Genotoxicity assessment of the novel antitussive agent Benzonatate and its major metabolite

Steve Teo; Wannie Madraymootoo; Emily Dakoulas; Rohan Kulkarni; Marie McKeon

doi:10.1016/j.mrgentox.2018.03.007

Genotoxicity assessment of the novel antitussive agent Benzonatate and its major metabolite

Mutat Res Genet Toxicol Environ Mutagen. 2018 May-Jun:829-830:19-25. doi: 10.1016/j.mrgentox.2018.03.007. Epub 2018 Mar 21.

Authors

Steve Teo¹, Wannie Madraymootoo², Emily Dakoulas², Rohan Kulkarni², Marie McKeon²

Affiliations

¹ Pfizer Inc., Madison, NJ, United States. Electronic address: steve.teo@pfizer.com.
² MilliporeSigma BioReliance(®) Toxicology Services, Rockville, MD, United States.

PMID: 29704989
DOI: 10.1016/j.mrgentox.2018.03.007

Abstract

Benzonatate (TESSALON^®) is a peripherally acting oral antitussive. It undergoes rapid ester hydrolysis producing 4-(butylamino) benzoic acid (BBA) and methylated polyethylene glycol (MPG) metabolites, which are eliminated in urine and feces. The nonclinical and clinical efficacy of Benzonatate has been demonstrated over the last 60 years, but its safety was not fully assessed. In this study, we tested the genotoxicity of Benzonatate and its major metabolite BBA in an in vitro bacterial reverse mutation and in vivo micronucleus assays. A chromosomal aberration assay was also performed on Benzonatate and BBA. In the reverse mutation assay, Benzonatate and BBA doses 1.5-5000 μg/plate ± S9 metabolic activation were used and the numbers of revertants/plate were compared to various controls. Chromosomal aberration assays with human peripheral blood lymphocytes used Benzonatate and BBA concentrations 25-2000 and 62.5-1930 μg/mL, respectively. A CByB6F1 mouse bone marrow micronucleus assay was performed as part of a 28-day oral toxicology study at up to 250 mg/kg/day. The frequencies of micronuclei in polychromatic erythrocytes in treated groups were compared with the control group. Neither Benzonatate nor BBA induced significant mutagenicity in any of the bacterial strains, with or without metabolic activation. They also did not produce any biologically relevant structural or numerical aberrations in human chromosomes. Benzonatate and its BBA and MPG metabolites rapidly produced from esterase activity did not produce any significant increase in the incidence of micronucleated polychromatic erythrocytes. In conclusion, Benzonatate and its major metabolite BBA were not mutagenic and did not cause numerical or structural chromosome alterations. While the MPG metabolite was not tested, studies on structural analogues indicated it was also unlikely to be genotoxic. This was supported by oral rodent carcinogenicity assays showing no increase in malignancies.

Keywords: Ames; Benzonatate; Carcinogenicity; Chromosomal aberration; Mouse micronucleus.

MeSH terms

Adult
Animals
Antitussive Agents / toxicity*
Bone Marrow Cells / cytology
Bone Marrow Cells / drug effects*
Butylamines / toxicity*
Chromosome Aberrations
Dose-Response Relationship, Drug
Escherichia coli / drug effects
Escherichia coli / genetics
Female
Humans
Lymphocytes / cytology
Lymphocytes / drug effects*
Male
Mice
Micronuclei, Chromosome-Defective / chemically induced
Micronucleus Tests
Mutagenicity Tests
Salmonella typhimurium / drug effects
Salmonella typhimurium / genetics
Young Adult

Substances

Antitussive Agents
Butylamines
benzonatate