Preclinical rodent toxicity studies for long term use of ceftriaxone

Preclinical rodent toxicity studies for long term use of ceftriaxone

A 6-months rodent toxicology and pharmacokinetic (PK) study was performed to provide supportive safety data for long-term use of intravenous ceftriaxone in a clinical trial in patients with amyotrophic lateral sclerosis (ALS). Ceftriaxone was administered by subcutaneous injection at up to 2 g/kg/da...

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Main Authors: Elena Ratti, James D. Berry, David J. Greenblatt, Lorena Loci, Amy Swartz Ellrodt, Jeremy M. Shefner, Merit E. Cudkowicz
Format: Article
Language:English
Published: Elsevier 2015-01-01
Series:Toxicology Reports
Subjects:
Ceftriaxone
Amyotrophic lateral sclerosis (ALS)
Rodent
Toxicology
Pharmacokinetics
Preclinical study
Online Access:http://www.sciencedirect.com/science/article/pii/S2214750015300640
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spelling doaj-995e71aa7ad644fdacb723b711f934522020-11-25T01:09:33ZengElsevierToxicology Reports2214-75002015-01-012C1396140310.1016/j.toxrep.2015.09.010Preclinical rodent toxicity studies for long term use of ceftriaxoneElena Ratti0James D. Berry1David J. Greenblatt2Lorena Loci3Amy Swartz Ellrodt4Jeremy M. Shefner5Merit E. Cudkowicz6Neurological Clinical Research Institute (NCRI), Massachusetts General Hospital, 165 Cambridge Street, Suite 600, Boston, MA 02114, USANeurological Clinical Research Institute (NCRI), Massachusetts General Hospital, 165 Cambridge Street, Suite 600, Boston, MA 02114, USATufts University School of Medicine, 136 Harrison Avenue, Boston, MA 02111, USANeurological Clinical Research Institute (NCRI), Massachusetts General Hospital, 165 Cambridge Street, Suite 600, Boston, MA 02114, USANeurological Clinical Research Institute (NCRI), Massachusetts General Hospital, 165 Cambridge Street, Suite 600, Boston, MA 02114, USAUpstate Medical University, 750 East Adams Street, Syracuse, NY 13210, USANeurological Clinical Research Institute (NCRI), Massachusetts General Hospital, 165 Cambridge Street, Suite 600, Boston, MA 02114, USAA 6-months rodent toxicology and pharmacokinetic (PK) study was performed to provide supportive safety data for long-term use of intravenous ceftriaxone in a clinical trial in patients with amyotrophic lateral sclerosis (ALS). Ceftriaxone was administered by subcutaneous injection at up to 2 g/kg/day to Sprague-Dawley Crl:CD (SD) rats. Ceftriaxone was found to be safe and well tolerated. Specifically, no significant differences in body weight and food consumption were observed between the treatment and control groups. With the exception of in red cell parameters decrease, there were no ceftriaxone-related changes in hematology, coagulation, clinical chemistry and urinalysis parameters. Injection site trauma and associated reversible anemia, likely due to chronic blood loss at the injection site, were all attributable to subcutaneous route of administration. Cecum dilatation and some skin changes were reversible after recovery period, while bile duct dilatation, observed only in a few animals, persisted. Changes in the non-glandular stomach do not have a human correlate. The no-observed-adverse-effect dose level (NOAEL) was 0.5 g/kg/day ceftriaxone in both sexes. Ceftriaxone showed rapid absorption with half-life values ranging between 1 and 1.5 h. Additionally, there was no evidence of accumulation and a virtually complete elimination by 16 h after the last dose. Overall there were no toxicologically meaningful drug-related animal findings associated with the long-term administration (6 months) of ceftriaxone. These results support safety of long-term use of ceftriaxone in human clinical trials.http://www.sciencedirect.com/science/article/pii/S2214750015300640CeftriaxoneAmyotrophic lateral sclerosis (ALS)RodentToxicologyPharmacokineticsPreclinical study
