Enhancement of the Cytotoxicity of Liposomal Ricin by the Carboxylic lonophore Monensin and the Lysosomotropic Amine NH4Cl in Chinese Hamster Ovary Cells.

Autor: Bharadwaj, Seemha, Rathore, Shailendra Singh, Ghosh, Prahlad C.
Zdroj: International Journal of Toxicology (Sage); Sep2006, Vol. 25 Issue 5, p349-359, 11p
Abstrakt: Ricin was encapsulated in negatively charged liposomes and its effect on the cytotoxicity was compared with native ricin in Chinese hamster ovarian (CHO) cells. The cytotoxicity of ricin, as measured by a marker protein synthesis (incorporation of 3H-leucine), was reduced markedly (300-fold) following encapsulation in liposomes. Lactose, a potent inhibitor of ricin cytotoxicity, had no effect on the binding, internalization, and cytotoxicity of lipo-somal ricin, indicating that liposomal ricin enter into mammalian cells by an alternative route, bypassing galactose-mediated endo-cytic pathway. Both monensin (a carboxylic ionophore) and NH4Cl (a lysosomotropic amine) markedly enhances the cytotoxicity of liposomal ricin, indicating endocytotic uptake of liposomal ricin. The degree of potentiation of the cytotoxicity of liposomal ricin by both monensin and NH4Cl was significantly higher (441- and 51-fold) as compared to native ricin (62.5- and 12.5-fold). The extent of exocytosis of free ricin was found to be much higher as compared to liposomal ricin; on the other hand, the extent of degradation of free and liposomal ricin was identical. Consequently, the intracel-lular level of liposomal ricin was increased to 3.5-fold. This higher level of intracellular liposomal ricin may allow more efficient ricin A-chain release into the cytosol under the influence of NH4Cl and monensin. Monensin-induced potentiation of liposomal ricin was prevented by brefeldin A, indicating that in the presence of mon-ensin, the liposomal ricin was efficiently routed through the Golgi apparatus en route to the cytosol. Thus, liposomal ricin in combination with monensin may have potential application for selective elimination of malignant cells. [ABSTRACT FROM PUBLISHER]
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