Your search keyword '"Abram MC"' showing total 3 results

1. Preferential decorporation of americium by pulmonary administration of DTPA dry powder after inhalation of aged PuO(2) containing americium in rats.

Author

Grémy O, Tsapis N, Chau Q, Renault D, Abram MC, and Van der Meeren A

Subjects

Animals, Chelating Agents administration & dosage, Chelating Agents pharmacology, Lung metabolism, Male, Plutonium chemistry, Powders, Pulmonary Alveoli drug effects, Pulmonary Alveoli metabolism, Rats, Rats, Sprague-Dawley, Time Factors, Americium pharmacokinetics, Inhalation, Lung drug effects, Lung physiology, Pentetic Acid administration & dosage, Pentetic Acid pharmacology, Plutonium pharmacokinetics

Abstract

After inhalation of plutonium oxides containing various percentages of americium in rats, we identified an acellular transient pulmonary compartment, the epithelial lining fluid (ELF), in which a fraction of actinide oxides dissolve prior to absorption and subsequent extrapulmonary deposit. Chelation therapy is usually considered to be poorly efficient after inhalation of actinide oxides. However, in the present study, prompt pulmonary administration of diethylenetraminepentaacetic acid (DTPA) as a dry powder led to a decrease in actinide content in ELF together with a limitation of bone and liver deposits. Because americium is more soluble than plutonium, higher amounts of americium were found in ELF, extrapulmonary tissues and urine. Our results also demonstrated that the higher efficacy of DTPA on americium compared to plutonium in ELF induced a preferential inhibition of extrapulmonary deposit and a greater urinary excretion of americium compared to plutonium. All together, our data justify the use of an early and local DTPA treatment after inhalation of plutonium oxide aerosols in which americium can be in high proportion such as in aged compounds.

Published

2010

2. Simplified structure of a new model to describe urinary excretion of plutonium after systemic, liver or pulmonary contamination of rats associated with Ca-DTPA treatments.

Author

Fritsch P, Sérandour AL, Grémy O, Phan G, Tsapis N, Abram MC, Renault D, Fattal E, Benech H, Deverre JR, and Poncy JL

Subjects

Analysis of Variance, Animals, Autoradiography, Bone and Bones chemistry, Bone and Bones drug effects, Bone and Bones radiation effects, Citric Acid toxicity, Feces chemistry, Half-Life, Kinetics, Liver chemistry, Liver drug effects, Liver radiation effects, Lung chemistry, Lung drug effects, Lung radiation effects, Male, Pentetic Acid administration & dosage, Pentetic Acid chemistry, Plutonium analysis, Plutonium chemistry, Radiation Injuries, Experimental urine, Radiation-Protective Agents administration & dosage, Rats, Rats, Sprague-Dawley, Time Factors, Models, Biological, Pentetic Acid therapeutic use, Plutonium toxicity, Plutonium urine, Radiation Injuries, Experimental prevention & control, Radiation-Protective Agents therapeutic use

Abstract

This study validates, by targeted experiments, several modeling hypotheses for interpretation of urinary excretion of plutonium after Ca-DTPA treatments. Different formulations and doses of Ca-DTPA were administered to rats before or after systemic, liver or lung contamination with various chemical forms of plutonium. The biokinetics of plutonium was also characterized after i.v. injection of Pu-DTPA. Once formed, Pu-DTPA complexes are stable in most biological environments. Pu-DTPA present in circulating fluids is rapidly excreted in the urine, but 2-3% is retained, mainly in soft tissues, and is then excreted slowly in the urine after transfer to blood. Potentially, all intracellular monoatomic forms of plutonium could be decorporated after DTPA internalization involving slow urinary excretion of Pu-DTPA with half-lives varying from 2.5 to 6 days as a function of tissue retention. The ratio of fast to slow urinary excretion of Pu-DTPA depends on both plutonium contamination and Ca-DTPA treatment. Fast urinary excretion of Pu-DTPA corresponds to extracellular decorporation that occurs beyond a threshold of the free DTPA concentration in circulating fluids. Slow excretion corresponds mostly to intracellular decorporation and depends on the amount of intracellular DTPA. From these results, the structure of a simplified model is proposed for interpretation of data obtained with Ca-DTPA treatments after systemic, wound or pulmonary contamination by plutonium.

Published

2009

3. Activation of alveolar macrophages after plutonium oxide inhalation in rats: involvement in the early inflammatory response.

Author

Van der Meeren A, Tourdes F, Grémy O, Grillon G, Abram MC, Poncy JL, and Griffiths N

Subjects

Animals, Bronchoalveolar Lavage Fluid cytology, Chemokine CCL2 biosynthesis, Chemokine CXCL2 biosynthesis, Dose-Response Relationship, Drug, Inhalation Exposure, Male, Rats, Tumor Necrosis Factor-alpha biosynthesis, Inflammation etiology, Macrophage Activation drug effects, Macrophages, Alveolar drug effects, Plutonium toxicity

Abstract

Alveolar macrophages play an important role in the distribution, clearance and inflammatory reactions after particle inhalation, which may influence long-term events such as fibrosis and tumorigenesis. The objectives of the present study were to investigate the early inflammatory events after plutonium oxide inhalation in rats and involvement of alveolar macrophages. Lung changes were studied from 3 days to 3 months after inhalation of PuO2 of different isotopic compositions (70% or 97% 239Pu) and initial lung deposits (range 2.1 to 43.4 kBq/rat). Analyses of bronchoalveolar lavages showed early increases in the numbers of granulocytes, lymphocytes and multinucleated macrophages. The activation of macrophages was evaluated ex vivo by measurement of inflammatory mediator levels in culture supernatants. TNF-alpha and chemokine MCP-1, MIP-2 and CINC-1 production was elevated from 7 days after inhalation and remained so up to 3 months. In contrast, IL-1beta, IL-6 and IL-10 production was unchanged. At 6 weeks, pulmonary macrophage numbers and activation state were increased as observed from an immunohistochemistry study of lung sections with anti-ED1. Similarly, histological analyses of lung sections also showed evidence of inflammatory responses. In conclusion, our results indicate early inflammatory changes in the lungs of PuO2-contaminated animals and the involvement of macrophages in this process. A dose-effect relationship was observed between the amount of radionuclide inhaled or retained at the time of analysis and inflammatory mediator production by alveolar macrophages 14 days after exposure. For similar initial lung deposits, the inflammatory manifestation appears higher for 97% 239Pu than for 70% 239Pu.

Published

2008