Liposomal formulation of α-tocopheryl maleamide: In vitro and in vivo toxicological profile and anticancer effect against spontaneous breast carcinomas in mice

Tuřánek, Jaroslav; Wang, Xiufang; Knotigová, Pavlína Turánek; Koudelka, Štěpán; Dong, Lan-Feng; Vrublová, Eva; Mahdavian, Elahe; Procházka, Lubomír; Sangsura, Smink; Vácek, A; Salvatore, Brian A.; Neužil, Jiřı́

doi:10.1016/j.taap.2009.01.027

Cited by 45 publications

(42 citation statements)

References 41 publications

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“…Their liposomal formulations were found to be well tolerated in mice of various strains and preserved the strong anticancer efficacy of the VE analogues, as shown using the transgenic FVB/N c-neu mice with spontaneous breast carcinomas. 26 Nonliposomal systems like vesiculated VE analogues formed by spontaneous vesiculation were found to be toxic for some analogues of VE, for example, a-tocopheryl oxalate, 18 or a-TAM. 26 Thus, entrapment of such analogues (as shown for a-TAM) minimises the secondary toxicity while the anticancer efficacy remains preserved.…”

Section: Discussionmentioning

confidence: 99%

“…26 Nonliposomal systems like vesiculated VE analogues formed by spontaneous vesiculation were found to be toxic for some analogues of VE, for example, a-tocopheryl oxalate, 18 or a-TAM. 26 Thus, entrapment of such analogues (as shown for a-TAM) minimises the secondary toxicity while the anticancer efficacy remains preserved. 26 Stable preparations of a-TOS and similar anticancer agents that could be stored for prolonged periods of time are needed.…”

Section: Discussionmentioning

confidence: 99%

“…26 Thus, entrapment of such analogues (as shown for a-TAM) minimises the secondary toxicity while the anticancer efficacy remains preserved. 26 Stable preparations of a-TOS and similar anticancer agents that could be stored for prolonged periods of time are needed. A plausible approach to this problem is the use of liposomes, which have been utilised as suitable carriers for a variety of drugs and vaccines.…”

Section: Discussionmentioning

confidence: 99%

“…Liposomal formulation of a-tocopheryl maleamide (a-TAM), an esterase-resistant analogue of the ester atocopheryl maleate, 25 was reported to eliminate the acute toxicity associated with administration of the free VE analogue. 26 The physico-chemical stability of liposomal nanoparticles depends on their composition and structure. Physical modifications of liposomes, including fusion and aggregation of the particles, as well as increase of the membrane permeability and the drug release can occur as the consequences of chemical degradation of the liposomal system.…”

Section: Introductionmentioning

confidence: 99%

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Lyophilised liposome‐based formulations of α‐tocopheryl succinate: Preparation and physico‐chemical characterisation

Koudelka

Mašek

Neužil

et al. 2010

Journal of Pharmaceutical Sciences

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Lyophilised liposome‐based formulations of α‐tocopheryl succinate: Preparation and physico‐chemical characterisation

Koudelka

Mašek

Neužil

et al. 2010

Journal of Pharmaceutical Sciences

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“…Las betaciclodextrinas son oligosacáridos cíclicos que forman complejos de inclusión en una variedad de moléculas hidrofóbicas (34), por lo cual se considera que confieren mayor solubilidad y estabilidad a las propiedades biológicas de las moléculas (30), efecto que se vería potenciado por las propiedades farmacológicas de los complejos de paladio (cuadro 1, 2) en la inhibición de la síntesis de ADN o por unión no covalente con el ADN, ocasionando así la muerte celular y logrando un mayor efecto con menores dosis, sin afectar de manera significativa las células linfoides normales.…”

