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Dive into the research topics where Jean Pommery is active.

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Featured researches published by Jean Pommery.


Biomedical Chromatography | 1999

Colchicine poisoning: report of a fatal case with body fluid and post-mortem tissue analysis by high-performance liquid chromatography

Betty Dehon; Jean-Luc Chagnon; Elisabeth Vinner; Jean Pommery; Daniel Mathieu; Michel Lhermitte

A case involving a suicide by the ingestion of colchicine tablets is presented. Liquid chromatography has been used to measure the drug level in blood and in post-mortem tissues of the patient (a 42-year-old man). Plasma concentration 24 h after ingestion was 4.5 ng/mL. On autopsy, the kidney showed the highest concentration (396 ng/g). High concentrations were also found in the liver (347 ng/g) and heart (334 ng/g). Low concentrations were detected in the lung (58 ng/g), muscle (10 ng/g) and brain (5 ng/g).


Clinical Toxicology | 1993

Atrazine in Plasma and Tissue Following Atrazine-Aminotriazole-Ethylene Glycol-Formaldehyde Poisoning

Jean Pommery; Monique Mathieu; Daniel Mathieu; Michel Lhermitte

A high performance liquid chromatography method has been used to study the plasma kinetics of atrazine in a human fatality after ingestion of a herbicide mix containing atrazine, aminotriazole, ethylene glycol and formaldehyde. A hemodialysis was performed in an effort to eliminate these toxic substances. The mean atrazine clearance over 4 h was 250 mL/min and the dialysance of atrazine was calculated as 76%. On autopsy, the kidney showed the highest concentration of atrazine (97.62 micrograms/g-1 wet tissue) with lesser concentrations in the lung, small intestine and liver, and the lowest concentration in the heart.


Heterocycles | 2006

Expeditious synthesis of 2-aryl substituted imidazolines and imidazoles

Sylvia Lauwagie; Régis Millet; Jean Pommery; Patrick Depreux; Jean-Pierre Hénichart

A versatile and efficient method for the synthesis of 2-aryl substituted imidazolines and imidazoles bearing a carboxylate group on C-4 is reported. Three different synthetic pathways were explored, compared and optimized. The selected procedure involves condensation of methyl 2,3-diaminopropionate with different imino ethers. The ring closure, monitored by LC-MS analysis, was facilitated by heating at reflux in ethanol leading to increase the rate of cyclization.


Cancer Chemotherapy and Pharmacology | 1991

High-performance liquid chromatography assay of bleomycin in human plasma and rat hepatocytes in culture

Rachid Mahdadi; Abdelraouf Kenani; Nicole Pommery; Jean Pommery; Jean-Pierre Hénichart; Michel Lhermitte

SummaryA sensitive and rapid linear-gradient, ionpaired, reversed-phase high-performance liquid chromatography technique using fluorescence detection was developed to quantify bleomycin (BLM) metabolites in the plasma of patients undergoing BLM therapy and in rat hepatocytes that had previously been incubated with 5×10−5m BLM. We could detect about 70 ng/ml using this procedure. BLM metabolites were assayed in the supernatant fractions of precipitated human plasma and in pellets of rat hepatocytes. Metabolite concentrations were below the level of detection in human plasma samples. In hepatocyte pellets, metabolites such as deamido-BLM A2 and deamido-BLM B2 were detected, indicating that isolated rat hepatocytes in culture can metabolize BLM analogues to the corresponding deamido-BLMs. The high-performance liquid chromatography procedure developed during this work can be used to study the metabolism of BLM in cell-culture systems.


Bioorganic & Medicinal Chemistry Letters | 2008

New NSAIDs-NO hybrid molecules with antiproliferative properties on human prostatic cancer cell lines.

Nicolas Bézière; Laurence Goossens; Jean Pommery; Hervé Vezin; Nadia Touati; Jean-Pierre Hénichart; Nicole Pommery

The design of profen hybrids containing a NO donor moiety connected to an aliphatic spacer led to compounds with a similar cyclooxygenase inhibition compared to their parent profen and with significant antiproliferative activities on PC3 cells. However, inhibition of COX-2 pathway alone did not seem sufficient to inhibit cancer cell proliferation, and NO-release in a time-dependent manner strongly contributes to this activity.


Medicinal Chemistry | 2012

Antioxidant Activity of New Benzo[de]quinolines and Lactams: 2DQuantitative Structure-Activity Relationships

Alina Ghinet; Amaury Farce; Souhila Oudir; Jean Pommery; Joseph Vamecq; Jean-Pierre Hénichart; Benoît Rigo; Philippe Gautret

In order to predict the antioxidant activity of 7 polycyclic lactams, a two dimensional quantitative-structure activity relationships (2D-QSAR) study based on a 5-descriptor model was performed. The synthetic compounds built from a condensed lactam scaffold were screened for their abilities to inhibit the autoxidation of pyrogallol, a superoxide anion radical-dependent process. The ketone 2 (8,9-dihydro-7H-benzo[de]pyrrolo[1,2-a]quinoline-7,10(7aH)-dione) exhibited the most potent antioxidant activity in vitro. The oxidation mechanism was proved by the isolation and characterization of alcohol 5 formed in the reaction of ketone 2 with dissolved oxygen in methanol.


Journal of Medicinal Chemistry | 2004

New COX-2/5-LOX inhibitors: apoptosis-inducing agents potentially useful in prostate cancer chemotherapy.

Nicole Pommery; Thierry Taverne; Aurélie Telliez; Laurence Goossens; Caroline Charlier; Jean Pommery; Jean-François Goossens; Raymond Houssin; François Durant; Jean-Pierre Hénichart


Journal of Medicinal Chemistry | 2004

Potent and Selective Farnesyl Transferase Inhibitors

Régis Millet; Juozas Domarkas; Raymond Houssin; Pauline Gilleron; Jean-François Goossens; Philippe Chavatte; Cédric Logé; Nicole Pommery; Jean Pommery; Jean-Pierre Hénichart


European Journal of Medicinal Chemistry | 2008

Synthesis and biological activities of a series of 4,5-diaryl-3-hydroxy-2(5H)-furanones

Fabrice Bailly; Clémence Queffélec; Gladys Mbemba; Jean-François Mouscadet; Nicole Pommery; Jean Pommery; Jean-Pierre Hénichart; Philippe Cotelle


Journal of Antimicrobial Chemotherapy | 1992

The binding of amikacin to macromolecules from the sputum of patients suffering from respiratory diseases

Véronique Bataillon; Michel Lhermitte; Jean-Jacques Lafitte; Jean Pommery; Philippe Roussel

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Gladys Mbemba

École normale supérieure de Cachan

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