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佛波酯与脂质双层的相互作用:荧光偏振、相变和钙离子载体转运的热致变化

Interaction of phorbol esters with lipid bilayers : thermotropic changes in fluorescence polarization, phase transition and calcium ionophoresis.

作者信息

Deleers M, Defrise-Quertain F, Ruysschaert J M, Malaisse W J

出版信息

Res Commun Chem Pathol Pharmacol. 1981 Dec;34(3):423-39.

PMID:6798652
Abstract

The influence of phorbol esters upon the thermotropic behaviour of multilamellar liposomes formed of dipalmitoylphosphatidylcholine (DPPC) or dimyristoylphosphatidylcholine (DMPC) was investigated, as a model for possible interferences of the phorbol esters with the phospholipid domain of biological membranes. Both biologically active (TPA, 12-O-tetradecanoylphorbol-13-acetate, PDD, phorbol-12,13-didecanoate) and inactive (4 alpha-PDD, 4 alpha-phorbol-12,13-didecanoate) phorbol esters lowered the temperature required to cause a fall in fluorescence polarization of a fluorescent probe inserted in the lipid matrix of the DMPC or DPPC liposomes and facilitated the process of calcium exchange-diffusion in DPPC liposomes containing the ionophore A23187. Both of these effects could be due to a decrease in viscosity of the liposomal matrix. However, differential scanning calorimetry revealed that the thermotropic changes evoked by each of these phorbol esters were not identical. In most cases, the phorbol esters decreased both the main phase transition temperature and enthalpy of melting. However, when TPA was incorporated in DMPC liposomes, i.e. when a myristoyl chain was present in both the phorbol ester and phospholipid, no change in the enthalpy of melting could be detected, whereas the main phase transition temperature decreased in proportion to the TPA content of the liposomes. These findings emphasize the view that phorbol esters indeed interact with phospholipids and that the characteristics of such an interaction may tightly depend on the precise chemical structure of both the phorbol ester and phospholipid under consideration.

摘要

研究了佛波酯对由二棕榈酰磷脂酰胆碱(DPPC)或二肉豆蔻酰磷脂酰胆碱(DMPC)形成的多层脂质体热致行为的影响,以此作为佛波酯可能干扰生物膜磷脂结构域的模型。具有生物活性的(TPA,12 - O - 十四烷酰佛波醇 - 13 - 乙酸酯,PDD,佛波醇 - 12,13 - 二癸酸酯)和无活性的(4α - PDD,4α - 佛波醇 - 12,13 - 二癸酸酯)佛波酯均降低了使插入DMPC或DPPC脂质体脂质基质中的荧光探针荧光偏振下降所需的温度,并促进了含有离子载体A23187的DPPC脂质体中的钙交换扩散过程。这两种效应可能都是由于脂质体基质粘度的降低。然而,差示扫描量热法表明,这些佛波酯各自引起的热致变化并不相同。在大多数情况下,佛波酯降低了主相变温度和熔化焓。然而,当TPA掺入DMPC脂质体中时,即当佛波酯和磷脂中都存在肉豆蔻酰链时,未检测到熔化焓的变化,而主相变温度随脂质体中TPA含量成比例降低。这些发现强调了这样一种观点,即佛波酯确实与磷脂相互作用,并且这种相互作用的特性可能紧密取决于所考虑的佛波酯和磷脂的精确化学结构。

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