Nathalie J. Morin scite author profile

Nathalie J. Morin

4Publications

22Citation Statements Received

73Citation Statements Given

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Affiliations

Université Laval, University of Mons, Centre hospitalier de l'Université Laval

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Temporal variation in nephrotoxicity of low doses of isepamicin in rats

Yoshiyama¹,

Grenier²,

Gourde³

et al. 1996

Antimicrob Agents Chemother

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The temporal variation in the nephrotoxicity of low doses of isepamicin was studied in male Sprague-Dawley rats treated with a single daily intraperitoneal injection of saline (NaCl, 0.9%) or isepamicin (80 mg/kg of body weight) at either 0800, 1400, 2000, or 0200 h for 4 and 10 days. On day 10, the cellular regeneration (incorporation of [3H] thymidine into DNA of renal cortex) and cortical accumulation of isepamicin were significantly higher in animals treated at 1400 h than at 0200 h (P < 0.01). Immunogold labeling studies showed that isepamicin was essentially localized in the lysosomes of proximal tubular cells in all treated groups, but the density of the gold particles over the lysosomes was higher in animals treated at 1400 than at 0200 h. The results of the present study show that the renal toxicity of isepamicin was maximal at 1400 h (midlight period) and minimal at 0200 h (middark period).

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Potentiation of Gentamicin Nephrotoxicity in the Rat by Infusion of Aprotinin

Morin

Frau

Nonclercq

et al. 1994

Experimental and Molecular Pathology

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Differential distributions in tissues and efficacies of aztreonam and ceftazidime and in vivo bacterial morphological changes following treatment

Turcotte

Simard

Morin

et al. 1997

Antimicrob Agents Chemother

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The differential tissue distributions of aztreonam and ceftazidime within fibrin clots infected with Pseudomonas aeruginosa, Enterobacter cloacae, and Serratia marcescens, their efficacies, and the in vivo bacterial morphological changes induced by these drugs were evaluated. Rabbits were given intravenously a single dose of 100 mg of either agents/kg of body weight. In the cores of the clots, the peak levels of both drugs were much lower than those observed in the peripheries and in serum. Aztreonam's half-lives within the peripheries and in the cores of the fibrin clots were up to six times higher than that observed in serum, while ceftazidime's half-lives in clots were twice that observed in serum. This resulted in a much greater penetration ratio for aztreonam than for ceftazidime. Both drugs controlled the growth of P. aeruginosa in vivo, but E. cloacae and S. marcescens responded better to ceftazidime. Morphological changes were more abundant in the peripheries than in the cores of the clots. In the control group, P. aeruginosa's morphology in the cores was different than that in the peripheries of the clots. Against P. aeruginosa, aztreonam did induce morphological changes in the cores while ceftazidime did not. Electron microscopic studies revealed that morphological changes associated with aztreonam seemed different than those of ceftazidime. Along with elongation of bacteria, more bow tie and herniated bacteria were observed with aztreonam. Though both agents selectively affect PBP 3, as manifested by elongated bacteria, they induce in the peripheries of the clots thickening, breaks, and detachment in bacterial cell walls, alterations which are generally associated with antibiotics affecting PBP 1a and 1b.

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Relationship between intrarenal Distribution and Efficacy of Fleroxacin in the Treatment of Escherichia coli Pyelonephritis in Rats

Leclerc

Morin

Bergeron

et al. 1998

Journal of Infection and Chemotherapy

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Nathalie J. Morin

Temporal variation in nephrotoxicity of low doses of isepamicin in rats

Potentiation of Gentamicin Nephrotoxicity in the Rat by Infusion of Aprotinin

Differential distributions in tissues and efficacies of aztreonam and ceftazidime and in vivo bacterial morphological changes following treatment

Relationship between intrarenal Distribution and Efficacy of Fleroxacin in the Treatment of Escherichia coli Pyelonephritis in Rats

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