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Verapamil prevents the effects of daunomycin on the thermotropic phase transition of model lipid bilayers.

机译:维拉帕米可预防道诺霉素对模型脂质双层的热致相变的影响。

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摘要

High-sensitivity differential scanning calorimetry and fluorescence-depolarization techniques were used to study how the presence of daunomycin and/or verapamil affect the thermotropic behaviour of dipalmitoyl phosphatidylcholine (DPPC) vesicles. Daunomycin, a potent anti-cancer agent, perturbs the thermodynamic parameters associated with the lipid phase transition: it decreases the enthalpy change, lowers the transition temperature and reduces the co-operative behavior of the phospholipid molecules. Verapamil, on the other hand, produces smaller alterations in the lipid phase transition. However, when daunomycin and verapamil are present simultaneously in the DPPC vesicles, it is observed that verapamil prevents, in a concentration-dependent manner, the alteration in the phospholipid phase transition expected from the presence of daunomycin in the bilayer. Furthermore, drug-binding studies suggest that the observed interference of verapamil in the daunomycin/phospholipid interaction occurs without a decrease in the amount of daunomycin bound to the lipid bilayer and without the formation of a daunomycin-verapamil complex. Because of the importance of drug-membrane interactions in anthracycline cytotoxicity, we speculate that the lipid bilayer of biological membranes may provide appropriate sites at which the presence of verapamil influences the activity of daunomycin.
机译:高灵敏度差示扫描量热法和荧光去极化技术被用于研究道诺霉素和/或维拉帕米的存在如何影响二棕榈酰磷脂酰胆碱(DPPC)囊泡的热致行为。道诺霉素是一种有效的抗癌药,会干扰与脂质相变有关的热力学参数:它降低了焓变,降低了转变温度并降低了磷脂分子的协同行为。另一方面,维拉帕米在脂质相变中产生较小的改变。然而,当道诺霉素和维拉帕米同时存在于DPPC囊泡中时,可以观察到维拉帕米以浓度依赖性的方式阻止了双层中存在道诺霉素的磷脂相变的改变。此外,药物结合研究表明,观察到维拉帕米对道诺霉素/磷脂相互作用的干扰发生,而与脂质双分子层结合的道诺霉素的量却没有减少,也没有形成道诺霉素-维拉帕米复合物。由于药物-膜相互作用在蒽环霉素的细胞毒性中具有重要意义,我们推测生物膜的脂质双层可能会提供适当的位点,维拉帕米的存在会影响道红霉素的活性。

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