A Pharmacokinetic Study of Mix-160 by LC-MS/MS: Oral Bioavailability of a Dosage Form of Citroflavonoids Mixture
Jesús Alfredo Araujo-León,
Rolffy Ortiz-Andrade,
Efrén Hernández-Baltazar,
Emanuel Hernández-Núñez,
Julio César Rivera-Leyva,
Víctor Yáñez-Pérez,
Priscila Vazquez-Garcia,
Carla Georgina Cicero-Sarmiento,
Juan Carlos Sánchez-Salgado,
Maira Rubí Segura-Campos
Affiliations
Jesús Alfredo Araujo-León
Laboratorio de Cromatografía, Facultad de Química, Universidad Autónoma de Yucatán, Merida 97069, Mexico
Rolffy Ortiz-Andrade
Laboratorio de Farmacología, Facultad de Química, Universidad Autónoma de Yucatán, Merida 97069, Mexico
Efrén Hernández-Baltazar
Laboratorio de Tecnología Farmacéutica, Facultad de Farmacia, Universidad Autónoma del Estado de Morelos, Cuernavaca 62209, Mexico
Emanuel Hernández-Núñez
Departamento de Recursos del Mar, Centro de Investigación y de Estudios Avanzados del Instituto Politécnico Nacional-Unidad Mérida, Merida 97205, Mexico
Julio César Rivera-Leyva
Laboratorio 4, Facultad de Farmacia, Universidad Autónoma del Estado de Morelos, Cuernavaca 62209, Mexico
Víctor Yáñez-Pérez
Bioterio de la Escuela de Medicina, Universidad Anáhuac-Mayab, Merida 97302, Mexico
Priscila Vazquez-Garcia
Laboratorio de Cromatografía, Facultad de Química, Universidad Autónoma de Yucatán, Merida 97069, Mexico
Carla Georgina Cicero-Sarmiento
Laboratorio de Farmacología, Facultad de Química, Universidad Autónoma de Yucatán, Merida 97069, Mexico
Juan Carlos Sánchez-Salgado
Hypermedic MX, Ciudad de Mexico 04930, Mexico
Maira Rubí Segura-Campos
Facultad de Ingeniería Química, Universidad Autónoma de Yucatán, Merida 97203, Mexico
This study was performed to evaluate and compare the pharmacokinetic parameters between two dosage formulations of hesperidin and naringenin: mixture and tablet. Our objective was to determine that the flavonoid tablet does not significantly modify the pharmacokinetic parameters compared with the mixture. For this study, we administered 161 mg/kg of either mixture (Mix-160) or tablet composed of hesperidin and by intragastric administration. Blood microsamples were collected from tail vein up to 24 h. Serum flavonoid extraction was performed by solid phase extraction and analyzed by LC-MS/MS of triple quadrupole (QqQ). Serum concentration vs. time plot showed that data fitted for a first-order model. The pharmacokinetic parameters were calculated by a noncompartmental model. The results showed that the absorption constant is higher than the elimination constant. The first concentration was found at five minutes, and minimal concentration at 24 h after administration, suggesting a enterohepatic recirculation phenomena and regulation of liver cytochromes’ activity. We did not find meaningful differences between the pharmacokinetic parameters of both samples. We concluded that tablet form did not interfere with the bioavailability of hesperidin and naringenin, and it could be a suitable candidate for developing a drug product.
