Acute and 28-day subchronic toxicity studies of mangiferin, a glucosyl xanthone isolated from Mangifera indica L. stem bark

Prado, Y; Merino, N; Acosta, J.; Herrera, JA; Luque Y.; Hernandez, I; Prado E.; Garrido G.; Delgado, R; Rodeiro I.

Keywords: mangiferin, xanthone, Acute dose, repetitive toxicity assay, toxicological studies

Abstract

Context: Pharmacological properties of mangiferin have been reported, but few studies have investigated mangiferin toxicity. Aims: To study the acute and 28-day toxicity effects of mangiferin in rodents. Methods: Single doses of mangiferin were administered by oral or i.p. route or were applied dermally to Sprague-Dawley rats and Balb/C mice. Clinical symptoms of animals were observed during 14 days after treatment. Animals also received single oral doses daily for 28 consecutive days. Blood biochemistry, hematology and pathology findings were reported. Results: In the acute study, no toxic effects were observed after dermal exposure to mangiferin 2000 mg/kg but transient dyspnea, flank position and piloerection were observed after oral administration to this xanthone. I.p. administration induced similar toxicity signs, but at the highest dose (2000 mg/kg) all mice, one female rat and one male rat died. Rats orally treated with mangiferin (250-1000 mg/kg) for 28 days did not show any abnormal clinical signs or hematology alterations, when compared to control group animals. Histopathological alterations like vacuolar degeneration, necrosis and increment of apoptosis of the acinar cells were observed in the exocrine pancreas of rats at 1000 mg/kg. This suggesting that exocrine pancreas was the target organ for mangiferin's toxicity. Conclusions: These studies indicated that acute and subchronic toxicities of mangiferin for oral exposure are low.

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Título de la Revista: JOURNAL OF PHARMACY AND PHARMACOGNOSY RESEARCH
Volumen: 3
Número: 1
Editorial: JOURNAL PHARMACY & PHARMACOGNOSY RESEARCH-JPPRES
Fecha de publicación: 2015
Página de inicio: 13
Página final: 23
Idioma: English
Notas: WOS-ESCI