Your search keyword '"Gerbod D"' showing total 3 results

1. Programmed cell death in parasitic protozoans that lack mitochondria.

Author

Chose O, Sarde CO, Gerbod D, Viscogliosi E, and Roseto A

Subjects

Animals, Mitochondria physiology, Necrosis, Symbiosis physiology, Trichomonas vaginalis physiology, Apoptosis physiology, Biological Evolution, Eukaryota physiology

Published

2003

2. Cell death in protists without mitochondria.

Author

Chose O, Sarde CO, Noël C, Gerbod D, Jimenez JC, Brenner C, Capron M, Viscogliosi E, and Roseto A

Subjects

Animals, Eukaryota ultrastructure, Giardia lamblia cytology, Giardia lamblia physiology, Humans, Hydrogen metabolism, Symbiosis, Trichomonas vaginalis cytology, Trichomonas vaginalis physiology, Apoptosis physiology, Cell Death physiology, Eukaryota physiology, Mitochondria physiology

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 H(2). 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.

Published

2003

3. A form of cell death with some features resembling apoptosis in the amitochondrial unicellular organism Trichomonas vaginalis.

Author

Chose O, Noël C, Gerbod D, Brenner C, Viscogliosi E, and Roseto A

Subjects

Animals, Apoptosis Inducing Factor, Carrier Proteins metabolism, Cell Death, Cell Nucleus ultrastructure, DNA Fragmentation, Flavoproteins analysis, Membrane Proteins analysis, Mitochondria physiology, Nucleosomes ultrastructure, Phosphatidylserines analysis, Trichomonas vaginalis chemistry, Trichomonas vaginalis ultrastructure, Apoptosis, Protozoan Proteins, Trichomonas vaginalis cytology

Abstract

One of hallmarks of apoptosis is the degradation and concomitant compaction of chromatin. It is assumed that caspases and caspase-independent pathways are rate limiting for the development of nuclear apoptosis. The caspase-independent pathway involves apoptosis-inducing factor (AIF) and leads to DNA fragmentation and peripheral chromatin condensation. Both pathways are the result of activation of death signals that the mitochondrion receives, integrates, and responds to with the release of various molecules (e.g., cytochrome c and AIF). In fact, both pathways have in common the final point of the DNA fragmentation and the mitochondrial origin of molecules that initiate the apoptotic events. Here, we examine the question of whether apoptosis or apoptotic-like processes exist in a unicellular organism that lacks mitochondria. We herein show that a form of cell death with some features resembling apoptosis is indeed present in Trichomonas vaginalis. Characterization of morphological aspects implicated in this event together with the preliminary biochemical data provided may lead to new insight about the evolutionary relationships between the different forms of programmed cell death identified so far.

Published

2002