Marianne Rooman
The iron- and manganese-containing superoxide dismutases (Fe/Mn-SOD) share the same chemical function and spatial structure but can be distinguished according to their modes of oligomerization and their metal ion specificity. They appear as homodimers or homotetramers and usually require a specific metal for activity. On the basis of 261 aligned SOD sequences and 12 superimposed x-ray structures, two phenetic trees were constructed, one sequence-based and the other structure-based. Their comparison reveals the imperfect correlation of sequence and structural changes; hyperthermophilicity requires the largest sequence alterations, whereas dimer/tetramer and manganese/iron specificities are induced by the most sizable structural differences within the monomers. A systematic investigation of sequence and structure characteristics conserved in all aligned SOD sequences or in subsets sharing common oligomeric and/or metal specificities was performed. Several residues were identified as guaranteeing the common function and dimeric conformation, others as determining the tetramer formation, and yet others as potentially responsible for metal specificity. Some form cation-π interactions between an aromatic ring and a fully or partially positively charged group, suggesting that these interactions play a significant role in the structure and function of SOD enzymes. Dimer/tetramer- and iron/manganese-specific fingerprints were derived from the set of conserved residues; they can be used to propose selected residue substitutions in view of the experimental validation of our in silico derived hypotheses.
Annals of the New York Academy of Sciences | 2003
Olivier Chose; Claude-Olivier Sarde; Christophe Noël; Delphine Gerbod; Juan-Carlos Jimenez; Catherine Brenner; Monique Capron; Eric Viscogliosi; Alberto Roseto
Abstract: Some protozoans, such as Trichomonad species, do not possess mitochondria. Most of the time, they harbor another type of membrane‐bounded organelle, called hydrogenosome from its capacity to produce H2. This is the case for the human parasite Trichomonas vaginalis. Some other parasites, such as the protist Giardia lamblia, do not harbor any of these organelles. From this observation arises naturally a naive question: How do cells die when the mitochondrion, the cornerstone of apoptotic process, is absent? Data strongly suggest that the mitochondrion and the hydrogenosome arose from a common ancestral endosymbiont. But hydrogenosomes do not appear to directly substitute for mitochondria in apoptotic functions. Thus, it appears judicious to examine more closely the genome of unicellular cells, which do not harbor mitochondria, and search for new molecules that could participate in the apoptotic process in these microorganisms.
Journal of Eukaryotic Microbiology | 2001
Christophe Noël; Delphine Gerbod; Naomi M. Fast; René Wintjens; Pilar Delgado-Viscogliosi; W. Ford Doolittle; Eric Viscogliosi
Abstract We have isolated and analysed an α-tubulin-encoding gene (atub1) in an early-diverging eukaryote, Trichomonas vaginalis. The complete atub1 open reading frame included 1,356 bp encoding a polypeptide of 452 amino-acyl residues. A second α-tubulin gene (atub2) was amplified by PCR using primers derived from consensus α-tubulin amino acid sequences. Both T. vaginalis α-tubulin sequences showed high identity to those described in other parabasalids (94.4%–97.3%), and exhibited a high degree of similarity to sequences from Metazoa (such as pig brain) and diplomonads (such as Giardia). Despite large evolutionary distances previously observed between trichomonads and mammals, the three-dimensional model of the T. vaginalis tubulin dimer was very similar to that of pig brain. Possible correlations between α-tubulin sequences and posttranslational modifications (PTMs) were examined. Our observations corroborated previous data obtained in T. vaginalis using specific anti-PTMs antibodies. As described in the related species Tritrichomonas mobilensis, microtubules are likely acetylated, non-tyrosinated, glutamylated, and non-glycylated in T. vaginalis. Evolutionary considerations concerning the time of appearance of these tubulin PTMs are also discussed since trichomonads are potentially one of the earliest diverging eukaryotic lineages.
Free Radical Biology and Medicine | 2006
Fabienne Dufernez; Cédric Yernaux; Delphine Gerbod; Christophe Noël; Mélanie Chauvenet; René Wintjens; Virginia P. Edgcomb; Monique Capron; Frederik Opperdoes; Eric Viscogliosi
Experimental Cell Research | 2002
Olivier Chose; Christophe Noël; Delphine Gerbod; Catherine Brenner; Eric Viscogliosi; Alberto Roseto
Molecular Phylogenetics and Evolution | 2004
Delphine Gerbod; Emily Sanders; Shigeharu Moriya; Christophe Noël; Hirotoshi Takasu; Naomi M. Fast; Pilar Delgado-Viscogliosi; Moriya Ohkuma; Toshiaki Kudo; Monique Capron; Jeffrey D. Palmer; Patrick J. Keeling; Eric Viscogliosi
Molecular Phylogenetics and Evolution | 2002
Delphine Gerbod; Christophe Noël; Michael F. Dolan; Virginia P. Edgcomb; Osamu Kitade; Satoko Noda; Fabienne Dufernez; Moriya Ohkuma; Toshiaki Kudo; Monique Capron; Mitchell L. Sogin; Eric Viscogliosi