collection DOAJ
language English
format Article
sources DOAJ
author Elena Ratti
James D. Berry
David J. Greenblatt
Lorena Loci
Amy Swartz Ellrodt
Jeremy M. Shefner
Merit E. Cudkowicz
spellingShingle Elena Ratti
James D. Berry
David J. Greenblatt
Lorena Loci
Amy Swartz Ellrodt
Jeremy M. Shefner
Merit E. Cudkowicz
Preclinical rodent toxicity studies for long term use of ceftriaxone
Toxicology Reports
Ceftriaxone
Amyotrophic lateral sclerosis (ALS)
Rodent
Toxicology
Pharmacokinetics
Preclinical study
author_facet Elena Ratti
James D. Berry
David J. Greenblatt
Lorena Loci
Amy Swartz Ellrodt
Jeremy M. Shefner
Merit E. Cudkowicz
author_sort Elena Ratti
title Preclinical rodent toxicity studies for long term use of ceftriaxone
title_short Preclinical rodent toxicity studies for long term use of ceftriaxone
title_full Preclinical rodent toxicity studies for long term use of ceftriaxone
title_fullStr Preclinical rodent toxicity studies for long term use of ceftriaxone
title_full_unstemmed Preclinical rodent toxicity studies for long term use of ceftriaxone
title_sort preclinical rodent toxicity studies for long term use of ceftriaxone
publisher Elsevier
series Toxicology Reports
issn 2214-7500
publishDate 2015-01-01
description A 6-months rodent toxicology and pharmacokinetic (PK) study was performed to provide supportive safety data for long-term use of intravenous ceftriaxone in a clinical trial in patients with amyotrophic lateral sclerosis (ALS). Ceftriaxone was administered by subcutaneous injection at up to 2 g/kg/day to Sprague-Dawley Crl:CD (SD) rats. Ceftriaxone was found to be safe and well tolerated. Specifically, no significant differences in body weight and food consumption were observed between the treatment and control groups. With the exception of in red cell parameters decrease, there were no ceftriaxone-related changes in hematology, coagulation, clinical chemistry and urinalysis parameters. Injection site trauma and associated reversible anemia, likely due to chronic blood loss at the injection site, were all attributable to subcutaneous route of administration. Cecum dilatation and some skin changes were reversible after recovery period, while bile duct dilatation, observed only in a few animals, persisted. Changes in the non-glandular stomach do not have a human correlate. The no-observed-adverse-effect dose level (NOAEL) was 0.5 g/kg/day ceftriaxone in both sexes. Ceftriaxone showed rapid absorption with half-life values ranging between 1 and 1.5 h. Additionally, there was no evidence of accumulation and a virtually complete elimination by 16 h after the last dose. Overall there were no toxicologically meaningful drug-related animal findings associated with the long-term administration (6 months) of ceftriaxone. These results support safety of long-term use of ceftriaxone in human clinical trials.
topic Ceftriaxone
Amyotrophic lateral sclerosis (ALS)
Rodent
Toxicology
Pharmacokinetics
Preclinical study
url http://www.sciencedirect.com/science/article/pii/S2214750015300640
work_keys_str_mv AT elenaratti preclinicalrodenttoxicitystudiesforlongtermuseofceftriaxone
AT jamesdberry preclinicalrodenttoxicitystudiesforlongtermuseofceftriaxone
AT davidjgreenblatt preclinicalrodenttoxicitystudiesforlongtermuseofceftriaxone
AT lorenaloci preclinicalrodenttoxicitystudiesforlongtermuseofceftriaxone
AT amyswartzellrodt preclinicalrodenttoxicitystudiesforlongtermuseofceftriaxone
AT jeremymshefner preclinicalrodenttoxicitystudiesforlongtermuseofceftriaxone
AT meritecudkowicz preclinicalrodenttoxicitystudiesforlongtermuseofceftriaxone
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