Grandisin induces apoptosis in leukemic K562 cells

Abstract In this study, the potential antileukemic activity of grandisin, a lignan extracted from Piper solmsianum, was evaluated against the leukemic line K562. The cytotoxicity of grandisin (0.018 to 2.365 µM) was evaluated in K562 and normal peripheral blood lymphocytes by Trypan Blue Exclusion and MTT methods after 48h exposure to the drug. In both methods, cellular viability was concentration-dependent and the IC50 values were lower than 0.85µM. Analysis of K562 cells after treatment with grandisin showed that the cell cycle was arrested in the G1 phase with a 12.31% increase, while both S and G2 phases decreased. Morphological studies conducted after the exposure of K562 to grandisin revealed changes consistent with the apoptosis process, which was confirmed by anexin V stain and caspase activation. Thus, lignan grandisin showed antileukemic activities against the K562 cell line and the cell death process occurred via apoptosis.

Actividad tripanocida de Piper solmsianum C. DC. sobre formas epimastigota y tripomastigota de Trypanosoma cruzi / Trypanocidal activity of Piper solmsianum C. DC. against epimastigote and trypomastigote forms of Trypanosoma cruzi

Introducción: la infección por Trypanosoma cruzi, conocida como enfermedad de Chagas, es un problema importante de salud pública en países de América Central y Sudamérica.Objetivo: evaluar la actividad de extractos crudos de acetato de etilo de plantas in vitro de 6-8 meses y 10-12 meses de edad, de tallos leñosos y hojas de plantas silvestres maduras y el lignano tetrahidrofurano grandisina, aislados de Piper solmsianum, sobre las formas epimastigota y tripomastigota de T. cruzi in vitro.Métodos: en la evaluación del efecto de diversos extractos crudos de acetato de etilo y grandisina de P. solmsianum, sobre la viabilidad de las formas epimastigota y tripomastigota de T. cruzi, se utilizó el método MTT (3-(4,5-dimetiltiazol-2-il)-2,5-difeniltetrazolium bromuro).Resultados: en la forma epimastigota, el mejor resultado en la inhibición del crecimiento fue obtenido con 50 µg/mL de extracto de tallo y en la forma tripomastigota con 25 y 50 µg/mL de grandisina y plantas in vitro de 6-8 meses de edad, respectivamente. En todos los casos los valores de inhibición oscilaron entre 86 a 96 por ciento. Plantas in vitro de 6-8 meses de edad y grandisina fueron más activas sobre las formas epimastigota y tripomastigota de T. cruzi con valores de CI50 de 0,018 y 0,360 µg/mL, respectivamente.Conclusiones: se demuestra la actividad tripanocida de extractos de plantas silvestres y plantas in vitro de P. solmsianum(AU)

Introduction: the infection by Trypanosoma cruzi, known as Chagas' disease, poses a major public health problem in Central and South America countries.Objective: to evaluate the activity of crude ethyl acetate extracts from in vitro plants of 6-8 and 10-12 months of age, stem barks and mature wild plant leaves and tetrahydrofuran lignin grandisin isolated from Piper solmsianum against the epimastigote and trypomastigote forms of T. cruzi in vitro.Methods: in the evaluation of the effect of various crude ethyl acetate extracts and grandisin from P. solmsianum on the viability of epimastigote and trypomastigote forms of T. cruzi, the MTT method (3-(4,5-dimethylthiazol-2-il)-2,5-diphenyltetrazolium bromide) was used.Results: in the epimastigote form, the best results in growth inhibition was obtained with 50 µg/mL of stem extract, and in the trypomastigote form, with 25 and 50 µg/mL of grandisin and 6-8 months-old in vitro plants, respectively. The inhibition values in all cases ranged from 86 to 96 percent. 6-8 months old in vitro plants and grandisin were found to be active against the epimastigote and trypomastigote forms of T. cruzi with IC50 of 0.018 µg/mL and 0.360 µg/mL, respectively.Conclusions: the trypanocidal activity of extracts from wild plants and in vitro plants of P. solmsianum was proved(AU)

Development and characterization of PLGA nanocapsules of grandisin isolated from Virola surinamensis: in vitro release and cytotoxicity studies

The most studied phyto constituent isolated from Virola surinamensis (Rol. ex Rottb.) Warb., Myristicaceae, is the tetrahydrofuran neolignan grandisin, which exhibits a series of biological activities, including trypanocidal, larvicidal and antitumoral. Due to its extremely low solubility, additional studies, including in vivo investigations are challenged by the difficulties in the development of an effective drug delivery system for grandisin. The encapsulation in polymeric nanoparticles is a very attractive alternative for overcoming some of these limitations. In this work, PLGA nanocapsules loaded with grandisin were developed in an attempt to optimize the efficacy of grandisin as an antitumoral drug, with high drug loading and efficiency, prolonged drug release and increased physical-chemical stability. Mean diameter of the nanocapsules was lower than 200 nm, with very low polydispersity. Encapsulation efficiency was above 90%. A sustained in vitro drug release was achieved for up to twenty days and cytotoxicity was markedly increased (IC50 for grandisin-NC and grandisin were 0.005 µM and 0.078 µM, respectively), indicating that polymeric nanocapsules are a potential drug delivery system for grandisin allowing the preparation of formulations viable for further in vivo studies.