Section: Discussionunclassified

Cytotoxic effect of palladium (II) inclusion compounds in beta-cyclodextrin

et al. 2016

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Introducción. Las tiosemicarbazonas y sus complejos de paladio (II) poseen actividad antineoplásica con pocos efectos secundarios, por lo cual se las considera como una nueva alternativa terapéutica. Sin embargo, existen diferencias en los rangos de la concentración inhibitoria media (CI50) asociada a la divergencia estructural y la solubilidad de los complejos, así como a la sensibilidad de los blancos celulares. La inclusión de fármacos en la beta-ciclodextrina con fines terapéuticos ha mejorado su solubilidad y estabilidad, pero los efectos de su combinación con los complejos de paladio (II) y las tiosemicarbazonas no se han comprobado aún.Objetivo. Estudiar el efecto citotóxico de los complejos de paladio en la beta-ciclodextrina.Materiales y métodos. La actividad citotóxica de los complejos de paladio en la beta-ciclodextrina se evaluó en la línea celular de cáncer de mama (MCF-7), empleando el método de la sulforodamina B.Resultados. Los ligandos MePhPzTSC y Ph2PzTSC, sus complejos de paladio (II) libres e incluidos en la beta-ciclodextrina y el cisplatino mostraron actividad citotóxica en la línea celular MCF-7; sin embargo, la citotoxicidad fue mayor con la inclusión en la beta-ciclodextrina ([Pd(MePhPzTSC)2]•ß-CD y [Pd(Ph2PzTSC)2]•ß-CD). La concentración inhibitoria media (CI50) para estos complejos se obtuvo en concentraciones de 0,14 y 0,49 μM, y con dosis hasta cinco veces inferiores comparadas con las concentraciones de los ligandos libres (1,4 y 2,9 μM), de los complejos de paladio (II) libres (0,57 y 1,24 μM) y del cisplatino (6,87 μM).Conclusiones. El uso de la beta-ciclodextrina mejoró significativamente la actividad citotóxica de las tiosemicarbazonas y sus complejos de paladio (II), lo cual probablemente está asociado al incremento de la solubilidad y biodisponibilidad del compuesto, estrategia que se puede sugerir para el diseño de futuros fármacos antineoplásicos.

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Mitochondrial‐dependent anticancer activity of δ‐tocotrienol and its synthetic derivatives in HER‐2/neu overexpressing breast adenocarcinoma cells

et al. 2013

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Anticancer activity and mitochondrial mechanism of the vitamin E form δ-tocotrienol (δ-T3) was investigated in HER-2/neu-overexpressing human SKBR3 and murine TUBO breast cancer cells. δ-T3 was confirmed to possess high cytotoxic and apoptotic activity in SKBR3 cells as compared with all natural forms of vitamin E and several synthetic forms that included novel derivatives with the same backbone of δ-T3 such as δ-tocotrienyl-succinyl amide (δ-T3AS) and the redox-active analogue δ-tocotrienyl amine (δ-T3NH2). As observed in the case of alpha-TOS, a prototypical anticancer drug derived from α-tocopherol, succinylation of δ-T3 enhanced citotoxicity and apoptotic activity of the vitamer. δ-T3 induced apoptosis of SKBR3 cells was associated with mitochondrial destabilization, energy failure, and unbalanced activity of stress/survival MAPKs, namely p38 and ERK1/2 pathways. An increased generation of ROS followed to such a series of early events. Enhanced activity of δ-T3 in this human carcinoma cell line was characterized by the sustained uptake and oxidative transformation to the quinone derivative δ-T3Q, thereby suggesting redox effects in SKBR3 mitochondria by this vitamer. Viability and uptake data show a different pattern of responses in TUBO cells with higher response to synthetic derivatives of δ-T3 than in SKBR3 cells. In conclusion, synthetic derivatives of δ-T3 with enhanced apoptotic activity in breast carcinoma cells are investigated for the first time in this study also describing mechanistic aspects of mitochondrial effects of δ-T3. Further investigation in preclinical models of HER2/neu-high breast adenocarcinoma is underway to identify other and more effective forms of VE in this type of cancer.

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Liposomal formulation of α-tocopheryl maleamide: In vitro and in vivo toxicological profile and anticancer effect against spontaneous breast carcinomas in mice

Cited by 45 publications

References 41 publications

Lyophilised liposome‐based formulations of α‐tocopheryl succinate: Preparation and physico‐chemical characterisation

Lyophilised liposome‐based formulations of α‐tocopheryl succinate: Preparation and physico‐chemical characterisation

Cytotoxic effect of palladium (II) inclusion compounds in beta-cyclodextrin

Mitochondrial‐dependent anticancer activity of δ‐tocotrienol and its synthetic derivatives in HER‐2/neu overexpressing breast adenocarcinoma cells

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