Gastric mucosal damage following repeat administration of melanocortin subtype-4 receptor ligands to Fischer 344 rats

Since the melanocortin system plays a role in the central control of feeding, melanocortin receptor ligands may be efficacious in treating human obesity. Ten structurally similar melanocortin subtype-4 receptor (MC4R) ligands from an aryl piperazine chemical platform were evaluated in female Fischer...

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Published inToxicologic pathology Vol. 34; no. 6; p. 738
Main Authors Williams, Tracy M, Donnelly, Kevin B
Format Journal Article
LanguageEnglish
Published United States 01.10.2006
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Abstract Since the melanocortin system plays a role in the central control of feeding, melanocortin receptor ligands may be efficacious in treating human obesity. Ten structurally similar melanocortin subtype-4 receptor (MC4R) ligands from an aryl piperazine chemical platform were evaluated in female Fischer 344 rats to assess the toxicity of this class of compounds. Rats were orally gavaged with 100, 250, or 500 mg/kg of each compound in 10% acacia and purified water daily for 4 days. In treated rats, notable clinical observations included a dose-dependent decrease in mean body weight and food consumption. A morphologically unique compound-related histologic lesion occurred in the nonglandular gastric mucosa. The lesions consisted of multiple, raised, sometimes ulcerated, white foci which, microscopically, were discrete, intraepithelial vesicles containing dense accumulations of neutrophils continuous with inflammation in the submucosa. Ruptured vesicles resulted in ulcers and occasionally gastric perforation. The morphologic characteristics of this acute lesion were described and concluded to be a direct toxicity of the compounds unrelated to melanocortin-mediated pharmacology.
AbstractList Since the melanocortin system plays a role in the central control of feeding, melanocortin receptor ligands may be efficacious in treating human obesity. Ten structurally similar melanocortin subtype-4 receptor (MC4R) ligands from an aryl piperazine chemical platform were evaluated in female Fischer 344 rats to assess the toxicity of this class of compounds. Rats were orally gavaged with 100, 250, or 500 mg/kg of each compound in 10% acacia and purified water daily for 4 days. In treated rats, notable clinical observations included a dose-dependent decrease in mean body weight and food consumption. A morphologically unique compound-related histologic lesion occurred in the nonglandular gastric mucosa. The lesions consisted of multiple, raised, sometimes ulcerated, white foci which, microscopically, were discrete, intraepithelial vesicles containing dense accumulations of neutrophils continuous with inflammation in the submucosa. Ruptured vesicles resulted in ulcers and occasionally gastric perforation. The morphologic characteristics of this acute lesion were described and concluded to be a direct toxicity of the compounds unrelated to melanocortin-mediated pharmacology.
Author Donnelly, Kevin B
Williams, Tracy M
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PublicationTitle Toxicologic pathology
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Snippet Since the melanocortin system plays a role in the central control of feeding, melanocortin receptor ligands may be efficacious in treating human obesity. Ten...
SourceID pubmed
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StartPage 738
SubjectTerms Animals
Anti-Obesity Agents - toxicity
Body Weight - drug effects
Cell Line
Cell Survival - drug effects
Dose-Response Relationship, Drug
Eating - drug effects
Female
Gastric Mucosa - drug effects
Gastric Mucosa - pathology
Inhibitory Concentration 50
Ligands
Muscle, Skeletal - drug effects
Muscle, Skeletal - pathology
Piperazines - toxicity
Rats
Rats, Inbred F344
Receptor, Melanocortin, Type 4 - agonists
Stomach Ulcer - chemically induced
Stomach Ulcer - pathology
Title Gastric mucosal damage following repeat administration of melanocortin subtype-4 receptor ligands to Fischer 344 rats
URI https://www.ncbi.nlm.nih.gov/pubmed/17162531
Volume 34
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