Fernandes Maria A S, Pereira Susana P S, Jurado Amália S, Custódio José B A, Santos Maria S, Moreno António J M, Duburs Gunars, Vicente Joaquim A F
IMAR, Departamento de Zoologia, Universidade de Coimbra, 3004-517 Coimbra, Portugal.
Chem Biol Interact. 2008 Jun 17;173(3):195-204. doi: 10.1016/j.cbi.2008.03.001. Epub 2008 Mar 15.
The 1,4-dihydropyridines OSI-1210, OSI-1211 (etaftoron), and OSI-3802 are compounds with similar chemical structure. They differ by the length of the alkoxyl chain in positions 3 and 5 of the dihydropyridine (DHP) ring and by their pharmacological action characteristics. However, as far as we know, a clear relationship between the effects of these compounds and the length of the alkoxyl chain in positions 3 and 5 of the DHP has not been established. The goal of this study was to compare the influence of OSI-1210, OSI-1211 (etaftoron), and OSI-3802 on rat liver mitochondrial bioenergetics and on the physical properties of membrane lipid bilayers, correlating their actions with the length of the alkoxyl chain in positions 3 and 5 of the DHP ring. Using either glutamate/malate or succinate as respiratory substrates, all the compounds, in concentrations of up to 500 microM, depressed state 3 and uncoupled respiration, respiratory control (RCR) and ADP/O ratios, and phosphorylation rate, whereas state 4 respiration was stimulated. However, the stimulatory effect on state 4 induced by OSI-3802, the compound with the longest chain in positions 3 and 5 of the DHP ring, as well as its inhibitory effects on RCR and ADP/O ratios and phosphorylation rate were more pronounced than that induced by OSI-1210 and OSI-1211 (etaftoron), the compounds with the shortest and intermediate chains, respectively. Moreover, OSI-3802 maximized state 4 stimulation and minimized RCR and ADP/O ratios, and phosphorylation rate at a concentration of 100 microM, whereas low graduate effects were detected with OSI-1210 and OSI-1211 (etaftoron) for concentrations of up to 500 microM. At low concentrations (< or =30 microM), OSI-3802, like its analogue OSI-1212 (cerebrocrast), reduced the phase transition temperature, the cooperative unit size, and the enthalpy associated with the phase transition temperature of dimyristoylphosphatidylcholine (DMPC) membrane bilayers. A good correlation was established between the effects of 200 microM OSI-1210, OSI-1211 (etaftoron), and OSI-3802 on glutamate/malate- and succinate-dependent RCR of rat liver mitochondria and on the enthalpy change (Delta H) for the thermotropic profile of DMPC membrane bilayers at a 0.2 drug/DMPC molar ratio, indicating that the changes induced by these compounds on both mitochondrial membrane integrity and physical properties of DMPC membrane bilayers are strongly related to the length of the alkoxyl chain in positions 3 and 5 of the DHP ring. A putative relationship between membrane physical perturbation, bioenergetics impairment and the molecular characteristics of the compounds will be established as an approach to better understand their differentiated toxicological and pharmacological actions.
1,4 - 二氢吡啶类化合物OSI - 1210、OSI - 1211(依他福龙)和OSI - 3802具有相似的化学结构。它们在二氢吡啶(DHP)环3位和5位的烷氧基链长度以及药理作用特性上存在差异。然而,据我们所知,这些化合物的作用与DHP环3位和5位烷氧基链长度之间尚未建立明确的关系。本研究的目的是比较OSI - 1210、OSI - 1211(依他福龙)和OSI - 3802对大鼠肝线粒体生物能量学以及膜脂双层物理性质的影响,并将它们的作用与DHP环3位和5位烷氧基链的长度相关联。以谷氨酸/苹果酸或琥珀酸作为呼吸底物时,所有化合物在浓度高达500微摩尔时,均会降低状态3呼吸、解偶联呼吸、呼吸控制率(RCR)和ADP/O比值以及磷酸化速率,而状态4呼吸则受到刺激。然而,DHP环3位和5位链最长的化合物OSI - 3802对状态4呼吸的刺激作用,以及对RCR、ADP/O比值和磷酸化速率的抑制作用,比分别具有最短链和中间链的化合物OSI - 1210和OSI - 1211(依他福龙)更为显著。此外,OSI - 3802在浓度为100微摩尔时使状态4呼吸刺激作用最大化,RCR、ADP/O比值和磷酸化速率最小化,而对于浓度高达500微摩尔的OSI - 1210和OSI - 1211(依他福龙),则检测到较低的逐渐变化效应。在低浓度(≤30微摩尔)时,OSI - 3802与其类似物OSI - 1212(脑迟缓素)一样,降低了二肉豆蔻酰磷脂酰胆碱(DMPC)膜双层的相变温度、协同单元大小以及与相变温度相关的焓。在0.2药物/DMPC摩尔比下,200微摩尔的OSI - 1210、OSI - 1211(依他福龙)和OSI - 3802对大鼠肝线粒体谷氨酸/苹果酸和琥珀酸依赖性RCR的影响与DMPC膜双层热致曲线的焓变(ΔH)之间建立了良好的相关性,表明这些化合物对线粒体膜完整性和DMPC膜双层物理性质的影响与DHP环3位和5位烷氧基链的长度密切相关。将建立膜物理扰动、生物能量学损伤与化合物分子特征之间的假定关系,作为更好地理解它们不同毒理学和药理学作用的一种方法。
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